Literature DB >> 29078393

HSPB7 is indispensable for heart development by modulating actin filament assembly.

Tongbin Wu1, Yongxin Mu1, Julius Bogomolovas1,2, Xi Fang1, Jennifer Veevers1, Roberta B Nowak3, Christopher T Pappas4, Carol C Gregorio4, Sylvia M Evans1,5, Velia M Fowler3, Ju Chen6.   

Abstract

Small heat shock protein HSPB7 is highly expressed in the heart. Several mutations within HSPB7 are associated with dilated cardiomyopathy and heart failure in human patients. However, the precise role of HSPB7 in the heart is still unclear. In this study, we generated global as well as cardiac-specific HSPB7 KO mouse models and found that loss of HSPB7 globally or specifically in cardiomyocytes resulted in embryonic lethality before embryonic day 12.5. Using biochemical and cell culture assays, we identified HSPB7 as an actin filament length regulator that repressed actin polymerization by binding to monomeric actin. Consistent with HSPB7's inhibitory effects on actin polymerization, HSPB7 KO mice had longer actin/thin filaments and developed abnormal actin filament bundles within sarcomeres that interconnected Z lines and were cross-linked by α-actinin. In addition, loss of HSPB7 resulted in up-regulation of Lmod2 expression and mislocalization of Tmod1. Furthermore, crossing HSPB7 null mice into an Lmod2 null background rescued the elongated thin filament phenotype of HSPB7 KOs, but double KO mice still exhibited formation of abnormal actin bundles and early embryonic lethality. These in vivo findings indicated that abnormal actin bundles, not elongated thin filament length, were the cause of embryonic lethality in HSPB7 KOs. Our findings showed an unsuspected and critical role for a specific small heat shock protein in directly modulating actin thin filament length in cardiac muscle by binding monomeric actin and limiting its availability for polymerization. Published under the PNAS license.

Entities:  

Keywords:  HSPB7; actin polymerization; heart development; sarcomere; thin filament assembly

Mesh:

Substances:

Year:  2017        PMID: 29078393      PMCID: PMC5692592          DOI: 10.1073/pnas.1713763114

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  61 in total

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Review 2.  Large potentials of small heat shock proteins.

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4.  HSPB7 is the most potent polyQ aggregation suppressor within the HSPB family of molecular chaperones.

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Journal:  Hum Mol Genet       Date:  2010-09-15       Impact factor: 6.150

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6.  Roles for alphaB-crystallin and HSPB2 in protecting the myocardium from ischemia-reperfusion-induced damage in a KO mouse model.

Authors:  Lisa E Morrison; Ross J Whittaker; Robert E Klepper; Eric F Wawrousek; Christopher C Glembotski
Journal:  Am J Physiol Heart Circ Physiol       Date:  2003-10-30       Impact factor: 4.733

7.  Characterization and in vivo functional analysis of splice variants of cypher.

Authors:  Chengqun Huang; Qiang Zhou; Peihua Liang; Melinda S Hollander; Farah Sheikh; Xiaodong Li; Marion Greaser; G Diane Shelton; Sylvia Evans; Ju Chen
Journal:  J Biol Chem       Date:  2002-12-23       Impact factor: 5.157

8.  The human genome encodes 10 alpha-crystallin-related small heat shock proteins: HspB1-10.

Authors:  Guido Kappé; Erik Franck; Pauline Verschuure; Wilbert C Boelens; Jack A M Leunissen; Wilfried W de Jong
Journal:  Cell Stress Chaperones       Date:  2003       Impact factor: 3.667

9.  Mechanisms of thin filament assembly in embryonic chick cardiac myocytes: tropomodulin requires tropomyosin for assembly.

Authors:  C C Gregorio; V M Fowler
Journal:  J Cell Biol       Date:  1995-05       Impact factor: 10.539

10.  Nesprin 1α2 is essential for mouse postnatal viability and nuclear positioning in skeletal muscle.

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Journal:  J Cell Biol       Date:  2017-05-22       Impact factor: 10.539

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  24 in total

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Journal:  JCI Insight       Date:  2019-02-21

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3.  Filamin C Cardiomyopathy Variants Cause Protein and Lysosome Accumulation.

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Review 5.  The Cardiac Sarcomere and Cell Cycle.

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6.  PRDM16 Is a Compact Myocardium-Enriched Transcription Factor Required to Maintain Compact Myocardial Cardiomyocyte Identity in Left Ventricle.

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Review 7.  Understanding the molecular basis of cardiomyopathy.

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8.  Hspb7 is a cardioprotective chaperone facilitating sarcomeric proteostasis.

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9.  Maternal protein restriction changes structural and metabolic gene expression in the skeletal muscle of aging offspring rats.

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Journal:  Histol Histopathol       Date:  2021-04-12       Impact factor: 2.303

10.  SRARP and HSPB7 are epigenetically regulated gene pairs that function as tumor suppressors and predict clinical outcome in malignancies.

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