ZA200406731B - Absorption enhancing agent. - Google Patents

Absorption enhancing agent. Download PDF

Info

Publication number
ZA200406731B
ZA200406731B ZA200406731A ZA200406731A ZA200406731B ZA 200406731 B ZA200406731 B ZA 200406731B ZA 200406731 A ZA200406731 A ZA 200406731A ZA 200406731 A ZA200406731 A ZA 200406731A ZA 200406731 B ZA200406731 B ZA 200406731B
Authority
ZA
South Africa
Prior art keywords
composition
peg
substance
composition according
mammal
Prior art date
Application number
ZA200406731A
Inventor
Sveinbjoern Gizurarson
Jakob Lindal Kristinsson
David Rurik Olafsson
Ellen Ruth Ingimundardottir
Sigriour Olafsdottir
Kolbrun Hrafnkelsdottir
Oddur Ingolfsson
Original Assignee
Lyfjathroun Hf
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Lyfjathroun Hf filed Critical Lyfjathroun Hf
Publication of ZA200406731B publication Critical patent/ZA200406731B/en

Links

Landscapes

  • Medicinal Preparation (AREA)

Description

ABSORPTION ENHANCING AGENT
FIELD OF THE INVENTION
The present invention relates to pharmaceutical compositions comprising one or more : mono- and diglycerides according to formula | as an absorption enhancing agent, a bioavailability improving agent and/or a bioadhesive agent. The pharmaceutical compositions are especially suitable for mucosal administration such as intranasal administration.
BACKGROUND OF THE INVENTION
Parenteral administration (intravenous, intramuscular and subcutaneous) of active substances, such as drugs, is normally regarded as the most effective route of administration. However, administration by injection has a number of disadvantages.
Injection of an active substance requires the use of sterile syringes and administration by trained personnel, and may cause pain and irritation, particularly in the case of repeated injections. This route of administration poses a risk of infection. More significantly, intramuscular injections are often poorly tolerated by the individual, and may possibly cause an induration (hardening of tissue), haemorrhage (bleeding) and/or necrosis (local death of tissue) at the injection site.
The mucosal membrane is connected to an extensive network of blood capillaries under the nasal mucosa, which makes the membrane highly suitable for drug delivery (delivery of active substances), particularly suited to provide rapid absorption of active substances, providing a rapid pharmacological response. One example of such a mucosal membrane is the nasal epithelial membrane, which consists essentially of a single layer of epithelial cells (pseudo-stratified epithelium), the mucosal membrane is therefore very suitable for drug delivery.
A variety of vehicle systems for intranasal drug delivery have been developed. One of the problems encountered in using such vehicle systems, is the local irritation and lack of rapid absorption. Without the rapid rate of absorption, the active substances, such as drug substances, may be cleared from the absorption site before they are absorbed into the systemic circulation, into the lymphatic system or into the brain, whichever is relevant.
It is contemplated that a vehicle that is bioadhesive as well as water-soluble would be an advantage for mucosal administration. However, to the best of the present inventors knowledge no such vehicle has yet been found. Thus, there is a need for developing a : bioadhesive agent, which may be used especially in hydrophilic compositions. It is also an advantage if it can be used in lipophilic compositions as well. The bioadhesive agent : should be suitable for mucosal delivery of active substances such as drug substances and/or vaccines.
A variety of vehicle systems for intranasal drug delivery have been developed. One of the problems encountered in using such vehicle systems, is the local irritation and malabsorption. A frequent problem is that the substance may be cleared from the absorption site before it may be absorbed into the systemic circulation, into the lymphatic system or into the brain. Many excipients such as polyethylene glycol and glycofurolum (Bechgaard, Gizurarson & Hjortkjaer, DK-1170/90 and Bechgaard, Gizurarson &
Hijortkjaer, US/5,397,771) are highly viscous and therefore not suitable for the purpose.
Thus, there is a need for an effective formulation for intranasal or mucosal drug delivery that may be used in low concentration without being affected by the viscosity.
WO 99/02186 describes antigen delivery systems comprising monogiyceride or diglyceride derivatives as adjuvants. The monoglyceride or diglyceride derivatives mentioned therein may contain a PEG polymer. However, there is no mention or indication that such derivatives are capable of promoting absorption of an active substance to obtain an increased and/or improved onset of action or to improve the bioavailability of an active substance. Furthermore, there is no disclosure mentioning or indication that such derivatives have an ability to adhere to a mucosal surface.
US 6,326,401 relates to a formulation for the oromucosal in particular the pernasal route. it describes pharmaceutical compositions comprising caprylcaproyl-macrogol glycerides for delivery of non-polypeptidic active substances. There is no mention or indication that the glycerides have bioadhesive properties.
The present invention provides pharmaceutical compositions, which - when administered to the mucosa such as intranasally to the nasal mucosa - enable the active substance ] rapidly to be absorbed into the circulatory system. The compositions comprise an absorption enhancing, a bioavailability improving and/or a bioadhesive agent that is a glyceride ester formed by esterification of glycerol with one or more polyethylene glycols and with one or more fatty acids. The absorption enhancing, bioavailability improving and/or bioadhesive agent does not irritate the nasal mucosa in the concentrations claimed. ’ SUMMARY OF THE INVENTION ’ The present invention is based on the observation that mono- and diglycerides according to formula | are absorption enhancing agents, bioavailability improving agents and/or bioadhesive agents. Furthermore, the mono- and diglycerides are water-soluble which means that the bioadhesive properties are present in a monophasic system such as an aqueous based system. This observation of the above-mentioned effects is extremely valuable in respect of design of pharmaceutical composition for administration to mucosal surfaces. Firstly, it is possible to ensure that the composition after administration will remain on the administration site for a prolonged period of time (i.e. a rapid clearance effect can be avoided) and, secondly, due to the water-solubility of the glycerides it is possible to formulate the compositions as a single phase composition, i.e. it is not necessary to add any surfactants (including emulsifiers) etc in order to stabilize a two or more phase composition and thereby it is possible to avoid any irritating effect arising from such surfactants. Moreover, it is envisaged that it is possible to obtain an enhanced onset of action and/or a controlled delivery of the active substance to the systemic circulation or to the site of action.
Thus the present invention relates to the use of a composition comprising one or more mono- or diglyceride having the formula (I):
H,G—0—R1
HC—O—R2 0
H,C—O—R3 wherein R1, R2, and R3 are selected from the group consisting of from C6 to C26 fatty acids, PEG polymers and hydrogen, provided that at least one of R1, R2 and R3 is a C6-C26 fatty acid residue and at least - one of R1, R2 and R3 is a PEG polymer residue . as an absorption enhancing, a bioavailability improving and/or a bioadhesive agent.
4 A
The term “PEG-C6/C26 glycerides” as used in the present context refers ta those reaction products derived from the co-reaction of polyoxyethylene glycol (or polymerizable precursor thereof, such as ethylene oxide) with a C6-C26 carboxylic acid and glycerol or a : C6-C26 carboxylic acid glyceride or glycerides. Resulting from such reactions are, typically, mixtures of a polyoxyethylene glycol-C8-C10 carboxylic acid diftri-glyceride : esters (e.g.; PEG-glycerol-caprate, PEG-glycerol-caprylate etc.) as principal components.
In another aspect, the invention relates to a pharmaceutical composition for nasal administration comprising i) one or more mono- or diglyceride having the formula (I):
CH;-0O-Ry4
CH-0O-R: 0]
CH;-0O-Rs wherein R1, R2, and R3 are selected from the group consisting of from C6 to C26 fatty acids, PEG polymers and hydrogen, provided that it contains at least one C6-C26 fatty acid and at least one PEG polymer, ii) a therapeutically, prophylactically and/or diagnostically active substance; and iii) optionally, a physiologically acceptable vehicle.
