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AuthorMikaeili, Hajar
AuthorHabib, Abdella M
AuthorYeung, Charlix Wai-Lok
AuthorSantana-Varela, Sonia
AuthorLuiz, Ana P
AuthorPanteleeva, Kseniia
AuthorZuberi, Sana
AuthorAthanasiou-Fragkouli, Alkyoni
AuthorHoulden, Henry
AuthorWood, John N
AuthorOkorokov, Andrei L
AuthorCox, James J
Available date2023-06-20T07:26:01Z
Publication Date2023-05-24
Publication NameBrain
Identifierhttp://dx.doi.org/10.1093/brain/awad098
CitationMikaeili, H., Habib, A. M., Yeung, C., Santana-Varela, S., Luiz, A. P., Panteleeva, K., ... & Cox, J. J. (2022). Molecular basis of FAAH-OUT-associated human pain insensitivity. bioRxiv, 2022-10.
ISSN0006-8950
URIhttp://hdl.handle.net/10576/44602
AbstractChronic pain affects millions of people worldwide and new treatments are needed urgently. One way to identify novel analgesic strategies is to understand the biological dysfunctions that lead to human inherited pain insensitivity disorders. Here we report how the recently discovered brain and dorsal root ganglia-expressed FAAH-OUT long non-coding RNA (lncRNA) gene, which was found from studying a pain-insensitive patient with reduced anxiety and fast wound healing, regulates the adjacent key endocannabinoid system gene FAAH, which encodes the anandamide-degrading fatty acid amide hydrolase enzyme. We demonstrate that the disruption in FAAH-OUT lncRNA transcription leads to DNMT1-dependent DNA methylation within the FAAH promoter. In addition, FAAH-OUT contains a conserved regulatory element, FAAH-AMP, that acts as an enhancer for FAAH expression. Furthermore, using transcriptomic analyses in patient-derived cells we have uncovered a network of genes that are dysregulated from disruption of the FAAH-FAAH-OUT axis, thus providing a coherent mechanistic basis to understand the human phenotype observed. Given that FAAH is a potential target for the treatment of pain, anxiety, depression and other neurological disorders, this new understanding of the regulatory role of the FAAH-OUT gene provides a platform for the development of future gene and small molecule therapies.
Sponsor- Medical Research Council/United Kingdom - grant No. [G1100340/MRC_]. - Medical Research Council/United Kingdom - grant No. [MR/R011737/1/MRC_]. - Versus Arthritis/United Kingdom [20200/VAC_]. - Medical Research Council grant [G1100340]. - Medical Research Council grant [MR/R011737/1]. - Qatar University grants [QUSD-CMED-2018/9-3] and [QUCG-CMED-19/20-4]. - Qatar National Research Fund [NPRP13S-0209-200315]. - Versus Arthritis grant [20200]. - Wellcome grant [200183/Z/15/Z].
Languageen
PublisherOxford University Press
Subjectanandamide
endocannabinoid system
pain
pseudogene
regulatory RNA
TitleMolecular basis of FAAH-OUT-associated human pain insensitivity.
TypeArticle
ESSN1460-2156


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