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    Microdeletion in a FAAH pseudogene identified in a patient with high anandamide concentrations and pain insensitivity

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    Microdeletion in a FAAH pseudogene identified in a patient with high anandamide concentrations and pain insensitivity.pdf (335.4Kb)
    Date
    2019-08
    Author
    Habib, Abdella M.
    Okorokov, Andrei L.
    Hill, Beta Matthew Nicholas
    Bras, Jose T.
    Lee, Man-Cheung
    Li, Shengnan
    Gossage, Samuel J.
    Drimmelen, Marie van
    Houlden, Henry H.
    Ramirez, Juan D.
    Bennett, David L.H.
    Srivastava, Devjit
    Cox, James J.
    ...show more authors ...show less authors
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    Abstract
    The study of rare families with inherited pain insensitivity can identify new human-validated analgesic drug targets. Here, a 66-yr-old female presented with nil requirement for postoperative analgesia after a normally painful orthopaedic hand surgery (trapeziectomy). Further investigations revealed a lifelong history of painless injuries, such as frequent cuts and burns, which were observed to heal quickly. We report the causative mutations for this new pain insensitivity disorder: the co-inheritance of (i) a microdeletion in dorsal root ganglia and brain-expressed pseudogene, FAAH-OUT, which we cloned from the fatty-acid amide hydrolase (FAAH) chromosomal region; and (ii) a common functional single-nucleotide polymorphism in FAAH conferring reduced expression and activity. Circulating concentrations of anandamide and related fatty-acid amides (palmitoylethanolamide and oleoylethanolamine) that are all normally degraded by FAAH were significantly elevated in peripheral blood compared with normal control carriers of the hypomorphic single-nucleotide polymorphism. The genetic findings and elevated circulating fatty-acid amides are consistent with a phenotype resulting from enhanced endocannabinoid signalling and a loss of function of FAAH. Our results highlight previously unknown complexity at the FAAH genomic locus involving the expression of FAAH-OUT, a novel pseudogene and long non-coding RNA. These data suggest new routes to develop FAAH-based analgesia by targeting of FAAH-OUT, which could significantly improve the treatment of postoperative pain and potentially chronic pain and anxiety disorders.
    DOI/handle
    http://dx.doi.org/10.1016/j.bja.2019.02.019
    http://hdl.handle.net/10576/23717
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