US20120070499A1 - Delayed-release glucocorticoid treatment of rheumatoid disease - Google Patents

Delayed-release glucocorticoid treatment of rheumatoid disease Download PDF

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US20120070499A1
US20120070499A1 US13/176,598 US201113176598A US2012070499A1 US 20120070499 A1 US20120070499 A1 US 20120070499A1 US 201113176598 A US201113176598 A US 201113176598A US 2012070499 A1 US2012070499 A1 US 2012070499A1
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prednisone
glucocorticoid
delayed
treatment
release
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Achim Schaeffler
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Horizon Pharma Switzerland GmbH
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Application filed by Horizon Pharma Switzerland GmbH filed Critical Horizon Pharma Switzerland GmbH
Priority to US13/176,598 priority Critical patent/US20120070499A1/en
Publication of US20120070499A1 publication Critical patent/US20120070499A1/en
Priority to US13/860,015 priority patent/US8920838B2/en
Priority to US14/563,000 priority patent/US9504699B2/en
Priority to US15/355,381 priority patent/US20170281648A1/en
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/56Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids
    • A61K31/57Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids substituted in position 17 beta by a chain of two carbon atoms, e.g. pregnane or progesterone
    • A61K31/573Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids substituted in position 17 beta by a chain of two carbon atoms, e.g. pregnane or progesterone substituted in position 21, e.g. cortisone, dexamethasone, prednisone or aldosterone
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K45/00Medicinal preparations containing active ingredients not provided for in groups A61K31/00 - A61K41/00
    • A61K45/06Mixtures of active ingredients without chemical characterisation, e.g. antiphlogistics and cardiaca
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P19/00Drugs for skeletal disorders
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P19/00Drugs for skeletal disorders
    • A61P19/02Drugs for skeletal disorders for joint disorders, e.g. arthritis, arthrosis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P21/00Drugs for disorders of the muscular or neuromuscular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P29/00Non-central analgesic, antipyretic or antiinflammatory agents, e.g. antirheumatic agents; Non-steroidal antiinflammatory drugs [NSAID]
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J5/00Normal steroids containing carbon, hydrogen, halogen or oxygen, substituted in position 17 beta by a chain of two carbon atoms, e.g. pregnane and substituted in position 21 by only one singly bound oxygen atom, i.e. only one oxygen bound to position 21 by a single bond
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K2121/00Preparations for use in therapy

Definitions

  • the present invention refers to the treatment of a rheumatic disease and/or osteoarthritis by administering a delayed-release dosage form of a glucocorticoid to a subject in need thereof.
  • RA rheumatoid rheumatoid arthritis
  • Glucocorticoids are widely used to treat the disease and are often administered in combination with other drugs, especially disease-modifying antirheumatic drugs (DMARDs) and non-steroidal anti-inflammatory drugs (NSAIDs) (Bijlsma 2003).
  • DMARDs disease-modifying antirheumatic drugs
  • NSAIDs non-steroidal anti-inflammatory drugs
  • Prednisone, prednisolone and methylprednisolone are among the most common glucocorticoids for the treatment of RA.
  • Glucocorticoids have a broad spectrum of anti-inflammatory and immunosuppressive effects. They act by inhibiting leukocyte traffic; interfering with functions of leukocytes, fibroblasts, and endothelial cells; and suppressing the synthesis and actions of inflammatory cytokines including interleukin-6 (IL-6) (Buttgereit 2005). When they were first introduced, glucocorticoids were administered to RA patients for long periods at high doses exceeding 10 mg/day prednisone or equivalent. These high-dose, long-term regimens were highly effective but were associated with pleiotropic effects and unacceptable adverse reactions. This led to the development of low-dose regimens in order to reduce the incidence of side effects and optimized the benefit:risk ratio (Buttgereit 2005).
  • High corticoid doses are now only considered suitable for short-term therapy in special cases (e.g. for treatment of a severe flare of RA). Decreases in prescribed corticoid dose are illustrated by an evaluation of patients who attended a US clinic between 1984 and 1986 (1985 cohort) or between 1999 and 2001 (2000 cohort) (Pincus 2005). The mean prednisone dose was 7.8 mg/day in 1985 compared to 4 mg/day in 2000, with median doses of 5 and 4 mg/day, respectively.
  • prednisolone In a double-blind, placebo-controlled study, 7.5 mg/day prednisolone reduced joint destruction when given for 2 years in combination with other standard RA treatments (Kirwan 1995). When prednisolone was stopped, joint destruction returned to the same level as in the control group (Hickling 1998). In a more recent double-blind, placebo-controlled study, prednisone (10 mg/day) slowed progression of joint damage over periods of 2 and 5 years in patients who had not been pretreated with DMARDs (van Everdingen 2002, Jacobs 2005).
  • Osteoporosis, obesity, hypertension, family history of diabetes or glaucoma were listed as risk factors requiring more careful observation.
  • adverse effects that may need regular checks were defined as Cushingoid syndrome, adrenal crisis of corticoid withdrawal, new onset of diabetes mellitus, worsening of glycemia control in patients with diabetes mellitus, cataracts, glaucoma, peptic ulcer (in combination with NSAIDs), and hypertension.
  • Patients with active RA suffer from clinical signs and symptoms that include joint stiffness, pain, and swelling. Patients have assessed these symptoms (and related factors such as disability and mobility) as being important outcomes of RA treatment (Ahlmen et al. 2005, Carr et al. 2003, Hewlett et al. 2005). Clinical symptoms vary during the day and are more severe early in the morning after awakening than in the afternoon or evening (Cutolo et al. 2003, Cutolo and Masi 2005). Indeed, morning stiffness is such a typical symptom of RA that it has become a standard diagnostic criterion for the disease (Arnett et al. 1988, ACR Guideline 2002).
  • RA patients have higher serum concentrations of interleukins (IL), especially IL-6, and tumor necrosis factor-alpha (TNF- ⁇ ) and levels display a pronounced circadian rhythm, with higher night-time concentrations that peak at 02:00 to 06:00 (Arvidson et al. 1994; Crofford 1997; Cutolo 2003, 2005).
  • IL interleukins
  • TNF- ⁇ tumor necrosis factor-alpha
  • IL-6 is a potent activator of the HPA axis and stimulates the release of cortisol from the adrenal cortex to counteract the inflammation (Cutolo 2005, Mastorakos 2000).
  • IL-6 is a potent activator of the HPA axis and stimulates the release of cortisol from the adrenal cortex to counteract the inflammation.
  • RA RA patients, it seems that the response of the permanently stimulated HPA axis is inadequate and levels of endogenous cortisol are insufficient to combat the inflammation (Gudbjöornsson 1996).
  • Administration of exogenous glucocorticoids acts—among other therapeutic effects—as a replacement therapy and supplements the inadequate levels of endogenous cortisol (Cutolo 2005).
  • Endogenous cortisol and exogenous therapeutic glucocorticoids inhibit the synthesis of IL-6 and other pro-inflammatory cytokines.
  • prednis(ol)one and methylprednisolone are ideally suited exogenous corticoid due to its comparatively short half-life of 3-4 h.
  • Low-dose oral prednis(ol)one or methylprednisolone are usually given for symptomatic relief as a single morning dose to minimize potential interference with the HPA axis.
  • the drug should be given shortly before the expected nocturnal increase of IL-6.
  • Karatay et al investigated in 2002 the administration of an IR low-dose prednisone tablet over a period of 6 months at 02:00 vs 07:30. The results were disappointing because a difference in morning stiffness could not be observed. One explanation of this could be that the short term effects observed by Arvidson disappear after several days or weeks of therapy. Thus, the effects on long term night time administration of glucocorticoids remained unclear.
  • U.S. Pat. No. 5,792,476 describes a pharmaceutical composition for peroral administration for rheumatoid arthritis, which comprises a glucocorticoid as active ingredient and which leads to release in the small intestine.
  • the composition is a granulate which is laminated with an inner layer which is resistant to a pH of 6.8, and with an outer layer which is resistant to a pH of 1.0.
  • U.S. Pat. No. 6,488,960 describes a pharmaceutical dosage form for controlled release of corticoids, reference being made to the formulations described in U.S. Pat. No. 5,792,476.
  • WO 01/08421 describes a tablet having a core which is coated by at least two layers, one of which completely encloses the other.
  • the coating layers can be produced by spray coating and/or pressing.
  • WO 01/68056 discloses a pharmaceutical preparation having a release profile with a time delay, comprising a core and at least one hydrophilic or lipophilic coating surrounding the core, where the coating is slowly swollen, dissolved, eroded or changed in its structure in another way through the water present in the release medium, so that the core or parts of the core become accessible to the release medium.
  • the coating may be formed for example as pressed coating.
  • WO 02/072034 discloses a pharmaceutical dosage form for delayed release, having a core which comprises as active ingredient a glucocorticoid and a material which brings about delayed release and includes at least one natural or synthetic gum.
  • WO 2004/093843 discloses a tablet with a specific core geometry to release the active ingredient in a specific delayed release manner.
  • WO 2006/027266 discloses a pharmaceutical dosage form with site-and time controlled gastrointestinal release of an active agent, particularly a corticosteroid.
  • the pharmaceutical dosage form is preferably a coated tablet having a core comprising the corticosteroid and a swellable/disintegration adjuvant, and an inert outer coating. The coating is compressed at a pressure chosen to result in the release of the corticosteroid at a predetermined position in the gastrointestinal tract.
  • the present inventors have carried out a clinical study in order to test the efficacy of a delayed-release prednisone tablet compared to a standard immediate-release tablet. It was found that long-term administration of the delayed-release prednisone tablet shows a surprisingly increased efficacy compared to the treatment with a standard immediate-release prednisone tablet.
  • a first aspect of the invention refers to the use of a delayed-release dosage form of a corticosteroid for the manufacture of a medicament for the long-term treatment of a rheumatic disease and/or osteoarthritis.
  • a further aspect of the invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of rheumatic diseases in
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in combination with at least one further medicament which is a NSAID, a DMARD, a TNF ⁇ inhibitor, an IL-6 inhibitor and/or an analgetic agent.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis without any further medicament.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for treatment of a rheumatic disease and/or osteoarthritis in combination with reduced doses of at least one further medicament which is a NSAID, a DMARD, a TNF ⁇ inhibitor, an IL-6 inhibitor and/or an analgetic agent.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of ankylosating spondylitis, polymyalgia rheumatica and/or osteoarthritis.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of morning stiffness, pain and/or inflammation parameters such as release of cytokines, e.g. in a rheumatic disease and/or osteoarthritis.
  • Still a further aspect of the present invention is a method for the treatment of a patient suffering from signs and symptoms of an underlying rheumatic disease and/or osteoarthritis, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at least about two weeks.
  • Still a further aspect of the present invention is a method for the treatment of a patient suffering from morning stiffness and pain due to an underlying rheumatic disease and/or osteoarthritis, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at lest about two weeks.
  • Still a further aspect of the present invention is a method for the treatment of a patient having circadian fluctuations in Interleukin 6 levels due to underlying inflammation, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at least about two weeks, and wherein said treatment is administered such that the glucocorticoid is released at or before the time when the patient's Interleukin 6 level is at a daily peak.
  • FIG. 1 shows duration of Morning Stiffness: Relative Change from Baseline in % (SEM) per week of treatment in the ITT population.
  • FIG. 2 shows duration of Morning Stiffness: Relative Change from Baseline in % (SEM) per month of treatment in the ITT population.
  • FIG. 3 shows IL 6 values (median) under treatment of Prednisone delayed release tablets.
  • the present invention refers to the use of a delayed-release dosage form of a glucocorticoid.
  • the release of the active ingredient is preferably delayed for a time period of 2-10 hours after intake, preferably 2-6, more preferably 3-5 hours after intake the active ingredient may be released in the upper sections of the intestine and/or in the lower sections of the intestine. More preferably, the active ingredient is released in the upper sections of the intestine within a period of 2-6 hours.
  • the delayed-release dosage form is preferably administered to the patient at or before bedtime, more preferably in the evening, e.g. from about 9:00 pm to about 11:00 pm. Because inflammation is accompanied with circadian fluctuations in the concentration of pro-inflammatory cytokines (such as Interleukin-6) which peaks during sleeping hours, bedtime administration allows an efficacious concentration of the active ingredient to be present when such concentration peaks.
  • pro-inflammatory cytokines such as Interleukin-6
  • the delayed-release dosage form is preferably a tablet, e.g. as described in WO 2006/027266, which is herein incorporated by reference.
  • the dosage form preferably comprises
  • the inert coating initially prevents release of the active ingredient or the active ingredient combination over an exactly defined period, so that no absorption can occur.
  • the water present in the gastrointestinal tract penetrates slowly in through the coating and, after a time which is previously fixed by the pressure for compression, reaches the core.
  • the coating ingredients show neither swelling nor diluting of parts of the coating.
  • the core is reached, the water penetrating in is very rapidly absorbed by the hydrophilic ingredients of the core, so that the volume of the core increases greatly and, as a consequence thereof, the coating completely bursts open, and the active ingredient and the active ingredient combination respectively is released very rapidly.
  • a particularly advantageous embodiment of this press-coated delayed-release tablet is achieved when a previously compressed core tablet is subsequently compressed with a multilayer tablet press to a press-coated tablet.
  • the tablet coating typically consists of the following materials in order to achieve a delayed release profile:
  • further adjuvants should also be added to these materials so that the tablet coating can be compressed.
  • fillers such as lactose, various starches, celluloses and calcium hydrogen phosphate or di-basic calcium phosphate.
  • the glidant used is normally magnesium stearate, and in exceptional cases also talc and glycerol behenate.
  • a plasticizer is often also added to the coating material, preferably from the group of polyethylene glycol, dibutyl phthalate, diethyl citrate or triacetin.
  • the tablet core In order to achieve an optimal release profile, the tablet core must also fulfil certain tasks and exhibit certain properties. Thus, after the lag phase has elapsed, a rapid release profile is achieved if typical disintegrants are added to the inner core, which are derived for example from the group of the following substances: cellulose derivatives, starch derivatives, crosslinked polyvinylpyrrolidone.
  • cellulose derivatives derived for example from the group of the following substances: cellulose derivatives, starch derivatives, crosslinked polyvinylpyrrolidone.
  • a blowing agent for example resulting from a combination of a weak acid and a carbonate or bicarbonate, may also promote rapid release.
  • the tablet core typically consists additionally of matrix or filling ingredients (e.g. lactose, cellulose derivatives, calcium hydrogen phosphate or other substances known from the literature) and lubricant or glidant (usually magnesium stearate, in exceptional cases also talc and glycerol behenate).
  • the size of the core tablet preferably should not exceed 6 mm (preferably 5 mm) in diameter, because otherwise the press-coated tablet becomes too large for convenient ingestion.
  • the dosages of the active ingredients are in the range from 0.1 to 50 mg, very particularly between 1 and 20 mg.
