eLife (Oct 2018)

Bid maintains mitochondrial cristae structure and function and protects against cardiac disease in an integrative genomics study

  • Christi T Salisbury-Ruf,
  • Clinton C Bertram,
  • Aurelia Vergeade,
  • Daniel S Lark,
  • Qiong Shi,
  • Marlene L Heberling,
  • Niki L Fortune,
  • G Donald Okoye,
  • W Gray Jerome,
  • Quinn S Wells,
  • Josh Fessel,
  • Javid Moslehi,
  • Heidi Chen,
  • L Jackson Roberts II,
  • Olivier Boutaud,
  • Eric R Gamazon,
  • Sandra S Zinkel

DOI
https://doi.org/10.7554/eLife.40907
Journal volume & issue
Vol. 7

Abstract

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Bcl-2 family proteins reorganize mitochondrial membranes during apoptosis, to form pores and rearrange cristae. In vitro and in vivo analysis integrated with human genetics reveals a novel homeostatic mitochondrial function for Bcl-2 family protein Bid. Loss of full-length Bid results in apoptosis-independent, irregular cristae with decreased respiration. Bid-/- mice display stress-induced myocardial dysfunction and damage. A gene-based approach applied to a biobank, validated in two independent GWAS studies, reveals that decreased genetically determined BID expression associates with myocardial infarction (MI) susceptibility. Patients in the bottom 5% of the expression distribution exhibit >4 fold increased MI risk. Carrier status with nonsynonymous variation in Bid’s membrane binding domain, BidM148T, associates with MI predisposition. Furthermore, Bid but not BidM148T associates with Mcl-1Matrix, previously implicated in cristae stability; decreased MCL-1 expression associates with MI. Our results identify a role for Bid in homeostatic mitochondrial cristae reorganization, that we link to human cardiac disease.

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