IE83435B1 - Method for the prevention of intrinsically aged skin with retinoids - Google Patents
Method for the prevention of intrinsically aged skin with retinoidsInfo
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- IE83435B1 IE83435B1 IE1990/0202A IE20290A IE83435B1 IE 83435 B1 IE83435 B1 IE 83435B1 IE 1990/0202 A IE1990/0202 A IE 1990/0202A IE 20290 A IE20290 A IE 20290A IE 83435 B1 IE83435 B1 IE 83435B1
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- retinoid
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- mice
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- symptoms
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Description
PATENTS ACT , 1992 202/90 METHOD FOR THE PREVENTION OF INTRINSICALLY AGED SKIN WITH RETINOIDS ORTHO PHARMACEUTICAL CORPORATION METHOD FOR THE TREATMENT OR PREVENTION OF INTRINSICALLY AGED SKIN WITH RETINOIDS The present invention relates to a method for the prevention of intrinsically (chronologically) aged skin by the topical administration of retinoids.
Cutaneous aging results from two distinct and independent processes: intrinsic aging and photoaging. Although the skin changes that occur in intrinsic aging may involve genetically programmed senescence mediated perhaps by as yet unidentified endogenous factors, an understanding of the clinical alterations as well as changes in the extracellular matrix and molecular biology is beginning to emerge. Clinically, intrinsic aging is characterized by having a thin, atrophic dermis, reduction in subcutaneous adipose tissue and by the presence of fine wrinkling. In addition, there appears an unblemished surface with some deepening of skin surface markings and some histopathologic and ultrastructural alterations as well. Compared to young skin, intrinsically aged skin manifests its most pronounced changes in the dermis.
The major changes in the elastic tissue include an increase in the number as well as thickness of fibers, loss of vertical fibers that insert into the basement membrane, and the presence of large irregular fibroblasts containing extensive rough endoplasmic reticulum, characteristic of elastogenesis.
Conversly, photodamaged skin is characterized by coarse wrinkling and furrowing and the skin appears loose, thickened and leathery. Photodamaged skin represents a state of mild chronic inflammation. Histologically, in photodamaged skin, there is excessive accumulation of elastotic material in the upper dermis, basophilic degeneration and homogenization of the collagen fibers accompanying the accumulation of glycosaminoglycan-proteoglycan complexes. Also, there appears to be a loss of collagen bundles. Biochemically, there is a decrease in mature (insoluble) collagen with a concomitant increase in soluble collagen. Mature collagen may be degraded by the chronic inflammatory infiltrate produced by ultraviolet—B irradiation. However, in intrinsically aged skin, mature collagen is more stable and resistant to enzymatic degradation, the bundles become larger forming disoriented rope—like structures. Also, there is marked thickening or acanthosis in the epidermis as well as the dermis and sebaceous glands become greatly enlarged. Electronmicroscopic studies reveal that early changes in photodamaged skin consist of an increase and enlargement of the microfibrillar component of the elastic fibers. In more advanced stages, the elastic fibers are highly disorganized.
Concerning microcirculation, there is a loss of vascular area in both intrinsic and photoaged skin, with distinct differences between the two. Intrinsically-aged skin experiences a uniform reduction in the vasculature with a progressive thinning of the vessel wall. The vessels are not dilated or deranged and have an undisturbed superficial plexus. In photoaged skin, the vasculature is almost totally missing in some areas of the dermis with the horizontal superficial plexus almost completely destroyed, while in other areas the vessels become dilated and tortuous and are seen on the surface of the skin as telangiectasias. In early photodamage, the vessel wall actually thickens and then progressively thins.
Thus, aging and photoaging. there are distinct differences between intrinsic Kligman, A.M. et al., "Cutaneous Aging: The Differences Between Intrinsic Aging and Photoaging", Journal of Cutaneous Aging and Cosmetic —l2 (1988). These differences are summarized in Table 1.
Dermatology, Vol. 1, No. 1, pp.
