Abstract

Protein kinase C (PKC) has been implicated in a number of cardiac functions, including regulation of the strength and rate of contraction and protection from hypoxia-induced cell death. We found that there are at least six different PKC isozymes in neonatal heart. These isozymes share long stretches of sequence homologies. In addition, each isozyme has unique sequences that are quite well conserved in evolution. It is therefore expected that individual PKC isozymes play specific roles in cardiac function and that the isozyme-unique sequences mediate this specificity. Our research has focused on identifying PKC isozyme-selective inhibitors. We have capitalized on observations that individual isozymes translocate to different subcellular sites following activation. We suggested that this isozyme-selective subcellular localization reflects the association of individual isozymes with their selective anchoring proteins, and that inhibition of isozyme translocation selectively inhibits the function mediated by each isozyme. To this end, we have designed translocation inhibitors that interfere with the association of each PKC isozyme and its selective anchoring protein. Recently, we have also identified activators of individual isozymes. We now have selective inhibitors for all the isozymes present in heart and selective activators for some of them. With the exception of one inhibitor, all were developed in our laboratory. In this proposal, we plan to apply these novel tools to identify the role of different PKC isozymes in cardiac functions that are altered in specific disease states. We will test a new working hypothesis that individual PKC isozymes have opposing effects in cardiac function. If correct, it may explain the current controversy in the field. Using isolated adult cells, intact heart and whole animal studies, we plan to determine the role of PKC isozymes in the response of cardiac myocytes and fibroblasts to hypoxia (AIM A) and in the regulation of chronotrophy (AIM B). We will also determine the role of PKC isozymes in the regulation of proliferation of cardiac fibroblasts (AIM C). Our published and preliminary data demonstrate the feasibility of these studies as well as our substantial progress in sorting out these complex events. Our overall goal is to relate these findings to human disease; identification of the individual PKC isozyme whose activity is required and sufficient to induce the tested cardiac function may reveal novel targets for therapy of heart diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL052141-06
Application #
6389354
Study Section
Pharmacology A Study Section (PHRA)
Program Officer
Reinlib, Leslie
Project Start
1996-04-05
Project End
2003-03-31
Budget Start
2001-04-01
Budget End
2002-03-31
Support Year
6
Fiscal Year
2001
Total Cost
$392,794
Indirect Cost

  Institution

Name
Stanford University
Department
Biology
Type
Schools of Medicine
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Deshwal, Soni; Forkink, Marleen; Hu, Chou-Hui et al. (2018) Monoamine oxidase-dependent endoplasmic reticulum-mitochondria dysfunction and mast cell degranulation lead to adverse cardiac remodeling in diabetes. Cell Death Differ 25:1671-1685
Kim, Jeewon; Chen, Che-Hong; Yang, Jieying et al. (2017) Aldehyde dehydrogenase 2*2 knock-in mice show increased reactive oxygen species production in response to cisplatin treatment. J Biomed Sci 24:33
Qvit, Nir; Kornfeld, Opher S; Mochly-Rosen, Daria (2017) Corrigendum: Engineered Substrate-Specific Delta PKC Antagonists to Enhance Cardiac Therapeutics. Angew Chem Int Ed Engl 56:2236
Campos, Juliane C; Queliconi, Bruno B; Bozi, Luiz H M et al. (2017) Exercise reestablishes autophagic flux and mitochondrial quality control in heart failure. Autophagy 13:1304-1317
Chang, Jeffrey S; Hsiao, Jenn-Ren; Chen, Che-Hong (2017) ALDH2 polymorphism and alcohol-related cancers in Asians: a public health perspective. J Biomed Sci 24:19
Ueta, Cintia B; Gomes, Katia S; Ribeiro, Márcio A et al. (2017) Disruption of mitochondrial quality control in peripheral artery disease: New therapeutic opportunities. Pharmacol Res 115:96-106
Qvit, Nir; Rubin, Samuel J S; Urban, Travis J et al. (2017) Peptidomimetic therapeutics: scientific approaches and opportunities. Drug Discov Today 22:454-462
Nene, Aishwarya; Chen, Che-Hong; Disatnik, Marie-Hélène et al. (2017) Aldehyde dehydrogenase 2 activation and coevolution of its ?PKC-mediated phosphorylation sites. J Biomed Sci 24:3
Cunningham, Anna D; Qvit, Nir; Mochly-Rosen, Daria (2017) Peptides and peptidomimetics as regulators of protein-protein interactions. Curr Opin Struct Biol 44:59-66
Chen, Che-Hong; Joshi, Amit U; Mochly-Rosen, Daria (2016) The Role of Mitochondrial Aldehyde Dehydrogenase 2 (ALDH2) in Neuropathology and Neurodegeneration. Acta Neurol Taiwan 25(4):111-123

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