RGS6 drives cardiomyocyte death following nucleolar stress by suppressing Nucleolin/miRNA-21

Abhishek Singh Sengar; Manish Kumar; Chetna Rai; Sreemoyee Chakraborti; Dinesh Kumar; Pranesh Kumar; Sukhes Mukherjee; Kausik Mondal; Adele Stewart; Biswanath Maity

doi:10.1186/s12967-024-04985-3

RGS6 drives cardiomyocyte death following nucleolar stress by suppressing Nucleolin/miRNA-21

J Transl Med. 2024 Feb 26;22(1):204. doi: 10.1186/s12967-024-04985-3.

Authors

Affiliations

¹ Centre of Biomedical Research (CBMR), SGPGI Campus, Raebareli Road, Lucknow, Uttar Pradesh, 226014, India.
² Forensic Science Laboratory, Department of Home and Hill Affairs, Kolkata, West Bengal, 700037, India.
³ Institute of Pharmaceutical Science, University of Lucknow, Lucknow, Uttar Pradesh, 226007, India.
⁴ Biochemistry, AIIMS Bhopal, Saket Nagar, Bhopal, Madhya Pradesh, 462026, India.
⁵ Zoology, University of Kalyani, Nadia, West Bengal, 741235, India.
⁶ Biomedical Science, Florida Atlantic University, Jupiter, FL, 33458, USA.
⁷ Centre of Biomedical Research (CBMR), SGPGI Campus, Raebareli Road, Lucknow, Uttar Pradesh, 226014, India. bmaity@cbmr.res.in.

Abstract

Background: Prior evidence demonstrated that Regulator of G protein Signaling 6 (RGS6) translocates to the nucleolus in response to cytotoxic stress though the functional significance of this phenomenon remains unknown.

Methods: Utilizing in vivo gene manipulations in mice, primary murine cardiac cells, human cell lines and human patient samples we dissect the participation of a RGS6-nucleolin complex in chemotherapy-dependent cardiotoxicity.

Results: Here we demonstrate that RGS6 binds to a key nucleolar protein, Nucleolin, and controls its expression and activity in cardiomyocytes. In the human myocyte AC-16 cell line, induced pluripotent stem cell derived cardiomyocytes, primary murine cardiomyocytes, and the intact murine myocardium tuning RGS6 levels via overexpression or knockdown resulted in diametrically opposed impacts on Nucleolin mRNA, protein, and phosphorylation.RGS6 depletion provided marked protection against nucleolar stress-mediated cell death in vitro, and, conversely, RGS6 overexpression suppressed ribosomal RNA production, a key output of the nucleolus, and triggered death of myocytes. Importantly, overexpression of either Nucleolin or Nucleolin effector miRNA-21 counteracted the pro-apoptotic effects of RGS6. In both human and murine heart tissue, exposure to the genotoxic stressor doxorubicin was associated with an increase in the ratio of RGS6/Nucleolin. Preventing RGS6 induction via introduction of RGS6-directed shRNA via intracardiac injection proved cardioprotective in mice and was accompanied by restored Nucleolin/miRNA-21 expression, decreased nucleolar stress, and decreased expression of pro-apoptotic, hypertrophy, and oxidative stress markers in heart.

Conclusion: Together, these data implicate RGS6 as a driver of nucleolar stress-dependent cell death in cardiomyocytes via its ability to modulate Nucleolin. This work represents the first demonstration of a functional role for an RGS protein in the nucleolus and identifies the RGS6/Nucleolin interaction as a possible new therapeutic target in the prevention of cardiotoxicity.

Keywords: Cardiotoxicity; Chemotherapy; G-protein; Nucleolar stress; RGS proteins.

MeSH terms

Animals
Cardiotoxicity
Humans
Mice
MicroRNAs* / genetics
Myocytes, Cardiac
Nucleolin
RGS Proteins* / genetics
Signal Transduction / physiology

Substances

MicroRNAs
MIRN21 microRNA, human
Nucleolin
RGS Proteins
RGS6 protein, human
NCL protein, human
Ncl protein, mouse
Rgs6 protein, mouse

Abstract

MeSH terms

Substances

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