CN101057973A - Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof - Google Patents

Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof Download PDF

Info

Publication number
CN101057973A
CN101057973A CNA2006101453767A CN200610145376A CN101057973A CN 101057973 A CN101057973 A CN 101057973A CN A2006101453767 A CNA2006101453767 A CN A2006101453767A CN 200610145376 A CN200610145376 A CN 200610145376A CN 101057973 A CN101057973 A CN 101057973A
Authority
CN
China
Prior art keywords
effective dose
composition
inflammation
patient body
compositions
Prior art date
Legal status (The legal status 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 status listed.)
Pending
Application number
CNA2006101453767A
Other languages
Chinese (zh)
Inventor
罗伯特·菲什曼
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
All Natural FMG Inc
Original Assignee
All Natural FMG Inc
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
Priority claimed from US11/407,387 external-priority patent/US7291591B2/en
Application filed by All Natural FMG Inc filed Critical All Natural FMG Inc
Publication of CN101057973A publication Critical patent/CN101057973A/en
Pending legal-status Critical Current

Links

Abstract

The invention relates to a transdermal drug delivery system composition containing a water-based excipient, including emu oil, at least one fatty acid alkyl ester, polyethylene glycol, at least one gelating agent/emulsifier and at least one analgesic ingredient, such as ibuprofen, and the invention further relates to a preparation and an application method.