Other aspects of the invention relates to a method for obtaining a relatively fast onset of a therapeutic effect or for improving the bioavailability of an active substance, the method comprises administering to a mammal including a human an efficient amount of a composition according to the invention.
DETAILED DISCLOSURE OF THE INVENTION
} As appears from the above, the present invention concerns the use of compositions comprising one or more mono- or diglycerides of formula | especially for administration to ’ a mucosal surface. The invention is based on the observation that specific glycerides can act as absorption enhancers, bioavailability improving agents and/or bioadhesive agents and at the same time they are non-irritating to the nasal mucosal. : Thus, the present invention relates to the use of a composition comprising 5 . one or more mono- or diglycerides having the formula (1):
H,G—O—Rt1
HC—O—R2 0
H,C—0O—R3 wherein R1, R2, and R3 are selected from the group consisting of from C6 to C26 fatty acids, PEG polymers and hydrogen, provided that at least one of R1, R2 and R3 is a C6-C26 fatty acid residue and at least one of R1, R2 and R3 is a PEG polymer residue as an absorption enhancing, a bioavailability improving and/or a bioadhesive agent.
The PEG polymer on the glycerides imparts the desired water-solubility of the bioadhesive agent. Thus, it the water-solubility of the bioadhesive agent is relatively high, i.e. at least 40% wiw such as at least 50% w/w or at least 60% w/w. As mentioned above the high water-solubility makes it possible to design pharmaceutical compositions in liquid form that are in the form of single phase aqueous systems and thereby it is possible to avoid side effects related to the presence of surfactants or other additives that stabilize e.g. emulsions or suspensions.
Any saturated or unsaturated C6-26 fatty acid can be used including, but not limited to, fatty acid residues derived from caproic acid, capric acid, caprylic acid, arachidonic acid, propionic acid, lauric acid, myristic acid, palmitic acid, oleic acid, linoleic acid and linolenic acid. Examples of suitable fatty acids are saturated or unsaturated C6-20, C6-C18, C6-14,
C6-12, C8-12 or C8-10 fatty acids. In one embodiment, the fatty acids are C6, C8 or C10 fatty acids.
The fatty acid residues may be a single residue or a mixture of two or more residues. ] They can be derived from natural or synthetic sources, such as fats and oils.
Commercially available glycerides can be used or they can be synthesized enzymatically by means of lipases, including both specific and non-specific lipases, which place the fatty acids on specific positions (R1, R2 and/or R3) such as Rt; R2; R1, R2; R1, R3; and ’ specific racemic structures as well etc. For example, glycerol (0.92 g) adsorbed onto 1 g silica gel is suspended with 20 hl tBuOMe. Vinyl caprylate (3.49) and lipase (50 mg) from : Rhizopus delemar were added © the suspension. The mixture was stirred at room temperature for 96 hours and the reaction progress was monitored by means of TLC.
After removal of the solid companents by filtration and evaporation of the solvent, a crude reaction mixture was obtained which contained about 91% of 1,3 dicaprylin glyceride.
The absorption enhancing, a bioavailability improving and/or a bioadhesive agent can be prepared by oligomerizing or polymerising ethylene oxide in the presence of an ester of glycerol and one or more of such C6-C26 carboxylic acids (glyceride esters). Still another route is by co-reacting a carboxylic acid glyceride ester or esters with a fully pre-formed polyoxyethylene glycerol under conditions to achieve alcoholysis. The term “carboxylic acid glyceride ester’, is employed in this description in the conventional sense to mean an ester which has been derived from glycerol and a carboxylic acid.
A suitable PEG polymer is one that is biocompatible with the tissue to which it is administered, particularly the cus membranes. Suitable PEG polymers having these properties include but are not ited to, polyethylene glycol, polyoxyethylene glycol, polyethylene glycol derivatives (including, but not limited to, amino-PEG, nucleophilic-
PEG, PEG-thial, PEG-succinate, PEG-succinimide, PEG-tresylate, carboxymethylated-
PEG, PEG-propionic acid, PEGsilanes, PEG-phospholipids, biotin-PEG and PEG- orthopyridyl-disulfide) and polyoxyethylene glycol derivatives.
The polyethylene glycol (PEG or PEO) component used in the formation of the absorption enhancing, bioavailability improving and/or adhesive agent is, typically, a medium to high molecular weight material having a molecular weight of from about 200 to about 1200 such as, e.g. from about 300 to about 600.
Preferred are polyethylene glycol polymers having from about 2 to about 30 polyethylene glycol units (PEG2-30) or PEG Solymers that have from 2 to about 15 residues such as, e.g., from 2 to about 10 residues, from 2 to about 8 residues or from about 3 to about 6 residues.
'
One or two PEG moieties can be incorporated into the giyceride formula. The water- soluble moiety can reside at any one of the R1, R2, and/or R3 positions of the glyceride. ] ; Thus, the composition for use according to the invention may comprise a mixture of at least a first and a second ayer, the first glyceride having one PEG polymer in position : R1, R2 or R3, and the second glyceride having two PEG polymers in position R1, R2 and/or R3.
The polymers can be attached to the glyceride via covalent bonds formed chemically or enzymatically. The polymers may be acylated to the glyceride or linked using ester bonds such as, for example, by esterase-mediated synthesis. For example, solketal can be mixed with polymerchloride in triethanolamine and trichloromethane, whereafter the free glycerol bonds are deprotected by heating in dilute aqueous acetic acid. With excess of caproyl chloride in the presence of triethylamine and 4- dimethylaminopyridine as catalyst, the fatty acids are linked to the free glycerol bonds. The results of this synthesis will be a caproyl/polymer glyceride. in one embodiment, the composition for use according to the invention comprises a mixture of mono- and diglycerides having formula I, such as a mixture of one or more monoglycerides and/or a mixture of one or more diglycerides. The v/v-% ratio of monoglycerides to diglycerides being from about 0.1:99.9 to about 99.9:0.1 such as, e.g., from about 1:99 to about 99:1, from about 2.5:97.5 to about 97.5:2.5, and preferably from about 5:95 to about 95:5.
In a second embodiment, the mono- or diglyceride has a structure selected from the group consisting of:
H,G1-0~R1
HCTO—R2 Q) iro-reo woro-r . HETO~PEG un
HCTo-R2
H,G—0O—PEG
HG—O—R1 (Iv)
H,C—O—PEG
H,C—O—R1
HC—O—PEG \
H,C—O—PEG
The PEG polymers in formulas 1I-V have from about 2 to about 30 polyethylene glycol units (PEG2-30). In a specific embodiment, the PEG in formula i-V is selected from the group consisting of PEG2, PEG3, PEG4, PEG5, PEG6, PEG7, PEGS, PEGY, PEG10, and in yet another specific embodiment, the PEG in formula 11-V is PEG3 or PEGG.
In another embodiment, the monoglyceride has the following structure i momen oH on VI)
H,C—-0C,H;-—OH and in yet another embodiment, the diglyceride has the following structure i og Teron
H romCr onan, (vin)
H,C1-OC;H;,-OH
In a specific embodiment, the composition contains a mixture of the two following . 20 structures i 0 ngmoeten CH, Hpmoe Ton CH,
Il yoeon Vv) and Hot reon (Vil)
H,C—-0C,H;—-OH H,C—F-OC,Hy|-—OH
In the formulas Vi and VII, x is from about 4 to about 20, such as e.g. from about 4 to about 12, or from about 6 to about 8, and y is from 2 to about 30, such as e.g. from 2 to about 10, or from 3 to about 6. In a specific embodiment of the invention, x is 6 and/or 8 andy is 3 and/or 6.
The total concentration of glycerides of formula | in the composition is at least about 90 % w/w such as, e.g., at least about 92.5% wiw, at least about 95% wiw, at least about 97.5% wiw, at least about 98% w/w or at least about 99% w/w and is normally from about 0.05- 89.95 of glyceride fatty acid diester of formula I and Ili such as, e.g. from about 5 to about” 95% glyceride fatty acid diesters of formula Il and lll and from about 0.05 to about 99.95% glyceride fatty acid mono esters of formula IV and V such as, e.g. from about 5 to about 95% glyceride fatty acid monoesters of formula IV and V. The fatty acid esters at the glycerides may contain about 30-90% octanoic acid esters (C8) and about 5-80% decanoic acid esters (C10).