  • the in vitro release profile of the dosage form according to the invention is preferably such that less than 5% of the active ingredient is released during the lag phase. After the release phase has started, preferably ⁇ 80%, particularly preferably ⁇ 90%, of the active ingredient is released within one hour. More preferably, the delayed-release dosage form has a dissolution time of equal to or less than about 2 hours after the lag time has been reached).
  • the in vitro release is preferably determined using the USP paddle dissolution model in water.
  • the employed active ingredients are derived from the group of glucocorticoids and all show comparable physicochemical properties.
  • Such include cortisone, hydrocortisone, prednisone, prednisolone, methylprednisolone, budesonide, dexamethasone, fludrocortisone, fluocortolone, cloprednole, deflazacort, triamcinolone, or the corresponding pharmaceutically acceptable salts and/or esters thereof.
  • prednisone prednisolone, methylprednisolone, budesonide, dexamethasone, fluocortolone, cloprednole, and deflazacort or the corresponding pharmaceutically acceptable salts and/or esters thereof.
  • the following combination of core materials and coating materials has proved to be particularly suitable for achieving a time- and site-controlled release with exclusion of pH and food influences:
  • the coating preferably comprises:
  • the core tablet preferably comprises:
  • the delayed-release dosage form is administered as a long-term treatment to a subject in need thereof for a time sufficient to reduce and/or abolish the disease and/or disease symptoms.
  • the long term treatment usually comprises daily administration of the medicament for an extended period of time, e.g. for at least two weeks, preferably for at least 4 weeks, more preferably for at least 8 weeks, even more preferably for at least 12 weeks, and most preferably for at least 6 months or at least 12 months.
  • the present invention refers to the novel treatment of groups of patients suffering from rheumatic diseases and/or osteoarthritis. These patient groups are selected from:
  • patient groups may be selected from:
  • patient groups may be selected from:
  • patient groups may be selected from:
  • patient groups may be selected from:
  • the daily dose of the glucocorticoid may be substantially reduced compared to an immediate-release tablet of the glucocorticoid.
  • the disease-inhibiting effect may be obtained by a significantly lower dose of the active ingredient, whereby the occurrence and/or intensity of site effect is diminished.
  • the daily dose of the glucocorticoid can be reduced by at least 10%, more preferably by at least 20%, e.g. by 10-50% compared to an immediate-release tablet.
  • the reduced daily dose of prednis(ol)one in Prednisone delayed-release is preferably in the range of 1 to 5 mg/day compared to 6-10 mg/day for a standard IR tablet.
  • the treatment according to the present invention may comprise the treatment of a rheumatic disease and/or osteoarthritis without any further medicament.
  • the invention may comprise the treatment of a rheumatic disease and/or osteoarthritis in combination with at least one further medicament which is preferably selected from the groups of NSAIDs, DMARDs, TNF ⁇ inhibitors, IL-6 inhibitors, analgetic agents or combinations thereof. Especially preferred is a combination with Tarenflurbil.
  • NSAIDs are preferably selected from arylalkanoic acids (Diclofenac, Indometacin, Sulindac) from 2-arylpropionic acids (Carprofen, Fenoprofen, Flurbiprofen, Ibuprofen, Ketoprofen, Ketorolac, Laxoprofen, Naproxen, Tiaprofenic acid), from N-arylanthranilic acids (Mefenamic acid, Meclofenamic acid), from Oxicams (Piroxicam, Meloxicam) or from Coxibs (Celecoxib, Parecoxib, Etoricoxib) or from combinations thereof. Especially preferred is a combination with Tarenflurbil.
  • arylalkanoic acids Diclofenac, Indometacin, Sulindac
  • 2-arylpropionic acids Carprofen, Fenoprofen, Flurbiprofen, Ibuprofen, Ketoprofen,
  • DMARDs are preferably selected from gold preparations, chloroquine, azathioprine, sulfasalazine, cyclophosphamide, penicillamine, hydroxychloroquine, methotrexate, thorium dioxide suspension, levamisole, cyclosporin, interferone, leflunomide or from combinations thereof.
  • TNF ⁇ inhibitors and IL 1 inhibitors are preferably selected from antibodies or soluble receptors such as etanercept, inflixima, anakinra, adalimumab and from cominations thereof.
  • IL-6 inhibitors are preferably selected from antibodies or soluble receptors such as tocilizumab.
  • Analgetic agents are preferably selected from salicylates (Aspirin, Methyl salicylate, Diflunisal, Benorylate, Faislamine, Amoxiprin), from pyrazolidine derivatives (Phenylbutazone, Oxyphenylbutazone) or paracetamol or from combinations thereof.
  • the dose of the at least one further medicament may be substantially reduced e.g. by at least 10%, preferably by at least 20%, e.g. by 10-50%.
  • the first usage of TNF ⁇ inhibitors or IL-6 inhibitors can be postponed to a later point in time.
  • the present invention particularly refers to the treatment of a rheumatic disease selected from rheumatoid arthritis, ankylosating spondylitis, polymyalgia rheumatica and/or to the treatment of osteoarthritis.
  • a rheumatic disease selected from rheumatoid arthritis, ankylosating spondylitis, polymyalgia rheumatica and/or to the treatment of osteoarthritis.
  • the delayed-release dosage form of a glucocorticoid particularly a long-term treatment
  • the administration of the delayed-release dosage form is effective without having undesired side effects.
  • the dose of the glucocorticoid may vary during the course of treatment.
  • the patient may be administered a relatively high dose during the initiation of therapy (e.g., about 10-40 mg/day or higher of prednisone, or an equivalent amount of another glucocorticoid), which may be reduced downward over a period of time (e.g., over 3-4 weeks) according to the patient's response, to a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid.
  • a relatively high dose during the initiation of therapy (e.g., about 10-40 mg/day or higher of prednisone, or an equivalent amount of another glucocorticoid)
  • a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid.
  • the patient may be started on a relatively low dose, which may be adjusted upward over a period of time (e.g., over 3-4 weeks) to a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid.
  • a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid.
  • Prednisone dose Patients were to continue on the same stable low dose of prednisone (or equivalent) that they received in the month before entering the study. During the study prednisone doses of 3 to 10 mg/day were achieved with appropriate combinations of Prednisone delayed-release or IR tablets containing 1 and 5 mg prednisone; daily doses of 2.5 and 7.5 mg prednisone were rounded to 3 and 8 mg, respectively. A constant low prednisone dose was given throughout the treatment phase to ensure that any differences between the treatment groups were not due to dose changes.
  • the primary objective of the study was to show whether administration of the new delayed-release formulation of prednisone (i.e. Prednisone delayed-release) in the evening was superior to the standard morning administration of immediate-release (IR) prednisone in reducing the duration of morning stiffness.
  • the patient diary card was appropriately designed to capture relevant clock times in minutes: wake-up, morning medication intake, resolution of morning stiffness.
  • the primary variable was “the relative change in duration of morning stiffness from baseline at individual study end in the double-blind treatment phase”, whereby the duration of morning stiffness was the difference between the time of resolution of morning stiffness and the time of awakening. Morning stiffness was chosen as the primary variable because it was expected to be directly affected by inhibition of night-time IL-6 peaks after delayed release of prednisone.
  • DAS 28 disease activity score
  • ACR20 responder rate The DAS 28 was computed from the joint scores, the ESR and the patient's global assessment of disease activity.
  • An ACR responder was defined as a patient with improvement of at least 20% of the baseline values in the tender joint count, swollen joint count and at least 3 of the following 5 variables: pain intensity, investigator global assessment, patient global assessment, HAQ disability index, or ESR.
  • Inclusion criteria were designed to enroll adult patients (18 to 80 years) with active RA who were typical of the general RA population being treated with a combination of stable corticoid medication and DMARDs. Patients had to have a documented history of RA and present with active symptoms of disease, i.e. morning stiffness of 45 min, pain ⁇ 30 mm (VAS), ⁇ 3 painful joints, ⁇ 1 swollen joints and elevated ESR and/or CRP.
  • active symptoms of disease i.e. morning stiffness of 45 min, pain ⁇ 30 mm (VAS), ⁇ 3 painful joints, ⁇ 1 swollen joints and elevated ESR and/or CRP.
  • the primary variable was “the relative change in duration of morning stiffness from baseline at individual study end in the double-blind treatment phase”, whereby the duration of morning stiffness was the difference between the time of resolution of morning stiffness and the time of awakening.
  • the reduction in duration of morning stiffness under Prednisone delayed-release treatment was higher than under standard IR prednisone throughout the 12-week treatment period.
  • Prednisone delayed-release was shown to be superior to standard prednisone IR tablet in a statistically significant manner (p ⁇ 0.025, one sided) and the primary study objective was met.
  • Table 4 shows the frequencies of starting stable doses of prednisone in the Predisone delayed-release and standard prednisone groups of the intention-to-treat (ITT) population.
  • the frequency profiles in both treatment groups were similar, with the most common dose being 5 mg (50% subjects), followed by 7 and 10 mg (approximately 20% each).
  • the median value of the mean daily prednisone dose across all subjects in the ITT population was 5.18 mg.
  • Subgroup analyses were performed on the primary efficacy variable (i.e. the relative change from baseline in duration of morning stiffness) in subjects with a mean daily prednisone dose ⁇ 5.18 mg and >5.18 mg.
  • Descriptive statistics for baseline demographics and the primary efficacy variable are presented for mean daily prednisone doses of >5.18 mg and ⁇ 5.18 mg in each of the treatment groups of the ITT population in Table 5.
  • the difference for the primary efficacy variable between the treatment groups is also given (as calculated by ANOVA, model A).
  • the intensity of pain was improved after 12 weeks of treatment by both treatments.
  • the treatment difference in the relative change in intensity of pain was calculated to be 4.91% (SD 8.08%).
  • a difference between the 2 groups in favour of Prednisone delayed-release has been observed, which was much more pronounced in the per-protocol set ( ⁇ 19% for Prednisone delayed-release vs ⁇ 5% for Prednisone standard).
  • the mean number of days with analgesics per week did not change notably after treatment start in both treatment groups. There is no difference between the two treatment groups after 2, 6, and 12 weeks of treatment.
  • the intensity of pain went down it can be assumed that in patients with early RA or under long-term treatment also a reduction of painkillers will be seen.
  • VAS mean daily quality of sleep
  • the Disease Activity Score (DAS 28) decreased in both treatment groups. After two weeks of treatment, the decreases were small, whereas after six and 12 weeks of treatment the decreases were more pronounced. Absolute and relative changes were similar between the two treatment groups after 2, 6, and 12 weeks of treatment.
  • the tender and swollen joint count decreased in both treatment groups. After two weeks of treatment, the decreases were notable and further decreases were observed in both treatment groups after six and 12 weeks of treatment.
  • VAS disease activity
  • HAQ-DI Health Assessment Questionnaire Disability Index
  • SF36 Quality of Life
  • HAQ-DI and SF36 scores were similar in both treatment groups at baseline as well as after 12 weeks of treatment.
  • IL-6 values decreased during the 12-week treatment in the Prednisone delayed-release treatment group, but remained unchanged in the prednisone standard treatment group. Median values seem to have been halved by the Prednisone delayed-release preparation and the overall range was much smaller after 12 weeks of treatment. The variability was very high in both groups. However, the change under Prednisone delayed-release from baseline to 12 weeks was significantly lower (p ⁇ 0.001). Also, there was a statistically significant difference between the two treatment groups after 12 weeks.
  • Osteocalcin is a sensitive measure to the bone metabolism (Heshmati 1998). The mean osteocalcin values at baseline (screening) as well as after 12 weeks of treatment and the respective relative changes are presented in Table 8.
  • the mean daily duration of morning stiffness was 153 min. After three months of treatment stiffness duration was reduced to a mean of 92 min and after six months further to 74 min. After nine months of prednisone delayed-release treatment mean daily duration of morning stiffness was 78 min.
  • IL-6 values decreased notably in the former prednisone standard group from 1050 IU/L to 570 IU/L. Thus, IL-6 concentrations were halved in the subjects of the former standard group. This decrease of IL-6 was similar to the decrease of IL-6 in the prednisone delayed-release group described in the double-blind phase. No further reduction was observed in the subjects of the former prednisone delayed-release group.
  • glucocorticoids in the treatment of rheumatoid arthritis (RA) is well established).
  • the main side effects consist of osteoporosis leading to fractures, gastrointestinal disorders, cardiovascular disorders, increased risk of infections, hyperglycemia, suppression of the HPA axis, and ophthalmologic disorders. It is accepted that many of these side effects are observed at high or medium doses but not at low doses (Bijlsma et al. 2003, Bijlsma et al. 2005, Boers 2004, Buttgereit et al 2005, Conn 2001, Da Silva et al. 2005, Saag et al. 1994).
  • Prednisone delayed-release is intended for the treatment of RA at low doses (3 to 10 mg prednisone/day) and contains the same active drug ingredient as standard low-dose IR products.
  • Prednisone delayed-release differs from standard products solely with respect to the recommended time of administration and timepoint of drug release within the gastrointestinal tract.
  • the safety profile of low-dose prednisone is well established and reflected in labeling for standard IR products. Clinically significant differences are not expected.
  • AE Treatment-emergent Adverse Event
  • prednisone standard died on study within 18 days after first dose of prednisone. Seven subjects (2.4%) experienced SAEs, and in one subject of these 7 subjects, the SAE was judged to be related to prednisone by the investigator.
  • Table 13 summarizes the number of subjects experiencing AEs by type of AE (MedDRA Preferred Term, in at least 1.0% of the treated group).
  • AEs The most frequently reported AEs (frequency >1.0% of the subjects of the safety set) by MedDRA Preferred Term were rheumatoid arthritis including several terms for worsening (deterioration, escalation, exacerbation, flare etc.) (24 subjects, 8.3%), abdominal pain upper (13 subjects, 4.5%) and nasopharyngitis (12 subjects, 4.2%). The incidences of these AEs were similar in both treatment groups.
  • AE treatment-emergent adverse event
  • Table 14 summarizes the most common AEs by type of AE (MedDRA Preferred Term, in more than 2% of the subjects).
  • AEs MedDRA Preferred Term
  • rheumatoid arthritis 36 subjects, 14.5%
  • flushing 13 subjects, 5.2%
  • Flushing was only reported by the subjects who participated in the CRH testing.
  • Upper respiratory tract infection, increased weight, or back pain were reported less frequently (seven subjects (2.8%) in each case).
  • Prednisone delayed-release is a novel, delayed-release tablet that has been developed to optimize the efficacy of orally administered low-dose prednisone in the treatment of RA.
  • Prednisone delayed-release has shown improved efficacy compared to standard prednisone in patients with RA without increasing their prednisone dose. This improvement has been solely obtained as a result of Prednisone delayed-release's unique release characteristics.
  • the safety profiles of Prednisone delayed-release and standard prednisone were comparable and the patients were thus not exposed to an increased risk.
  • Prednisone delayed-release tablets can be used in patients with severe, moderate or mild disease.
  • Prednisone delayed-release tablets can be used in patients with short, mid-term or long-lasting disease duration.
  • Prednisone delayed-release tablets can be used in patients pre-treated with corticosteroids, in those who are refractory to treatment or in corticoid na ⁇ ve patients.
  • Prednisone delayed-release tablets can be used as monotherapy or more likely in combination with DMARDs, NSAIDs, TNF ⁇ Inhibitors and/or analgetics.
  • Prednisone delayed-release tablets can be used for short, mid or long-term treatment.
  • Buttgereit F Burmester G-R, Lipworth B J. Optimised glucocorticoid therapy: the sharpening of an old spear. Lancet 2005;365:801-3.
  • Buttgereit F Saag K G, Cutolo M, da Silva J A P, Bijlsma J W J.
  • Buttgereit F Straub R H, Wehling M, Burmester G R. Glucocorticoids in the treatment of rheumatic diseases: an update on the mechanisms of action. Arthritis Rheum 2004;50:3408-17.
  • Kirwan J R The effect of glucocorticoids on joint destruction in rheumatoid arthritis.
  • Mastorakos G, Ilias I Relationship between interleukin-6 (IL-6) and hypothalamic-pituitary-adrenal axis hormones in rheumatoid arthritis.
  • IL-6 interleukin-6