Description

The transdermal analgesic compositions and the methods for making and using same thereof that do not have alcohol
The cross reference of related application
The application is the partial continuous application of U.S. Patent application 10/412,626 co-pending when submitting on April 11st, 2003, and its content is hereby incorporated by.
Technical field
The present invention relates to be used for percutaneous dosing with the bonded analgesic composition of percutaneous drug delivery system that does not have alcohol with and methods for making and using same.
Background technology
Disease treatment often need be taken in a large amount of drug components.Especially, to there being the active component of certain level in the treatment of pain requirement blood samples of patients, its concentration is enough to keep pain relieving or antiinflammatory effect.In order to realize this point, the patient must take in a large amount of tablets, capsule or analog every day for several times.This therapy usually is difficult to keep, and is because active component, relevant with gastrointestinal stimulation as aspirin and triethanolamine Salicylate or NSAIDs such as ibuprofen (ibuprofen), naproxen (naprosyn) etc.The stimulation of even now may only cause chronic indigestion, and in some cases, stimulation can promptly cause spontaneous gastrorrhagia, and this may bring life danger.
Another problem relevant with oral drug therapy is must possess significant concentration level in order effectively to treat the periphery of pain or inflammation in the blood.These levels often such as the fruit medicine more accurately during the specific site of targeting pain or wound necessary level much higher.Therefore needing can the tip administration and can local ease the pain and the transdermal analgesic prescription of inflammation.
Prior art
United States Patent (USP) 6,416,772 have instructed the local skin anaesthetic composition that eases the pain, and said composition contains the alcohol of about 57-91wt%; The glycerol of about 1-12wt%; The analgesic of about 2-28wt%, this analgesic comprises salicylic derivant; The dimethyl sulfone of about 0.02-5wt%; And Dromaius novaehollandiae (Emu) oil of about 0.01-3wt%.This component produces percutaneous pain when analgesic is applied directly to afflicted areas.
Alcohol, preferred alcohol or isopropyl alcohol according to announcement, are effectively to dissolve analgesic that it can be absorbed by skin is necessary.Secondly, need the stabilizing agent of glycerol, thus the sale effect duration that alcohol can the appreciable impact component as aspirin, triethanolamine Salicylate or other analgesic.It is essential that glycerol also is considered to abundant dispersion analgesic, so needn't rock or stir component before use the part.Introduce dimethyl sulfone and fat of Oromaius norvaehollandeae and be considered to help to quicken the absorption of skin component, and because the feature that eases the pain of itself, they make analgesic more effective, have improved the effect of component.
The compositions that this patent can effectively ease the pain when instruction is not used for the regional tip of various trigger point, uncomfortable real sensation.In addition, ' 772 patent need be used alcohol when percutaneous dosing, and alcohol causes the degraded of analgesic, needs glycerol to stop the alcohol degraded as stabilizing agent thus.
United States Patent (USP) 6,346,278 have instructed lipid-soluble extract with blue or green limit mussel (Perna canaliculus) or Mytilus edulis (Mytilus edulis) as the active component in the compositions that is applicable to percutaneous dosing, said composition comprises ointment or lotion base material or excipient, can comprise that skin penetration enhancer is to assist the administration of active component.Suitable base material or excipient are oil, as olive oil or fat of Oromaius norvaehollandeae, and can be separately or with penetrating agent such as eucalyptole or limonene administration.
United States Patent (USP) 6,444,234 have instructed a kind of pharmaceutical composition that contains alcohol, carry out the percutaneous dosing of medicine or other active agent by the topical to the skin of people or other animal.The method of preparing these components is based on transdermal delivery system (TDS), this system's Chinese medicine modified and specific solvent and solvent and solute dressing agent and skin combination of stabilizers formation mixture true solution, this method makes medicine by fast Absorption, shift and, simultaneously skin irritation and/or immunoreation are minimized by skin arrival fatty tissue or vascular system.Analgesic such as ibuprofen and analog thereof, MSM and fat of Oromaius norvaehollandeae are considered to and can be used in combination with transdermal delivery system.
United States Patent (USP) 6,528,040 has instructed the prescription based on fat of Oromaius norvaehollandeae as analgesic, anesthetis and pruritus.Prescription contains 0.01 to 13wt% Arrcostab; And 20 to 70wt% fat of Oromaius norvaehollandeae; 10 to 33wt% benzyl alcohol; 10 to 33% Benzoinum; 0.2 allantoin to 2wt%; 0.25 to the nipagin of 1.25wt% and 0.01 to 0.30wt% propyl parabene.This prescription can be made into spraying or percutaneous prescription, can be used to treat chronic skin ulcer and burn wound.
United States Patent (USP) 5,885,597 have instructed a kind of local prescription that is used to alleviate the patient suffering, and this prescription basic composition is the combination of at least a corticoid class analgesic of effective dose, at least a aromatic acid class analgesic and at least a para-aminobenzoic acid ester type local anesthetic; With the capsaicin compositions of the raising pain relief effect of effective dose, and at least a phospholipid of its skin turn-over capacity of the raising of effective dose and at least a polyoxyethylene polyoxypropylene copolymer.