In one embodiment, the glyceride has a chiral carbon, and in a specific embodiment the chiral carbon is S- or R-form.
Suitable absorption enhancing, a bioavailability improving and/or bioadhesive agents for use in this invention, which are commercially available, are Softigen® 767, produced by
Condea Chemie GmbH (Witten, Germany). Softigen® 767 contains following specifications:
Specification Value . Acid value : <1 mg KOH/g
Saponification value 90-100 mg KOH/g ) 30 lodine value <1 mg 1/100 mg
Colour <150 APHA
Freeze test Clear solution at 0°C (24h)
Water content max. 0.5% (Carl Fisher te)
Viscosity 150-175 mPaes
Refractive index 1.464-1.466 "Dg : EP-0351651 describes the use of PEG-C8/C10-glycerides as an absorption promoter for insulin. Especially for orally and buccally administered insulin. From the disclosure it appears that an increase in concentration of PEG-C8/C10-glycerides results in an increase in absorption. With respect to a nasal composition the composition described has a relatively high concentration of absorption enhancer, namely about 50% w/w.
The present invention provides glycerides according to formula 1, which can be used as an absorption enhancing, a bioavailability improving and/or a bioadhesive agent in the concentrations claimed in the appended claims. It is especially interesting that the present inventors have observed that also very low concentrations lead to a suitable therapeutic response. Thus, even concentrations in a range corresponding to from 0.005 to about 2.5 %, or from 0.01 to 2.0% v/v are suitable for the administration of active substances, such as drugs, through the mucosal membrane such as the nasal membrane. This agent is fully water-soluble and produces a non-viscous solution together with water or saline. The agent of the present invention provides enhanced absorption of the active substance through the nasal mucosal membrane. Use of the invention provides the ability to achieve a significant controllable systemic absorption of active substances such as drugs, into the systemic circulation, without causing unacceptable irritation of the epithelial membrane.
As mentioned above, the disclosure in EP-B-0 351 651 (Hoffmann-La Roche) is focused on oral and buccal insulin composition. The present invention is mainly directed to nasal compositions, but as discussed above, it has been found that even very small : concentrations of glycerides according to the invention may lead to a suitable therapeutic response.
Therefore in another aspect, the invention relates to a pharmaceutical composition for nasal administration comprising i) a composition comprising one| or more mono- or diglycerides according to the invention, i) a therapeutically, prophylactically and/or diagnostically active substance; and iii) optionally, a physiologically acceptable vehicle.
The present invention is also directed to compositions in general, in which the concentration of the absorption enhancing, bioavailability improving and/or bioadhesive agent is relatively low, namely in concentrations ranging from 0.005 - 2.5 % v/v such as, : e.g., 0.01 - 2% v/v of chemically modified glycerides selected from the group consisting of monoglycerides, diglycerides, and mixtures thereof, said glycerides having the formula (1):
CH.-O-R1
CH-0-R2 {)
CH;-0-R3 wherein R1, R2, and R3 are as defined above.
In a composition according to the present invention for nasal administration the concentration of component i) in the composition is at the most 50% v/v such as, e.g., from about 0.005% to about 50% v/v, from about 0.005% to about 40% v/v, from about 0.01% to about 30% v/v, from about 0.01% to about 25% v/v, from about 0.01 to about 20% v/v, from about 0.01 to about 15% v/v, from about 0.01 to about 10% v/v.
Alternatively, the concentration of component i) in the composition is at the most about 10% viv such as, e.g., at the most about 7.5% v/v, at the most about 5% v/v, at the most 2.5% viv.
Irrespective of the route of administration, the invention relates to a composition having a concentration of component i) in the composition is from about 0.01% to about 2% viv such as, e.g. from about 0.1 to about 1.5% v/v such as from about 0.2% to about 1% viv.
As mentioned above, a composition according to the invention leads fo a relatively fast onset of the active substance contained in the composition. Thus, tna - when nasally administered - takes places relatively fast after administration compared to tax obtained after administration of a similar composition containing saline instead of component i). In other words, in a composition according to the invention, the mono- or diglycerides are used as an absorption enhancing, a bioavailability improving and/or a bioadhesive agent, providing a desired trax.
A further advantage of a composition according to the invention is that an increase in bioavailability is obtained. Thus, - when nasally administered — the bioavailability is increased with a factor of at least 2 such as, e.g., at least 5, at least 10, at least 20, at least 40 compared with the bioavailability obtained after administration of a similar composition containing saline instead of component i).
In a particular embodiment, a composition according to the invention contains the active substance ii) is in a dissolved form.
In addition to the above-described effects, the composition of the invention mediates adhesion of active substances to the nasal mucosa and thereby prolongs the residence time of the substance at the administration site. Furthermore the composition of the invention promotes absorption of active substances, such as drugs, across the nasal membrane, that is, the drug is capable of being absorbed into the systemic circulation with sufficient speed and quantity to be biologically active. This can be accomplished, since an absorption promoter increases the rate of absorption allowing a rapid onset of the drug and increases the amount absorbed across the nasal membrane.
A composition according to the invention may further comprising one or more components selected from the group consisting of: surfactants, water absorbing polymers, substances which inhibit enzymatic degradation, alcohols, organic solvents, oils, pH-controlling agents, solubilizers, stabilizers, HLB-controlling agents, viscosity controlling agents, preservatives, osmotic pressure controlling agents, propellants, air displacement, water, and mixtures thereof.
For intranasal administration, an active substance must be applied to the mucosa in such a manner that it is able to penetrate or be absorbed through the mucosa into the systemic circulation before it is washed away by the nasal secretions or ciliary beat clearance. In order to penetrate the mucus, the delivery vehicle must have a certain degree of biocompatibility with the mucus membrane and hence have a certain degree of hydrophilicity and hydrophobicity. Work described herein relates to the utility of compositions described herein as absorption enhancing, bioavailability improving and/or ] bioadhesive agents. Accordingly, this invention also pertains to compositions, e.g. drug compositions, comprising an active substance and an absorption enhancing, bioavailability improving and/or bioadhesive agent containing 0.01-2% v/v of glycerides selected from the group consisting of PEG-C8/C10-glycerides.
The PEG-C8/C10 glycerides are products derived from the co-reaction of polyoxyethylene glycol (or poly merizable precursor thereof, such as ethylene oxide) C6-C26 carboxylic acid glyceride or glycerides or by oligomerizing or polymerising ethylene oxide in the presence of an ester of glycerol and one or more of such C6-C26 carboxylic acids (glyceride esters). Resulting from such reactions are, typically, mixtures of a polyoxyethylene glycol-C6-C26 carboxylic acid mono-/di- glyceride esters (e.g.; PEG-
C8/C10-glycerol-dicaprate, diPEG-glycerol-caprate, PEG-glycerol-dicaprylate etc.) as principal components.
The absorption enhancing, bioavailability improving and/or bioadhesive agents of the invention mediates the adhesion of an active substance to a mucosal surface and also modulates the absorption of the substance such as a drug in order to generate successful absorption and absorption rate into the systemic circulation.