Abstract

The present invention refers to the treatment of a rheumatic disease and/or osteoarthritis by administering a delayed-release dosage form of a glucocorticoid to a subject in need thereof.

Description

  • The present invention refers to the treatment of a rheumatic disease and/or osteoarthritis by administering a delayed-release dosage form of a glucocorticoid to a subject in need thereof.
    • BACKGROUND OF THE INVENTION Role of Low-Dose Corticoid Therapy in Clinical Practice
  • Diseases of rheumatoid nature like rheumatoid arthritis (RA) are chronic, autoimmune disorders in which inflammation of the synovial joint lining is accompanied by joint pain and stiffness and usually leads to bone and joint destruction, deformity, disability, and even death. RA affects about 1% of the population and is 2 to 3 times more common in women than in men (CPMP/EWP/556/95). Early diagnosis, suppression of inflammation, and aggressive treatment strategies are regarded as important requisites for a favorable outcome (Pincus 2005). Glucocorticoids are widely used to treat the disease and are often administered in combination with other drugs, especially disease-modifying antirheumatic drugs (DMARDs) and non-steroidal anti-inflammatory drugs (NSAIDs) (Bijlsma 2003). Prednisone, prednisolone and methylprednisolone are among the most common glucocorticoids for the treatment of RA.
  • Use and types of oral corticoid RA therapy differ according to region and published estimates vary. According to one source, in 2002 about 40 to 50% of patients in France, Germany, Italy and Spain received such therapy compared to about 20% in the United Kingdom (UK). Prednisone was the most common corticoid in France, Italy and Spain (94%, 59% and 43% of treated patients, respectively) whereas prednisolone was the most common in Germany and the UK (50 and 100%, respectively). A study in 150 patients who attended a US clinic during the period 1999 to 2001 showed that 144 (96%) patients took prednisone in combination with DMARDs (86%) or alone (10%) (Pincus 2005).
  • Glucocorticoids have a broad spectrum of anti-inflammatory and immunosuppressive effects. They act by inhibiting leukocyte traffic; interfering with functions of leukocytes, fibroblasts, and endothelial cells; and suppressing the synthesis and actions of inflammatory cytokines including interleukin-6 (IL-6) (Buttgereit 2005). When they were first introduced, glucocorticoids were administered to RA patients for long periods at high doses exceeding 10 mg/day prednisone or equivalent. These high-dose, long-term regimens were highly effective but were associated with pleiotropic effects and unacceptable adverse reactions. This led to the development of low-dose regimens in order to reduce the incidence of side effects and optimized the benefit:risk ratio (Buttgereit 2005). High corticoid doses are now only considered suitable for short-term therapy in special cases (e.g. for treatment of a severe flare of RA). Decreases in prescribed corticoid dose are illustrated by an evaluation of patients who attended a US clinic between 1984 and 1986 (1985 cohort) or between 1999 and 2001 (2000 cohort) (Pincus 2005). The mean prednisone dose was 7.8 mg/day in 1985 compared to 4 mg/day in 2000, with median doses of 5 and 4 mg/day, respectively.
  • Long-term, low-dose, corticoid therapy (defined as daily doses of ≦10 mg prednisone or equivalent) is currently recognized as an important part of standard treatment for RA (ACR guideline, Conn 2001). Below 10 mg the daily dose should be decreased stepwise until the lowest, still effective dose for disease control is reached. In addition to providing immediate relief of symptoms such as morning stiffness and pain, the low-dose corticoid regimen also prevents progression of disease. Several randomized studies performed since the mid-1990s have shown that low-dose prednis(ol)one slows the rate of joint damage (as measured by radiographic images) in patients with early, active RA. In a double-blind, placebo-controlled study, 7.5 mg/day prednisolone reduced joint destruction when given for 2 years in combination with other standard RA treatments (Kirwan 1995). When prednisolone was stopped, joint destruction returned to the same level as in the control group (Hickling 1998). In a more recent double-blind, placebo-controlled study, prednisone (10 mg/day) slowed progression of joint damage over periods of 2 and 5 years in patients who had not been pretreated with DMARDs (van Everdingen 2002, Jacobs 2005). In a double-blind, placebo-controlled study (Wassenberg 2005) and an open-label, DMARD-controlled study (Svensson 2005), prednisolone at doses of 5 and 7.5 mg/day, respectively, decreased radiographic progression when given in combination with DMARDs for 2 years. The increasing evidence for the disease-modifying effects of low-dose corticoid treatment has certainly contributed to renewed interest in this treatment regimen and increased use in clinical practice.
    • Safety of Low-Dose Long-Term Corticoid Therapy
  • Soon after glucocorticoids were introduced for the treatment of RA in the 1950s it became apparent that long-term use of high doses was associated with clinically significant side effects that included osteoporosis, glucose intolerance, infections, peptic ulcers and gastrointestinal bleeding, cataracts and glaucoma, as well as atherosclerotic disease. Several clinical studies and literature reviews have been performed to assess the safety profile of low-dose, long-term corticoid therapy. It is generally agreed that side effects can be reduced by using as low a dose as possible for each individual patient. One study that compared RA patients with and without prednisone treatment concluded that long-term prednisone use at doses ≧5 mg/day was associated with the dose-dependent development of specific AEs (Saag 1994). However, this study was retrospective with historical case controls and included prednisone doses up to 15 mg/day. A working group of rheumatologists and experts from other therapeutic areas has recently conducted a comprehensive literature review of the adverse effects of low-dose (≦10 mg/day prednisolone equivalent), long-term glucocorticoid therapy by a primary search of textbooks and review papers (da Silva 2006). Their review also included analysis of data from 4 prospective, randomized, controlled studies in which prednisolone (5 to 10 mg/day) was given to RA patients for 2 years (Capell 2004, Kirwan 1995, van Everdingen 2002, Wassenberg 2005). Common side effects seen at high doses were not observed at low doses or were less frequent. The experts concluded that “the overall fear of glucocorticoid toxicity in RA, as quoted in textbooks and review articles, is probably overestimated based on observations with higher dose therapy. The balance of risks and benefits of low-dose therapy clearly differs from that of medium- and high-dose therapy . . . ”. Osteoporosis, obesity, hypertension, family history of diabetes or glaucoma were listed as risk factors requiring more careful observation. In addition to osteoporosis, adverse effects that may need regular checks were defined as Cushingoid syndrome, adrenal crisis of corticoid withdrawal, new onset of diabetes mellitus, worsening of glycemia control in patients with diabetes mellitus, cataracts, glaucoma, peptic ulcer (in combination with NSAIDs), and hypertension.
    • Delayed-Release Prednisone Tablets
  • Patients with active RA suffer from clinical signs and symptoms that include joint stiffness, pain, and swelling. Patients have assessed these symptoms (and related factors such as disability and mobility) as being important outcomes of RA treatment (Ahlmen et al. 2005, Carr et al. 2003, Hewlett et al. 2005). Clinical symptoms vary during the day and are more severe early in the morning after awakening than in the afternoon or evening (Cutolo et al. 2003, Cutolo and Masi 2005). Indeed, morning stiffness is such a typical symptom of RA that it has become a standard diagnostic criterion for the disease (Arnett et al. 1988, ACR Guideline 2002).
  • The mechanisms responsible for the circadian variation of RA symptoms are complex and involve the HPA axis and endogenous inflammatory mediators. Inflammation causes increased production of inflammatory cytokines. In comparison with healthy subjects, RA patients therefore have higher serum concentrations of interleukins (IL), especially IL-6, and tumor necrosis factor-alpha (TNF-α) and levels display a pronounced circadian rhythm, with higher night-time concentrations that peak at 02:00 to 06:00 (Arvidson et al. 1994; Crofford 1997; Cutolo 2003, 2005).
  • Increased levels of IL-6 are produced in response to inflammation but IL-6 is a potent activator of the HPA axis and stimulates the release of cortisol from the adrenal cortex to counteract the inflammation (Cutolo 2005, Mastorakos 2000). In RA patients, it seems that the response of the permanently stimulated HPA axis is inadequate and levels of endogenous cortisol are insufficient to combat the inflammation (Gudbjöornsson 1996). Administration of exogenous glucocorticoids acts—among other therapeutic effects—as a replacement therapy and supplements the inadequate levels of endogenous cortisol (Cutolo 2005).
  • Endogenous cortisol and exogenous therapeutic glucocorticoids inhibit the synthesis of IL-6 and other pro-inflammatory cytokines. In this context, prednis(ol)one and methylprednisolone are ideally suited exogenous corticoid due to its comparatively short half-life of 3-4 h. Low-dose oral prednis(ol)one or methylprednisolone are usually given for symptomatic relief as a single morning dose to minimize potential interference with the HPA axis. However, in order to provide optimal relief of morning stiffness and joint pain it has been proposed that the drug should be given shortly before the expected nocturnal increase of IL-6. A randomized study has investigated the efficacy of standard IR (Immediate Release) low-dose prednisolone (5 or 7.5 mg/day) given at 02:00 or at 07:30 for 4 days in 26 patients with active RA who were being treated with standard anti-rheumatic drugs (predominantly NSAIDs) but who had not received glucocorticoids in the 3 months before the study (Arvidson et al. 1997). Night-time administration of prednisolone at 02:00 resulted in highly statistically significant improvements in morning stiffness, joint pain, as well as suppression of serum concentrations of IL-6 (p<0.01). Much smaller effects (p<0.05) were only observed for morning stiffness and IL-6 concentrations after conventional morning dosing at 07:30. The authors concluded that low doses of glucocorticoids improved acute RA symptoms if they were administered before the circadian flare of increased IL-6 synthesis and inflammatory activity. However, it remained unclear what would happen to the patients if they would be treated for a longer period of time.
  • Karatay et al investigated in 2002 the administration of an IR low-dose prednisone tablet over a period of 6 months at 02:00 vs 07:30. The results were disappointing because a difference in morning stiffness could not be observed. One explanation of this could be that the short term effects observed by Arvidson disappear after several days or weeks of therapy. Thus, the effects on long term night time administration of glucocorticoids remained unclear.
  • Furthermore, all patients in both study (Arvidson 1997; Karatay 2002) were corticoid naïve. Thus, the question has arisen, how low-dose night-time prednisone would work in patients already pre-treated with low-dose corticoids and what would happen if they would get the night-time dose over a longer time with a higher compliance rate.
  • Although administration of glucocorticoids at 02:00 resulted in improved efficacy in one of two studies, in practice this would be highly inconvenient for the patient and likely to result in poor quality of sleep and/or compliance.
  • U.S. Pat. No. 5,792,476 describes a pharmaceutical composition for peroral administration for rheumatoid arthritis, which comprises a glucocorticoid as active ingredient and which leads to release in the small intestine. The composition is a granulate which is laminated with an inner layer which is resistant to a pH of 6.8, and with an outer layer which is resistant to a pH of 1.0.
  • U.S. Pat. No. 6,488,960 describes a pharmaceutical dosage form for controlled release of corticoids, reference being made to the formulations described in U.S. Pat. No. 5,792,476.
  • WO 01/08421 describes a tablet having a core which is coated by at least two layers, one of which completely encloses the other. The coating layers can be produced by spray coating and/or pressing.
  • WO 01/68056 discloses a pharmaceutical preparation having a release profile with a time delay, comprising a core and at least one hydrophilic or lipophilic coating surrounding the core, where the coating is slowly swollen, dissolved, eroded or changed in its structure in another way through the water present in the release medium, so that the core or parts of the core become accessible to the release medium. The coating may be formed for example as pressed coating.
  • WO 02/072034 discloses a pharmaceutical dosage form for delayed release, having a core which comprises as active ingredient a glucocorticoid and a material which brings about delayed release and includes at least one natural or synthetic gum.
  • WO 2004/093843 discloses a tablet with a specific core geometry to release the active ingredient in a specific delayed release manner.
  • WO 2006/027266 discloses a pharmaceutical dosage form with site-and time controlled gastrointestinal release of an active agent, particularly a corticosteroid. The pharmaceutical dosage form is preferably a coated tablet having a core comprising the corticosteroid and a swellable/disintegration adjuvant, and an inert outer coating. The coating is compressed at a pressure chosen to result in the release of the corticosteroid at a predetermined position in the gastrointestinal tract.
    • SUMMARY OF THE INVENTION
  • The present inventors have carried out a clinical study in order to test the efficacy of a delayed-release prednisone tablet compared to a standard immediate-release tablet. It was found that long-term administration of the delayed-release prednisone tablet shows a surprisingly increased efficacy compared to the treatment with a standard immediate-release prednisone tablet.
  • Thus, a first aspect of the invention refers to the use of a delayed-release dosage form of a corticosteroid for the manufacture of a medicament for the long-term treatment of a rheumatic disease and/or osteoarthritis.
  • A further aspect of the invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
      • (i) patients with severe diseases,
      • (ii) patients with moderate diseases,
      • (iii) patients with mild diseases,
      • (iv) patients with short disease duration (<2 years),
      • (v) patients with mid-term disease duration (2-5 years) or
      • (vi) patients with long-lasting disease duration (>5 years).
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
      • (i) patients with severe, long lasting morning stiffness
      • (ii) patients with moderate morning stiffness;
      • (iii) patients with mild morning stiffness;
      • (iv) patients with severe, long lasting pain
      • (v) patients with moderate pain;
      • (vi) patients with mild pain.
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
      • (i) patients with high Interleukin 6 levels;
      • (ii) patients with medium Interleukin 6 levels or
      • (iii) patients with low Interleukin 6 levels.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in
      • (i) patients who have been pre-treated with an immediate release dosage form of a glucocorticoid,
      • (ii) patients who are refractory to treatment with an immediate release dosage form of a glucocorticoid, or
      • (iii) glucocorticoid naive patients.
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of rheumatic diseases in
      • (i) patients who have been pre-treated with other medicaments like a NSAID, a DMARD, a TNFα inhibitor, an IL-6 inhibitor and/or an analgetic agent or any combination thereof, or
      • (ii) patients who have not been pre-treated with any other medicaments like a NSAID, a DMARD, a TNFα inhibitor, an IL-6 inhibitor and/or an analgetic agent.
  • Still a further aspect of the present invention refers to the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis in combination with at least one further medicament which is a NSAID, a DMARD, a TNFα inhibitor, an IL-6 inhibitor and/or an analgetic agent.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of a rheumatic disease and/or osteoarthritis without any further medicament.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for treatment of a rheumatic disease and/or osteoarthritis in combination with reduced doses of at least one further medicament which is a NSAID, a DMARD, a TNFα inhibitor, an IL-6 inhibitor and/or an analgetic agent.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of ankylosating spondylitis, polymyalgia rheumatica and/or osteoarthritis.
  • Still a further aspect of the present invention is the use of a delayed-release dosage form of a glucocorticoid for the manufacture of a medicament for the treatment of morning stiffness, pain and/or inflammation parameters such as release of cytokines, e.g. in a rheumatic disease and/or osteoarthritis.
  • Still a further aspect of the present invention is a method for the treatment of a patient suffering from signs and symptoms of an underlying rheumatic disease and/or osteoarthritis, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at least about two weeks.
  • Still a further aspect of the present invention is a method for the treatment of a patient suffering from morning stiffness and pain due to an underlying rheumatic disease and/or osteoarthritis, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at lest about two weeks.
  • Still a further aspect of the present invention is a method for the treatment of a patient having circadian fluctuations in Interleukin 6 levels due to underlying inflammation, which comprises administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at least about two weeks, and wherein said treatment is administered such that the glucocorticoid is released at or before the time when the patient's Interleukin 6 level is at a daily peak.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • FIG. 1 shows duration of Morning Stiffness: Relative Change from Baseline in % (SEM) per week of treatment in the ITT population.
  • FIG. 2 shows duration of Morning Stiffness: Relative Change from Baseline in % (SEM) per month of treatment in the ITT population.
  • FIG. 3 shows IL 6 values (median) under treatment of Prednisone delayed release tablets.
    •  DETAILED DESCRIPTION OF THE INVENTION
  • The present invention refers to the use of a delayed-release dosage form of a glucocorticoid. The release of the active ingredient is preferably delayed for a time period of 2-10 hours after intake, preferably 2-6, more preferably 3-5 hours after intake the active ingredient may be released in the upper sections of the intestine and/or in the lower sections of the intestine. More preferably, the active ingredient is released in the upper sections of the intestine within a period of 2-6 hours. The delayed-release dosage form is preferably administered to the patient at or before bedtime, more preferably in the evening, e.g. from about 9:00 pm to about 11:00 pm. Because inflammation is accompanied with circadian fluctuations in the concentration of pro-inflammatory cytokines (such as Interleukin-6) which peaks during sleeping hours, bedtime administration allows an efficacious concentration of the active ingredient to be present when such concentration peaks.
  • The delayed-release dosage form is preferably a tablet, e.g. as described in WO 2006/027266, which is herein incorporated by reference. The dosage form preferably comprises
      • (a) a core having at least one glucocorticoid-active ingredient and having at least one swellable adjuvant and/or a disintegrant such that the active ingredient is rapidly released from the dosage form when the core is contacted with gastrointestinal fluids, and
      • (b) an inert, e.g. a non-soluble and non-swellable coating pressed onto the core, said coating being capable of preventing substantial release of the active ingredient for a defined time period following ingestion of the dosage form.
  • The inert coating initially prevents release of the active ingredient or the active ingredient combination over an exactly defined period, so that no absorption can occur. The water present in the gastrointestinal tract penetrates slowly in through the coating and, after a time which is previously fixed by the pressure for compression, reaches the core. The coating ingredients show neither swelling nor diluting of parts of the coating. When the core is reached, the water penetrating in is very rapidly absorbed by the hydrophilic ingredients of the core, so that the volume of the core increases greatly and, as a consequence thereof, the coating completely bursts open, and the active ingredient and the active ingredient combination respectively is released very rapidly.