U.S. Patent application 20030031724 has been instructed from Dromaius novaehollandiae, the cost-effective component that Dromiceiusnovaehollandiae derives or prepares, and this component can be used as the intravital antiinflammatory of patient.This application is not imagined MSM or analgesic in the percutaneous dosing environmental applications.
U.S. Patent application 20010033838 has been instructed fat of Oromaius norvaehollandeae and various fraction thereof the carrier as antifungal, antibacterium and antiviral drugs and preparation.This application has instructed being used in combination of MSM and fat of Oromaius norvaehollandeae, but when the needs percutaneous dosing, fat of Oromaius norvaehollandeae is substituted by liposome component or oiliness percutaneous composition.
Summary of the invention
Research has shown when NSAIDs and nutrient during by orally ingestible, has had only 5% arrival to need their areas of inflammation.This is to wherein much resetting and abandoning because of stomach, liver and digestive system.
The invention discloses a kind of percutaneous drug delivery set of systems compound that comprises water base excipient, comprise at least a fatty acid alkyl esters, Polyethylene Glycol-8 (PEG-8), fat of Oromaius norvaehollandeae and gellant with 13 to 30 six carbon atoms.
The example of suitable fatty acid alkyl esters comprises, but be not limited to methyl laurate, methyl myristate, methyl hexadecanoate, methyl stearate, methyl behenate, ethyl oleate, Ethyl linoleate, butyl oleate, butyl stearate, isopropyl myristate, isopropyl palmitate, dodecyl acetate, sad tetradecane ester, cetyl palmitate and stearic stearolactone.
Above-mentioned fatty acid alkyl esters promotes chemical combination and can add in the prescription that its amount is the about 31.0wt% of about 0.001-of compositions, preferably approximately 3wt%.
Can be used for suitable gelling/emulsifying agent of the present invention and comprise guar gum, xanthan gum, carrageenan (carrageenan), cellulose, hydroxy alkyl cellulose, carboxycellulose sodium, SEPIGEL 305, gelatin, agar, starch or analog.SEPIGEL 305 is trade marks, and (Fairfield NJ) makes by Seppic company.SEPIGEL 305 is a kind of gelling/emulsifying agents, comprises about 40% polyacrylamide, about 15% C 13-C 14Isoparaffin and about 5% laureth-7 and suitable quantity of water.
Add gelling/emulsifying agent reaching required viscosity in this prescription, its amount can be about 0.001 to about 31.0wt%, preferably approximately 3wt%.
The preferred Polyethylene Glycol that uses among the present invention is that (trade mark PROTACHEM400 is by Protameen Chemical, Inc. for PEG-8, Totawa, NJ makes), its addition in this prescription be compositions about 0.001 to approximately to about 31.0wt%, preferably approximately 3wt%.In this prescription, add fat of Oromaius norvaehollandeae and promote the absorption of said composition in skin.Fat of Oromaius norvaehollandeae the amount in the present invention prescription of can adding is about 0.001 to about 31.0wt%.
In a preferred implementation, the present invention openly comprises the percutaneous drug delivery set of systems compound of water base excipient, comprise fat of Oromaius norvaehollandeae (U.S.), isopropyl palmitate (trade mark PROTACHEMIPP, by Protameen Chemical, Inc., Totawa, NJ makes), PEG-8, dimethyl sulfone (MSM) and SEPIGEL 305 (by the sale of Seppic company).
In this water base excipient, add analgesic, be example with the ibuprofen but be not limited thereto.
According to the present invention, analgesic composition should be understood that to comprise any can minimizing or the pharmaceutical composition of prevent irritation, inflammation etc.These compositionss include but not limited to gentle analgesic such as aspirin and acetaminophen, and NSAIDS (non-steroid anti-inflammation drugs) is as indometacin (Indomethacin), ibuprofen, naproxen, fenoprofen (Fenoprofen), tolmetin (Tolmetin), sulindac (Sulindac), meclofenamic acid (Meclofenamate), ketoprofen (Ketoprofen), Luo Xika (Proxicam), flurbiprofen (Flurbiprofen) and diclofenac (Diclofenac) and various DMARDS (amelioration of disease antirheumatic) are as corticosteroid, methotrexate and analog.
In addition, percutaneous drug delivery of the present invention system can add any can minimizing or the allopathy of prevent irritation, inflammation etc. with chemical compound or medical herbs chemical compound.Specifically, all percutaneous dosings less than the chemical compound of insulin molecule size can be used for compositions of the present invention.In addition, all nanotechnology products well known in the prior art can join in the present composition and not deviate from the scope of the invention.
Opposite with the agent of use oral pain alleviating, local cream of the present invention has some benefits.
These benefits comprise:
1) uses the more active component of a small amount of;
2) avoid liver metabolism;
3) avoid the degraded of active component in gastrointestinal tract;
4) avoid gastrointestinal is stimulated.
Percutaneous drug delivery system in this explanation does not contain alcohol, does not therefore have the problem of the effect duration shortening relevant with the prior art formula that contains alcohol.Because do not use alcohol, the existence of glycerol is optional equally.Therefore, provide a kind of percutaneous drug delivery system of no alcohol of uniqueness, this system has improved the penetration to skin, become thus replace capsule and tablet safer, effect rapidly and the method that is easy to realize.
In the various experiments of between prior art formula and the present invention's prescription, carrying out, have been found that current disclosed prescription needn't directly be used in the pain perception source.Correspondingly, compositions can be applied to various trigger point, pain perception point tip still will be realized alleviating of pain.