In this invention, an active substance is combined with one or more glycerides according to this present invention, and this formulation can be used to mediate adhesion of the substance to a mucosal surface of a subject such as a mammal and elicit absorption of the drug into the subject. Examples of active substances and drugs are anti-emetics and anti-nausea and drugs for the treatment of motion sickness such as ondansetron, granisetron, tropisetron, scopolamine, metopimazine; anti-migraine drugs such as sumatriptan, zolmitriptan, naratriptan, rizatriptan, eletriptan, almotriptan, frovatriptan; sex hormones, such as androgen hormones e.g testosteron and derivatives thereof; anti- narcotic treatment drugs such as nicotine, hormones such as calcitonin, drugs for the treatment of erectile dysfunction such as apomorphine, sildenafil, drugs for pain management such as morphine, drugs for sleep induction such as melatonin and the benzodiazepines, drugs for sedation, preanaestesia and treatment of epileptic seizures from the group of benzodiazepines such as diazepam, alprazolam, fiunitrazepam, lorazepam, triazolam, nitrazepam, lormetazepam, midazolam, desmethyldiazepam, flurazepam; drugs for ntithromobotic treatment such as heparin, dalteparin, enoxaparin and tranexamic acid; drugs for fertility treatment such as choriogonadotropin, menotropin, follitropin alpha, follitropin beta and lutropin alpha. ) Other active substances do include but are not limited to materials having antiviral, antiprion, antibacterial, antineoplastic, antiparasitic, anti-inflammatory and/or antifungal activity. They may act as neurotfansmiter, neuromodulators, hormone, hormone releasing factor, hormone receptor agonist or antagonist. The substance may also be an activator or inhibitor of a specific enzyme, an antioxidant, a free radical scavenger or a metal chelating agent. The active substance may further be any substance which is capable of acting as a stimulant, sedative, hypnotic, analgesic, anticonvulsant, antiemetic, anxiolytic, antidepressant, tranquilliser, cognition enhancer, agents preventing or healing amnesia, ’ metabolic stimulator or inhibitor, appetite stimulator or inhibitor and/or narcotic antagonist or agonist. The substance may furthermore be any bioactive material found to be deficient : in conjunction with the disorder being treated or prevented, for example, nutrients such as glucose, ketone bodies, and the like, or metabolic precursors such as lecithin, choline or acetyl coenzyme A for producing neurotransmitters for the treatment of Alzheimer's disease or insulin for the treatment of obesity and diabetes. The substance may also be an antibody for the treatment of viral, bacterial, prion, parasitic infections or tumours and/or cancer or for diagnosis of diseases or disorders where polyclonal or monocional antibodies and/or/with biochemical markers characteristic of the diseases or disorder are used. Such diagnostic antibodies may be labelled with any labelling agent who may be suitable according to the invention. Gene manipulated micro-organisms may also be used for the treatment of tumours and/or cancer. The active substance may also comprise of substances selected from the group consisting of adrenal hormones, corticosteroids and derivatives, amino acids, anorectics, antibiotics, anti-allergic agents, antibodies, anti- cholinergic agents, anti-depressants, anti-epileptica and anti-spasmolytica, anti-histaminic agents, anti-hypertensive agents, anti-inflammatory agents (enzymatic or non-steroidal or steroidal), anti-neoplastic agents, antiseptics, anti-tumor, anti-tussive expectorant (asthamtic agents), anti-viral and anti-cancer agents, beta-adrenergic blocking agents, blood factors such as factor VII, factor VIII etc, metabolism controlling agents, bone- metabolism controlling agents, bronchodilators, cardiotonics, cardiovascular regulatory hormones, chemoterapeutic agents, CNS-stimulants, diagnostic drugs, dopaminergic agents, enzymes, gastrointestinal hormones, hypothalamus hormones and derivatives, hypotensives, local anesthetics, migraine treatment substances, narcotics, antagonists and analgetics, pancreatic hormones and derivatives, parasympathomimetics, parasympatholytics, Parkinson's disease substances, pituitary gland hormones and derivatives, prostaglandines, protease inhibitors, sedatives, sex-hormones, sympathomimetics, thyroid gland hormones and derivatives, tranquillisers, vasoconstrictors, vasodilators, and vitamins.
The active substance such as drugs may be used in a particulate form or dissolved. The formulation is especially suitable for dissolved drugs.
The absorption enhancing effect of an absorption enhancing, bioavailability improving and/or bioadhesive agent according to this invention can be monitored with methods known in the art, such as HPLC, LC-MS, LC-MS-MS, GC, GC-MS, spectroscopy and/or
ELISA assays. As used herein, "absorption enhancing effect” is intended to mean the ability to increase and/or accelerate the absorption of an active substance into the systemic circulation. Absorption enhancing effect includes, but is not limited to, the ability to enhance the absorption of the active substance by increasing the transport of the substance across the nasal mucosal membrane and to accelerate this transport.
Typically the administration of the absorption enhancing, bioavailability improving and/or bioadhesive agent of the invention will also cause or result in an enhanced pharmacological response to the active substance of interest. In this context, "enhancing" is intended to mean that the absorption of an active substance is quantitatively greater and/or qualitatively better in the presence of the absorption enhancing agent than in the absence of the absorption enhancing agent. Furthermore, the absorption dynamics of the active substance can be controlled through the concentration of the absorption enhancer, to tailor the pharmacokinetics to achieve the optimal biologically active response.
Comparisons of absorption in the presence and absence of the absorption enhancing agent can be performed by routine methods, such as titres comparisons by HPLC, L.C-
MS, LC-MS-MS, GC, GC-MS, spectroscopy or ELISA assays, and appropriate controls.
The enhanced absorption can be a result of a direct effect on the mucosal membrane or due to a more advantageous presentation of the biologically active agent to the mucus membrane.
The bioadhesive effect of the absorption enhancing, bioavailability improving and/or bioadhesive agents according to the invention, with a particular active substance, can be assessed using methods known in the art, such as bioadhesiometer, radioactive tracers, fluorescence tracers. As used herein, "bioadhesive effect” is intended to mean the ability to increase the duration of an active substance at the site of absorption. Bioadhesive effects include, but are not limited to, the ability to prolong the duration of the active substance by decreasing the clearance of the active substance from the site of absorption, such as the nasal cavity. . Typically the administration of the absorption enhancing, bioavailability improving and/or bioadhesive agent of the invention will also cause or result in a controlled release and . 35 prolonged pharmacological response to the active substance of interest. In this context, "prolonged" is intended to mean that the pharmacological effect of an active substance is quantitatively longer and/or therefore qualitatively better in the presence of the agent of the invention than in the absence of the agent. Comparisons of the effect in the presence and absence of the bioadhesive agent can be performed by routine methods, such as monitoring the clearance of radiolabelled tracers or fluorescence labelled tracers and an ) appropriate control. The prolonged duration can be a result of a biocompatibility with the mucosal environment and/or direct effect on the mucosal membrane of due to a more ’ advantageous presentation of the active substance to the mucus membrane.
The method of the present invention comprises administering to a mammal, particularly a human or other primate, a pharmacologically effective dose of a pharmaceutical composition according to the invention comprising an active substance and an absorption enhancing, bioavailability improving and/or bioadhesive agent according to the invention.
The concentration of the absorption enhancing, bioavailability improving and/or bioadhesive agent ranges from high concentrations to low concentrations of about 0.01% to about 2% viv, and more particularly from about 0.2% to about 1.5% v/v and more preferably between 0.2% and 1% v/v, will typically be effective to provide absorption enhancing, bioavailability improving and/or bioadhesive effects; however, variations in these dosage ranges will occur depending upon the active agent. Moreover, the particular dosage will depend upon the age, weight and medical condition of the mammal to be treated, as well as on the method of administration. The skilled artisan will readily determine suitable doses.