  • A particularly advantageous embodiment of this press-coated delayed-release tablet is achieved when a previously compressed core tablet is subsequently compressed with a multilayer tablet press to a press-coated tablet.
  • The tablet coating typically consists of the following materials in order to achieve a delayed release profile:
      • polymer or copolymer of acrylic acid, methacrylic acid etc. (e.g. Eudragits or Carbopol),
      • cellulose derivatives such as hydroxypropylmethylcellulose, hydroxypropylcellulose, carboxymethylcellulose, ethylcellulose, cellulose acetate,
      • polyvinyl alcohol,
      • polyethylene glycol,
      • salts of higher fatty acids, esters of monohydric or polyhydric alcohols with short-, medium- or long-chain, saturated or unsaturated fatty acids. Specifically, stearic acid triglycerides (e.g. Dynersan) or glycerol behenate (e.g. Compritol) are used.
  • In addition, further adjuvants should also be added to these materials so that the tablet coating can be compressed. Typically used here are fillers such as lactose, various starches, celluloses and calcium hydrogen phosphate or di-basic calcium phosphate. The glidant used is normally magnesium stearate, and in exceptional cases also talc and glycerol behenate. A plasticizer is often also added to the coating material, preferably from the group of polyethylene glycol, dibutyl phthalate, diethyl citrate or triacetin.
  • In order to achieve an optimal release profile, the tablet core must also fulfil certain tasks and exhibit certain properties. Thus, after the lag phase has elapsed, a rapid release profile is achieved if typical disintegrants are added to the inner core, which are derived for example from the group of the following substances: cellulose derivatives, starch derivatives, crosslinked polyvinylpyrrolidone. The use of a blowing agent, for example resulting from a combination of a weak acid and a carbonate or bicarbonate, may also promote rapid release. The tablet core typically consists additionally of matrix or filling ingredients (e.g. lactose, cellulose derivatives, calcium hydrogen phosphate or other substances known from the literature) and lubricant or glidant (usually magnesium stearate, in exceptional cases also talc and glycerol behenate).
  • The size of the core tablet preferably should not exceed 6 mm (preferably 5 mm) in diameter, because otherwise the press-coated tablet becomes too large for convenient ingestion. As a result thereof, the dosages of the active ingredients are in the range from 0.1 to 50 mg, very particularly between 1 and 20 mg.
  • The in vitro release profile of the dosage form according to the invention is preferably such that less than 5% of the active ingredient is released during the lag phase. After the release phase has started, preferably ≧80%, particularly preferably ≧90%, of the active ingredient is released within one hour. More preferably, the delayed-release dosage form has a dissolution time of equal to or less than about 2 hours after the lag time has been reached). The in vitro release is preferably determined using the USP paddle dissolution model in water.
  • The employed active ingredients are derived from the group of glucocorticoids and all show comparable physicochemical properties. Such include cortisone, hydrocortisone, prednisone, prednisolone, methylprednisolone, budesonide, dexamethasone, fludrocortisone, fluocortolone, cloprednole, deflazacort, triamcinolone, or the corresponding pharmaceutically acceptable salts and/or esters thereof. This applies in particular to prednisone, prednisolone, methylprednisolone, budesonide, dexamethasone, fluocortolone, cloprednole, and deflazacort or the corresponding pharmaceutically acceptable salts and/or esters thereof.
  • In the present case of the delayed-release tablet, the following combination of core materials and coating materials has proved to be particularly suitable for achieving a time- and site-controlled release with exclusion of pH and food influences:
  • The coating preferably comprises:
      • hydrophobic, waxy substances with an HLB value of less than about 5, preferably around 2. Carnauba wax, paraffins, cetyl ester waxes are preferably employed therefor. Glycerol behenate has proved to be particularly suitable. The use of about 20-60%, in particular about 30-50%, in the coating has proved to be very advantageous;
      • non-fatty, hydrophobic filling materials such as calcium phosphate salts, e.g. dibasic calcium phosphate. The use of about 25-75% of these filling materials, in particular of about 40-60%, in the coating has proved to be very advantageous here;
      • in addition, the tablet coating preferably also consists of binders, e.g. polyvinylpyrrolidone (PVP), typically in concentrations of about 4-12%, specifically about 7-10%, and glidants such as magnesium stearate, in concentrations of about 0.1-2%, in the specific case of about 0.5-1.5%. Colloidal silicon dioxide can for example be used as flow regulator, normally in concentrations of about 0.25-1%. In addition, to distinguish different dosages, a colorant can be added to the tablet coating, preferably an iron oxide pigment in concentrations of about 0.001-1%.
  • The core tablet preferably comprises:
      • an active ingredient or an active ingredient combination from the group of glucocorticoids, preferably prednisone, prednisolone, methylprednisolone, budesonide, dexamethasone, fludrocortisone, fluocortolone, cloprednole, deflazacort, and triamcinolone, and the corresponding salts and esters thereof. The dosages of the active ingredients are in the region of about 0.1-50 mg, very especially between about 1 and 20 mg;
      • in addition, the core tablet preferably comprises a filler such as, for example, lactose, starch derivatives or cellulose derivatives. Lactose is preferably employed. The filler is typically present in concentrations of about 50-90%, specifically of about 60-80%. A disintegrant is additionally present and is typically crosslinked PVP or sodium carboxymethylcellulose, typically in concentrations of about 10-20%. It is additionally possible for a binder, e.g. PVP, to be present, typically in concentrations of about 2-10%, specifically of about 5.5-9%, and a lubricant such as magnesium stearate, in concentrations of about 0.1-2%, in the specific case of about 0.5-1.5%. Colloidal silicon dioxide is normally used as flow regulator, normally in concentrations of about 0.25-1%. It is additionally possible, for visually distinguishing the core from the coating, to add a colorant, preferably an iron oxide pigment in concentrations of about 0.01-1%.
  • Preferably, the delayed-release dosage form is administered as a long-term treatment to a subject in need thereof for a time sufficient to reduce and/or abolish the disease and/or disease symptoms. The long term treatment usually comprises daily administration of the medicament for an extended period of time, e.g. for at least two weeks, preferably for at least 4 weeks, more preferably for at least 8 weeks, even more preferably for at least 12 weeks, and most preferably for at least 6 months or at least 12 months.
  • According to the present invention refers to the novel treatment of groups of patients suffering from rheumatic diseases and/or osteoarthritis. These patient groups are selected from:
      • (i) patients with severe diseases characterized by a Disease Activity Score (DAS) of >5.1 (Le Loet 2006) and/or a Physicians Assessment;
      • (ii) patients with moderate diseases characterized by a Disease Activity Score (DAS) of >3.2 but <5.1 and/or a Physicians Assessment;
      • (iii) patients with mild diseases characterized by a Disease Activity Score (DAS) of <3.2 and/or a Physicians Assessment;
      • (iv) patients with short disease duration of less than 2 years,
      • (v) patients with mid-term disease duration of 2-5 years, and
      • (vi) patients with long-lasting disease duration of more than 5 years.
  • Further patient groups may be selected from:
      • (i) patients with severe, long lasting morning stiffness characterized by a duration of morning stiffness >180 min,
      • (ii) patients with moderate morning stiffness between 100 and 180 min,
      • (iii) patients with mild morning stiffness of less than 100 min,
      • (iv) patients with severe, long lasting pain characterized by a VAS scale with >70 mm,
      • (v) patients with moderate pain characterized by a VAS scale with >50-70 mm,
      • (vi) patients with mild pain characterized by a VAS scale with <50 mm.
  • Further patient groups may be selected from:
      • (i) patients with high Interleukin 6 levels, e.g. more than 3000 IU/l;
      • (ii) patients with medium Interleukin 6 levels, e.g. between 3000 and 1000 IU/l;
      • (iii) patients with low Interleukin 6 levels, e.g. less than 1000 IU/l.
  • Further patient groups may be selected from:
      • (i) patients who have been pre-treated with an immediate release dosage form of a glucocorticoid;
      • (ii) patients who are refractory to treatment with an immediate-release dosage form of a glucocorticoid, and
      • (iii) glucocorticoid naive patients.
  • Further patient groups may be selected from:
      • (i) patients who have been pre-treated with other medicaments like a NSAID, a DMARD, a TNFα inhibitor and/or an analgetic agent or any combination thereof, and
      • (ii) patients who have not been pre-treated with any other medicaments like a NSAID, a DMARD, a TNFα inhibitor, an Interleukin 6 inhibitor and/or an analgetic agent.
  • By means of administering a delayed-release tablet, the daily dose of the glucocorticoid may be substantially reduced compared to an immediate-release tablet of the glucocorticoid. Thus, the disease-inhibiting effect may be obtained by a significantly lower dose of the active ingredient, whereby the occurrence and/or intensity of site effect is diminished. For example, the daily dose of the glucocorticoid can be reduced by at least 10%, more preferably by at least 20%, e.g. by 10-50% compared to an immediate-release tablet. Thus, the reduced daily dose of prednis(ol)one in Prednisone delayed-release is preferably in the range of 1 to 5 mg/day compared to 6-10 mg/day for a standard IR tablet.
  • The treatment according to the present invention may comprise the treatment of a rheumatic disease and/or osteoarthritis without any further medicament. On the other hand, the invention may comprise the treatment of a rheumatic disease and/or osteoarthritis in combination with at least one further medicament which is preferably selected from the groups of NSAIDs, DMARDs, TNF α inhibitors, IL-6 inhibitors, analgetic agents or combinations thereof. Especially preferred is a combination with Tarenflurbil.
  • NSAIDs are preferably selected from arylalkanoic acids (Diclofenac, Indometacin, Sulindac) from 2-arylpropionic acids (Carprofen, Fenoprofen, Flurbiprofen, Ibuprofen, Ketoprofen, Ketorolac, Laxoprofen, Naproxen, Tiaprofenic acid), from N-arylanthranilic acids (Mefenamic acid, Meclofenamic acid), from Oxicams (Piroxicam, Meloxicam) or from Coxibs (Celecoxib, Parecoxib, Etoricoxib) or from combinations thereof. Especially preferred is a combination with Tarenflurbil.
  • DMARDs are preferably selected from gold preparations, chloroquine, azathioprine, sulfasalazine, cyclophosphamide, penicillamine, hydroxychloroquine, methotrexate, thorium dioxide suspension, levamisole, cyclosporin, interferone, leflunomide or from combinations thereof.
  • TNF α inhibitors and IL 1 inhibitors are preferably selected from antibodies or soluble receptors such as etanercept, inflixima, anakinra, adalimumab and from cominations thereof.
  • IL-6 inhibitors are preferably selected from antibodies or soluble receptors such as tocilizumab.
  • Analgetic agents are preferably selected from salicylates (Aspirin, Methyl salicylate, Diflunisal, Benorylate, Faislamine, Amoxiprin), from pyrazolidine derivatives (Phenylbutazone, Oxyphenylbutazone) or paracetamol or from combinations thereof.
  • The dose of the at least one further medicament may be substantially reduced e.g. by at least 10%, preferably by at least 20%, e.g. by 10-50%. Alternatively, the first usage of TNF α inhibitors or IL-6 inhibitors can be postponed to a later point in time.
  • The present invention particularly refers to the treatment of a rheumatic disease selected from rheumatoid arthritis, ankylosating spondylitis, polymyalgia rheumatica and/or to the treatment of osteoarthritis. Based on the results of the clinical trials described in the present application, it is evident that the delayed-release dosage form of a glucocorticoid, particularly a long-term treatment, is of therapeutic benefit. Particularly in the case of osteoarthritis or a rheumatic disease having an osteoarthritic component, the administration of the delayed-release dosage form is effective without having undesired side effects.
  • The dose of the glucocorticoid may vary during the course of treatment. For example, the patient may be administered a relatively high dose during the initiation of therapy (e.g., about 10-40 mg/day or higher of prednisone, or an equivalent amount of another glucocorticoid), which may be reduced downward over a period of time (e.g., over 3-4 weeks) according to the patient's response, to a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid. Alternatively, the patient may be started on a relatively low dose, which may be adjusted upward over a period of time (e.g., over 3-4 weeks) to a maintenance therapy dose of about 10 mg/day or less of prednisone, or an equivalent amount of another glucocorticoid.
  • Further, the present invention is described in more detail by the following examples.
    • EXAMPLE
  • Clinical studies. The clinical development program supporting the present application for the delayed-release prednisone tablet “Prednisone delayed-release” comprised 3 phase I studies and 1 phase III study:
      • Phase I studies: These 3 randomized, open-label, crossover studies on 69 healthy men investigated the comparative bioavailability and pharmacokinetic characteristics of 6 experimental galenic delayed-release formulations each containing 5 mg prednisone. The studies were performed to allow selection of a delayed-release tablet with appropriate characteristics for evening administration to RA patients (i.e. a suitable lag time and high bioavailability that was not affected by food). Single doses of each of the delayed-release tablets were compared to a single dose of a reference immediate release (IR) prednisone tablet (Decortin® 5 mg tablets marketed by Merck KGaA).
      • Phase III study: In this randomized, parallel-group, double-blind, double-dummy study on 288 adult RA patients, the final prednisone delayed-release tablet formulation was administered in the evening for 12 weeks. The daily prednisone dose of 3 to 10 mg was achieved with 1 and 5 mg tablets. Efficacy and safety were compared with the reference IR product given in the morning.
  • This is a novel study design which was not used by Arvidson (1997) or Karatay (2002) as patients in these studies were corticoid naïve. In those studies the administration of a standard IR prednis(ol)one tablet at 2.00 and 8.00 was compared.
    • Study Design and Methodology
  • Study design. The studies were specifically designed to compare the efficacy and safety of Prednisone delayed-release given in the evening with standard IR prednisone (Decortin®, Merck KGaA) given in the morning at 08:00 over a period of 12 weeks. Prednisone delayed-release and the reference product both contained the same drug (prednisone) and differed solely with respect to the timepoint at which this was released in the gastrointestinal tract. Timing of the evening dose (22:00±30 min) was based on results from a previous pharmacokinetic study with Prednisone delayed-release which showed first detectable plasma concentrations of prednisone and its active metabolite prednisolone after 4 hours and maximal plasma concentrations about 6 h after administration. This specific plasma profile with Cmax at 04:00 is expected to suppress the known early morning increase of pro-inflammatory cytokines, and thus reduce morning stiffness.
  • Inclusion of a placebo arm was not considered necessary or ethical due to the proven efficacy of prednisone. Blinding was essential in this study to avoid bias. As the Prednisone delayed-release tablets and reference product tablets differed in appearance a double-dummy technique was used to maintain the treatment blind.
  • The study had a 1-to 2-week screening period that was followed by a 12-week double-blind treatment period with visits after 2 and 6 weeks. This 12-week period was considered to be sufficiently long to demonstrate any differences in the primary and secondary efficacy endpoints (see below). At the end of the 12-week double blind period, patients who completed the 12-week double-blind period were offered to continue in an open-label 9-month follow up period, during which all patients received active treatment with Prednisone delayed-release.
  • Prednisone dose. Patients were to continue on the same stable low dose of prednisone (or equivalent) that they received in the month before entering the study. During the study prednisone doses of 3 to 10 mg/day were achieved with appropriate combinations of Prednisone delayed-release or IR tablets containing 1 and 5 mg prednisone; daily doses of 2.5 and 7.5 mg prednisone were rounded to 3 and 8 mg, respectively. A constant low prednisone dose was given throughout the treatment phase to ensure that any differences between the treatment groups were not due to dose changes.
  • Primary objective and efficacy endpoint. The primary objective of the study was to show whether administration of the new delayed-release formulation of prednisone (i.e. Prednisone delayed-release) in the evening was superior to the standard morning administration of immediate-release (IR) prednisone in reducing the duration of morning stiffness. The patient diary card was appropriately designed to capture relevant clock times in minutes: wake-up, morning medication intake, resolution of morning stiffness. The primary variable was “the relative change in duration of morning stiffness from baseline at individual study end in the double-blind treatment phase”, whereby the duration of morning stiffness was the difference between the time of resolution of morning stiffness and the time of awakening. Morning stiffness was chosen as the primary variable because it was expected to be directly affected by inhibition of night-time IL-6 peaks after delayed release of prednisone.
  • Secondary efficacy endpoints. In addition to morning stiffness, the study included a comprehensive battery of supportive secondary endpoints that were based on regulatory recommendations (CPMP/EWP/556/95 rev 1). Patients assessed their quality of sleep, pain intensity (VAS), and global disease activity (VAS). They also documented their use of analgesics and completed validated questionnaires on their health status (HAQ) and quality of life (SF36). Investigators counted the numbers of swollen and tender joints (28 joints) and assessed global disease activity (5-point scale). Laboratory variables (ESR, CRP, IL-6) were assessed from blood samples taken as early as possible in the morning to investigate the inflammatory state of the disease. Osteocalcin was also measured as an indicator of bone metabolism.
  • Two validated composite variables were used: the disease activity score (DAS 28) and the ACR20 responder rate. The DAS 28 was computed from the joint scores, the ESR and the patient's global assessment of disease activity. An ACR responder was defined as a patient with improvement of at least 20% of the baseline values in the tender joint count, swollen joint count and at least 3 of the following 5 variables: pain intensity, investigator global assessment, patient global assessment, HAQ disability index, or ESR.
  • Inclusion criteria were designed to enroll adult patients (18 to 80 years) with active RA who were typical of the general RA population being treated with a combination of stable corticoid medication and DMARDs. Patients had to have a documented history of RA and present with active symptoms of disease, i.e. morning stiffness of 45 min, pain ≧30 mm (VAS), ≧3 painful joints, ≧1 swollen joints and elevated ESR and/or CRP.
  • Patients had to have been treated with the following state-of-the-art RA medications for at least 3 months before entering the study:
      • DMARDs (unless they were not tolerated)
      • Prednis(ol)one, with a low, stable dose of 2.5 to 10 mg prednisone (or equivalent) for at least 1 month prior to screening
  • Patients were to continue on their RA medications at the same dose throughout the 12-week double-blind treatment phase. These restrictions are considered appropriate because they ensure that any differences between the treatment groups were due to the different dosing modalities of prednisone not to dose changes in the corticoid or concomitant DMARDs.