Trigger point be intramuscular stress over-drastic fibre bundle, they since the injured tuberosity and do not have elasticity of becoming can not shrink or unfold.Trigger point has multiple inducement, as overuse, injured, disease or or even daily pressure.Intramuscular trigger point shortens and tension muscle, stretch tendon and ligament and reduce intramuscular blood circulation singularly.When muscle was strained, muscle lacked oxygen, and human body discharges the chemical compound that triggers pain.Thus, the present inventor has been found that the percutaneous drug delivery system that will comprise the local analgesia agent is used for these trigger point and will reduces or remove pain in the relevant range of health.
Therefore, the purpose of this invention is to provide not containing of a kind of percutaneous dosing that is used for analgesic composition of fast skin drug-supplying system alcohol, cream, said composition can effectively be treated arthralgia and stiff.
Another object of the present invention provides analgesic composition, and when being applied to the terminal in uncomfortable impression source, said composition can systematicness ease the pain and/or the discomfort of inflammation.
Another purpose of the present invention provides a kind of method for preparing the percutaneous drug delivery system.
A further object of the present invention provides the prescription that is used for skin that a kind of effective minimizing prostaglandin produces.
In conjunction with appended accompanying drawing, by illustration of the present invention and embodiment, specific implementations, other purpose of the present invention and benefit are conspicuous according to following explanation.
The specific embodiment
The percutaneous drug delivery system that can improve dermal osmosis power in order to simplify the operation is necessary to understand the parameter that influences this phenomenon.
Influence the various factors of dermal osmosis power:
1) oil-soluble (J Pharm Sci " Linear relationships between lipophiliccharacter and biological activity of drugs. " 1972 Jan; 61 (1): 1-19) oil-soluble of material (lipotropy) is good more, and dermal osmosis power is strong more;
2) molecular weight (molecule is more little, easy more infiltration);
3) penetration of cream, gel and liquid is better than solid;
4) penetration enhancers improves local absorption (Targeted drug delivery tothe skin and deeper tissues:role of physiology, the solute structure and disease of lipophilic substance; Clin Exp Pharmacol Physiol 1997 Nov; 24 (11): 874-9).
Embodiment 1
This paper provides indefiniteness explanation embodiment; Following just embodiment and can not independently represent notion of the present invention disclosed herein.
According to preferred implementation of the present invention, the batching of excipient base material has following composition:
Component Amount (wt%)
U.S. fat of Oromaius norvaehollandeae isopropyl palmitate PEG-8 SEPIGEL 305 dimethyl sulfone water (deionized water) ~3% ~3% ~4% ~3% *~0.75% surplus
( *Gelling if desired additionally increases by 1%)
Preparation steps:
At least a active component such as ibuprofen are added in the above-mentioned excipient.In this embodiment, expection adds about 10% active component.
1, active component is weighed, and uses mortar that it is fully mixed;
2, measure U.S.'s fat of Oromaius norvaehollandeae of 3%, add high-speed mixing device;
3, active component is added fat of Oromaius norvaehollandeae.Mixing enters oil until all powder.Mixture will be very dry;
4, measure isopropyl palmitate and PEG-8, add the fat of Oromaius norvaehollandeae mixture;
5, mix half an hour;
6, add sterilized water, mixed 5 minutes, scraping mixes vessel wall once in a while;
7, the SEPICEL 305 of adding 3% mixes 5 minutes (if the denseness of also not realizing ideal, the SEPIGEL 305 of increase by 1% is until obtaining ideal denseness).
All patents and the publication mentioned in this description have illustrative for those skilled in the art in the invention.Quoted by reference with same degree in these all patents and publication, illustrated by reference respectively specially as each publication and quote.
Illustrated that particular form of the present invention, the present invention are not limited in the particular form of this description and demonstration or the arrangement of each several part although be understood that.In the case without departing from the scope of the present invention, it is apparent to one skilled in the art to carry out various modifications, and should not think that the present invention is subjected in the description showing and the restriction of the content of explanation.
One of ordinary skill in the art will readily recognize that the present invention is very suitable for realizing goal of the invention, obtain to mention and itself inherent result and benefit.Any chemical compound, method, step and technology in this explanation are the representatives of current preferred specific embodiments, be intended to the explanation and scope is not limited.That those skilled in the art will carry out that spirit of the present invention comprised and by variation and other application of the scope definition of claims.Although the present invention is illustrated in conjunction with specific preferred specific embodiments, be understood that the present invention who declares should not be subjected to the improper restriction of these specific specific embodiments.In fact, conspicuous to those skilled in the art should be within the scope of the appended claims to carrying out various modifications that described pattern of the present invention carries out.