Tretinoin, all trans retinoic acid, has been described _3a_. mcmohamompoum .m©m umC©o>HmocHEmmOo>Hm \mw oapmuomamcmamu Ucm Hmeuocnm \mmoa ummmw wcom NCQHU £#H3 mamoummaw HQHOW ®HQHUHH%CH %HOH@EE®H%Cfl Uwxflg ~U®mm®MUCH %HU®MH@E maamo ummz m>auomHmQ>s \U®mm®HUQH mpmmanongam mflmoummam .Um:wxoHnB U®m®®HUCH >HU®MH®2 mumflflw Ucm mwavcsn mo mmmwwomb Umxumz mwmE WDOQQHOEQ OMCH mwummmcwmwb .®mm®HoqH mSOUC®E®HH mHQ>pm umasaamo \mHmo£ucmom Umxwmz >uHoflumma® mo mmoa ucmoflwacmflm mmaxcamz mama m:H3oaa®> \m®£ouoaQ £#H3 womwuzm %H®QU©®H \HmHSUOZ mmoa wummwfioz wcom NCGHU oz COHMEEEQHMCH oc \Ummmmuo®U maamo ummz ®>HuowcH \UwmmwuowU WHWMHQOHQHM Hmcsane UQWMGHUQU husaaam uwucoflgomflv .xoHgu mmawcsm HGEMOE UWOEHM usfl \U®WM®HOCH mHnmH> Ucm cfige xpaoflummam wo mmoa mEom mmcaxumfi womwnsm caxm wo mcacmmmmv mfiom momwuzm U®£mHE®HQC3 ~£HOOEm ®H3u®HSUm®>OHOHE mflEH®U xwmaaflamm mHEH®U Hmasoaumm mmwm ‘memo cmomaaoo msmmwu oaummam WHEHGUHQM wocmnmmmam Hmoacaao mfiammouonm m:fim¢ UflmfiflHuGH H mqm¢a ®H5Um0h as being effective in the treatment of photoaged skin (Weiss, J. J. et al., "Topical Tretinoin Improves Photoaged Skin," Journal of the American Medical Association, Vol. 259, No. 4, pp. 527-532, (1988).
Little is known, however, of the effectiveness of retinoids in the treatment or prevention of intrinsically aged skin.
Vitamin—A acid has been suggested as being useful in the treatment of wrinkles, sun damaged and sagging skin (WO 86/06275; Saline, C., "Adventures in the Skin Trade." Philadelphia Magazine, pp. 120-133 (1980)). However, no method is described for the prevention of the symptoms of intrinsically aged skin by the topical administration prior to the appearance of said symptoms of an effective amount of a retinoid in a pharmaceutically acceptable carrier.
The use of retinoids in the treatment of photoaged skin is also disclosed in EP—A—0229561, EP—A—O274104 and GB—A—1466062.
Summary of the Invention The present invention is directed to a method for the prevention of the symptoms of intrinsically (chronologically) aged skin by the topical administration prior to the appearance of said symptoms of an effective amount of a retinoid in a pharmaceutically acceptable carrier. The retinoids employed may be any natural and/or synthetic compound which possesses the biological activity of vitamin A.
Detailed Description of the Invention The invention relates to the use of retinoids for the prevention of the symptoms of intrinsically (chronologically) aged skin.
Retinoids have been defined narrowly as comprising simply (retinol) and its derivatives, vitamin A such as vitamin A aldehyde (retinal) and vitamin A acid (retinoic acid), which comprise so- called natural retinoids. However, subsequent research has resulted in a much larger class of chemical compounds that are deemed retinoids due to their biological similarity to vitamin A and its derivatives. Compounds useful in the present invention include all natural and/or synthetic analogs of vitamin A. or retinol-like compounds which possess the biological activity of vitamin A in the skin. These include: regulation of epithelial cell differentiation of ketatinocytes in the epidermis; stimulation of new collagen synthesis in the dermis, and production of new blood vessels (angiogenesis). Accordingly, as used herein for purposes of the present invention, the term 'retinoid' will be understood to include any of the foregoing compounds. Examples of suitable retinoids in the present invention are set forth in Table 2, although it will be understood that the invention is not limited thereto.
