Frontiers in Cardiovascular Medicine (Aug 2020)

Association of Genetic Variants at TRPC6 With Chemotherapy-Related Heart Failure

  • Nadine Norton,
  • Julia E. Crook,
  • Liwei Wang,
  • Janet E. Olson,
  • Jennifer M. Kachergus,
  • Daniel J. Serie,
  • Brian M. Necela,
  • Paul G. Borgman,
  • Pooja P. Advani,
  • Jordan C. Ray,
  • Carolyn Landolfo,
  • Damian N. Di Florio,
  • Damian N. Di Florio,
  • Anneliese R. Hill,
  • Katelyn A. Bruno,
  • Katelyn A. Bruno,
  • DeLisa Fairweather,
  • DeLisa Fairweather

DOI
https://doi.org/10.3389/fcvm.2020.00142
Journal volume & issue
Vol. 7

Abstract

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Background: Our previous GWAS identified genetic variants at six novel loci that were associated with a decline in left ventricular ejection fraction (LVEF), p < 1 × 10−5 in 1,191 early breast cancer patients from the N9831 clinical trial of chemotherapy plus trastuzumab. In this study we sought replication of these loci.Methods: We tested the top loci from the GWAS for association with chemotherapy-related heart failure (CRHF) using 26 CRHF cases from N9831 and 984 patients from the Mayo Clinic Biobank which included CRHF cases (N = 12) and control groups of patients treated with anthracycline +/– trastuzumab without HF (N = 282) and patients with HF that were never treated with anthracycline or trastuzumab (N = 690). We further examined associated loci in the context of gene expression and rare coding variants using a TWAS approach in heart left ventricle and Sanger sequencing, respectively. Doxorubicin-induced apoptosis and cardiomyopathy was modeled in human iPSC-derived cardiomyocytes and endothelial cells and a mouse model, respectively, that were pre-treated with GsMTx-4, an inhibitor of TRPC6.Results:TRPC6 5′ flanking variant rs57242572-T was significantly more frequent in cases compared to controls, p = 0.031, and rs61918162-T showed a trend for association, p = 0.065. The rs61918162 T-allele was associated with higher TRPC6 expression in the heart left ventricle. We identified a single TRPC6 rare missense variant (rs767086724, N338S, prevalence 0.0025% in GnomAD) in one of 38 patients (2.6%) with CRHF. Pre-treatment of cardiomyocytes and endothelial cells with GsMTx4 significantly reduced doxorubicin-induced apoptosis. Similarly, mice treated with GsMTx4 had significantly improved doxorubicin-induced cardiac dysfunction.Conclusions: Genetic variants that are associated with increased TRPC6 expression in the heart and rare TRPC6 missense variants may be clinically useful as risk factors for CRHF. GsMTx-4 may be a cardioprotective agent in patients with TRPC6 risk variants. Replication of the genetic associations in larger well-characterized samples and functional studies are required.

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