Literature DB >> 27039070

BRG1 and BRM SWI/SNF ATPases redundantly maintain cardiomyocyte homeostasis by regulating cardiomyocyte mitophagy and mitochondrial dynamics in vivo.

Scott J Bultman1, Darcy Wood Holley2, Gustaaf G de Ridder3, Salvatore V Pizzo3, Tatiana N Sidorova4, Katherine T Murray4, Brian C Jensen5, Zhongjing Wang5, Ariana Bevilacqua6, Xin Chen7, Megan T Quintana8, Manasi Tannu9, Gary B Rosson2, Kumar Pandya10, Monte S Willis11.   

Abstract

There has been an increasing recognition that mitochondrial perturbations play a central role in human heart failure. Mitochondrial networks, whose function is to maintain the regulation of mitochondrial biogenesis, autophagy ('mitophagy') and mitochondrial fusion/fission, are new potential therapeutic targets. Yet our understanding of the molecular underpinning of these processes is just emerging. We recently identified a role of the SWI/SNF ATP-dependent chromatin remodeling complexes in the metabolic homeostasis of the adult cardiomyocyte using cardiomyocyte-specific and inducible deletion of the SWI/SNF ATPases BRG1 and BRM in adult mice (Brg1/Brm double mutant mice). To build upon these observations in early altered metabolism, the present study looks at the subsequent alterations in mitochondrial quality control mechanisms in the impaired adult cardiomyocyte. We identified that Brg1/Brm double-mutant mice exhibited increased mitochondrial biogenesis, increases in 'mitophagy', and alterations in mitochondrial fission and fusion that led to small, fragmented mitochondria. Mechanistically, increases in the autophagy and mitophagy-regulated proteins Beclin1 and Bnip3 were identified, paralleling changes seen in human heart failure. Evidence for perturbed cardiac mitochondrial dynamics included decreased mitochondria size, reduced numbers of mitochondria, and an altered expression of genes regulating fusion (Mfn1, Opa1) and fission (Drp1). We also identified cardiac protein amyloid accumulation (aggregated fibrils) during disease progression along with an increase in pre-amyloid oligomers and an upregulated unfolded protein response including increased GRP78, CHOP, and IRE-1 signaling. Together, these findings described a role for BRG1 and BRM in mitochondrial quality control, by regulating mitochondrial number, mitophagy, and mitochondrial dynamics not previously recognized in the adult cardiomyocyte. As critical to the pathogenesis of heart failure, epigenetic mechanisms like SWI/SNF chromatin remodeling seem more intimately linked to cardiac function and mitochondrial quality control mechanisms than previously realized.
Copyright © 2016 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Autophagy; BRG1; BRM; CHOP; Cardiomyocyte; GRP78; IRE-1; Mitochondrial dynamics; Mitophagy; SWI/SNF complex; Unfolded protein response

Mesh:

Substances:

Year:  2016        PMID: 27039070      PMCID: PMC4860071          DOI: 10.1016/j.carpath.2016.02.004

Source DB:  PubMed          Journal:  Cardiovasc Pathol        ISSN: 1054-8807            Impact factor:   2.185


  73 in total

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2.  Fluorescent dye ProteoStat to detect and discriminate intracellular amyloid-like aggregates in Escherichia coli.

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3.  Quantitative Imaging of Preamyloid Oligomers, a Novel Structural Abnormality, in Human Atrial Samples.

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Journal:  J Histochem Cytochem       Date:  2014-04-30       Impact factor: 2.479

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Authors:  Gerald W Dorn
Journal:  J Cardiovasc Transl Res       Date:  2010-03-16       Impact factor: 4.132

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Authors:  David C Rubinsztein; Guillermo Mariño; Guido Kroemer
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6.  Altered control of cellular proliferation in the absence of mammalian brahma (SNF2alpha).

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7.  Avoidance of transient cardiomyopathy in cardiomyocyte-targeted tamoxifen-induced MerCreMer gene deletion models.

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8.  The chromatin remodeler ISWI regulates the cellular response to hypoxia: role of FIH.

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Journal:  Mol Biol Cell       Date:  2011-09-07       Impact factor: 4.138

Review 9.  Functional Amyloid Signaling via the Inflammasome, Necrosome, and Signalosome: New Therapeutic Targets in Heart Failure.

Authors:  Traci L Parry; Jason H Melehani; Mark J Ranek; Monte S Willis
Journal:  Front Cardiovasc Med       Date:  2015-05-19

10.  Impaired mitochondrial biogenesis is a common feature to myocardial hypertrophy and end-stage ischemic heart failure.

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Journal:  Cardiovasc Pathol       Date:  2015-09-30       Impact factor: 2.185

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  9 in total

1.  BRG1 and BRM function antagonistically with c-MYC in adult cardiomyocytes to regulate conduction and contractility.

Authors:  Monte S Willis; Darcy Wood Holley; Zhongjing Wang; Xin Chen; Megan Quintana; Brian C Jensen; Manasi Tannu; Joel Parker; Darwin Jeyaraj; Mukesh K Jain; Julie A Wolfram; Hyoung-Gon Lee; Scott J Bultman
Journal:  J Mol Cell Cardiol       Date:  2017-02-21       Impact factor: 5.000

2.  Brahma safeguards canalization of cardiac mesoderm differentiation.

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Review 3.  Current Understanding of the Pivotal Role of Mitochondrial Dynamics in Cardiovascular Diseases and Senescence.

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Review 4.  Mitochondrial-Shaping Proteins in Cardiac Health and Disease - the Long and the Short of It!

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Review 5.  Chromatin remodelling and epigenetic state regulation by non-coding RNAs in the diseased heart.

Authors:  F De Majo; M Calore
Journal:  Noncoding RNA Res       Date:  2018-03-02

Review 6.  The roles and mechanisms of epigenetic regulation in pathological myocardial remodeling.

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Review 7.  Epigenetics in heart failure phenotypes.

Authors:  Alexander Berezin
Journal:  BBA Clin       Date:  2016-05-30

Review 8.  Epigenetics in Cardiac Hypertrophy and Heart Failure.

Authors:  Chia-Feng Liu; W H Wilson Tang
Journal:  JACC Basic Transl Sci       Date:  2019-12-23

Review 9.  The Role of BRG1 in Antioxidant and Redox Signaling.

Authors:  Shilong You; Ying Zhang; Jiaqi Xu; Hao Qian; Shaojun Wu; Boquan Wu; Saien Lu; Yingxian Sun; Naijin Zhang
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  9 in total

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