Abstract

Regenerative potential is inextricably tied to youthfulness and declines with aging, prompting research into mechanisms of rejuvenation to enhance myocardial repair, particularly in the middle aged to elderly patients suffering from acute myocardial injury or chronic heart failure. Regenerative potential and cellular pluripotency is linked to regulation of the Lin28 / let-7 signaling axis, which is also associated with myocardial protection from pathologic injury. Lin28 is employed in this proposal to define a novel heterogeneous cardiac interstitial cell (CIC) population possessing youthful characteristics and enhanced functional competency. The Lin28 interstitial population (LIP) defies categorization as a specific cell type, consisting of a combinatorial mix used as a foundation to select for naturally occurring CICs with youthful phenotype. This proposal advances fundamental innovative principles of CIC and cardiac stem cell (CSC) biology by revealing a new conceptual approach to the problem of identifying, propagating, and deploying the most biologically active cells to effect reparative and regenerative processes. Implementation is facilitated by our expertise in working with fresh and cultured CICs from both murine and human sources coupled with our legacy of over a decade engaged in seminal CSC research. The long term goal of this proposal is to deliver novel insight regarding CIC biology that can be modified, enhanced, and altered to promote myocardial healing. The short term goal is to contextualize LIPs and their inherent Lin28 / let-7 signaling axis relative to CIC and CSC in pursuit of mitigating myocardial damage and enhancing reparative processes.
Specific Aims are: 1) LIPs are a cardiac interstitial cell population with distinct but heterogeneous phenotypic and functional signature 2) Lin28 expression and LIPs change in response to pathological injury as well as aging, 3) Derivation of LIP cultures resulting from in vitro expansion amplifies a subpopulation with phenotypic characteristics influenced by passage number and co- culture environment, and 4) Functional adaptation of LIPs depends upon and is regulated by the Lin28 / let-7 signaling axis. The innovation of this proposal is discovery and advancement of novel CIC biology through identification, characterization, and manipulation of a heterogeneous cell population coupled with a canonical regeneration-associated signaling axis to potentiate myocardial reparative processes. The significance of these studies is implementation of a marker that defines a novel CIC subset defined by pluripotent ?youthful? characteristics rather than traditional cell type-specific markers, advancing use of a combinatorial cell treatment approach defined by inherent population reparative potential rather than compartmentalized functional activity of any single cell category. These studies provide fundamental knowledge to generate novel hypotheses and approaches to enhance myocardial response to pathologic injury.

Public Health Relevance

Myocardial repair and regeneration is compromised by age and condition of the interstitial cells responsible for mediating responses to damage. These interstitial cells lose their ?youthfulness? over the passage of time and become functionally impaired. The goal of these studies is to identify the population of interstitial cells with preserved ?youthfulness? in the heart and develop novel approaches to rejuvenate old cardiac interstitial cells as a preclinical approach or treatment of heart failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL067245-15
Application #
9615659
Study Section
Cardiac Contractility, Hypertrophy, and Failure Study Section (CCHF)
Program Officer
Wong, Renee P
Project Start
2001-06-01
Project End
2022-05-31
Budget Start
2018-07-01
Budget End
2019-05-31
Support Year
15
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
San Diego State University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
073371346
City
San Diego
State
CA
Country
United States
Zip Code
92182

  Publications

Gude, Natalie A; Sussman, Mark A (2018) Chasing c-Kit through the heart: Taking a broader view. Pharmacol Res 127:110-115
Gude, Natalie A; Firouzi, Fareheh; Broughton, Kathleen M et al. (2018) Cardiac c-Kit Biology Revealed by Inducible Transgenesis. Circ Res 123:57-72
Kubli, Dieter A; Sussman, Mark A (2018) Editorial commentary: Mitochondrial autophagy in cardiac aging is all fluxed up. Trends Cardiovasc Med 28:261-262
Matsumoto, Collin; Jiang, Yan; Emathinger, Jacqueline et al. (2018) Short Telomeres Induce p53 and Autophagy and Modulate Age-Associated Changes in Cardiac Progenitor Cell Fate. Stem Cells 36:868-880
Broughton, Kathleen M; Wang, Bingyan J; Firouzi, Fareheh et al. (2018) Mechanisms of Cardiac Repair and Regeneration. Circ Res 122:1151-1163
Broughton, Kathleen M; Sussman, Mark A (2018) Enhancement Strategies for Cardiac Regenerative Cell Therapy: Focus on Adult Stem Cells. Circ Res 123:177-187
Eschenhagen, Thomas; Bolli, Roberto; Braun, Thomas et al. (2017) Cardiomyocyte Regeneration: A Consensus Statement. Circulation 136:680-686
Monsanto, Megan M; Wang, Bingyan J; Sussman, Mark A (2017) Synthetic MSC? Nothing Beats the Real Thing. Circ Res 120:1694-1695
Khalafalla, Farid G; Greene, Steven; Khan, Hashim et al. (2017) P2Y2 Nucleotide Receptor Prompts Human Cardiac Progenitor Cell Activation by Modulating Hippo Signaling. Circ Res 121:1224-1236
Fernández-Avilés, Francisco; Sanz-Ruiz, Ricardo; Climent, Andreu M et al. (2017) Global position paper on cardiovascular regenerative medicine. Eur Heart J 38:2532-2546

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