The composition according to the invention can be optionally administered in a pharmaceutically or physiologically acceptable vehicle, such as physiological or phosphate buffered saline, water, dextrose, ethanol polyols (such as glycerol or propylene glycol), and combinations thereof. The formulation according to the invention can be in admixture with a dispersing or wetting agent, suspending agent, and/or one or more preservatives. Suitable dispersing or wetting agents are, for example, naturally occurring phosphatides, e.g., lecithin, or soybean lecithin; condensation products of ethylene oxide with e.g. a fatty acid, a long chain aliphatic alcohol, or a partial ester derived from fatty acids and a hexitol or a hexitol anhydride, for example polyoxyethylene stearate, polyoxyethylene sorbitol monooleate, polyoxyethylene sorbitan monooleate etc. Suitable suspending agents are, e.g., naturally occurring gums such as, e.g., gum acacia, xanthan } gum, or gum tragacanth; celluloses such as, e.g., sodium carboxymethyicellulose, microcrystalline cellulose (e.g. Avice! RC 591), methylcellulose; alginates such as, e.g., sodium alginate, etc. Suitable dxamples of preservatives for use in formulations according to the invention are parabens, such as methyl or propyl p-hydroxybenzoate, and benzalkonium chloride.
For application to the nasal mucosa nasal sprays or inhalation formulations are suitable compositions for use according to the invention. In a typical nasal formulation, the active substance is present in the form of a solution. The pharmaceutically acceptable vehicles and excipients and optional other pharmaceutically acceptable materials present in the composition such as diluents, flavouring agents, preservatives and the like are all selected in accordance with conventional pharmaceutical practice in a manner understood by the persons skilled in the art. After administration of a nasal formulation according to the invention, the active substance may be absorbed through the nasal mucosa.
Pharmaceutically acceptable excipients may include, antioxidants, buffering agents, preservatives, humectants and perfumes. Examples of antioxidants are ascorbic acid and derivatives thereof, tocopherol and derivatives thereof, butylated hydroxy anisole (BHA), and cysteine. Examples of preservatives are parabens, such as methyl or propyl p- hydroxybenzoate, and benzalkonium chloride. Examples of humectants are glycerin, propylene glycol, sorbitol, and urea. Examples of other excipients are edible oils like almond oil, castor oil, cacao butter, coconut oil, corn oil, cottonseed oil, linseed oil, olive oil, palm oil, peanut oil, poppy seed oil, rapeseed oil, sesame oil, soybean oil, sunflower oil, and tea seed oil; and of polymers such as carmelose, sodium carmelose, hydroxypropylmethylcellulose, hydroxyethyicellylose, hydroxypropyicellulose, chitosane, pectin, xanthan gum, carragenan, locust bean gum, acacia gum, gelatin, and alginates.
Many mucosal formulations need some specialized mixture of excipients. Therefore formulations may comprise one or more surfactants and/or water absorbing polymers and/or substances which inhibit enzymatic degradation and/or alcohols, organic solvents, oils, pH-controlling agents, solubilizers, stabilisers, HLB-controlling agents, viscosity controlling agents, preservatives, osmotic pressure controlling agents, propellants, air displacement, water and mixture thereof. The surfactants may be selected from nonoxynol, octoxynol, tweens, spans sodium lauryl sulfate, sorbitan monopalmitate; water absorbing polymers may be selected from glycofurols and derivatives thereof, polyethylene glycol 200-7500 and derivatives thereof, polyvinylpyrrolidone, polyacrylic acid, propylene glycol, gelatine, cellulose and derivatives thereof, substances which inhibit . enzymatic degradation may be Selected from aprotinin, DFP, carbopol; oils may be selected from vegetable oil, soybean oil, peanut oil, coconut oil, maize oil, olive oil, ) 35 sunflower oil, Miglyols; pH-controlling agents may be selected from acetic acid, hydrochloric acid, nitric acid, potassium metaphosphate, potassium phosphate, sodium acetate, ammonia, sodium carbonate, sodium hydroxide, sodium borate, trolamine;
solubilizers may be selected from alcohol, isopropyl alcohol, water, glycofurol, polyethylene glycol 200-7500; stabilisers such as cyclodextrins; HLB controlling agents may be selected from Tween 20-85, Span 20- 80, Brij 30-98, acacia; viscosity controlling agents may be selected from cellulose and derivatives thereof, Tweens and derivatives thereof, polyethylene glycol and derivatives thereof, cetyl alcohol, glycerine, propylene glycol, sorbitol, gelatin; preservatives may be selected from benzalkonium salt, benzyl alcohol, phenol, thimerosal, phenylmercuric nitrate, phenylethyl alcohol, chiorobutanol, cetylpyridinium chloride; osmotic pressure controlling agents may be selected from dextrose, sodium chloride, mannitol; and propellants may be selected from dichlorodifluoromethane, dichlorotetrafluoroethane, trichloromonofluoromethane and other non-ozone damaging propellants such as butane; air displacement may be nitrogen.
It is essential that the effective amount of the active substance can be administered in an appropriate volume. The volume should not exceed about 300 ul for a human subject when the composition is administered by the nasal route. A larger volume can be disagreeable to the patient and will drain out anteriorly through the nostrils or posteriorly toward the pharynx. The result is that a part of the active substance is lost from the absorption site. The volume is preferably from about 20 pl to about 125 pl and preferably administered into one nostril).
Adjustment and manipulation of established dosage ranges used with desired pharmacological responses, is within the ability of those skilled in the art. The active substances of the present invention are intended for use in the treatment of both immature and adult warm-blooded animals, and, in particular, humans, but also for diagnostic or prophylactic use.
The mucosal absorption enhancing, bioavailability improving and/or bioadhesive agent according to the invention, has a number of important implications. The agent can be used to tailor the absorption of an active substance or drug to achieve optimal concentration overtime, and hence desired physiological response. More specific, variations in the concentrations of the absorption enhancing, bioavailability improving and/or bioadhesive agent even in a low concentration range of 0.01-2% can be used to manipulate the blood . concentration of the drug over time. As a result, effective therapy, diagnosis or prophylactic treatment may be dehieved. Additionally, the use of an absorption enhancing, . 35 bioavailability improving and/or pioadhesive agent of the invention can promote the ability of poorly absorbable substances to be transported across the mucosal membrane. It may also provide for safer drug delivery as the concentration can be controlled to meet the requirement for therapeutically concentration but may still be low enough to minimise the risk of toxic reaction. When the active substance is toxic at the concentration normally required for effective therapy. By reducing the dose, the risk of toxic reaction is reduced.
It may also provide for safer drug delivery. Furthermore, the absorption enhancing, bioavailability improving and/or bioadhesive agent according to the invention can increase the duration of mucosally administered antigens in the vaccinated organism, providing appropriate time for the antigen presenting cells to recognize the antigen. This is due to bioadhesive effect of the agent. As a result, effective vaccination can be achieved with a smaller quantity of antigen than would be normally required. This reduction in the required amount of antigen may lead to more widespread use of vaccines, which are difficult and costly to prepare.
Typically, an effective serum concentration of an active substance is gained over a period of weeks or months. A clinically relevant concentration may be generated with much reduced time course by the mean of this invention. In some instances, it may result in the generation of a successful response in a single dose.
