Modulating Innate and Adaptive Immunity by (R)-Roscovitine: Potential Therapeutic Opportunity in Cystic Fibrosis

Laurent Meijer(ManRos Therapeutics (France)), Deborah J. Nelson(University of Chicago), Vladimir Riazanski(University of Chicago), Aida G. Gabdoulkhakova(University of Chicago), Geneviève Héry-Arnaud(Laboratoire de Biodiversité et Biotechnologies Microbiennes), Rozenn Le Berre(Laboratoire de Biodiversité et Biotechnologies Microbiennes), Nadège Loaëc(ManRos Therapeutics (France)), Nassima Oumata(ManRos Therapeutics (France)), Hervé Galons(Inserm), Emmanuel Nowak(Hôpital Maison Blanche), L. Guéganton(Fondation FondaMental), Guillaume Dorothée(Sorbonne Université), Michaela Prochazkova(National Institute of Dental and Craniofacial Research), Bradford Hall(National Institute of Dental and Craniofacial Research), Ashok B. Kulkarni(National Institute of Dental and Craniofacial Research), Robert D. Gray(Centre for Inflammation Research), Adriano G. Rossi(Centre for Inflammation Research), Véronique Witko‐Sarsat(Centre National de la Recherche Scientifique), Caroline Norez(Université de Poitiers), Frédéric Becq(Université de Poitiers), Denis Ravel(MNM Consulting (France)), Dominique Mottier(Hôpital Maison Blanche), G. Rault(Station Biologique de Roscoff)
Journal of Innate Immunity
January 1, 2016
Cited by 4,998Open Access
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Abstract

(R)-Roscovitine, a pharmacological inhibitor of kinases, is currently in phase II clinical trial as a drug candidate for the treatment of cancers, Cushing's disease and rheumatoid arthritis. We here review the data that support the investigation of (R)-roscovitine as a potential therapeutic agent for the treatment of cystic fibrosis (CF). (R)-Roscovitine displays four independent properties that may favorably combine against CF: (1) it partially protects F508del-CFTR from proteolytic degradation and favors its trafficking to the plasma membrane; (2) by increasing membrane targeting of the TRPC6 ion channel, it rescues acidification in phagolysosomes of CF alveolar macrophages (which show abnormally high pH) and consequently restores their bactericidal activity; (3) its effects on neutrophils (induction of apoptosis), eosinophils (inhibition of degranulation/induction of apoptosis) and lymphocytes (modification of the Th17/Treg balance in favor of the differentiation of anti-inflammatory lymphocytes and reduced production of various interleukins, notably IL-17A) contribute to the resolution of inflammation and restoration of innate immunity, and (4) roscovitine displays analgesic properties in animal pain models. The fact that (R)-roscovitine has undergone extensive preclinical safety/pharmacology studies, and phase I and II clinical trials in cancer patients, encourages its repurposing as a CF drug candidate.


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