Abstract

A well-patterned and functioning heart is required for the growth and survival of embryos. While many genes critical for early cardiogenesis have been identified by previous genetic studies, genetic networks required for establishing and maintaining embryonic cardiac function remain to be explored. We have previously shown that calcium homeostasis has an important role in maintaining embryonic cardiac rhythmicity in zebrafish and that loss of function of NCX1h, one of the primary molecules responsible for calcium extrusion in the heart, abolishes synchronized cardiac contraction and leads to chaotic cardiac movements known as cardiac fibrillation. Consistent with the role of NCX1 in calcium homeostasis, we observed abnormal calcium transients in NCX1h null zebrafish embryonic hearts. These observations suggest that the NCX1h mutant zebrafish can serve as a tool for studying the calcium- regulatory networks important for embryonic cardiac function. From a chemical-based suppression screen on the zebrafish tremblor/NCX1h genetic model, we identified a critical component of the gene network governing embryonic cardiac function. We discovered that OK-F7, a novel small molecule suppresses cardiac fibrillation in the tremblor/NCX1 null genetic background, and our biochemical study indicated that the mitochondrial protein VDAC2 is the protein target of OK-F7. Furthermore, over expression of VDAC2 restores rhythmic cardiac contractions in embryos lacking NCX1h activity, suggesting a critical role for VDAC2 and mitochondria in calcium regulation and embryonic cardiac rhythmicity. As the first step toward understanding the role for VDAC2 in embryonic cardiac rhythmicity, we propose to evaluate the requirement of VDAC2 in cardiac development by both gain-of-function and loss-of-function approaches (Aim1). Second, to understand how the interaction of OK-F7 and VDAC modulates calcium homeostasis, we propose to evaluate whether OK-F7 treatment changes VDAC2 channel activity. We will also investigate the impact of OK-F7 on mitochondrial calcium influx. Information obtained from this line of study will provide insight into the mechanism by which OK-F7 and VDAC2 suppress cardiac fibrillation (Aim2). Finally, we will investigate whether OK-F7 treatment can restore rhythmic calcium waves in tremblor and other zebrafish embryos that have calcium-handling defects. We will also determine whether forced expression of other VDAC proteins can restore rhythmic cardiac contractions in embryos lacking NCX1h activity. The success of this line of study will further our understanding of the role for VDAC proteins in embryonic cardiac rhythmicity at the molecular level (Aim3). Our overall goal of this research program is to gain insight into gene networks important for calcium homeostasis and embryonic cardiac rhythmicity through multi-disciplinary studies. Information obtained from this research program will reveal previously unrecognized roles for VDAC and mitochondria in embryonic cardiac function.

Public Health Relevance

Cardiac fibrillation is a form of cardiac arrhythmia that poses serious health threats. We hypothesize that the fundamental mechanisms regulating cardiac rhythmicity are conserved among vertebrates and that the zebrafish tremblor mutant can serve as a good animal model for cardiac fibrillation. The studies in this proposal will help elucidate cellular and molecular mechanisms underlying cardiac fibrillation and ultimately contribute to the development of new preventive and therapeutic approaches.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL096980-01A1
Application #
7889281
Study Section
Cardiovascular Differentiation and Development Study Section (CDD)
Program Officer
Kaltman, Jonathan R
Project Start
2010-04-15
Project End
2014-02-28
Budget Start
2010-04-15
Budget End
2011-02-28
Support Year
1
Fiscal Year
2010
Total Cost
$368,316
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Biochemistry
Type
Schools of Arts and Sciences
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Lu, Fei; Langenbacher, Adam; Chen, Jau-Nian (2017) Tbx20 drives cardiac progenitor formation and cardiomyocyte proliferation in zebrafish. Dev Biol 421:139-148
Shimizu, Hirohito; Langenbacher, Adam D; Huang, Jie et al. (2017) The Calcineurin-FoxO-MuRF1 signaling pathway regulates myofibril integrity in cardiomyocytes. Elife 6:
Lu, Fei; Langenbacher, Adam D; Chen, Jau-Nian (2016) Transcriptional Regulation of Heart Development in Zebrafish. J Cardiovasc Dev Dis 3:
Gao, Chen; Ren, Shuxun; Lee, Jae-Hyung et al. (2016) RBFox1-mediated RNA splicing regulates cardiac hypertrophy and heart failure. J Clin Invest 126:195-206
Shimizu, Hirohito; Schredelseker, Johann; Huang, Jie et al. (2015) Mitochondrial Ca(2+) uptake by the voltage-dependent anion channel 2 regulates cardiac rhythmicity. Elife 4:
Cavanaugh, Ann M; Huang, Jie; Chen, Jau-Nian (2015) Two developmentally distinct populations of neural crest cells contribute to the zebrafish heart. Dev Biol 404:103-12
Zhang, Yixuan; Shimizu, Hirohito; Siu, Kin Lung et al. (2014) NADPH oxidase 4 induces cardiac arrhythmic phenotype in zebrafish. J Biol Chem 289:23200-8
Lin, Chuwen; Yao, Erica; Wang, Kevin et al. (2014) Regulation of Sufu activity by p66? and Mycbp provides new insight into vertebrate Hedgehog signaling. Genes Dev 28:2547-63
Monte, Emma; Mouillesseaux, Kevin; Chen, Haodong et al. (2013) Systems proteomics of cardiac chromatin identifies nucleolin as a regulator of growth and cellular plasticity in cardiomyocytes. Am J Physiol Heart Circ Physiol 305:H1624-38
Langenbacher, Adam D; Huang, Jie; Chen, Yi et al. (2012) Sodium pump activity in the yolk syncytial layer regulates zebrafish heart tube morphogenesis. Dev Biol 362:263-70

Showing the most recent 10 out of 15 publications