4.7 Article

TTTCA repeat insertions in an intron of YEATS2 in benign adult familial myoclonic epilepsy type 4

Journal

BRAIN
Volume 142, Issue -, Pages 3360-3366

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/brain/awz267

Keywords

epilepsy; myoclonic epilepsy; movement disorders; molecular genetics; whole-genome sequencing

Funding

  1. Chulalongkorn Academic Advancement Into Its 2nd Century Project
  2. Grants for Development of New Faculty Staff
  3. Ratchadaphiseksomphot Endowment Fund, Medical Genomics Cluster, Chulalongkorn University
  4. Thailand Research Fund [MRG6080186, DPG6180001]

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Epilepsy is a common neurological disorder and identification of its causes is important for a better understanding of its pathogenesis. We previously studied a Thai family with a type of epilepsy, benign adult familial myoclonic epilepsy type 4 (BAFME4), and localized its gene to chromosome 3q26.32-q28. Here, we used single-molecule real-time sequencing and found expansions of TTTTA and insertions of TTTCA repeats in intron 1 of YEATS2 in one affected member of the family. Of all the available members in the family-comprising 13 affected and eight unaffected-repeat-primed PCR and long-range PCR revealed the cosegregation of the TTTCA repeat insertions with the TTTTA repeat expansions and the disease status. For 1116 Thai control subjects, none were found to harbour the TTTCA repeats while four had the TTTTA repeat expansions. Therefore, our findings suggest that BAFME4 is caused by the insertions of the intronic TTTCA repeats in YEATS2. Interestingly, all four types of BAFMEs for which underlying genes have been found (BAFMEs 1, 4, 6 and 7) are caused by the same molecular pathology, suggesting that the insertions of non-coding TTTCA repeats are involved in their pathogenesis.

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