The composition according to the invention is especially suitable for humans, including toddlers, adolescents, teenagers, adults and elderly. The nature of the composition provides the ability to enhance and control the absorption of a variety of active substances and the ability to prolong the duration of residence time of the substance at the administration site, and therefore the formulation may be used for subjects with various conditions such as humans with disease, e.g., splenectomized subjects, subjects with cancer, subjects using anticancer drugs, subjects using antiasthmatic drugs, subjects using anti-inflammatory drugs, subjects with hyper- and hypothyroidea, subjects having problems with malabsorption such as diarrhoea or emesis in addition to humans with nausea or those who have problems swallowing.
The composition according to the invention is also suitable for administration to animals such as horses, sheep, dogs, cats, cows, pigs, goats, rabbits, wild animals and laboratory animals such as mice, rats, guinea pigs, hamsters, rabbits, dogs, cats or monkeys; to birds such as chickens, turkeys; ducks, ostrich, tropical birds or wild birds. For animals, the concentration of each component may need to be adjusted. For example for sheep, the nasal cavity has extremely high humidity, which may require addition of water absorbing excipients to the composition. A person skilled in the art will know how to adjust the composition and the dosage amount in order to achieve a desired effect.
in a specific embodiment, the invention relates to a composition comprising a drug substance for the treatment of migraine, such as the triptans like e.g. sumatriptan; or for the treatment of emesis and nausea, such as ondansetron, or a hormone, such as testosteron.
In a further embodiment, the invention relates to a composition comprising i) from about 0.01% to about 2.5% v/v of a mixture of i i rotten CH, ogo CH, {l
OG on vp. and rom eto vi) . H,C—-0C,Hz]—-oH H,C—-OC Hy ,-OH wherein x is from about 4 to about 20, such as e.g. from about 4 to about 12, or from about 6 to about 8, and y is from 2 to about 30, such as e.g. from 2 to about 10, or from 3 to about 6. ii) a triptan such as, e.g., sumatriptan, iii) optionally, a physiologically acceptable vehicle, and iv) water.
The invention further relates to a method of eliciting a therapeutic, prophylactic and/or diagnostic effect in a mammal, comprising administering to the mammal an effective amount of a composition according to invention. in one embodiment, the invention relates to a method for obtaining a fast onset of a : therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, comprising Rdministering to the mammal an effective amount of a . 30 composition according to the invention, the onset being faster when compared with a similar compasition containing saline instead of component i) and using trax and/or Cray as measures for the onset.
In a second embodiment, the invention relates to a method for improving the bioavailability of a therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, comprising administering to the mammal an effective amount of a composition according to the invention, the bioavailability being improved when compared with a similar composition containing saline instead of component i) and using AUC. ininty 2S a measure.
In a specific embodiment, the administration is nasal administration, and in a further embodiment, the volume to be administered to humans ranges from about 20 to about 300 pl.
Further interesting embodiments appear from the appended claims.
The following Examples are included to illustrate the present invention and are not to be construed to limit the scope of this invention. The contents of all references, patents and published patent applications cited throughout this application are hereby incorporated by reference.
EXAMPLES
Example 1
Preparation of compositions according to the invention and in vivo behaviour in rabbits
Two formulations, A and B, were made. Formulation A contains Sumatriptan, 1% Softigen 767 (PEG-C8/C10-glyceride) in water; and Formulation B contains Sumatriptan in phosphate buffered saline, as Imigran®. These formulations were administered intranasally to rabbits and the sumatriptan serum concentration was determined as a function of time. The results show a significant improvement of Crax, tmax, bioavailability and clinical response when softigen was used over the use of Imigran®. Figure 1 shows the results. Cmax was improved from 40 ng/mi to 600 ng/mi and tna was improved from 30- 45 min and down to 3-5 minutes.
Example 2
Relationship between the concentration of absorption promoting substance and the in vivo behaviour
Four formulations, I, Il and iif, were made. Formulation I contains Sumatriptan, 1%
Softigen 767 (PEG-C8/C10-glyceride) in water; Formulation Il contains Sumatriptan, 0,5%
Softigen 767 (PEG-C8/C10-glyceride) in water; Formulation lif contains Sumatriptan, 0,2% Softigen 767 (PEG-C8/C10-glyceride) in water; and Formulation IV contains
Sumatriptan in phosphate buffered saline, as Imigran®. These formulations were administered intranasally to rabbits and the sumatriptan serum concentration was determined as a function of time. The results show that the time to tx may be controlled with the use of right concentration of Softigen 767. Table 1 shows the results. There was a linear relationship between the concentration of Softigen 767 and time to trax.
TABLE 1
DRUG/Formulation timax
IMIGRAN 31min (n=8) 0.2% SOFTIGEN 12.5 min (n=4) 0.5% SOFTIGEN 8.5 min (n=3) 1.0% SOFTIGEN 4.1min (n=7)
Example 3 :
Demonstration of a significant improved effect when Softigen® is applied as an absorption promoter and a bioadhesive agent according to the invention
In a cross-over study, 4 rabbits received drug A in a formulation containing 1% Softigen® (Sasol GmbH, Germany) (n=4) and 1% Labrasol® (Gattefosse, France) (n=4) and were sampled for blood samples after 0, 2, 5, 10, 15, 30, 45 and 60 min. Comparison of these two formulations showed that Softigen® had AUC = 4.875 and tmax = 6 min whereas
Labrasol® had AUC = 2.552 and tmax was 10 min. See Figure 2.
By the manufacturer Labrasol® is denoted caprylocaproyl macrogolglycerides that are mixtures, mainly of the following compounds i Ii Ii
HG—0-C~F-CHz CH, H,G-0-C—-CHz CH Hg-0-C-{-cr] oH,
X X X
9 9
HC—OH He-0-G--orzf oH, HG—0—C--cHz cry xX X ny
H.C— I
H,C—OH } H,C—OH ) 0-C—{oH; {oH ,
X i | i i nofons]-¢ focus fon o-fonsf-E-focfo-c- fon on : x y | AND x y x !
x = 6 or 8 (capric and caprylic acids), y = 8 on average, free glycerol is less 5%.
Accordingly, Labrasol® is not a composition according to the present invention as it is not included in the definition of compounds of formula
In contrast to Labrasol®, Softigen is a composition according to formula I.
Softigen® is denoted macrogol-6-giycerol-caprylocaprate and is mixtures, mainly of the following compounds: 1 i
HG—0-C—-CH|-Ch HG-0-C~|-CHz CH,
X | 9 X
HG FOC, OH AND HG—0~GC--CH; OH,
H.G— 00,150 HEF oc, Hyon y y x = 6 or 8 (capric and caprylic acids) and the sum of y on each molecule is on average 6.
Softigen consists of octanoic/decanoic macrogol-6 glycerides, which are made by ethoxylation of mono and diglycerides of octanoic and decanoic acids. Labrasol on the other hand is a mixture of macrogol-8 octanoic/decanoic mono or diester and mono-, di- and triesters of glycerol. This composition results from the partial alcoholysis of the corresponding triglycerides using macrogol 400.
In the following table is given a comparison of Softigen® and Labrasol®.
Softigen 767® Labrasol®
Sasol GmbH GATTEFOSSE www.condea.com hitp://www.gattefosse.c
Softigen 767® om ; Labrasol®
Chemical Macrogol-6-glycerol Caprylocaproyi composition caprylocaprate isa macrogol-8 glycerides mixture of mono and is a well defined - diesters, made of mixture of mono-, di- polyoxyethyl glycerol and triglycerides and ethers | mono and di-fatty acid . esters of polyethylene glycol ‘Macrogol-6-glycerol Caprylocaproyi caprylocaprate macrogolglycerides
[0120001443 [01/2002:1184
Average # of | Average number of Eight (8). Applies only ethoxy units ethoxy units per for the mono and di- molecule is six (6). fatty acid esters of ’ polyethylene glycol (PEG 400
Methods of Ethoxylation of mono and | The substance is made ) synthesis di glycerides from capric- | by an and caprylic acid that are alcoholysis/esterificatio synthesized through n reaction using esterification of glycerol | medium chain with destilled coconut or | triglycerides from palm-core fatty acids coconut oil and PEG 400 as starting material. 20°C
HPBvalue [ca 19 [14