    • Study Results
  • 288 randomized patients were treated in total, 144 patients with Prednisone delayed-release and 144 with the IR reference product. The baseline characteristics of the two treatment groups were comparable (mean values for the overall population): age (55 years), gender (85% female), morning stiffness (173 min), disease duration (115 months), DAS 28 (5.9), daily dose of prednis(ol)one (6.6 mg), medications prior to screening (DMARDs 94%, non-steroidal anti-inflammatory drugs [NSAIDs] 80% patients). Also the medical history of the patients in both treatments are comparable. Table 1 summarizes the Disease characteristics. Patients with different disease duration (short, mid-term and long-lasting) and different disease activity (DAS: mild, moderate and severe) were included.
  • TABLE 1
    Disease characteristics at baseline (ITT population)
    Prednisone Standard IR
    Disease characteristics delayed-release prednisone Total
    at baseline (N = 144) (N = 144) (N = 288)
    RA
    No. of subjects n (%) 144 (100.0) 144 (100.0) 288 (100.0)
    Mean Duration Months 115.1  115.4  115.3 
    Duration <2 years, n (%) 19 (13.2) 18 (12.5) 37 (12.8)
    2-5 years, n (%) 37 (25.7) 37 (25.7) 74 (25.7)
    5-10 years, n (%) 33 (22.9) 31 (21.5) 64 (22.2)
    >10 years, n (%) 55 (38.2) 58 (40.3) 113 (39.2) 
    Pre-treatment (yes) 144 (100.0) 144 (100.0) 288 (100.0)
    Stable dose [mg] Mean 6.5 6.7 6.6
    of prednis(ol)one
    DAS28 Mean 5.8 5.9 5.9
    SD 0.8 0.9 0.8
    Range 3.3-8.1 3.7-7.7 3.3-8.1
    Disease Asymptomatic 0 (0.0) 0 (0.0) 0 (0.0)
    activity Mild 13 (9.0)  14 (9.7)  27 (9.4) 
    (physician's Moderate 103 (71.5)  102 (70.8)  205 (71.2) 
    assessment) Severe 28 (19.4) 28 (19.4) 56 (19.4)
    [n (%)] Very severe 0 (0.0) 0 (0.0) 0 (0.0)
    Pain intensity mean 57.9  59.7  58.8 
    (HAQ-VAS) [mm] SD 14.8  15.8  15.3 
    Range 18-95 25-96 18-96
    HAQ-DI score mean 1.5 1.5 1.5
    SD 0.6 0.5 0.5
    Range 0.0-2.9 0.0-2.8 0.0-2.9
    • Efficacy Results
  • Primary efficacy variable and morning stiffness. As planned, the primary efficacy analysis in the study was performed on the intention-to-treat population (i.e. all randomized patients as randomized) using “last observation carried forward” methodology.
  • TABLE 2
    Duration of morning stiffness after 12 weeks
    of treatment (intention-to-treat population)
    Duration of morning Prednisone delayed- Prednisone Standard
    stiffness (mean (SD)) release (N = 144) (N = 144)
    Baseline [min] 164.1 (101.4) 182.5 (125.0)
    (N = 125) (N = 129)
    At Week 12 (Final week) 120.9 (140.5) 157.4 (145.6)
    [min] (N = 127) (N = 131)
    Relative change [%] −22.66 (89.1)  −0.39 (89.0) 
    (N = 125) (N = 129)
    Treatment difference
    LS mean (SD) [%] 22.4 (11.1)
    Lower limit of 95% CI 0.493
    p-value 0.0226 (one-sided)
  • The primary variable was “the relative change in duration of morning stiffness from baseline at individual study end in the double-blind treatment phase”, whereby the duration of morning stiffness was the difference between the time of resolution of morning stiffness and the time of awakening. The reduction in duration of morning stiffness under Prednisone delayed-release treatment was higher than under standard IR prednisone throughout the 12-week treatment period.
  • At the end of the first week of treatment there was a difference of 10% between the two treatment groups. The relative reduction between baseline and final week of treatment was 22.7% in the Prednisone delayed-release group and 0.4% in the standard prednisone group. Thus, Prednisone delayed-release was shown to be superior to standard prednisone IR tablet in a statistically significant manner (p<0.025, one sided) and the primary study objective was met.
  • A difference between the two groups is obvious from the first week on, however the longer the treatment the more pronounced are the differences in favour for Prednisone delayed-release. This is illustrated in Table 3 and FIG. 1:
  • TABLE 3
    Mean daily duration of morning stiffness
    per week (intention-to-treat population)
    Mean daily duration
    of morning stiffness Prednisone
    per week (mean delayed-release Prednisone Standard
    (SD)) (N = 144) (N = 144)
    Baseline [min] 164.1 (101.4) (N = 125) 182.5 (125.0) (N = 129)
    At Week 1 [min] 159.4 (127.3) (N = 126) 186.4 (135.6) (N = 131)
    Relative change [%] −1.4 (62.4) (N = 124) 9.3 (60.2) (N = 129)
    At Week 2 [min] 144.9 (136.4) (N = 123) 187.7 (154.4) (N = 131)
    Relative change [%] −12.5 (70.0) (N = 121) 8.1 (71.6) (N = 129)
    At Week 3 [min] 138.3 (137.1) (N = 122) 164.2 (137.2) (N = 127)
    Relative change [%] −13.8 (73.9) (N = 120) 0.3 (63.6) (N = 125)
    At Week 4 [min] 129.5 (128.3) (N = 117) 163.7 (124.2) (N = 123)
    Relative change [%] −23.3 (54.7) (N = 115) 3.5 (72.5) (N = 121)
    At Week 5 [min] 126.0 (126.9) (N = 117) 159.7 (128.5) (N = 121)
    Relative change [%] −25.9 (55.1) (N = 115) 6.0 (85.1) (N = 119)
    At Week 6 [min] 117.9 (128.2) (N = 112) 154.2 (123.7) (N = 119)
    Relative change [%] −28.3 (59.8) (N = 110) 5.3 (82.5) (N = 117)
    At Week 7 [min] 109.0 (113.9) (N = 109) 156.5 (144.9) (N = 119)
    Relative change [%] −33.5 (49.1) (N = 107) −2.6 (74.2) (N = 117)
    At Week 8 [min] 98.7 (93.8) (N = 105) 152.1 (125.3) (N = 116)
    Relative change [%] −37.1 (45.8) (N = 103) −5.2 (62.5) (N = 114)
    At Week 9 [min] 90.7 (87.5) (N = 107) 146.4 (123.1) (N = 116)
    Relative change [%] −41.3 (46.5) (N = 105) −5.6 (68.8) (N = 115)
    At Week 10 [min] 92.7 (90.8) (N = 105) 147.9 (134.1) (N = 117)
    Relative change [%] −40.5 (46.9) (N = 103) −5.0 (83.0) (N = 116)
    At Week 11 [min] 95.9 (97.2) (N = 103) 148.9 (136.4) (N = 116)
    Relative change [%] −37.7 (50.1) (N = 101) −1.2 (95.8) (N = 115)
    At Week 12 [min] 98.1 (100.5) (N = 102) 149.5 (134.8) (N = 111)
    Relative change [%] −33.1 (75.4) (N = 100) −3.4 (92.1) (N = 111)
  • The weekly assessment of the mean daily duration of morning stiffness revealed that the decrease and thus the improvement begins already after 2 weeks of treatment in the Prednisone delayed-release group. The mean daily duration of morning stiffness continues to decrease steadily thereafter, whereas in the prednisone standard group, there was no clear tendency for the changes during the 12-week treatment.
  • This result is surprising as Karatay showed in 2002 that such an effects could not be expected.
  • Due to the superiority of Prednisone delayed-release against standard Prednisone of a reduction in the daily dose of e.g. 25-30% could be possible under
  • In the Phase III trial the superiority of a very low dose of Prednisone in the new delayed-release tablet compared to standard IR prednisone could be shown supporting the proposed dose reduction.
  • Table 4 shows the frequencies of starting stable doses of prednisone in the Predisone delayed-release and standard prednisone groups of the intention-to-treat (ITT) population. The frequency profiles in both treatment groups were similar, with the most common dose being 5 mg (50% subjects), followed by 7 and 10 mg (approximately 20% each).
  • TABLE 4
    Frequencies of stable doses of prednisone
    at start of study (ITT population)
    Number (%) subjects
    Stable Prednisone Standard
    prednisone dose delayed-release prednisone
    (mg) (N = 144) (N = 144)
    2 1 (0.7) 0 (—)
    3 8 (5.6) 2 (1.4)
    4 1 (0.7) 1 (0.7)
    5 72 (50.0) 73 (50.7)
    6 1 (0.7) 0 (—)
    7 28 (19.4) 30 (20.8)
    8 4 (2.8) 3 (2.1)
    9 0 (—) 0 (—)
    10 29 (20.1) 35 (24.3)
  • The median value of the mean daily prednisone dose across all subjects in the ITT population was 5.18 mg. Subgroup analyses were performed on the primary efficacy variable (i.e. the relative change from baseline in duration of morning stiffness) in subjects with a mean daily prednisone dose ≦5.18 mg and >5.18 mg.
  • In order to investigate the comparability of subgroups, selected demographic and baseline characteristics were analyzed: age, gender, ethnic origin, body weight, body height, duration of RA, HAQ-DI, pain intensity (VAS), SF36, and DAS28. Comments on age, duration of RA, and DAS28 as the most clinically relevant parameters are included below. There were no clinically relevant imbalances between subgroups in the other baseline variables.
  • Descriptive statistics for baseline demographics and the primary efficacy variable are presented for mean daily prednisone doses of >5.18 mg and ≦5.18 mg in each of the treatment groups of the ITT population in Table 5. The difference for the primary efficacy variable between the treatment groups is also given (as calculated by ANOVA, model A).
  • TABLE 5
    Baseline demographic variables and primary efficacy variable in subjects
    with a mean daily prednisone dose ≦5.18 mg or >5.18 mg* (ITT population)
    Prednisone delayed-release Standard prednisone
    (N = 144) (N = 144)
    Variable/subgroup N Mean (SD) n Mean (SD)
    Baseline demographic variables
    Age, years
    Mean daily dose ≦5.18 mg* 78 55.1 (10.5) 65 54.6 (11.9)
    Mean daily dose >5.18 mg* 65 54.3 (12.0) 77 56.1 (10.9)
    Duration of RA, months
    Mean daily dose ≦5.18 mg* 77 115.5 (98.4) 65 113.0 (111.4)
    Mean daily dose >5.18 mg* 65 116.3 (86.8) 77 117.1 (75.1)
    DAS28 score
    Mean daily dose ≦5.18 mg* 78 5.8 (0.8) 64 5.8 (0.9)
    Mean daily dose >5.18 mg* 65 5.8 (0.7) 76 6.0 (0.8)
    Duration of morning stiffness
    Mean daily dose ≦5.18 mg*
    Baseline, min 67 163.54 (109.92) 59 174.79 (132.47)
    Final week, min 69 119.25 (132.40) 60 169.36 (174.47)
    Relative change from 67 −26.93 (67.72) 59 7.88 (106.38)
    baseline to final week, %
    Difference between groups
    LS mean (SE), % 34.98 (15.57)
    95% CI 4.13, 65.83
    p-value 0.0134 (one-sided)
    Mean daily dose >5.18 mg*
    Baseline, min 57 164.81 (92.36) 68 189.74 (120.43)
    Final week, min 57 122.81 (152.12) 69 144.22 (113.49)
    Relative change from 57 −17.64 (110.12) 68 −8.76 (70.83)
    baseline to final week, %
    Difference between groups
    LS mean (SE), % 15.45 (16.14)
    95% CI −16.54, 47.45 
    p-value 0.1702 (one-sided)
    *5.18 mg is the median value of the mean daily prednisone dose across all subjects in the ITT population.
    LS = least square, SE = standard error
  • There were no differences in mean age, mean duration of RA, or mean DAS28 score between subjects receiving a mean daily prednisone dose of ≦5.18 mg and those receiving a mean daily dose of >5.18 mg in either of the 2 treatment groups.
  • In the Prednisone delayed-release group, morning stiffness decreased in both dose subgroups, with a larger decrease in subjects with a mean daily prednisone dose ≦5.18 mg than in subjects with a daily dose >5.18 mg.
  • In the standard prednisone group, subjects with a mean daily dose ≦5.18 mg showed an increase in the duration of morning stiffness. In subjects with a mean daily dose >5.18 mg, morning stiffness decreased but the decrease was not as large as in either of the Prednisone delayed-release dose subgroups.
    • Recurrence of Stiffness During the Day
  • In about 58% of the subjects in both treatment groups, recurrence of stiffness during the day was reported at baseline. After two weeks of treatment, the percentage was slightly lower in both treatment groups; after six weeks of treatment, the percentages were notably lower in both treatment groups with no major difference between the treatments; after 12 weeks of treatment, the percentage of subjects concerned was again notably lower compared to the 6-week value in both treatment groups.
    • Secondary Efficacy Variables.
  • TABLE 6
    Intensity of pain (VAS) after 12 weeks of
    treatment (intention-to-treat population)
    Prednisone
    Intensity of pain (VAS) delayed-release Prednisone Standard
    (mean (SD)) (N = 144) (N = 144)
    Baseline [mm] 50.9 (15.2) 52.3 (17.2)
    (N = 141) (N = 143)
    At Week 12 (Final week) 45.7 (24.1) 45.1 (23.1)
    [mm]
    (N = 142) (N = 144)
    Relative change [%] −8.57 (55.0)  −6.53 (83.9) 
    (N = 141) (N = 143)
  • According to the relative changes, the intensity of pain (VAS) was improved after 12 weeks of treatment by both treatments. In the ITT set, the treatment difference in the relative change in intensity of pain (VAS) was calculated to be 4.91% (SD 8.08%). A difference between the 2 groups in favour of Prednisone delayed-release has been observed, which was much more pronounced in the per-protocol set (−19% for Prednisone delayed-release vs −5% for Prednisone standard). The mean number of days with analgesics per week did not change notably after treatment start in both treatment groups. There is no difference between the two treatment groups after 2, 6, and 12 weeks of treatment. However, as under Prednisone delayed-release the intensity of pain went down it can be assumed that in patients with early RA or under long-term treatment also a reduction of painkillers will be seen.
  • No differences were observed in all other efficacy variables as listed in the following.
    • Quality of Sleep
  • The mean daily quality of sleep (VAS) did not improve in both treatment groups. There were no marked differences between baseline of the two treatment groups and the means of absolute changes after 2, 6, and 12 weeks of treatment.
    • Disease Activity Score (DAS 28)
  • The Disease Activity Score (DAS 28) decreased in both treatment groups. After two weeks of treatment, the decreases were small, whereas after six and 12 weeks of treatment the decreases were more pronounced. Absolute and relative changes were similar between the two treatment groups after 2, 6, and 12 weeks of treatment.
    • Tender and Swollen Joint Count
  • The tender and swollen joint count decreased in both treatment groups. After two weeks of treatment, the decreases were notable and further decreases were observed in both treatment groups after six and 12 weeks of treatment.
    • Subject's Global Assessment of Disease Activity
  • The mean subject's global assessment of disease activity (VAS) decreased in both treatment groups after start of the treatment with no relevant differences between timepoints and treatments.
    • Health Assessment Questionnaire Disability Index (HAQ-DI) and Quality of Life (SF36)
  • The HAQ-DI and SF36 scores were similar in both treatment groups at baseline as well as after 12 weeks of treatment.
    • Physician's Global Assessment of Disease Activity
  • In both treatment groups, the number and percentage of subjects whose disease activity was assessed by the physician as mild increased during the course of the treatment; the number and percentage of subjects whose disease activity was assessed by the physician as severe decreased.
    • Inflammatory Signs
  • The mean values of the inflammatory signs CRP and IL-6 at baseline as well as after 2, 6 and 12 weeks of treatment and the respective relative changes are presented in Table 7.
  • TABLE 7
    Inflammatory signs (CRP, IL-6) (intention-to-treat population)
    Inflammatory signs Prednisone
    (median (min, max)) delayed-release Prednisone Standard
    CRP [mg/L]
    Baseline (Visit 2) 9.9 (1.0, 105.1) 12.2 (1.0, 177.5)
    At Week 2 (Visit 3) 10.2 (1.0, 159.0) 11.2 (1.0, 106.3)
    Relative change [%] 13.0 (−96.1, 543.2) 0.0 (−93.1, 1535.4)
    At Week 6 (Visit 4) 9.9 (1.0, 90.3) 10.7 (1.0, 152.5)
    Relative change [%] 8.0 (−93.4, 695.2) 0.0 (−94.2, 2377.8)
    At Week 12 (Visit 5*) 9.1 (1.0, 185.0) 11.5 (1.0, 145.3)
    Relative change [%] 2.4 (−98.2, 1419.6) 0.0 (−93.0, 2605.6)
    IL-6 [IU/L]
    Baseline (Visit 1) 860 (200, 23000) 1110 (200, 20800)
    At Week 12 (Visit 5*) 470 (200, 9530) 1080 (200, 22700)
    Absolute change −160 (−13460, 9080) 0.0 (−16190, 18100)
    Relative change [%] −28.6 (−96.8, 2018) 0.0 (−98.1, 3017)
  • The median CRP values did not change notably during the 12-week treatment in both treatment groups.
  • IL-6 values decreased during the 12-week treatment in the Prednisone delayed-release treatment group, but remained unchanged in the prednisone standard treatment group. Median values seem to have been halved by the Prednisone delayed-release preparation and the overall range was much smaller after 12 weeks of treatment. The variability was very high in both groups. However, the change under Prednisone delayed-release from baseline to 12 weeks was significantly lower (p<0.001). Also, there was a statistically significant difference between the two treatment groups after 12 weeks.
    • Osteocalcin
  • Osteocalcin is a sensitive measure to the bone metabolism (Heshmati 1998). The mean osteocalcin values at baseline (screening) as well as after 12 weeks of treatment and the respective relative changes are presented in Table 8.
  • TABLE 8
    Osteocalcin (intention-to-treat population)
    Osteocalcin [ng/mL] Prednisone
    (mean (SD)) delayed-release Prednisone Standard
    Baseline (Visit 1) 20.95 (11.31) 20.04 (9.95)
    At Week 12 (Visit 5*) 20.40 (12.82) 19.43 (9.49)
    Relative change [%] −1.7 (33.0)  3.9 (46.4)
  • There were no differences between baseline and endpoints or between the two treatments. Thus, it can be concluded that night-time administration of low dose prednisone does not have a negative impact on bone metabolism and risk of osteoporosis.
    • Continued Efficacy Over During 9 Month Open Follow Up
  • Out of 288 patients enrolled into the double blind treatment period, a total of 249 subjects entered the open follow-up phase of the study, 219 subjects completed this phase (see Table 9).
  • TABLE 9
    Disposition of Subjects
    Number of subjects
    Criterion n (%)
    Enrolled into double-blind phase 288
    Enrolled in open follow-up 249 (100)
    Withdrawn  30 (12.0*)
    Who completed open follow-up 219 (88.0*)
  • Although efficacy was not the main objective of this open follow-up study, the order of reporting was kept the same as in the previous study report on the double-blind phase. In the open follow-up phase the interpretation of the efficacy data was focused on the following three aspects:
      • maintenance of the effects on stiffness duration achieved by prednisone delayed-release during the double-blind phase in the former prednisone delayed-release group
      • reduction of morning stiffness to the same extent in the subjects of the former prednisone standard group after three months of treatment with prednisone delayed-release at Visit 6
      • further reduction of morning stiffness in the study population after Visit 6 up to 9 months (Visit 8) or after 12 months of treatment with prednisone delayed-release, respectively.
    Mean Daily Duration of Morning Stiffness
  • The mean daily duration of morning stiffness at start of the double-blind period (Visit 2), at start of the open follow-up period (Visit 5) and at end of study (Visit 8) as well as the relative changes are presented in Table 10 and FIG. 2 for the study population.
  • TABLE 10
    Mean Daily Duration of Morning Stiffness at Month 9 of Follow-Up (Visit 8)
    Number of subjects
    Prednisone Prednisone
    delayed-release Standard Total
    (N = 120) (N = 129) (N = 249)
    mean (SD) mean (SD) mean (SD)
    median median median
    Duration of morning stiffness [min] (min; max) (min; max.) (min; max)
    Visit 2 (Start of Double-blind Period) 156.27 (97.25) 182.40 (127.43) 169.80 (114.38)
    137.14 149.29 143.21
    (41.43; 659.29) (32.14; 720.0)  (32.14; 720.0)
    (n = 107) (n = 115) (n = 222)
    Visit 5 (Start of Follow-up Period)  98.20 (100.22) 150.31 (139.48) 125.56 (124.92)
     75.36 116.07  83.93
     (0.0; 470.0) (0.0; 720.0)  (0.0; 720.0)
    (n = 114) (n = 126) (n = 240)
    Relative change [%] to Visit 2 −34.47 (68.99) −1.44 (93.07) −17.10 (83.99) 
    −37.29 −19.05 −28.75
    (−100.00; 433.53)  (−100.00; 609.86)   (−100.00; 609.86) 
    (n = 101) (n = 112) (n = 213)
    Visit 8* (Month 9 of Follow-up)  73.43 (92.32)  92.88 (124.59)  83.63 (110.60)
     42.14 60.0  46.43
     (0.0; 502.5) (0.0; 720.0)  (0.0; 720.0)
    (n = 97)  (n = 107) (n = 204)
    Relative change [%] to Visit 2 −55.07 (44.79) −44.90 (63.73)  −49.71 (55.67) 
    −63.13 −62.96 −63.02
    (−100; 133.33) (−100; 269.44)  (−100; 269.44)
    (n = 87)  (n = 97)  (n = 184)
    Relative change [%] to Visit 5  −7.81 (144.62) −13.90 (146.98) −11.22 (145.56)
    −38.33 −40.70 −40.70
    (−100; 783.75) (−100; 950)   (−100; 950) 
    (n = 78)  (n = 99)  (n = 177)
    *Incl. premature termination
  • Starting treatment with prednisone delayed-release with longer stiffness duration at Visit 5, the former prednisone standard group achieved almost identical reduction, when percent relative change is calculated from Visit 8 to Visit 5 or from Visit 8 to Visit 2. For all subjects of the study population in the follow-up phase, a further mean reduction of 11.22% (Visit 8 compared to Visit 5) was gained. The total reduction of stiffness duration by 49.71% was observed on long term treatment between Visit 2 and 8.
  • Mean Daily Duration of Morning Stiffness After Start of Treatment with Prednisone Delayed-Release (Visit 2/Visit 5)