Table 2 all-trans-retinoic acid l3—cis-retinoic acid (all—E)—9—(4-methoxy-2,3,6- trimethy1phenyl)—3,7-dimethy1—2,4,6,8- nonatetraenoic acid ethyl ester (all—E)-9—(4—methoxy-2,3,6- trimethylphenyl—3,7—dimethyl—2,4,6,8- nonatetraenoic acid N—ethyl—9-(4-methoxy—2,3,6-trimethyl— pheny1)—3,7—dimethyl-2,4,6,8— nonatetraenamide (E,E)—9—(2,6~dichloro—4-methoxy—3— methylphenyl)—3,7-dimethyl-2,4,6,8- nonatetraenoic acid ethyl ester Table 2 (continued) ,8-didehydroretinoic acid (E,E)—4-[2—methy1—4-(2,6,6—trimethy1— l—cyc1ohexen—1—y1)~1,3-butadienyllbenzoic acid (E)-4—[4—methy1—6—(2,6,6-trimethy1— 1—cyc1ohexen—1—y1)—1,3,5-hexa- trienyllbenzoic acid (a1l—E)-3,7-dimethy1-(3—thieny1)- 2,4,6,8-nonatetraenoic acid (E,E,E)—3—methy1—7—(5,6,7,8—tetrahydro— ,5,8,8-tetramethy1~2—naphthaleny1)— 2,4,6-octatrienoic acid (E)—6—[2—(2,6,6-trimethy1cyc1ohexen— 1—y1)etheny1]-2—naphtha1enecarboxy1ic acid methyl-1H—inden-5—y1)—3—methy1— 2,4,6—octatrienoic acid (E)-4—[2~(2,3—dihydro—1,l,3,3-tetramethy1- 1H—inden—S—y1)-1—propeny1]benzoic acid (E)—4—[2—(5,6,7,8—tetrahydro-5,5,8,8- tetramethy1—2—naphtha1enyl—1— propenyllbenzoic acid (E)—4-[2—(5,6,7,8—tetrahydromethy1- ,5,8,8-tetramethyl—2—naphthalenyl propenyllbenzoic acid Table 2 (continued) (E)—1,2,3,4-tetrahydro-1,1,4,4-tetramethy1— 6-(l—methy1—2—pheny1etheny1)naphthalene —(1,2,3,4~tetrahydro—1,1,4,4-tetramethy1- 6—naphthyl)naphthalenecarboxylic acid (E)—6—[2—(4-(ethylsu1fonyl)phenyl]—l— methylethenyl]—l,2,3,4—tetrahydro- 1,1,4,4-tetramethylnaphthalene —[(5,6,7,8—tetrahydro-5,5,8,8—tetramethyl- 2—naphthalenyl)ethyny1]benzoic acid (E)—2—(1,1,4,4-tetramethy1—l,2,3,4—tetra— hydronaphth—7-y1)—l—[4-tetrazo1— —yl)pheny1]—l—propene (E)—4-[2—(5,6,7,8-tetrahydro—7—hydroxy— ,5,8,8—tetramethy1—2—naphthalenyl)- 1-propenyllbenzyl alcohol Included among the compounds which can be employed are the pharmaceutically acceptable addition salts and esters of the retinoids such as the palmitates etc. Also encompassed within the term 'retinoid" are geometric and stereoisomers of the retinoids.
A pharmacological composition containing a retinoid as the active ingredient in intimate admixture with a pharmaceutical carrier can be prepared according to conventional pharmaceutical compounding techniques, such as, for example, those known for topical application of a11—trans—retinoid acid. The carrier may take a wide variety of physical forms such as, for example, creams, dressings, gels, lotions, ointments or liquids. The retinoid will be present in the composition in an amount from about 0.0000l% by weight to about 0.2% by weight, depending on the potency of the retinoid. A suitable topical retinoid preparation in a gel vehicle is Retin-A", which contains 0.01% to 0.1% by weight of the active ingredient, (produced by Ortho Pharmaceutical Corporation).
The following example describes the invention in greater particularity, and is intended to be a way of illustrating but not limiting the invention.
EXAMPLE 1 lLifetime Application of all—trans—Retinoic Acid to Albino Hairless Mice.
Materials and Methods Female Albino hairless mice (Skh-hair1ess—l), age 8-11 weeks, were treated topically, three times a week, for the remainder of their life span as follows: Group 1. 0.025% all-trans-retinoic acid (100 pl) 12 mice Group 2. Cream vehicle (100 pl) 12 mice ‘Group 3. Untreated 12 mice The mice were examined monthly for skin changes and possible weight loss that might indicate a toxic effect.
Toward the end of the study, mice were photographed to show the condition of the skin. A few mice were sacrificed at about 70, 80 and 90 weeks, with dorsal skin taken for histochemical evaluation. The remainder were allowed to live out their life span which ranged from 91-106 weeks and were biopsied when moribound, if possible. The histochemical stains were: H&E for general histology, Luna's for elastic fibers, Van Gieson's for collagen and Mowry's for proteoglycans. l!;e_s_u.l1:s A. Tgxigity . There was no difference in the weights of mice within the three groups.
. There was no difference in mortality within the three groups.
. At biopsy and necropsy there was no indication that the mice suffered any adverse or unusual effects.
Therefore: treatment with either a1l—trans—retinoic acid or vehicle over a lifetime produced no detectable toxic effects.
B. 'ni rva i n Mice treated with all-trans—retinoic acid had thinner, pinker, more uniform skin than the controls. closely resembled far younger, untreated mice. controls had thicker, yellower skin. had extremely thick, They more Vehicle Untreated controls sagging, yellowed skin, typical of such aged mice (Figure l).
Figure l. is a photograph which illustrates the results of lifetime application of vehicle or all-trans—retinoic acid to female albino hairless (Skh—1) mice. T = vehicle, T1 = untreated, T1? = all—trans-retinoic acid. photograph.
Mice were 91-106 weeks of age at All—trans—retinoic acid mice had thinner, pinker, more uniform skin than controls or untreated mice.