Claims (57)

  1. PCT/1S2003/000010 ® 2 CLAMS / : S 1. Use of a compositicn comprising ons or more mono- or diglyceride having the formula (1): HC—O-R2 ~(D : H,C—0O—R3 wherein R1, R2, and R3 are selected from the group consisting of from CB to C28 fatty acids, PEG polymers and hydrogen, | : provided that at least one of R1, R2 and R3 is a C6-C26 fatty acid residue and at least Co one of R1, R2 and R3 is a PEG polymer residue 15, as an absorption enhancing agent for drug substances.
  2. 2. Use of a composition according to claim 1 as a bioavailability improving agent.
  3. 3. Use of a composition according to claim 1 and 2 as a bioadhesive agent.
  4. 4. Use according to any of the preceding claims, wherein the PEG polymer has a molecular weight of from about 200 to about 1200.
  5. 5. Use according to any of the preceding claims, wherein the PEG contains from 2 to about 30 residues of ethylene glycol or derivatives thereof.
  6. 6. Use according to any of the preceding claims, whersin the PEG has from 2 to 20 residues such as, e.g. from 2 to about 15 residues, from 2 to about 10 residues, from 3 to 10 residues, from 2 to about 8 residues or from about 3 to about 6 residues.
  7. 7. Use according to any of the preceding claims, wherein the composition comprises a mixture of mono- and diglycerides. AMENDED SHEET CLEAN COPY :
    PCT/1S2003/000010 ® 27
  8. 8. Use according to any of the preceding claims, wherein the composition comprises a mixture of at least a first and a second glyceride, the first glyceride having one PEG : polymer in pasition R1, R2 or R3, and the second glyceride having two PEG polymers in position R1, R2 and/or R3.
  9. 8. Use according to claim 7 or 8, wherein the v/v-% ratio of monoglycerides to diglycerides is from about 0.1:99.9 to about 99.9:0.1 such as, e.g., from about 1:99 to about 99:1, from about 2.5:97.5 to about 97.5:2.5, and preferably from about 5:85 to about 95:5. :
  10. 10. Use according to any of the preceding claims, wherein the mono- or diglyceride has a structure selected from the group consisting of: H,C—0—R1 HC—0—R2 m H,C—O—PEG H,C—0—R1 HC—O—PEG uy H,C—O—R2 HG —O—PEG HE—O0—R1 Vv) H,C—-0—PEG H,C—O—R1 : ] HE—O—PEG M. : C—0— H,C—O—PEG
  11. 11. Use according to any of the preceding claims, wherein PEG is selected from the group consisting of PEG2, PEG3, PEG4, PEGS, PEGE, PEG7, PEGS. PEG9, PEG10.
    : .
  12. 12. Use according to claim 11, wherein PEG is PEG3 or PEGG. AMENDED SHEET CLEAN COPY
    PCT/1S2003/000010
  13. 13. Use according to any of the preceding claims, wherein at least one of R1, R2, and R3 is selected from saturated C6-26 fatty acids such as, e.g., saturated C68-20, saturated C6-C18, saturated C6-14, saturated C8-12, saturated C8-12 or saturated C8- 10 fatty acids. | :
  14. 14. Use according to claim 13, wherein at least one of R1,R2and R3is a Cs, C8or C10 fatty acid. : 15. Use according to any of the preceding claims, wherein the total concentration of : glycerides in the composition is at least about 80 % w/w such as. e.g., at least about :
  15. 92.5% wiw, at least about 95% w/w, at least about 97.5% wiw, at least about 98% wiw or at least about 99% wiw such as, e.g., front about 5 to about 95% glyceride fatty acid diesters of formula Il and Hl and from about 5 to about 95% glyceride fatty acid monoesters of formula [V and V.
  16. 16. Usa according fo any of the preceding claims, wherein the glyceride has a chiral carbon.
  17. 17. Use according to claim 16, wherein the chiral carbon is S- or R-form.
  18. 18. Usa according to any of the preceding claims, wherein the glyceride has the following structure : Homereseen 1 reson oD H,C—-0C,Hy-OH
  19. 19. Use according io any of the preceding claims, wherein the glyceride has the following structure AMENDED SHEET CLEAN COPY
    PC1/152003/000010 ® 29 f-o-geriron I HpmomGronen (vin) H,C—-0C,Hzf-OH
  20. 20. Use according to claim 18 or 19, wherein the composition contains a mixture of 0 | i Hpmo-C er CH, SE TE pl Ts Es OCH; L0H (iy and IE vin H,C——0C Hz ]—OH H,C—{-0C HOH
  21. 21. Use according to claims 18-20, wherein x is from about 4 to about 20, such as e.g. from about 4 to about 12, or from about 6 to about 8.
    .
  22. 22. Use according to claims 18-21, wherein y is from 2 to about 30, such as e.g. from 2 to about 10, or from 3 to about 8. :
  23. 23. Use according to claims 18-22, wherein x is 6 and/or 8 and y is 3 and/or 6. . . 15
  24. 24. A pharmaceutical composition for nasal administration comprising i) a composition according to any of claims 1-23, ii) a therapeutically, prophylactically and/or diagnostically active substance; and iii) optionally, a physiologically acceptable vehicle.
  25. 25. A pharmaceutical composition according to claim 24 comprising from about 0.005% to about 2.5% vivofa composition according to any of claims 1-23. AMENDED SHEET oo CLEAN COPY
  26. PCT/IS2003/000010 ® 30 : 28. A composition according to claim 24, wherein the concentration of component i)in the composition is at the most 50% v/v such as, e.qg., from about 0.005% to about 50% viv, from about 0.005% to about 40% v/v, from about 0.01% to about 30% v/v, from about 0.01% to about 25% viv, from about 0.01 to about 20% v/v, from about 0.01 to about 15% v/v, from about 0.01 to about 10% v/v.
  27. 27. A composition according to claim 26, wherein the concentration of component i) in the composition is at the most about 10% v/v such as, e.q., at the most about 7.5% viv, at tha most about 5% v/v, at the most 2.5% viv.
  28. 28. A composition according to any of claims 24-27, wherein the concentration of : component i} inthe composition is from-about 0.01% to.about 2% viv. .
  29. 29. A composition according to any of claims 24-28, wherein the-concentration of componenti) is fron about 0.1 to about 1.5% v/v such as from about 0.2% to about 1% viv,
  30. 30. A composition according to any of claims 24-29, wherein tmax - When nasally : administered - takes places relatively fast after administration compared to ty.. obtained after administration of a similar composition containing saline instead of . component i).
  31. 31. A composition according to any of claims 24-30, wherein the bioavailability - when nasally administered - is increased with a factor of at least 2 such as, e.g, atleast 5, at least 10, at least 20, at least 30, at least 40 compared with the bioavailability obtained : after administration of a similar composition containing saline instead of component i). .
  32. 32. A composition according to any of claims 24-31, wherein the active substance ii) is : in a dissolved form. : 33. A composition according to any of claims 24-32, further comprising one or more components selected from the group consisting of: surfactants, water absorbing polymers, substances which inhibit enzymatic degradation, alcohols, organic solvents, oils, pH-controlling agents, solubilizers, stabilizers, HLB-controlling agents, viscosity controlling agents, preservatives, osmotic pressure controlling agents, propellants, air displacemant, water. and mixtures thersof. AMENDED SHEET : CLEAN COPY
  33. PCT/IS2003/000010 ® )
  34. 34.A composition according to any. of claims 24-33, wherein the component i) is used as an absorption enhancing, bioavailability improving and/or bicadhesjve agent, providing a desired tp.
  35. 35. A composition according to any of claims 24-34 for administration of the active - substance ii} to the systemic circulation. ~ 38.
  36. A composition according to arty of claims 24-35, wherein the active substance is a drug substance for the treatment of migraine, such as the triptans ike 2.g. sumatriptan; or for the treatment of ernesis and nausea, such as cndansetron, ora hormone, such as testosteron. :
  37. 37. A composition according to any of claims 24-36 comprising i i) from about 0.01% fo about 2.5% viv of a mixture of oo SER oC ero i toon vp and romero en vin H,G—-0C Hs |-oH H,C—-0C HOH wherein x and y are as defined in claims 21-23, oo ii) a triptan such as, e.g., sumatriptan, : fii) optionally, a physiologically acceptable vehicle, and : iv) water. .
  38. 38. A method of eliciting a prophylactic effect in a mammal, comprising administering to the mammal an effective amount of a composition according to "any of claims 24-37. oo Co AMENDED SHEET
    PCT/1S2003/000010 ® *
  39. 39. A method for obtaining a fast onset of a prophylactic effect of an active substance in a mammal including a human, comprising administering to the mammal an effective amount of a composition according to any of claims 24-37, the onset being faster when compared with a similar composition containing saline instead of component i} and using t,, and/or C_,, as measures for the onset.
  40. 40. A method for improving the bioavailability of a prophylactic effect of an active substance in a mammal including a human, comprising administering to the mammal an effective amount of a composition according to any of claims 24-37, the bioavailability being improved when compared with a similar composition containing saline instead of component i) and using AUC; .,y 85 a measure.
  41. 41. A method according to any of claims 38-40, wherein the administration is nasal administration.
  42. 42. A method according to any of claims 38-41, wherein the volume to be administered to humans ranges from about 20 to about 300 uL.
  43. 43. Use of a composition according to any of claims 24-37 in the manufacture of a preparation for eliciting a therapeutic, prophylactic and/or diagnostic effect in a mammal.
  44. 44. Use of a composition according to any of claims 24-37 in the manufacture of a preparation for obtaining a fast onset of a therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, the onset being faster when compared with a similar composition containing saline instead of component i) and using t,,,, and/or C,., as measures for the onset.
  45. 45. Use of a composition according to any of claims 24-37 in the manufacture of a preparation for improving the bioavailibility of a therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, the bioavailability being improved when compared with a similar composition containing saline instead of component i} and using AUC, ., @s a measure. - AMENDED SHEET
    PCT/iIS2003/000010
  46. 46. Use according to any of claims 43-45, wherein said preparation is suitable for nasal administration.
  47. 47. Use according to any of claims 43-46, wherein said preparation is administrable to humans in a range of volumes from about 20 to about 300 yl.
  48. 48. A substance or composition for use in a method of eliciting a therapeutic, prophylactic and/or diagnostic effect in a mammal, said substance or composition comprising a composition according to any of claims 24-37, and said method comprising administering an effective amount of said substance or composition to the mammal. :
  49. 49. A substance or composition for use in a method for obtaining a fast onset of a therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, the onset being faster when compared with a similar composition containing saline instead of component i) and using t,,, and/or C_,, as measures for the onset, said substance or composition comprising a composition according to any of claims 24-37, and said method comprising administering an effective amount of said substance or composition to the mammal.
  50. 50. A substance or composition for use in a method for improving the bioavailability of a therapeutic, prophylactic and/or diagnostic effect of an active substance in a mammal including a human, the bioavailability being improved when compared with a similar composition containing saline instead of component i) and using AUC, xinity as a measure, said substance or composition comprising a composition according to any of claims 24-37, and said method comprising administering an effective amount of said substance or composition to the mammal.
  51. 51. A substance or composition for use in a method of treatment or prevention according to any of claims 48-50, wherein the administration is nasal administration.
  52. 52. A substance or composition for use in a method of treatment or prevention according to any of claims 48-51, wherein the volume to be administered to humans ranges from about 20 to about 300 uL. AMENDED SHEET
    PCT/1IS2003/000010
  53. 53. Use according to ary one of claims 1, or 43 to 45, substantially as herein described and illustrated.
  54. 54. A composition according to claim 24, substantially as herein described and illustrated.
  55. 55. A method according to any one of claims 38 to 40, substantially as herein described and illustrated.
  56. 56. A substance or composition for use in a method of treatment or prevention according to any one of claims 48 to 50, substantially as herein described and illustrated.
  57. 57. A new use of a composition according to claim 1, a new use of a composition according to any one of claims 24 to 37, a new composition, a new non-therapeutic method of treatment, or a substance or composition for a new use in a method of treatment or prevention, substantially as herein described. AMENDED SHEET
ZA200406731A 2002-02-25 2004-08-24 Absorption enhancing agent. ZA200406731B (en)