Claims (10)

  1. One kind reduce and/or prevention patient body in the analgesic composition of no alcohol of inflammation, comprising:
    The gellant of at least a fatty acid alkyl esters of the fat of Oromaius norvaehollandeae of effective dose, effective dose, the Polyethylene Glycol of effective dose, gelling effective dose, the pain relieving composition of effective dose and the sterilized water of enough supplying 100%.
  2. 2. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body, wherein said fatty acid alkyl esters comprises that at least one is selected from the composition in methyl laurate, methyl myristate, methyl hexadecanoate, methyl stearate, methyl behenate, ethyl oleate, Ethyl linoleate, butyl oleate, butyl stearate, isopropyl myristate, isopropyl palmitate, dodecyl acetate, sad tetradecane ester, cetyl palmitate and the stearic stearolactone.
  3. 3. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body, wherein said pain relieving composition comprises that at least one is selected from the composition of aspirin and acetaminophen, indometacin, ibuprofen, naproxen, fenoprofen, tolmetin, sulindac, meclofenamic acid, ketoprofen, a Luo Xika, flurbiprofen, diclofenac, corticosteroid and methotrexate.
  4. 4. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body, wherein said gellant comprises that at least one is selected from the composition of guar gum, xanthan gum, carrageenan, cellulose, hydroxy alkyl cellulose, carboxycellulose sodium, SEPIGEL 305, gelatin, agar, starch or analog.
  5. 5. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body, wherein said Polyethylene Glycol is a Polyethylene Glycol-8.
  6. 6. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body also comprises the dimethyl sulfone of effective dose.
  7. 7. the compositions of inflammation in minimizing as claimed in claim 1 and/or the prevention patient body also comprises at least a composition that is selected from allopathy with chemical compound, medical herbs chemical compound or nanotechnology product of effective dose.
  8. One kind reduce and/or prevention patient body in the method for inflammation and pain, comprising:
    The position of pain and/or inflammation in the identification patient body;
    Discern the trigger point relevant with described position; And
    With analgesic composition at least one place of described position or described trigger point percutaneous dosing, described compositions basic composition is the fat of Oromaius norvaehollandeae of effective dose, at least a fatty acid alkyl esters of effective dose, the Polyethylene Glycol of effective dose, the dimethyl sulfone of effective dose, the gellant of gelling effective dose, the pain relieving composition of effective dose, and the sterilized water of enough supplying 100%;
    The treatment that realizes described pain and/or inflammation is thus alleviated.
  9. 9, a kind of preparation is effective to the method for analgesic composition of the no alcohol of percutaneous dosing, comprising:
    The described analgesic composition of effective dose is provided;
    The fat of Oromaius norvaehollandeae of effective dose is provided in high-speed mixing device;
    Described analgesic composition is added the component of also mixing in the described fat of Oromaius norvaehollandeae until the formation mix homogeneously;
    In described homogeneous mixture, add the Polyethylene Glycol of the fatty acid alkyl esters of effective dose and effective dose and mix the sufficiently long time;
    Add sterilized water and be mixed to even;
    At least a gellant that adds effective dose is mixed to evenly and is gel-like consistency; With
    If desired, add extra gellant, until the gel consistency of realizing ideal.
  10. 10. by the product of the described method of claim 9 preparation.
CNA2006101453767A 2006-04-18 2006-11-24 Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof Pending CN101057973A (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US11/407,387 2006-04-18
US11/407,387 US7291591B2 (en) 2003-04-11 2006-04-18 Alcohol-free transdermal insulin composition

