HIV-1 Nef-induced cardiotoxicity through dysregulation of autophagy

Manish K Gupta,Tricia H Burdo,Joseph Y Cheung,Kamel Khalili,Arthur M Feldman,Jennifer Gordon,Rafal Kaminski,Brian Mullen,Muniswamy Madesh

doi:10.1038/s41598-017-08736-x

Manish K Gupta, Tricia H Burdo + Show 7 more

Open Access

https://doi.org/10.1038/s41598-017-08736-x

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Journal: Scientific Reports	Publication Date: Aug 17, 2017
Citations: 29	License type: open-access

Affiliation: Temple University

Abstract

Cardiovascular disease is a leading cause of co-morbidity in HIV-1 positive patients, even those in whom plasma virus levels are well-controlled. The pathogenic mechanism of HIV-1-associated cardiomyopathy is unknown, but has been presumed to be mediated indirectly, owing to the absence of productive HIV-1 replication in cardiomyocytes. We sought to investigate the effect of the HIV-1 auxiliary protein, Nef, which is suspected of extracellular release by infected CD4+ T cells on protein quality control and autophagy in cardiomyocytes. After detection of Nef in the serum of HIV-1 positive patients and the accumulation of this protein in human and primate heart tissue from HIV-1/SIV-infected cells we employed cell and molecular biology approaches to investigate the effect of Nef on cardiomyocyte-homeostasis by concentrating on protein quality control (PQC) pathway and autophagy. We found that HIV-1 Nef-mediated inhibition of autophagy flux leads to cytotoxicity and death of cardiomyocytes. Nef compromises autophagy at the maturation stage of autophagosomes by interacting with Beclin 1/Rab7 and dysregulating TFEB localization and cellular lysosome content. These effects were reversed by rapamycin treatment. Our results indicate that HIV-1 Nef-mediated inhibition of cellular PQC is one possible mechanism involved in the development of HIV-associated cardiomyopathy.

Highlights

A large number of HIV-1 infected individuals develop cardiovascular diseases (CVD) with abnormal heart function causing significant morbidity and mortality[1, 2]
Prior to the introduction of combined anti-retroviral therapy, a major cause of death in HIV-1 infected patients was the development of HIV-1-related cardiomyopathy
The improved viral control achieved in HIV-1 infected patients on combined anti-retroviral therapy (cART) has only decreased the prevalence of HIV-1-associated heart failure by about 30%, Figure 8

Summary

Introduction

A large number of HIV-1 infected individuals develop cardiovascular diseases (CVD) with abnormal heart function causing significant morbidity and mortality[1, 2]. HIV-1 has been detected in the heart, yet the mechanisms of any such direct HIV-mediated cardiomyopathy, and progression towards heart failure, are unknown[11,12,13] Infected cells such as CD4+ T lymphocytes often release viral and cellular proteins with toxic activities that can be taken up by uninfected bystander cells leading to cell injury and death[14,15,16]. Infected macaques: (A) Representative images show the localization of Nef protein in heart tissue of HIV-1 positive patients treated (HIV+/ART) or not treated with ART (HIV+) but not in HIV-1 negative (HIV−). Blots were probed with antibody against SIV Nef (E) Nef was detectable in the serum of HIV-1+ patients with or without ART, but not control subjects, by ELISA

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