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
IS6283 2002-02-25

Publications (1)

Publication Number Publication Date
ZA200406731B true ZA200406731B (en) 2005-10-11

Family

ID=35986277

Family Applications (1)

Application Number Title Priority Date Filing Date
ZA200406731A ZA200406731B (en) 2002-02-25 2004-08-24 Absorption enhancing agent.

Country Status (1)

Country Link
ZA (1) ZA200406731B (en)

Similar Documents

Publication Publication Date Title
US6855332B2 (en) Absorption promoting agent
JP5551540B2 (en) Stabilized reverse micelle composition and use thereof
JP4592250B2 (en) Novel pharmaceutical composition for administering N-0923
CN1202863C (en) Antigen delivery system comprising monoglyceride or diglyceride derivatives as adjuvant
US20240050535A1 (en) Topical therapeutic formulations
US7820722B2 (en) Permeation enhancers
JPH09508614A (en) Pharmaceutical preparation for topical transmucosal administration of antigens and / or vaccines to mammals
CN1515245A (en) Vaccine containing saponin and sterol
AU2003215885B2 (en) Absorption enhancing agent
ES2611995T3 (en) Methods and compositions for the delivery of a therapeutic agent
US20030018085A1 (en) Isostearic acid salts as permeation enhancers
CN111195230B (en) Method for preparing flexible liposome
CN104797252A (en) Skin wound healing and scar reduction with prostaglandin ep4 agonist combinations
CN1688296A (en) Injectable 2, 6-diisopropylphenol-containing anesthetic composition and methods
Nagai et al. Bioadhesive dosage forms for buccal/gingival administration
WO2003047494A2 (en) Reverse micelle compositions and uses thereof
CN109496152B (en) Intramuscular inventory of decoquinate compositions and methods for their prevention and treatment
ZA200406731B (en) Absorption enhancing agent.
JP2810730B2 (en) Motilin preparation
WO2002009670A1 (en) Liquid or semi-solid pharmaceutical excipient and pharmaceutical composition comprising the same