WIPI1 is a conserved mediator of right ventricular failure
Christos Tzimas, Christoph D. Rau, Petra E. Buergisser, Gaston Jean-Louis Jr., Katherine Lee, Jeffrey Chukwuneke, Wen Dun, Yibin Wang, Emily J. Tsai
Christos Tzimas, Christoph D. Rau, Petra E. Buergisser, Gaston Jean-Louis Jr., Katherine Lee, Jeffrey Chukwuneke, Wen Dun, Yibin Wang, Emily J. Tsai
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Research Article Cardiology

WIPI1 is a conserved mediator of right ventricular failure

Abstract

Right ventricular (RV) dysfunction is highly prevalent across cardiopulmonary diseases and independently predicts death in both heart failure (HF) and pulmonary hypertension (PH). Progression towards RV failure (RVF) can occur in spite of optimal medical treatment of HF or PH, highlighting current insufficient understanding of RVF molecular pathophysiology. To identify molecular mechanisms that may distinctly underlie RVF, we investigated the cardiac ventricular transcriptome of advanced-HF patients, with and without RVF. Using an integrated systems genomic and functional biology approach, we identified an RVF-specific gene module, for which WIPI1 served as a hub and HSPB6 and MAP4 as drivers, and confirmed the ventricular specificity of Wipi1, Hspb6, and Map4 transcriptional changes in adult murine models of pressure overload–induced RV versus left ventricular failure. We uncovered a shift towards noncanonical autophagy in the failing RV that correlated with RV-specific Wipi1 upregulation. In vitro siRNA silencing of Wipi1 in neonatal rat ventricular myocytes limited noncanonical autophagy and blunted aldosterone-induced mitochondrial superoxide levels. Our findings suggest that Wipi1 regulates mitochondrial oxidative signaling and noncanonical autophagy in cardiac myocytes. Together with our human transcriptomic analysis and corroborating studies in an RVF mouse model, these data render Wipi1 a potential target for RV-directed HF therapy.

Authors

Christos Tzimas, Christoph D. Rau, Petra E. Buergisser, Gaston Jean-Louis Jr., Katherine Lee, Jeffrey Chukwuneke, Wen Dun, Yibin Wang, Emily J. Tsai

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Figure 7

Silencing Wipi1 decreases mitochondrial superoxide (O2˙) levels in in vitro neurohormonal model of right ventricular failure (RVF).

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Silencing Wipi1 decreases mitochondrial superoxide (O2˙) levels in in vi...
Neonatal rat ventricular myocytes (NRVMs) were transfected with scramble or Wipi1-specific siRNAs and then stimulated with aldosterone (Aldo, 1 μM, 48 hours) or hydrogen peroxide (H2O2, 50 μM, 2 hours). (A) Brightfield and MitoSOX Red imaging of NRVMs transfected with si-Scramble versus si-Wipi1, with and without Aldo stimulation. H2O2 was used as a positive control. Scale bars: 75 μm. (B) Summary analysis of mitochondrial O2˙ levels (n = 41–44 per group from 6 independent experiments). (C) Cell viability as assessed by MTT assay (n = 24 per group from 3 independent experiments). *P < 0.0001 versus respective unstimulated baseline unless indicated otherwise by comparison bar, by Tukey’s multiple-comparison test following 2-way ANOVA. Box-and-whisker plots show mean (+), median (midline), 25th and 75th percentiles (box), minimum and maximum values (whiskers).