AI Article Synopsis

  • - Fuchs endothelial corneal dystrophy (FECD) is a hereditary eye disorder that commonly leads to vision loss in older adults, primarily linked to polymorphisms in the TCF4 gene and an expanded CTG repeat (CTG18.1) in most patients.
  • - Several potential mechanisms have been proposed for how this repeat expansion causes or worsens the disease, including issues with TCF4 regulation and toxic effects from abnormal RNA and protein processes, although the specifics of their contributions are still unclear.
  • - The review discusses current research connecting the CTG18.1 expansion to disease manifestations, explores various research tools available for studying FECD, and outlines ongoing efforts to develop new treatments while addressing critical unanswered questions in

Article Abstract

Fuchs endothelial corneal dystrophy (FECD) is a common cause for heritable visual loss in the elderly. Since the first description of an association between FECD and common polymorphisms situated within the transcription factor 4 (TCF4) gene, genetic and molecular studies have implicated an intronic CTG trinucleotide repeat (CTG18.1) expansion as a causal variant in the majority of FECD patients. To date, several non-mutually exclusive mechanisms have been proposed that drive and/or exacerbate the onset of disease. These mechanisms include (i) TCF4 dysregulation; (ii) toxic gain-of-function from TCF4 repeat-containing RNA; (iii) toxic gain-of-function from repeat-associated non-AUG dependent (RAN) translation; and (iv) somatic instability of CTG18.1. However, the relative contribution of these proposed mechanisms in disease pathogenesis is currently unknown. In this review, we summarise research implicating the repeat expansion in disease pathogenesis, define the phenotype-genotype correlations between FECD and CTG18.1 expansion, and provide an update on research tools that are available to study FECD as a trinucleotide repeat expansion disease. Furthermore, ongoing international research efforts to develop novel CTG18.1 expansion-mediated FECD therapeutics are highlighted and we provide a forward-thinking perspective on key unanswered questions that remain in the field.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7988464PMC
http://dx.doi.org/10.1016/j.preteyeres.2020.100883DOI Listing

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