Abstract

Atherosclerosis is the underlying cause of the majority of cardiovascular diseases including myocardial infarction, strokes, and heart failure leading to tremendous morbidity and mortality worldwide. Risk factor modification such as weight loss, reductions in hyperlipidemia and hypertension constitute the only preventive strategy available for this vexing disease. Thus, there is an active effort to identify the culprit cellular processes that provide mechanistic insight. Recent work by us and others has renewed interest in the role of the autophagy-lysosomal system in atherosclerosis. Various lines of evidence demonstrate a progressive dysfunction in the autophagy-lysosome system of plaque macrophages suggesting that attempts at reprogramming the degradative capacity of macrophages might be a fruitful therapeutic area. Our work with TFEB, the predominant transcription factor regulating autophagy-lysosomal biogenesis, shows that enhancing its function in macrophages leads to reductions in atherosclerosis. A critical TFEB target is the autophagy chaperone p62/SQSTM1 which mediates the removal of cytotoxic protein aggregates. Our work has shown that clearance of the p62-enriched cargo in macrophages is a novel therapeutic strategy.
In specific aim 1, we will determine the predominant p62-dependent autophagic processes in macrophages that underlie TFEB- mediated atheroprotection.
In specific aim 2, we explore the potential atheroprotective benefits of HSP104, a novel disaggregase system mostly studied in simple organisms. This approach will be complementary to the autophagy studies since it is a completely autophagy-independent mechanism of clearing macrophage protein aggregates. Overall, this proposal will test the hypothesis that harnessing the macrophage degradative response to clear protein aggregates can be a novel approach to treat atherosclerosis.

Public Health Relevance

Atherosclerotic vascular disease remains the leading cause of death in the United States with the majority of mortality due to coronary artery disease and myocardial infarction. Macrophages are primary cells that specialize in removing the excess lipids and other debris present in the atherosclerotic plaque. We have found that macrophages have the ability to augment their degradation machinery and when this response is stimulated genetically in mice, they have reduced atherosclerosis. We have also learned of a parallel degradation mechanism best described in simple organisms that can potentially be leveraged to clear excess debris in macrophages. Thus, we propose to evaluate the various mechanisms of stimulating the macrophage degradation machinery both in vitro and in vivo with the goal of developing a completely novel strategy of treating atherosclerosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL125838-06
Application #
10052352
Study Section
Atherosclerosis and Inflammation of the Cardiovascular System Study Section (AICS)
Program Officer
Chen, Jue
Project Start
2014-11-04
Project End
2025-06-30
Budget Start
2020-07-15
Budget End
2021-06-30
Support Year
6
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Zhang, Xiangyu; Evans, Trent D; Jeong, Se-Jin et al. (2018) Classical and alternative roles for autophagy in lipid metabolism. Curr Opin Lipidol 29:203-211
Sergin, Ismail; Evans, Trent D; Zhang, Xiangyu et al. (2017) Exploiting macrophage autophagy-lysosomal biogenesis as a therapy for atherosclerosis. Nat Commun 8:15750
Zhang, Hanrui; Shi, Jianting; Hachet, Melanie A et al. (2017) CRISPR/Cas9-Mediated Gene Editing in Human iPSC-Derived Macrophage Reveals Lysosomal Acid Lipase Function in Human Macrophages-Brief Report. Arterioscler Thromb Vasc Biol 37:2156-2160
Liu, Haiyan; Javaheri, Ali; Godar, Rebecca J et al. (2017) Intermittent fasting preserves beta-cell mass in obesity-induced diabetes via the autophagy-lysosome pathway. Autophagy 13:1952-1968
Fang, Liang; Hodge, Johnie; Saaoud, Fatma et al. (2017) Transcriptional factor EB regulates macrophage polarization in the tumor microenvironment. Oncoimmunology 6:e1312042
Mildenberger, Jennifer; Johansson, Ida; Sergin, Ismail et al. (2017) N-3 PUFAs induce inflammatory tolerance by formation of KEAP1-containing SQSTM1/p62-bodies and activation of NFE2L2. Autophagy 13:1664-1678
Lee, YouJin; Chou, Tsui-Fen; Pittman, Sara K et al. (2017) Keap1/Cullin3 Modulates p62/SQSTM1 Activity via UBA Domain Ubiquitination. Cell Rep 19:188-202
Lanza, Gregory M; Jenkins, John; Schmieder, Anne H et al. (2017) Anti-angiogenic Nanotherapy Inhibits Airway Remodeling and Hyper-responsiveness of Dust Mite Triggered Asthma in the Brown Norway Rat. Theranostics 7:377-389
Evans, Trent D; Sergin, Ismail; Zhang, Xiangyu et al. (2017) Target acquired: Selective autophagy in cardiometabolic disease. Sci Signal 10:
Sergin, Ismail; Bhattacharya, Somashubhra; Emanuel, Roy et al. (2016) Inclusion bodies enriched for p62 and polyubiquitinated proteins in macrophages protect against atherosclerosis. Sci Signal 9:ra2

Showing the most recent 10 out of 14 publications