Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders

Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders

Abstract Background Retinoid‐based therapies are commonly used in the treatment of disorders of keratinization and other skin disorders but can result in non‐specific effects and adverse reactions. Use of retinoic acid metabolism blocking agents (RAMBAs) such as DX308 may address these shortcomings....

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Main Authors: J.G.S. Veit, Y. Poumay, D. Mendes, J. Kreitinger, L. Walker, A. Paquet, C. Menigot, F. Zolezzi, A.S. Paller, P. Diaz
Format: Article
Language:English
Published: Wiley 2021-06-01
Series:Skin Health and Disease
Online Access:https://doi.org/10.1002/ski2.22
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spelling doaj-03ec128546f642f9afab1da8c7c816d22021-09-14T19:05:42ZengWileySkin Health and Disease2690-442X2021-06-0112n/an/a10.1002/ski2.22Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disordersJ.G.S. Veit0Y. Poumay1D. Mendes2J. Kreitinger3L. Walker4A. Paquet5C. Menigot6F. Zolezzi7A.S. Paller8P. Diaz9Department of Biomedical and Pharmaceutical Sciences University of Montana Missoula Montana USAURPHYM‐NARILIS University of Namur Namur BelgiumR&D DermaXon LLC Missoula Montana USAR&D DermaXon LLC Missoula Montana USAR&D DermaXon LLC Missoula Montana USASyneos Health Biot FranceSyneos Health Biot FranceSyneos Health Biot FranceDepartment of Dermatology Northwestern University Feinberg School of Medicine Chicago Illinois USADepartment of Biomedical and Pharmaceutical Sciences University of Montana Missoula Montana USAAbstract Background Retinoid‐based therapies are commonly used in the treatment of disorders of keratinization and other skin disorders but can result in non‐specific effects and adverse reactions. Use of retinoic acid metabolism blocking agents (RAMBAs) such as DX308 may address these shortcomings. Objectives Characterize the therapeutic potential of recently discovered, CYP26‐selective RAMBA, DX308. Materials and Methods Preliminary in vitro assessment of potential off‐target activity, metabolic and toxicologic profiling. Studies to assess safety and efficacy of topical treatment in correcting abnormal skin morphology in rhino mice. Extensive gene expression profiling by RNA sequencing and qPCR in 3D epidermis grown with keratinocytes (KCs) from keratinization disorders and healthy controls, to investigate modulation of retinoid biopathways. Results In vitro, DX308 does not interact with off‐target nuclear receptors or CYP450s, is not genotoxic, and is stable in skin, despite vigorous hepatic metabolism. In vivo, topical DX308 induces comedolysis and epidermal thickening without apparent adverse effects. Gene expression profiling shows potent modulation of retinoid‐responsive genes by DX308 in both healthy and keratinization disorder KCs. Pathway analysis suggests DX308 may inhibit inflammatory and immune responses in KCs. Conclusions These preliminary studies suggest that DX308 is an efficacious topical therapeutic with a favourable metabolic and safety profiles. DX308 may present an improved therapeutic alternative for the treatment of keratinization disorders and other retinoid‐responsive skin ailments.https://doi.org/10.1002/ski2.22
collection DOAJ
language English
format Article
sources DOAJ
author J.G.S. Veit
Y. Poumay
D. Mendes
J. Kreitinger
L. Walker
A. Paquet
C. Menigot
F. Zolezzi
A.S. Paller
P. Diaz
spellingShingle J.G.S. Veit
Y. Poumay
D. Mendes
J. Kreitinger
L. Walker
A. Paquet
C. Menigot
F. Zolezzi
A.S. Paller
P. Diaz
Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
Skin Health and Disease
author_facet J.G.S. Veit
Y. Poumay
D. Mendes
J. Kreitinger
L. Walker
A. Paquet
C. Menigot
F. Zolezzi
A.S. Paller
P. Diaz
author_sort J.G.S. Veit
title Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
title_short Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
title_full Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
title_fullStr Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
title_full_unstemmed Preclinical assessment of dual CYP26[A1/B1] inhibitor, DX308, as an improved treatment for keratinization disorders
title_sort preclinical assessment of dual cyp26[a1/b1] inhibitor, dx308, as an improved treatment for keratinization disorders
publisher Wiley
series Skin Health and Disease
issn 2690-442X
publishDate 2021-06-01
description Abstract Background Retinoid‐based therapies are commonly used in the treatment of disorders of keratinization and other skin disorders but can result in non‐specific effects and adverse reactions. Use of retinoic acid metabolism blocking agents (RAMBAs) such as DX308 may address these shortcomings. Objectives Characterize the therapeutic potential of recently discovered, CYP26‐selective RAMBA, DX308. Materials and Methods Preliminary in vitro assessment of potential off‐target activity, metabolic and toxicologic profiling. Studies to assess safety and efficacy of topical treatment in correcting abnormal skin morphology in rhino mice. Extensive gene expression profiling by RNA sequencing and qPCR in 3D epidermis grown with keratinocytes (KCs) from keratinization disorders and healthy controls, to investigate modulation of retinoid biopathways. Results In vitro, DX308 does not interact with off‐target nuclear receptors or CYP450s, is not genotoxic, and is stable in skin, despite vigorous hepatic metabolism. In vivo, topical DX308 induces comedolysis and epidermal thickening without apparent adverse effects. Gene expression profiling shows potent modulation of retinoid‐responsive genes by DX308 in both healthy and keratinization disorder KCs. Pathway analysis suggests DX308 may inhibit inflammatory and immune responses in KCs. Conclusions These preliminary studies suggest that DX308 is an efficacious topical therapeutic with a favourable metabolic and safety profiles. DX308 may present an improved therapeutic alternative for the treatment of keratinization disorders and other retinoid‐responsive skin ailments.
url https://doi.org/10.1002/ski2.22
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