  • The mean daily duration of morning stiffness at start of the double-blind period (Visit 2) as well as at start of the follow-up period (Visit 5) and after 3, 6, 9, and 12 months (3-month intervals) of prednisone delayed-release treatment including respective relative changes are presented in Table 11.
  • TABLE 11
    Mean Daily Duration of Morning Stiffness after Start of Treatment
    with Prednisone delayed-release (Visit 2/Visit 5)
    Number of subjects
    Prednisone Prednisone
    delayed-release Standard Total
    Mean daily duration of morning (N = 249) (N = 249) (N = 249)
    stiffness mean (SD) mean (SD) mean (SD)
    Visit 2 (Start of Double-blind Period) [min] 156.27 (97.25) 153.04 (121.71)
    (n = 107) (n = 233)
    Visit 5 (Start of Follow-up Period) [min] 150.31 (139.48)
    (n = 126)
    after 3 months of Prednisone delayed-  98.20 (100.22)  85.17 (112.45) 91.92 (106.25)
    release treatment [min]  (n = 114) (n = 106) (n = 220)
    Relative change [%] −34.47 (68.99) −46.06 (46.86)  −40.18 (59.27) 
     (n = 101) (n = 98)  (n = 199)
    after 6 months of Prednisone delayed-  65.70 (100.95)  81.08 (104.79) 74.08 (103.10)
    release treatment [min] (n = 96) (n = 115) (n = 211)
    Relative change [%] −56.06 (54.20) −32.83 (116.64) −43.13 (94.71) 
    (n = 86) (n = 108) (n = 194)
    after 9 months of Prednisone delayed-  62.43 (87.49)  92.88 (124.59) 78.10 (108.99)
    release treatment* [min]  (n = 101) (n = 107) (208)
    Relative change [%] −61.35 (45.67) −13.90 (146.98) −36.23 (113.67) 
    (n = 88) (n = 99)  (n = 187
    after 12 months of Prednisone delayed-  73.43 (92.32)
    release treatment* [min] (n = 97)
    Relative change [%] −55.07 (44.79)
    (n = 87)
    Relative changes refer to values given in bold case
    *Incl. premature termination
  • In Table 11 the duration of morning stiffness is presented as treatment duration of prednisone delayed-release independent from Visits. Relative changes were calculated from the data at Visit 2 for the former prednisone delayed-release group and from the data of Visit 5 for the former prednisone standard group. Taking advantage of the higher number of available data, the interpretation of the results was carried out for the total numbers.
  • Before starting with the treatment of prednisone delayed-release the mean daily duration of morning stiffness was 153 min. After three months of treatment stiffness duration was reduced to a mean of 92 min and after six months further to 74 min. After nine months of prednisone delayed-release treatment mean daily duration of morning stiffness was 78 min. For the subjects of the former prednisone delayed-release group data were also available after 12 months of prednisone delayed-release treatment. For these subjects stiffness duration was similar to those after six and nine months of treatment (73 min). No weaning of effects was observed. Thus, the mean duration of morning stiffness was reduced to the half after six months of prednisone delayed-release treatment.
    • Inflammatory Signs
  • The median values of the inflammatory signs CRP and IL-6 during the open follow-up period (Visit 5 to Visit 8) and the respective absolute changes are presented in Table 12 and FIG. 3.
  • TABLE 12
    Inflammatory Signs (CRP, IL-6)
    Number of subjects
    Prednisone Prednisone Total
    delayed-release Standard (N = 249)
    (N = 120) (N = 129) median
    Inflammatory signs median (min; max) median (min; max) (min; max)
    CRP* [mg/L]
    Visit 5 (Start of Follow-up) 8.60 (n = 120) 10.90 (n = 129) 9.40 (n = 249)
     (1.00; 139.80)  (1.00; 145.30) (1.00; 145.30)
    Visit 6 (Month 3 of Follow-up) 8.55 (n = 108)  8.15 (n = 118) 8.35 (n = 226)
    (1.00; 81.40)  (1.00; 152.40) (1.00; 152.40)
    Absolute change −0.45 (n = 108)  −1.20 (n = 118) −0.70 (n = 226) 
    (−131.20; 77.70)   (−123.20; 95.00)   −131.20; 95.00)  
    Visit 7 (Month 6 of Follow-up) 7.00 (n = 109)  9.05 (n = 118) 8.00 (n = 227)
    (1.00; 71.00) (1.00; 69.70) (1.00; 71.00) 
    Absolute change −0.60 (n = 109)  −0.95 (n = 118) −0.80 (n = 227) 
    (−122.60; 49.00)   (−108.10; 25.80)   (−122.60; 49.00)  
    Visit 8*** (Month 9 of Follow-up) 8.40 (n = 112)  8.35 (n = 124) 8.35 (n = 236)
    (1.00; 83.30) (1.00; 86.50) (1.00; 86.50) 
    Absolute change −0.25 (n = 112)  −0.25 (n = 124) −0.25 (n = 236) 
    (−129.10; 68.30)   (−76.90; 68.70)  (−129.10; 68.70)  
    IL-6** [IU/L]
    Visit 5 (Start of Follow-up)  460 (n = 120)  1050 (n = 127) −710 (n = 247)
    (200; 9530)  (200; 22700) (200; 22700)
    Visit 8*** (Month 9 of Follow-up)  510 (n = 111)   570 (n = 123) −525 (n = 234)
     (200; 18300) (200; 8100) (200; 18300)
    Absolute change   0 (n = 111)   −300 (n = 121)  −45 (n = 232)
    (−6830; 16110)  (−20600; 6270)   (−20600; 16110)  
    *Values <1.0 mg/L were set to 1.0 for analysis
    **Values <200 IU/L were set to 200 for analysis
    ***Incl. premature termination.
  • The median CRP values did not change notably during the nine months of open follow-up treatment with prednisone delayed-release, except in the former prednisone standard group at Visit 6 where the CRP value was decreased most compared to Visit 5.
  • As the variability of the IL-6 values was high in both groups, the median was chosen for comparison rather than the mean values. IL-6 values decreased notably in the former prednisone standard group from 1050 IU/L to 570 IU/L. Thus, IL-6 concentrations were halved in the subjects of the former standard group. This decrease of IL-6 was similar to the decrease of IL-6 in the prednisone delayed-release group described in the double-blind phase. No further reduction was observed in the subjects of the former prednisone delayed-release group.
    • Overview of Safety
  • The safety profile of glucocorticoids in the treatment of rheumatoid arthritis (RA) is well established). The main side effects consist of osteoporosis leading to fractures, gastrointestinal disorders, cardiovascular disorders, increased risk of infections, hyperglycemia, suppression of the HPA axis, and ophthalmologic disorders. It is accepted that many of these side effects are observed at high or medium doses but not at low doses (Bijlsma et al. 2003, Bijlsma et al. 2005, Boers 2004, Buttgereit et al 2005, Conn 2001, Da Silva et al. 2005, Saag et al. 1994).
  • Prednisone delayed-release is intended for the treatment of RA at low doses (3 to 10 mg prednisone/day) and contains the same active drug ingredient as standard low-dose IR products. Prednisone delayed-release differs from standard products solely with respect to the recommended time of administration and timepoint of drug release within the gastrointestinal tract. The safety profile of low-dose prednisone is well established and reflected in labeling for standard IR products. Clinically significant differences are not expected.
    • Brief Summary of Adverse Events in Phase III Trial Under Prednisone Delayed-Release
  • In this study, 59 (41.0%) subjects of the Prednisone delayed-release treatment group and 59 (41.0%) subjects of the prednisone standard treatment group experienced at least one treatment-emergent Adverse Event (AE). A total of 35 subjects (12.2%) experienced AEs that were considered by the investigator to be related to prednisone. AEs causing discontinuation of prednisone were experienced by 22 subjects (7.6%).
  • One subject receiving prednisone standard died on study within 18 days after first dose of prednisone. Seven subjects (2.4%) experienced SAEs, and in one subject of these 7 subjects, the SAE was judged to be related to prednisone by the investigator.
  • Table 13 summarizes the number of subjects experiencing AEs by type of AE (MedDRA Preferred Term, in at least 1.0% of the treated group).
  • TABLE 13
    Most common AEs and drug-related AEs in study 003
    No. (%) subjects with AE
    Prednisone Standard
    delayed-release prednisone Total
    Preferred term (N = 144) (N = 144) (N = 288)
    All Aes 59 (41.0) 59 (41.0) 118 (41.0)
    Rheumatoid arthritis 11 (7.6)  13 (9.0)  24 (8.3)
    Abdominal pain 5 (3.5) 8 (5.6) 13 (4.5)
    upper
    Nasopharyngitis 4 (2.8) 8 (5.6) 12 (4.2)
    Headache 6 (4.2) 4 (2.8) 10 (3.5)
    Flushing 4 (2.8) 6 (4.2) 10 (3.5)
    Nausea 5 (3.5) 4 (2.8)  9 (3.1)
    Drug-related AEs 19 (13.2) 16 (11.1)  35 (12.2)
    Abdominal pain 3 (2.1) 4 (2.8)  7 (2.4)
    upper
    Nausea 3 (2.1) 3 (2.1)  6 (2.1)
    Headache 4 (2.8) 2 (1.4)  6 (2.1)
    Rheumatoid arthritis 1 (0.7) 4 (2.8)  5 (1.7)
  • The most frequently reported AEs (frequency >1.0% of the subjects of the safety set) by MedDRA Preferred Term were rheumatoid arthritis including several terms for worsening (deterioration, escalation, exacerbation, flare etc.) (24 subjects, 8.3%), abdominal pain upper (13 subjects, 4.5%) and nasopharyngitis (12 subjects, 4.2%). The incidences of these AEs were similar in both treatment groups.
  • During the 9 month open follow-up period, 127 subjects (51.0%) experienced at least one treatment-emergent adverse event (AE). A total of 27 subjects (10.8%) experienced AEs that were considered by the investigator to be related to prednisone delayed-release. AEs causing discontinuation of prednisone delayed-release were experienced by 13 subjects (5.2%); 68 subjects (27.3%) had AEs not known to be recovered at the end of the study.
  • Table 14 summarizes the most common AEs by type of AE (MedDRA Preferred Term, in more than 2% of the subjects).
  • TABLE 14
    Most Common Adverse Events (Frequency >1.0% Overall)
    Total
    (N = 249)
    Adverse Event (preferred term) n (%)
    Rheumatoid arthritis 36 (14.5)
    Flushing 13 (5.2) 
    Upper respiratory tract infection 7 (2.8)
    Weight increased 7 (2.8)
    Back pain 7 (2.8)
    Bronchitis 6 (2.4)
    Hypercholesterolemia 6 (2.4)
    Arthralgia 6 (2.4)
    Nasopharyngitis 6 (2.4)
    Feeling hot 5 (2.0)
  • The most frequently reported AEs (MedDRA Preferred Term) were rheumatoid arthritis (36 subjects, 14.5%) and flushing (13 subjects, 5.2%). Flushing was only reported by the subjects who participated in the CRH testing. Upper respiratory tract infection, increased weight, or back pain were reported less frequently (seven subjects (2.8%) in each case).
    • Benefits and Risks Conclusions
  • Prednisone delayed-release is a novel, delayed-release tablet that has been developed to optimize the efficacy of orally administered low-dose prednisone in the treatment of RA. Prednisone delayed-release has shown improved efficacy compared to standard prednisone in patients with RA without increasing their prednisone dose. This improvement has been solely obtained as a result of Prednisone delayed-release's unique release characteristics. The safety profiles of Prednisone delayed-release and standard prednisone were comparable and the patients were thus not exposed to an increased risk.
  • The benefits and main features of Prednisone delayed-release can be summarized as follows:
  • A significant reduction of morning stiffness was obtained in patients with long-standing RA who were pretreated with prednisone and DMARDs. A decrease of 10% compared to baseline was already apparent at week 2 of treatment. Under continued treatment this reduction increased in magnitude and plateaued at about 30% to 40% from week 7 onwards. In 50% of the patients (median values), the duration of morning stiffness was reduced by at least one third (33.9%) during the double blind treatment phase. At the end of the 9 month open label follow-up period, a decrease in the duration of morning stiffness of 49% compared to baseline was observed (mean baseline duration of morning stiffness was 3 hours). Morning stiffness is one of the most distressing symptoms for RA patients and thus the observed sustained reduction for at least 12 months under Prednisone delayed-release can be considered a clinically meaningful improvement.
  • Both in the double blind and the 9 month open follow-up period, the reduction in morning stiffness was accompanied by a sustained parallel decrease in the pro-inflammatory cytokine IL-6, thus confirming the proposed pharmacological rationale for adapting the timing of prednisone administration to the circadian rhythm of RA.
  • These results are surprising because it could not be expected from former investigations (Karatay 2002). Also the long lasting effect of prednisone delayed-release over 12 months on reducing IL-6 levels is unexpected. Further, the long term correlation of IL-6 reduction and morning stiffness reduction could not be expected from former investigations.
  • Maximum plasma levels of prednisone in the early morning hours are obtained by administration of Prednisone delayed-release at about 22:00 which is an acceptable time for the patient.
  • Prednisone delayed-release tablets can be used in patients with severe, moderate or mild disease.
  • Prednisone delayed-release tablets can be used in patients with short, mid-term or long-lasting disease duration.
  • Prednisone delayed-release tablets can be used in patients pre-treated with corticosteroids, in those who are refractory to treatment or in corticoid naïve patients.
  • Prednisone delayed-release tablets can be used as monotherapy or more likely in combination with DMARDs, NSAIDs, TNF α Inhibitors and/or analgetics.
  • Prednisone delayed-release tablets can be used for short, mid or long-term treatment.
    • LITERATURE REFERENCES
  • ACR (American College of Rheumatology) Subcommittee on Rheumatoid Arthritis Guidelines. Guidelines for the management of rheumatoid arthritis. Arthritis Rheum 2002;46:328-46.
  • Ahlmén M, Nordenskiöld U, Archenholtz B, Thyberg I, Rönnqvist R, Lindén L, et al. Rheumatology outcomes: the patient's perspective. A multicentre focus group interview study of Swedish rheumatoid arthritis patients. Rheumatology 2005;44:105-10.
  • Arnett F C, Edworthy S M, Bloch D A, McShane D J, Fries J F, Cooper N S, et al. The American Rheumatism Association 1987 revised criteria for the classification of rheumatoid arthritis. Arthritis Rheum 1988;31:315-24.
  • Arvidson NG, Gudbjörnsson B, Elfman L, Rydén A C, Tötterman T H, Hällgren R. Circadian rhythm of serum interleukin-6 in rheumatoid arthritis. Ann Rheum Dis 1994;53:521-4.
  • Arvidson N G, Gudbjörnsson B, Larsson A, Hällgren R. The timing of glucocorticoid administration in rheumatoid arthritis. Ann Rheum Dis 1997;56:27-31.
  • Bijlsma J W J, Boers M, Saag K G, Furst D E. Glucocorticoids in the treatment of early and late RA. Ann Rheum Dis 2003;62:1033-7.
  • Bijlsma J W J, Saag, K G, Buttgereit F, da Silva J A P. Developments in glucocorticoid therapy. Rheum Dis Clin N Am 2005;31:1-17.
  • Boers M. Glucocorticoids in rheumatoid arthritis: a senescent research agenda on the brink of rejuvenation? Best Practice Research Clin Rheumatol 2004;18 (1):21-9.
  • Buttgereit F, Burmester G-R, Lipworth B J. Optimised glucocorticoid therapy: the sharpening of an old spear. Lancet 2005;365:801-3.
  • Buttgereit F, Saag K G, Cutolo M, da Silva J A P, Bijlsma J W J. The molecular basis for the effectiveness, toxicity, and resistance to glucocorticoids: focus on the treatment of rheumatoid arthritis. Scand J Rheumatol 2005;34:14-21.
  • Buttgereit F, Straub R H, Wehling M, Burmester G R. Glucocorticoids in the treatment of rheumatic diseases: an update on the mechanisms of action. Arthritis Rheum 2004;50:3408-17.
  • Capell H A, Madhok R, Hunter J A, Porter D, Morrison E, Larkin J, et al. Lack of radiological and clinical benefit over two years of low dose prednisolone for rheumatoid arthritis: results of a randomised controlled trial. Ann Rheum Dis 2004;63:797-803.
  • Carr A, Hewlett S, Hughes R, Mitchell H, Ryan S, Carr M, et al. Rheumatology outcomes: the patient's perspective. J Rheumatol 2003;30:880-3.
  • Conn D L. Resolved: Low-dose prednisone is indicated as a standard treatment in patients with rheumatoid arthritis. Arthritis Rheum 2001;45:462-7.
  • Crofford L J, Kalogeras K T, Mastorakos G, Magiakou M A, Wells J, Kanik K S, et al. Circadian relationships between interleukin (IL)-6 and hypothalamic-pituitary-adrenal axis hormones: failure of IL-6 to cause sustained hypercortisolism in patients with early untreated rheumatoid arthritis. J Clin Endocrinol Metab 1997;82:1279-83.
  • Cutolo M, Maestroni G J M, Otsa K, Aakre O, Villaggio B, Capellino S, et al. Circadian melatonin and cortisol levels in rheumatoid arthritis patients in winter time: a north and south Europe comparison. Ann Rheum Dis 2005;64:212-6.
  • Cutolo M, Masi A T. Circadian rhythms and arthritis. Rheum Dis Clin N Am 2005;31:115-29.
  • Cutolo M, Seriolo B, Craviotto C, Pizzorni C, Sulli A. Circadian rhythms in RA. Ann Rheum Dis 2003;62:593-6.
  • Da Silva J A P, Jacobs J W G, Kirwan J R, Boers M, Saag K G, Ines L B S, et al. Safety of low dose glucocorticoid treatment in rheumatoid arthritis: published evidence and prospective trial data. Ann Rheumatol Dis 2006;65:285-93.
  • Gudbjörnsson B, Skogseid B, Öberg K, Wide L, Hällgren R. Intact adrenocorticotropic hormone secretion but impaired cortisol response in patients with active rheumatoid arthritis. Effect of glucocorticoids. J Rheumatol 1996;23:596-602.
  • Heshmati H M, Riggs B L, Burritt M F, McAlister C A, Wollan P C, Khosla S. Effects of the circadian variation in serum cortisol on markers of bone turnover and calcium homeostasis in normal postmenopausal women. J Clin Endocrinol Metab 1998;83:751-6.
  • Hewlett S, Carr M, Ryan S, Kirwan J, Richards P, Carr A, et al. Outcomes generated by patients with rheumatoid arthritis: How important are they? Musculoskeletal Care 2005;3:131-42.
  • Hickling P, Jacoby R K, Kirwan J R. Joint destruction after glucocorticoids are withdrawn in early rheumatoid arthritis. Arthritis and Rheumatism Council Low Dose Glucocorticoid Study Group. Br J Rheumatol 1998;37:930-6.
  • Hudson M, Baron M. Morning stiffness is a better predictor of function in early inflammatory arthritis than are swollen and tender joints. Arthritis Rheum 2005;52 Suppl 9: abstract 1036.
  • Jacobs J W G, van Everdingen A A, Verstappen S M M, Bijlsma J W J. Followup radiographic data on patients with rheumatoid arthritis who participated in a two-year trial of prednisone therapy or placebo. Arthritis Rheum 2006;54:1422-8.
  • Karatay S. et al, The timing of low dose glucocorticoid therapy in the treatment of rheumatoid arthritis, The Pain Clinic, 2002, 13, 4, 305-312
  • Kirwan J R. The effect of glucocorticoids on joint destruction in rheumatoid arthritis. The Arthritis, and Rheumatism Council Low-Dose Glucocorticoid Study Group. N Engl J Med 1995;333:142-6.
  • Kirwan J R, Boers M, Shea B. Glucocorticoids strongly suppress joint damage in rheumatoid arthritis: A meta-analysis of 1,414 patients in 15 trials. Arthritis Rheum 2005; 52 Suppl 9: abstract 891.
  • LeLoet X et al, Clinical practice decision tree for the coice of the first disease modifying antirheumatic drug for very early rheumatoid arthritis: a 2004 proposal of the French Society of Rheumatology, Annals of Rheum Dis 2006; 65:45-50
  • Mastorakos G, Ilias I. Relationship between interleukin-6 (IL-6) and hypothalamic-pituitary-adrenal axis hormones in rheumatoid arthritis. Z Rheumatol 2000;59(Suppl 2):75-9.
  • Petrovsky N, McNair P, Harrison L C. Diurnal rhythms of pro-inflammatory cytokines: regulation by plasma cortisol and therapeutic implications. Cytokine 1998;10:307-12.
  • Pincus T, Sokka T, Kautiainen H. Patients seen for standard rheumatoid arthritis care have significantly better articular, radiographic, laboratory, and functional status in 2000 than in 1985. Arthritis Rheum 2005;52:1009-19.
  • Saag K G, Criswell L A, Sems K M, Nettleman M D, Kolluri S. Low-dose corticosteroids in rheumatoid arthritis—A meta-analysis of their moderate-term effectiveness. Arthritis Rheum 1996;39:1818-25.
  • Saag K G, Koehnke R, Caldwell J R, Brasington R, Burmeister L F, Zimmerman B, et al. Low dose long-term corticoid therapy in rheumatoid arthritis: an analysis of serious adverse events. Am J Med 1994;96:115-23.
  • Stucki G, Cieza A. The international classification of functioning, disability and health (ICF) core sets for rheumatoid arthritis: a way to specify functioning. Ann Rheum Dis 2004;63(Suppl 2):40-5.
  • Svensson B, Boonen A, Albertsson K, van der Heijde D, Keller C, Hafstrom J. Low-dose prednisolone in addition to the initial disease-modifying antirheumatic drug in patients with early active rheumatoid arthritis reduces joint destruction and increases the remission rate: a two-year randomized trial. Arthritis Rheum 2005;52:3360-70.
  • van Everdingen A A, Jacobs J W G, Siewertsz van Reesema D R, Bijlsma J W J. Low-dose prednisone therapy for patients with early active rheumatoid arthritis: clinical efficacy, disease-modifying properties, and side effects. A randomized, double-blind, placebo-controlled clinical trial. Ann Intern Med 2002;136:1-12.
  • van Staa T P, Leufkens H G M, Abenhaim L, Zhang B, Cooper C. Oral corticosteroids and fracture risk: relationship to daily and cumulative doses. Rheumatology 2000;39:1383-9.
  • Wassenberg S, Rau R, Steinfeld P, Zeidler H. Very low-dose prednisolone in early rheumatoid arthritis retards radiographic progression over two years. Arthritis Rheum 2005;52:3371-80.

