TY - JOUR
T1 - Mechanical dysfunction of the sarcomere induced by a pathogenic mutation in troponin t drives cellular adaptation
AU - Clippinger, Sarah R.
AU - Cloonan, Paige E.
AU - Wang, Wei
AU - Greenberg, Lina
AU - Stump, W. Tom
AU - Angsutararux, Paweorn
AU - Nerbonne, Jeanne M.
AU - Greenberg, Michael J.
N1 - Funding Information:
This work was supported by the National Institutes of Health (grant R01 HL141086 to M.J. Greenberg and grants R01 HL034161 and R01 HL142520 to J.M. Nerbonne), the March of Dimes Foundation (grant FY18-BOC-430198 to M.J. Greenberg), the Children’s Discovery Institute of Washington University and St. Louis Children’s Hospital (grant PM-LI-2019-829 to M.J. Greenberg), the Washington University Institute of Materials Science, and the Washington University Center for Cellular Imaging (grant CDI-CORE-2015-505 to M.J. Greenberg). S.R. Clippinger was supported through a National Institutes of Health institutional training grant (T32 EB018266). The authors declare no competing financial interests.
Funding Information:
The authors thank Jonathan Davis for the troponin CT53C plasmid. This work was supported by the National Institutes of Health (grant R01 HL141086 to M.J. Greenberg and grants R01 HL034161 and R01 HL142520 to J.M. Nerbonne), the March of Dimes Foundation (grant FY18-BOC-430198 to M.J. Greenberg), the Children?s Discovery Institute of Washington University and St. Louis Children?s Hospital (grant PM-LI-2019-829 to M.J. Greenberg), the Washington University Institute of Materials Science, and the Washington University Center for Cellular Imaging (grant CDI-CORE-2015-505 to M.J. Greenberg). S.R. Clippinger was supported through a National Institutes of Health institutional training grant (T32 EB018266).
Publisher Copyright:
© 2021 Clippinger et al.
PY - 2021/5/3
Y1 - 2021/5/3
N2 - Familial hypertrophic cardiomyopathy (HCM), a leading cause of sudden cardiac death, is primarily caused by mutations in sarcomeric proteins. The pathogenesis of HCM is complex, with functional changes that span scales, from molecules to tissuesThis makes it challenging to deconvolve the biophysical molecular defect that drives the disease pathogenesis from downstream changes in cellular function. In this study, we examine an HCM mutation in troponin T, R92Q, for which several models explaining its effects in disease have been put forward. We demonstrate that the primary molecular insult driving disease pathogenesis is mutation-induced alterations in tropomyosin positioning, which causes increased molecular and cellular force generation during calcium-based activation. Computational modeling shows that the increased cellular force is consistent with the molecular mechanism. These changes in cellular contractility cause downstream alterations in gene expression, calcium handling, and electrophysiology. Taken together, our results demonstrate that molecularly driven changes in mechanical tension drive the early disease pathogenesis of familial HCM, leading to activation of adaptive mechanobiological signaling pathways.
AB - Familial hypertrophic cardiomyopathy (HCM), a leading cause of sudden cardiac death, is primarily caused by mutations in sarcomeric proteins. The pathogenesis of HCM is complex, with functional changes that span scales, from molecules to tissuesThis makes it challenging to deconvolve the biophysical molecular defect that drives the disease pathogenesis from downstream changes in cellular function. In this study, we examine an HCM mutation in troponin T, R92Q, for which several models explaining its effects in disease have been put forward. We demonstrate that the primary molecular insult driving disease pathogenesis is mutation-induced alterations in tropomyosin positioning, which causes increased molecular and cellular force generation during calcium-based activation. Computational modeling shows that the increased cellular force is consistent with the molecular mechanism. These changes in cellular contractility cause downstream alterations in gene expression, calcium handling, and electrophysiology. Taken together, our results demonstrate that molecularly driven changes in mechanical tension drive the early disease pathogenesis of familial HCM, leading to activation of adaptive mechanobiological signaling pathways.
UR - http://www.scopus.com/inward/record.url?scp=85104379575&partnerID=8YFLogxK
U2 - 10.1085/jgp.202012787
DO - 10.1085/jgp.202012787
M3 - Article
C2 - 33856419
AN - SCOPUS:85104379575
SN - 0022-1295
VL - 153
JO - Journal of General Physiology
JF - Journal of General Physiology
IS - 5
M1 - e202012787
ER -