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Non-Synonymous Variants in the Premelanosome Protein (PMEL) Gene are Associated with Pigment Dispersion Syndrome/Pigmentary Glaucoma and Cause Biochemical Defects

  • Author / Creator
    Lahola-Chomiak, Adrian

  • Pigmentary Glaucoma (PG) is a common glaucoma subtype that results from release of pigment from the iris (Pigment Dispersion Syndrome) and its deposition throughout the anterior chamber of the eye. Although PG has a substantial heritable component, no causative gene variants have yet been identified in humans. Whole Exome Sequencing (WES) of two independent pedigrees identified the first candidate gene for heritable PDS/PG - premelanosome protein (PMEL), which encodes a key component of the organelle (melanosome) essential for melanin synthesis, storage and transport. Targeted screening of PMEL in three independent replication cohorts (n= 394) identified nine additional PDS/PG-associated variants. These variants exhibited either defective post-translational processing of the PMEL (5/9), altered amyloid fibril formation (5/9), or both (3/9). Suppresion of the homologous pmela in zebrafish caused profound pigmentation and ocular defects further supporting PMEL’s role in PDS/PG. Taken together, these data support a model in which protein altering PMEL variants represent dominant negative mutations that impair PMEL’s normal ability to form functional amyloid fibrils. While PMEL mutations have previously been shown to cause pigmentation and ocular defects in animals, this research is the first report of mutations in PMEL that cause human eye disease.

  • Subjects / Keywords
  • Graduation date
    Fall 2018
  • Type of Item
    Thesis
  • Degree
    Master of Science
  • DOI
    https://doi.org/10.7939/R35H7C919
  • License
    Permission is hereby granted to the University of Alberta Libraries to reproduce single copies of this thesis and to lend or sell such copies for private, scholarly or scientific research purposes only. Where the thesis is converted to, or otherwise made available in digital form, the University of Alberta will advise potential users of the thesis of these terms. The author reserves all other publication and other rights in association with the copyright in the thesis and, except as herein before provided, neither the thesis nor any substantial portion thereof may be printed or otherwise reproduced in any material form whatsoever without the author's prior written permission.