Claims (25)

1-79. (canceled)
80. A method for treatment of a patient suffering from signs and symptoms of polymyalgia rheumatica comprising administering to said patient an effective amount of a glucocorticoid contained in a delayed-release dosage form, wherein said treatment is administered once daily for at least about two weeks.
81. The method of claim 80, wherein the treatment comprises administration of the glucocorticoid for at least about four weeks.
82. The method of claim 81, wherein the treatment comprises administration of the glucocorticoid for at least about eight weeks.
83. The method of claim 82, wherein the treatment comprises administration of the glucocorticoid for at least about twelve weeks.
84. The method of claim 83, wherein the treatment comprises administration of the glucocorticoid for at least about twelve months.
85. The method of claim 80, wherein the glucocorticoid dose is greater than about 10 mg/day of prednisone, or an equivalent amount of another glucocorticoid, at the initiation of the therapy.
86. The method of claim 80, wherein the glucocorticoid dose is equal to or less than about 10 mg/day of prednisone, or an equivalent amount of another glucocorticoid, for maintenance therapy.
87. The method of claim 80, wherein said patient has not previously been treated with one or more of an oral immediate release glucocorticoid, an NSAID, a DMARD, a TNFα inhibitor, an IL-1 inhibitor, an IL-6 inhibitor, and an analgetic agent.
88. The method of claim 80, wherein said patient has previously undergone treatment with one or more of an oral immediate release dosage form of a glucocorticoid, an NSAID, a DMARD, a TNFα inhibitor, an IL-1 inhibitor, an IL-6 inhibitor, and an analgetic agent.
89. The method of claim 88, wherein said patient is refractory to said treatment with an oral immediate release dosage form of a glucocorticoid.
90. The method of claim 80, which further comprises administering to said patient an effective amount of one or more of an NSAID, a DMARD, a TNFα inhibitor, an IL-1 inhibitor, an IL-6 inhibitor, and an analgetic agent.
91. The method of claim 80, wherein the delayed-release dosage form has a lag time of from about 2 hours to about 6 hours after administration.
92. The method of claim 80, wherein the delayed-release dosage form has a lag time of from about 3 hours to about 5 hours after administration.
93. The method of claim 80, wherein the delayed-release dosage form has a dissolution time of equal to or less than about 2 hours after the lag time is reached.
94. The method of claim 80, wherein the delayed-release dosage form has a drug release behavior which is independent of pH.
95. The method of claim 80, wherein the delayed release dosage form is a tablet or a capsule.
96. The method of claim 80, wherein the delayed-release dosage form comprises a non-soluble/non-swellable coating and a core comprising the active agent and a disintegrant and/or a swelling agent.
97. The method of claim 80, wherein the glucocorticoid is cortisone, hydrocortisone, prednisone, prednisolone, methylprednisolone, budesonide, dexamethasone, fludrocortisone, fluocortolone, cloprednole, deflazacort, or triamcinolone, or a pharmaceutically acceptable salt thereof.
98. The method of claim 97, wherein the glucocorticoid is prednisone, prednisolone, methylprednisolone, dexamethasone, fluocortolone, cloprednole, or deflazacort, or a pharmaceutically acceptable salt thereof.
99. The method of claim 80, wherein said delayed-release dosage form is effective at a lower dose of glucocorticoid as compared to the administration of said glucocorticoid in an immediate release dosage form.
100. The method of claim 80, wherein said patient suffers from inflammation.
101. The method of claim 80, wherein the glucocorticoid is administered in the evening.
102. The method of claim 101, wherein the glucocorticoid is administered between about 9:00 pm and about 11:00 pm.
103. The method of claim 80, wherein the signs and symptoms of polymyalgia rheumatica comprise morning stiffness and pain.
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US14/563,000 US9504699B2 (en) 2006-08-03 2014-12-08 Delayed-release glucocorticoid treatment of rheumatoid disease
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Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US8920838B2 (en) 2006-08-03 2014-12-30 Horizon Pharma Ag Delayed-release glucocorticoid treatment of rheumatoid disease