They resemble young mice. Vehicle control mice had thicker, yellow skin. Untreated mice had very thick, sagging, yellowed skin.
C. H’ h mi 1 V ' n H&E for General Histology (See Figures 2, 3 and 4) Figure 2. is a picture of a normal old mouse, at 80 weeks of age. H & E stain.
Figure 3 is a picture which illustrates cream vehicle mice at 85 weeks of age.
Figure 4 is a picture which illustrates mice treated with all—trans—retinoic acid. (Lifetime of treatment).
Hyperplastic epidermis and strongly granular layer of approximately 4 cells. Cells are plump, cytologically normal and have abundant cytoplasm and an abundance of new blood vessels. Sample was taken from a mouse 95 weeks of age.
In a1l—trans~retinoic acid-treated specimens, the epidermis was hyperplastic (about 8 cell layers) including a strongly granular layer of about 4 cell layers. The cells were plump, cytologically normal and had an abundant cytoplasm. Control specimens had the usual 2-4 compressed—looking cells. Blood vessels were readily seen in the all—trans—retinoic acid group, unlike in the controls. Areas of new collagen were apparent by the parallel array of the bundles and the presence of numerous large fibroblasts. These regions were free of inflammation despite a mild inflammatory infiltrate in the mid—dermis. No repair areas were seen in the controls and dermal inflammation was present but variable from specimen to specimen.
Luna's fitain for Elastic Fibers This stain confirmed the presence of new collagen in the sub-epidermal dermis of Retin—A"~treated mice. These areas, termed repair zones, are identified by elastic fibers at their lower border, having been displaced downward by the deposition of new collagen. Repair zones were intermittent across the specimen, unlike in photodamaged skin where they are continuous. In controls, no repair zones were found (Figure 2). In addition, mice treated with all—trans—retinoic acid appeared to have an increased amount of new elastic fibers (Figure 4).
V ‘ n‘ in f r 1 n Collagen in the repair zones stained mainly as normal, mature collagen.
M w ' in f l ‘n — r n There was little or no increase in dermal glycosaminoglycans or proteoglycans in any of the groups except for intermittent deposits at the dermal- epidermal junction. These deposits are typically found in aging mice. Fewer deposits were found in the retinoid treated group.
Claims (6)
1. A cosmetic method for the prevention of the symptoms of intrinsically aged skin which comprises the topical administration prior to the appearance of said symptoms of an effective amount of a retinoid in a pharmaceutically acceptable carrier.
2. The method of claim 1 wherein the retinoid is all trans retinoic acid.
3. The method of claim 1 wherein the retinoid is 13- cis—retinoic acid.
4. The method of claim 1 wherein the retinoid is retinol.
5. The method of claim 1 wherein the retinoid is selected from the group consisting of: (E)~4-[4—methyl—6—(2,6,6~trimethyl—1~cyclohexen— 1~yl)—1,3,5~hexatrienyl]benzoic acid (E)—6—[2—(4—(ethylsulfonyl)phenyl]—1—methylethenyl]— 1,2,3,4—tetrahydro—1,1,4,4—tetramethylnaphthalene 4-[(5,6,7,8—tetrahydro—5,5,8,8—tetramethyl—2— naphthalenyl)ethynyl]benzoic acid and (E)—4—[2—(5,6,7,8—tetrahydro—7—hydroXy—5,5,8,8- tetramethyl—2-naphthalenyl)—1—propenyl]benzyl alcohol. The method of claim 1 wherein the retinoid is present in an amount from about 0.0000l% by weight to 0.2% by weight. The use of a retinoid in the manufacture of a medicament for the therapeutic prevention of the symptoms of intrinsically aged skin, said method comprising administering said retinoid topically in a pharmaceutically acceptable carrier prior to the appearance of said symptoms. The use of a retinoid as claimed in claim 7, wherein said retinoid is as specified in any of claims 2 to
6. F. R. KELLY & C0,, AGENTS FOR THE APPLICANTS
Applications Claiming Priority (2)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| USUNITEDSTATESOFAMERICA19/01/19892 | |||
| US29911989A | 1989-01-19 | 1989-01-19 |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| IE83435B1 true IE83435B1 (en) | |
| IE900202L IE900202L (en) | 1990-07-19 |
Family
ID=23153383
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| IE20290A IE900202L (en) | 1989-01-19 | 1990-01-18 | Skin treatment |
Country Status (2)
| Country | Link |
|---|---|
| IE (1) | IE900202L (en) |
| ZA (1) | ZA90369B (en) |
-
1990
- 1990-01-18 IE IE20290A patent/IE900202L/en not_active IP Right Cessation
- 1990-01-18 ZA ZA90369A patent/ZA90369B/en unknown
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