Publications (1)

Publication Number Publication Date
CN101057973A true CN101057973A (en) 2007-10-24

Family

ID=38864376

Family Applications (1)

Application Number Title Priority Date Filing Date
CNA2006101453767A Pending CN101057973A (en) 2006-04-18 2006-11-24 Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof

Country Status (1)

Country Link
CN (1) CN101057973A (en)

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101977598B (en) * 2008-03-25 2012-07-18 帝国制药株式会社 Water-based adhesive skin patch comprising ketoprofen lysine salt
CN103356700A (en) * 2012-03-26 2013-10-23 朱晓明 Joint maintaining ointment

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101977598B (en) * 2008-03-25 2012-07-18 帝国制药株式会社 Water-based adhesive skin patch comprising ketoprofen lysine salt
CN103356700A (en) * 2012-03-26 2013-10-23 朱晓明 Joint maintaining ointment
CN103356700B (en) * 2012-03-26 2014-10-29 朱晓明 Joint maintaining ointment

Similar Documents

Publication Publication Date Title
US7052715B2 (en) Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof
RU2467759C2 (en) Composition for local use and its applications
CN103948927B (en) The topical vasoconstrictor preparations and method of cell are protected in cancer chemotherapy and radiotherapy
EP1248613B1 (en) Clonidine preparations
ES2318233T3 (en) IMPROVEMENT SYSTEMS OF PENETRATION AND IRRITATION REDUCERS THAT INCLUDE TESTOSTERONE.
EP1425381B1 (en) Emu-based formulations for wound treatment related application information
EP2373346B1 (en) Ibuprofen for topical administration
US7033998B2 (en) Alcohol-free transdermal insulin composition and processes for manufacture and use thereof
CN101790370A (en) A novel non-aqueous topical solution of diclofenac and process for preparing the same
JP2003171301A (en) Andrographis paniculata gel as adjunct in treatment of periodontitis
EP2588100A1 (en) Topical pharmaceutical composition comprising flurbiprofen
US20090082738A1 (en) Natural Anti-Inflammatory Agents for Reducing Pain
US20130209585A1 (en) Topical NMDA Antagonist Formulations for the Treatment of Peripheral Neuropathy
US7291591B2 (en) Alcohol-free transdermal insulin composition
CN1141929C (en) Medicament and method of treating an organism with medicaments
CN101057973A (en) Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof
WO2014176417A1 (en) Topical preparation for bypassing gi tract, delivery of therapeutics, and trans-epithelial drug delivery system
US20040121023A1 (en) Composition to alleviate pain and topical method of applying same
CN101036660A (en) Estrogen gelatin medicine and the method for preparing the same
US6663874B2 (en) Composition to alleviate pain and topical method of applying same
RU2381810C1 (en) Wound healing gel balm
CN101057972A (en) Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof
US20060263439A1 (en) Alcohol-free transdermal analgesic composition and processes for manufacture and use thereof
CN108785398A (en) A kind of analgesia compound oil and the preparation method and application thereof containing peony seed oil
KR100347883B1 (en) New pharmaceutical composition of gel preparation containing local anaesthetic agents

Legal Events

Date Code Title Description
C06 Publication
PB01 Publication
C02 Deemed withdrawal of patent application after publication (patent law 2001)
WD01 Invention patent application deemed withdrawn after publication