Families Citing this family (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2010084188A1 (en) 2009-01-26 2010-07-29 Nitec Pharma Ag Delayed-release glucocorticoid treatment of asthma
NZ582836A (en) * 2009-01-30 2011-06-30 Nitec Pharma Ag Delayed-release glucocorticoid treatment of rheumatoid arthritis by improving signs and symptoms, showing major or complete clinical response and by preventing from joint damage
JP5860032B2 (en) * 2010-04-28 2016-02-16 キンバリー クラーク ワールドワイド インコーポレイテッド Device for the delivery of rheumatoid arthritis drugs
WO2013053767A1 (en) * 2011-10-10 2013-04-18 Medimmune Limited Treatment for rheumatoid arthritis
GB201202433D0 (en) * 2012-02-13 2012-03-28 Diurnal Ltd Controlled drug release
US9012432B2 (en) * 2013-03-08 2015-04-21 Levolta Pharmaceuticals, Inc. Co-administration of steroids and zoledronic acid to prevent and treat osteoarthritis

Family Cites Families (173)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3048526A (en) 1958-08-04 1962-08-07 Wander Company Medicinal tablet
GB972128A (en) 1960-01-21 1964-10-07 Wellcome Found Pellets for supplying biologically active substances to ruminants and the manufacture of such pellets
US3125491A (en) 1962-04-06 1964-03-17 Chew able hematinic vitamin tablet
FR1603314A (en) 1965-02-23 1971-04-05 Pharmaceutical tablets - having a core and a matrix material
US3870790A (en) 1970-01-22 1975-03-11 Forest Laboratories Solid pharmaceutical formulations containing hydroxypropyl methyl cellulose
FR2100858B1 (en) 1970-07-03 1975-06-06 Daiichi Seiyaku Co
DE2445971A1 (en) 1974-09-24 1976-04-08 Schering Ag MEDICINAL INGREDIENTS CARRIERS II
US4797288A (en) 1984-10-05 1989-01-10 Warner-Lambert Company Novel drug delivery system
GB8518301D0 (en) 1985-07-19 1985-08-29 Fujisawa Pharmaceutical Co Hydrodynamically explosive systems
US5519057A (en) 1986-11-14 1996-05-21 Johnson & Johnson--Merck Pharmaceuticals Co. Ibuprofen-containing medicament
IT1201136B (en) 1987-01-13 1989-01-27 Resa Farma TABLET FOR PHARMACEUTICAL USE SUITABLE FOR THE RELEASE OF SUBSTANCES OF ACTIVE SUBSTANCES
GB8705083D0 (en) 1987-03-04 1987-04-08 Euro Celtique Sa Spheroids
GB8820353D0 (en) 1988-08-26 1988-09-28 Staniforth J N Controlled release tablet
US5047246A (en) 1988-09-09 1991-09-10 Bristol-Myers Company Direct compression cyclophosphamide tablet
IT1230576B (en) 1988-10-20 1991-10-28 Angeli Inst Spa ORAL PHARMACEUTICAL FORMULATIONS WITH SELECTIVE LIBERATION IN THE COLON
US4966770A (en) 1989-07-26 1990-10-30 Himedics, Inc. Prednisone microencapsulated granules
DE3930770A1 (en) 1989-09-14 1991-03-28 Wolfgang F Dr Schoener IMPLANTABLE CATHETERS MADE FROM MEDICAL COMPATIBLE ELASTIC PLASTIC
IT1246382B (en) 1990-04-17 1994-11-18 Eurand Int METHOD FOR THE TARGETED AND CONTROLLED DELIVERY OF DRUGS IN THE INTESTINE AND PARTICULARLY IN THE COLON
JP2558396B2 (en) 1990-06-28 1996-11-27 田辺製薬株式会社 Controlled release formulation
HU219341B (en) 1990-07-02 2001-03-28 Roche Diagnostics Gmbh Process for producing pressed, moulded, delayed release dose units and dose units thus produced
JP2521848B2 (en) 1990-07-02 1996-08-07 ベーリンガー マンハイム ゲーエムベーハー Method for preparing shaped and compressed sustained release unit dosage form and compressed unit dosage form thus obtained
IE61651B1 (en) 1990-07-04 1994-11-16 Zambon Spa Programmed release oral solid pharmaceutical dosage form
US5310578A (en) 1990-09-17 1994-05-10 Merck Patent Gesellschaft Deposition of cosmetically functional material onto pigments and fillers
US5316772A (en) 1990-12-19 1994-05-31 Solvay & Cie, S.A. (Societe Anonyme) Bilayered oral pharmaceutical composition with pH dependent release
CA2100272A1 (en) 1991-01-03 1992-07-04 Thomas Patrick Molloy Method for production of solid pharmaceutical preparation
DE4100920A1 (en) * 1991-01-15 1992-07-16 Degussa ACTIVE SUBSTANCE PREPARATION FOR ORAL ADMINISTRATION TO Ruminants
DE69222006T2 (en) 1991-10-30 1998-01-22 Glaxo Group Ltd Multilayer compositions containing histamine or serotonin antagonists
AU3949093A (en) 1992-03-31 1993-11-08 Benzon Pharma A/S A pharmaceutical formulation
GB9215908D0 (en) 1992-07-27 1992-09-09 Wellcome Found Water dispersible tablets
JPH07507564A (en) 1992-09-30 1995-08-24 ファイザー・インク. Articles containing a core and a coating of variable thickness
WO1994008589A1 (en) 1992-10-09 1994-04-28 The Board Of Trustees Of The Leland Stanford Junior University Treatment of systemic lupus erythematosus with dehydroepiandrosterone
TW272942B (en) 1993-02-10 1996-03-21 Takeda Pharm Industry Co Ltd
DK66493D0 (en) 1993-06-08 1993-06-08 Ferring A S PREPARATIONS FOR USE IN TREATMENT OF INFLAMMATORY GAS DISORDERS OR TO IMPROVE IMPROVED HEALTH
IL110376A (en) 1993-08-02 1998-08-16 Bristol Myers Squibb Co Pharmaceutical compositions containing ifetroban salts and methods for the preparation thereof
DE4332394A1 (en) 1993-09-23 1995-03-30 Falk Pharma Gmbh Controlled release budesonide pellets and method of making the same
US5482718A (en) 1994-03-23 1996-01-09 Hoffmann-La Roche Inc. Colon-targeted delivery system
US5464633A (en) 1994-05-24 1995-11-07 Jagotec Ag Pharmaceutical tablets releasing the active substance after a definite period of time
US5702723A (en) 1994-08-02 1997-12-30 Griffin; David Multi-stage delivery system for ingestible medications or nutrients
US5811388A (en) 1995-06-07 1998-09-22 Cibus Pharmaceutical, Inc. Delivery of drugs to the lower GI tract
US5709880A (en) 1995-07-10 1998-01-20 Buckman Laboratories International, Inc. Method of making tabletized ionene polymers
IT1276031B1 (en) 1995-10-31 1997-10-24 Angelini Ricerche Spa PHARMACEUTICAL COMPOSITION FOR THE TREATMENT OF AUTOIMMUNE DISEASES
JP3220373B2 (en) 1995-11-28 2001-10-22 バイエル薬品株式会社 Long-acting nifedipine preparation
US6645988B2 (en) 1996-01-04 2003-11-11 Curators Of The University Of Missouri Substituted benzimidazole dosage forms and method of using same
US5840332A (en) 1996-01-18 1998-11-24 Perio Products Ltd. Gastrointestinal drug delivery system
WO1997027843A2 (en) 1996-01-30 1997-08-07 Advanced Polymer Systems, Inc. Targeted delivery of drugs to the lower gastrointestinal tract
IT1282576B1 (en) 1996-02-06 1998-03-31 Jagotec Ag PHARMACEUTICAL TABLET SUITABLE TO GIVE THE ACTIVE SUBSTANCE IN SUBSEQUENT AND PREDETERMINABLE TIMES
HRP970493A2 (en) 1996-09-23 1998-08-31 Wienman E. Phlips Oral delayed immediate release medical formulation and method for preparing the same
ATE277739T1 (en) 1996-10-28 2004-10-15 Gen Mills Inc EMBEDDING AND ENCAPSULATING PARTICLES FOR CONTROLLED DELIVERY
US5792476A (en) * 1996-12-19 1998-08-11 Abigo Medical Ab Sustained release glucocorticoid pharmaceutical composition
US5788987A (en) 1997-01-29 1998-08-04 Poli Industria Chimica Spa Methods for treating early morning pathologies
US6210710B1 (en) 1997-04-28 2001-04-03 Hercules Incorporated Sustained release polymer blend for pharmaceutical applications
NZ501251A (en) 1997-07-01 2001-09-28 Pfizer Sertraline salts and sustained-release dosage forms of sertraline
US6013280A (en) 1997-10-07 2000-01-11 Fuisz Technologies Ltd. Immediate release dosage forms containing microspheres
JP2001519379A (en) 1997-10-09 2001-10-23 ペリオ、プロダクツ、リミテッド Delayed total release gastrointestinal drug delivery system
US7201923B1 (en) 1998-03-23 2007-04-10 General Mills, Inc. Encapsulation of sensitive liquid components into a matrix to obtain discrete shelf-stable particles
US6365185B1 (en) * 1998-03-26 2002-04-02 University Of Cincinnati Self-destructing, controlled release peroral drug delivery system
CA2327685C (en) 1998-04-03 2008-11-18 Bm Research A/S Controlled release composition
US6602521B1 (en) 1998-09-29 2003-08-05 Impax Pharmaceuticals, Inc. Multiplex drug delivery system suitable for oral administration
US6375986B1 (en) 2000-09-21 2002-04-23 Elan Pharma International Ltd. Solid dose nanoparticulate compositions comprising a synergistic combination of a polymeric surface stabilizer and dioctyl sodium sulfosuccinate
ATE433318T1 (en) 1999-02-10 2009-06-15 Pfizer Prod Inc OSMOTIC SYSTEM FOR ADMINISTRATION OF ACTIVE INGREDIENTS CONTAINING SOLID AMORPHOUS DISPERSIONS
US6761903B2 (en) 1999-06-30 2004-07-13 Lipocine, Inc. Clear oil-containing pharmaceutical compositions containing a therapeutic agent
US6267985B1 (en) 1999-06-30 2001-07-31 Lipocine Inc. Clear oil-containing pharmaceutical compositions
US6294192B1 (en) 1999-02-26 2001-09-25 Lipocine, Inc. Triglyceride-free compositions and methods for improved delivery of hydrophobic therapeutic agents
US6248363B1 (en) 1999-11-23 2001-06-19 Lipocine, Inc. Solid carriers for improved delivery of active ingredients in pharmaceutical compositions
US6677326B2 (en) 1999-03-15 2004-01-13 Arakis, Ltd. Corticosteroid formulation comprising less than 2.5 mg prednisolone for once daily administration
GB9905898D0 (en) 1999-03-15 1999-05-05 Darwin Discovery Ltd Controlled-dose formulation
US6245352B1 (en) 1999-04-27 2001-06-12 Eli Lilly And Company Pharmaceutical formulation
JP2001010950A (en) 1999-06-29 2001-01-16 Taiyo Yakuhin Kogyo Kk Medicinal composition having stable and good drug releasability
US6458383B2 (en) 1999-08-17 2002-10-01 Lipocine, Inc. Pharmaceutical dosage form for oral administration of hydrophilic drugs, particularly low molecular weight heparin
US6309663B1 (en) 1999-08-17 2001-10-30 Lipocine Inc. Triglyceride-free compositions and methods for enhanced absorption of hydrophilic therapeutic agents
US6500459B1 (en) 1999-07-21 2002-12-31 Harinderpal Chhabra Controlled onset and sustained release dosage forms and the preparation thereof
EP1074249A1 (en) 1999-07-27 2001-02-07 Jagotec Ag A pharmaceutical tablet system for releasing at least one active substance during a release period subsequent to a no-release period
US6428809B1 (en) 1999-08-18 2002-08-06 Microdose Technologies, Inc. Metering and packaging of controlled release medication
AR026148A1 (en) 2000-01-21 2003-01-29 Osmotica Argentina S A OSMOTIC DEVICE WITH PREFORMED PASSAGE THAT INCREASES SIZE
DE10012555A1 (en) 2000-03-15 2001-09-20 Merck Patent Gmbh Composition for rapid release of corticoid drugs after delay period, useful for drug delivery during the night, e.g. for preventing asthma, or for delivery to colon for treating inflammatory bowel disease
DE10014588A1 (en) 2000-03-27 2001-10-04 Basf Ag Sustained-release oral dosage form that floats in gastric fluid includes a blend of polyvinyl acetate and polyvinylpyrrolidone
DE10015479A1 (en) 2000-03-29 2001-10-11 Basf Ag Solid oral dosage forms with delayed release of active ingredient and high mechanical stability
US20020028240A1 (en) 2000-04-17 2002-03-07 Toyohiro Sawada Timed-release compression-coated solid composition for oral administration
WO2001080824A2 (en) 2000-04-19 2001-11-01 Eurand America, Inc. Dual mechanism timed release dosage forms for low dose drugs
DE10029201A1 (en) 2000-06-19 2001-12-20 Basf Ag Retarded release oral dosage form, obtained by granulating mixture containing active agent and polyvinyl acetate-polyvinyl pyrrolidone mixture below the melting temperature
US6476006B2 (en) 2000-06-23 2002-11-05 Teva Pharmaceutical Industries, Ltd. Composition and dosage form for delayed gastric release of alendronate and/or other bis-phosphonates
US6720005B1 (en) 2000-07-07 2004-04-13 The State Of Oregon Acting By And Through The State Board Of Higher Education On Behalf Of Oregon State University Coated, platform-generating tablet
US6620439B1 (en) 2000-10-03 2003-09-16 Atul M. Mehta Chrono delivery formulations and method of use thereof
US6565873B1 (en) 2000-10-25 2003-05-20 Salvona Llc Biodegradable bioadhesive controlled release system of nano-particles for oral care products
US6887493B2 (en) 2000-10-25 2005-05-03 Adi Shefer Multi component controlled release system for oral care, food products, nutraceutical, and beverages
US6589562B1 (en) 2000-10-25 2003-07-08 Salvona L.L.C. Multicomponent biodegradable bioadhesive controlled release system for oral care products
ES2436523T3 (en) 2001-03-13 2014-01-02 Endo Pharmaceuticals Inc. Therapeutic dosage forms
NZ528607A (en) 2001-03-15 2007-11-30 Enteron Pharmaceuticals Inc Method of treating inflammatory GI disorders using topically active corticosteroids to reduce symptoms without causing the side effects associated with systemic steroid administration
IN191028B (en) 2001-05-17 2003-09-13 Sun Pharmaceutical Ind Ltd
WO2003004009A1 (en) 2001-07-02 2003-01-16 Geneva Pharmaceuticals, Inc. Pharmaceutical composition
BR0211317A (en) 2001-07-04 2004-12-14 Sun Pharmaceutical Ind Ltd System for controlled drug release through gastric retention
WO2003011254A1 (en) 2001-07-31 2003-02-13 Capricorn Pharma Inc. Amorphous drug beads
US20030044458A1 (en) 2001-08-06 2003-03-06 Curtis Wright Oral dosage form comprising a therapeutic agent and an adverse-effect agent
EP2957281A1 (en) 2001-09-21 2015-12-23 Egalet Ltd. Polymer release system
US20040253310A1 (en) 2001-09-21 2004-12-16 Gina Fischer Morphine polymer release system
ATE404179T1 (en) 2001-09-28 2008-08-15 Mcneil Ppc Inc DOSAGE FORMS WITH CORE AND OUTER SHELL
WO2003030872A2 (en) 2001-10-12 2003-04-17 Elan Pharma International Ltd. Compositions having a combination of particles for immediate release and for controlled release
US20080145438A1 (en) 2001-12-20 2008-06-19 Beuford Arlie Bogue Micro- and nano-particulate drugs and methods of making thereof
JP5105697B2 (en) 2002-01-18 2012-12-26 シヴィダ・インコーポレイテッド Co-drug polymer delivery system for controlled delivery
EP1478349A1 (en) 2002-02-21 2004-11-24 Amarin Development AB A method for releasing nanosized particles of an active substance from a diffusion-controlled pharmaceutical composition for oral use
WO2003075919A1 (en) 2002-03-14 2003-09-18 Daiichi Suntory Pharma Co.,Ltd. Tablet containing pilsicainide hydrochloride (dry)
WO2003080027A1 (en) 2002-03-20 2003-10-02 Elan Pharma International, Ltd. Nanoparticulate compositions of angiogenesis inhibitors
US7074426B2 (en) 2002-03-27 2006-07-11 Frank Kochinke Methods and drug delivery systems for the treatment of orofacial diseases
US7985422B2 (en) 2002-08-05 2011-07-26 Torrent Pharmaceuticals Limited Dosage form
US20040062778A1 (en) 2002-09-26 2004-04-01 Adi Shefer Surface dissolution and/or bulk erosion controlled release compositions and devices
RU2005108576A (en) 2002-09-28 2005-09-20 МакНЕЙЛ-ППС, ИНК. (US) POLYMERIC COMPOSITION AND CONTAINING ITS MEDICINAL FORMS
US20080220074A1 (en) 2002-10-04 2008-09-11 Elan Corporation Plc Gamma radiation sterilized nanoparticulate docetaxel compositions and methods of making same
US20040132826A1 (en) * 2002-10-25 2004-07-08 Collegium Pharmaceutical, Inc. Modified release compositions of milnacipran
US7704527B2 (en) 2002-10-25 2010-04-27 Collegium Pharmaceutical, Inc. Modified release compositions of milnacipran
EP1585502B9 (en) 2002-11-12 2012-05-09 Elan Pharma International Limited Fast-disintegrating solid dosage forms being not friable and comprising pullulan
US20040185097A1 (en) 2003-01-31 2004-09-23 Glenmark Pharmaceuticals Ltd. Controlled release modifying complex and pharmaceutical compositions thereof
US20070148229A1 (en) 2003-04-24 2007-06-28 Jagotec Ag Tablet with coloured core
MXPA05011446A (en) 2003-04-24 2006-05-31 Jagotec Ag Delayed release tablet with defined core geometry.
US8029822B2 (en) 2003-05-22 2011-10-04 Osmotica Kereskedelmi és Seolgáltató KFT Rupturing controlled release device having a preformed passageway
UY28326A1 (en) 2003-05-22 2004-06-30 Osmotica Argentina S A BREAKDOWN DEVICE CONTROLLED WITH A PREFORMED PASSAGE
US20060177507A1 (en) 2003-05-22 2006-08-10 Joaquina Faour Controlled release device containing lercanidipine
JP2007001865A (en) 2003-09-16 2007-01-11 Ltt Bio-Pharma Co Ltd Fine particle enclosing fat-soluble medicine, method for producing the same and preparation containing the same
EP1663156A2 (en) 2003-09-19 2006-06-07 Penwest Pharmaceuticals Company Chronotherapeutic dosage forms
DE102004035936A1 (en) 2004-07-23 2006-03-16 Röhm GmbH & Co. KG Multilayer dosage form
KR101363563B1 (en) * 2004-09-10 2014-02-14 자고텍 아게 Tablets with site and time-controlled gastrointestinal release of active ingredient
DE102004043863A1 (en) 2004-09-10 2006-03-16 Nitec Pharma Ag Tablets with local and time-controlled drug release in the gastrointestinal tract
GB0427455D0 (en) 2004-12-15 2005-01-19 Jagotec Ag Dosage forms
US20090110633A1 (en) 2005-03-14 2009-04-30 Shiladitya Sengupta Nanocells for Diagnosis and Treatment of Diseases and Disorders
US9149439B2 (en) 2005-03-21 2015-10-06 Sandoz Ag Multi-particulate, modified-release composition
JP5095615B2 (en) 2005-06-27 2012-12-12 バリアント・インターナショナル・(バルバドス)・ソサイアティーズ・ウィズ・リストリクティッド・ライアビリティ Modified release of bupropion salt
EP1898886B1 (en) 2005-07-01 2019-09-04 Rubicon Research Pvt Ltd. Novel sustained release dosage form
UA91376C2 (en) 2005-08-24 2010-07-26 Рубикон Рисеч Пвт Лтд. Controlled release formulation
FR2891459B1 (en) 2005-09-30 2007-12-28 Flamel Technologies Sa MICROPARTICLES WITH MODIFIED RELEASE OF AT LEAST ONE ACTIVE INGREDIENT AND ORAL GALENIC FORM COMPRISING THE SAME
WO2008134071A1 (en) 2007-04-26 2008-11-06 Theraquest Biosciences, Inc. Multimodal abuse resistant extended release formulations
US8324192B2 (en) 2005-11-12 2012-12-04 The Regents Of The University Of California Viscous budesonide for the treatment of inflammatory diseases of the gastrointestinal tract
EP1968548A2 (en) 2005-12-02 2008-09-17 Elan Pharma International Limited Mometasone compositions and methods of making and using the same
TW200820991A (en) 2006-07-10 2008-05-16 Elan Pharma Int Ltd Nanoparticulate sorafenib formulations
US20080014272A1 (en) 2006-07-11 2008-01-17 Phil Skolnick Compositions and Methods for Treatment of Chronic Pain Conditions
US20080026040A1 (en) 2006-07-31 2008-01-31 Isaac Farr Active agent-releasing dosage forms
EA015304B1 (en) 2006-08-03 2011-06-30 Нитек Фарма Аг Delayed-release glucocorticoid treatment of rheumatoid disease
AU2007281433A1 (en) 2006-08-04 2008-02-07 Nastech Pharmaceutical Company Inc. Compositions for intranasal delivery of human insulin and uses thereof
CL2007002214A1 (en) 2006-08-14 2008-03-07 Boehringer Ingelheim Int PHARMACEUTICAL COMPOSITION IN THE FORM OF COMPRESSED, WHERE AT LEAST THE LENGTH OF THE COMPRESSED IN THE PREVIOUS STATE OF THE APPLICATION IS AT LEAST 7/12 OF THE PILOR DIAMETER OF THE PATIENT AND AFTER INGERING IT IN THE FOOD STATE, THE LENGTH OF THE COMP
US20080057123A1 (en) 2006-08-30 2008-03-06 Jagotec Ag Controlled Release Formulations
WO2008028193A2 (en) 2006-09-01 2008-03-06 Pharmion Corporation Colon-targeted oral formulations of cytidine analogs
MX2009002536A (en) 2006-09-08 2009-04-14 Foamix Ltd Colored or colorable foamable composition and foam.
WO2008033351A2 (en) 2006-09-11 2008-03-20 Theraquest Biosciences, Inc. Multimodal abuse resistant and extended release formulations
AU2007320737B2 (en) 2006-11-14 2014-04-03 Celsus Therapeutics Plc Contact lens compositions
WO2008079963A2 (en) 2006-12-22 2008-07-03 Cambrex Charles City, Inc. Pharmaceutical compositions comprising ionic complexes of active pharmaceutical ingredients
WO2008085484A2 (en) 2006-12-28 2008-07-17 Jacobus Pharmaceutical Company, Inc. Treatment of inflammatory bowel disease with enteric coated formulations comprising 5-aminosalicylic acid or 4-aminosalicylic acid
GB2445539A (en) 2006-12-29 2008-07-16 Ardana Bioscience Ltd Bigel composition
WO2008094877A2 (en) 2007-01-30 2008-08-07 Drugtech Corporation Compositions for oral delivery of pharmaceuticals
US20100016322A1 (en) 2007-02-28 2010-01-21 Nagesh Nagaraju Water Dispersible Pharmaceutical Formulation and Process for Preparing The Same
US20090068236A1 (en) 2007-04-13 2009-03-12 Chemgenex Pharmaceuticals, Inc. Oral Cephalotaxine Dosage Forms
CN101657186B (en) 2007-04-13 2012-07-18 陶氏环球技术公司 Granular material for dosage forms
US20080311162A1 (en) 2007-05-16 2008-12-18 Olivia Darmuzey Solid form
WO2008140460A1 (en) 2007-05-16 2008-11-20 Fmc Corporation Solid form
WO2008140459A1 (en) 2007-05-16 2008-11-20 Fmc Corporation Solid form
US20080286343A1 (en) 2007-05-16 2008-11-20 Dzenana Cengic Solid form
EP2167033B1 (en) 2007-05-30 2017-04-19 Veloxis Pharmaceuticals A/S Once daily oral dosage form comprising tacrolimus
NZ580972A (en) 2007-06-04 2012-02-24 Egalet Ltd Controlled release pharmaceutical compositions for prolonged effect
EP2008651A1 (en) 2007-06-26 2008-12-31 Drug Delivery Solutions Limited A bioerodible patch
AU2008288106B2 (en) 2007-08-13 2012-03-15 Panacea Biotec Limited Extended release compositions comprising mycophenolate sodium and processes thereof
US9254268B2 (en) 2007-09-25 2016-02-09 Solubest Ltd. Compositions comprising lipophilic active compounds and method for their preparation
US20110091566A1 (en) 2007-09-25 2011-04-21 Nirmal Mulye Controlled release pharmaceutical compositions
AR068745A1 (en) 2007-10-08 2009-12-02 Panacea Biotec Ltd A COMPOSITION IN THE FORM OF ORAL PHARMACEUTICAL DOSAGE OF HIGH DOSAGE UNIT OF SODIUM MYCOPHENOLATE, METHOD FOR USING SUCH COMPOSITION AND ITS USES
JP2011500553A (en) 2007-10-10 2011-01-06 ルピン・リミテッド Controlled release bioadhesive formulation targeting 5-colon of 5-aminosalicylic acid or its salts or metabolites
US20090143343A1 (en) 2007-11-13 2009-06-04 Meritage Pharma, Inc. Compositions for the treatment of inflammation of the gastrointestinal tract
CA2710387A1 (en) 2007-12-21 2009-07-09 Coda Therapeutics, Inc. Treatment of fibrotic conditions
EP2242844A2 (en) 2007-12-21 2010-10-27 Coda Therapeutics, Inc. Use of anti-connexin peptides, alone or in combination with anti-connexin polynucleotides, for the treatment of orthopedic conditions
US20130184220A1 (en) 2007-12-21 2013-07-18 Bradford James Duft Treatment of abnormal or excessive scars
CN101969931A (en) 2008-03-05 2011-02-09 万能药生物有限公司 Modified release pharmaceutical compositions comprising mycophenolate and processes thereof
WO2009142772A2 (en) 2008-05-23 2009-11-26 Mastcell Pharmaceuticals, Inc. Methods and treatment for allergies and inflammation associated with gastrointestinal diseases
US8648119B2 (en) 2008-05-23 2014-02-11 Otonomy, Inc. Controlled release immunomodulator compositions and methods for the treatment of otic disorders
WO2010005687A1 (en) 2008-06-12 2010-01-14 University Of Alabama Huntsville Compositions comprising nitric oxide or nitric oxide donors for the treatment of neurodegenerative diseases or trauma
GB2462022B (en) 2008-06-16 2011-05-25 Biovascular Inc Controlled release compositions of agents that reduce circulating levels of platelets and methods thereof
CL2009001884A1 (en) 2008-10-02 2010-05-14 Incyte Holdings Corp Use of 3-cyclopentyl-3- [4- (7h-pyrrolo [2,3-d] pyrimidin-4-yl) -1h-pyrazol-1-yl) propanonitrile, janus kinase inhibitor, and use of a composition that understands it for the treatment of dry eye.
WO2010084188A1 (en) 2009-01-26 2010-07-29 Nitec Pharma Ag Delayed-release glucocorticoid treatment of asthma
NZ582836A (en) 2009-01-30 2011-06-30 Nitec Pharma Ag Delayed-release glucocorticoid treatment of rheumatoid arthritis by improving signs and symptoms, showing major or complete clinical response and by preventing from joint damage

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
Cutolo et al.; Ann. N.Y. Acad. Sci. 966: 91-96 (2002). *

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US8920838B2 (en) 2006-08-03 2014-12-30 Horizon Pharma Ag Delayed-release glucocorticoid treatment of rheumatoid disease
US9504699B2 (en) 2006-08-03 2016-11-29 Hznp Limited Delayed-release glucocorticoid treatment of rheumatoid disease

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