Abstract

This Program Project Grant application challenges the accepted but never proven paradigm that the adult heart is a post-mitotic organ composed of an irreplaceable number of parenchymal cells, which is established at birth. The common theme of this proposal is based on the premise that the heart is a self renewing organ in which a stem cell compartment controls the physiologic turnover of cardiac cells and conditions myocardial aging and tissue regeneration in pathologic states. The long-term goal is the understanding of the origin and developmental control of cardiac stem cells (CSCs), their distribution in the heart and mechanisms of aging, the etiology of their death and senescence, and their therapeutic potential for the aged and aged-infarcted heart. The recognition that CSCs are present in the heart imposes a reconsideration of the various theories of cardiac development, maturation and, most importantly, myocardial aging. The notion that cardiomyocytes age at the same pace, and the age of the cells, organ and organism coincides is no longer acceptable and will be proven wrong by the interrelated studies to be performed in the five projects included in this application. We will try to ascertain the origin of CSCs and, more specifically, whether they are remnants of the embryonic cardiogenic plates that remain in the myocardium or whether they derive from the bone marrow and colonize the heart through the circulation and continuously replenish the CSC pool. The time-dependent decrease in the number of functionally competent CSCs mediated by critical shortening of telomeres and alterations of chromosomal proteins may result in CSC aging with forced entry into an irreversible state of quiescence. The complex process of stem cell senescence is expected to involve loss of locomotion, growth and differentiation, limiting cell turnover and expanding the population of old poorly functioning myocytes. Thus, CSC senescence leads to the old heart phenotype. If this were the case, genetic manipulation increasing the CSC pool and their survival should delay aging and the impairment in cardiac performance with time. The ability to activate and mobilize CSCs from the site of storage to areas of damage and promote myocardial regeneration may postpone the remodeling of the aged and aged-infarcted heart and the onset of terminal failure in the elderly. If successful, this research will make the impossible dream of myocardial regeneration a feasible reality.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG023071-03
Application #
7091414
Study Section
Special Emphasis Panel (ZAG1-ZIJ-2 (O1))
Program Officer
Kohanski, Ronald A
Project Start
2004-07-01
Project End
2009-06-30
Budget Start
2006-07-15
Budget End
2007-06-30
Support Year
3
Fiscal Year
2006
Total Cost
$1,922,579
Indirect Cost

  Institution

Name
New York Medical College
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
041907486
City
Valhalla
State
NY
Country
United States
Zip Code
10595

  Publications

Signore, Sergio; Sorrentino, Andrea; Borghetti, Giulia et al. (2015) Late Na(+) current and protracted electrical recovery are critical determinants of the aging myopathy. Nat Commun 6:8803
Leri, Annarosa; Rota, Marcello; Hosoda, Toru et al. (2014) Cardiac stem cell niches. Stem Cell Res 13:631-46
Sanada, Fumihiro; Kim, Junghyun; Czarna, Anna et al. (2014) c-Kit-positive cardiac stem cells nested in hypoxic niches are activated by stem cell factor reversing the aging myopathy. Circ Res 114:41-55
Signore, Sergio; Sorrentino, Andrea; Ferreira-Martins, João et al. (2014) Response to letter regarding article ""Inositol 1,4,5-trisphosphate receptors and human left ventricular myocytes"". Circulation 129:e510-1
Anversa, Piero; Leri, Annarosa (2013) Innate regeneration in the aging heart: healing from within. Mayo Clin Proc 88:871-83
Signore, Sergio; Sorrentino, Andrea; Ferreira-Martins, João et al. (2013) Inositol 1, 4, 5-trisphosphate receptors and human left ventricular myocytes. Circulation 128:1286-97
Goichberg, Polina; Kannappan, Ramaswamy; Cimini, Maria et al. (2013) Age-associated defects in EphA2 signaling impair the migration of human cardiac progenitor cells. Circulation 128:2211-23
Kajstura, Jan; Bai, Yingnan; Cappetta, Donato et al. (2012) Tracking chromatid segregation to identify human cardiac stem cells that regenerate extensively the infarcted myocardium. Circ Res 111:894-906
Anversa, Piero; Leri, Annarosa; Kajstura, Jan (2012) Biased DNA segregation during stem cell division. Circ Res 110:1403-7
Leri, Annarosa; Kajstura, Jan (2012) Created equal? The many facets of cell reprogramming. Circ Res 111:152-5

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