| Literature DB >> 26084806 |
Gaurav Kaushik1, Alice Spenlehauer1, Ayla O Sessions2, Adriana S Trujillo3, Alexander Fuhrmann1, Zongming Fu4, Vidya Venkatraman5, Danielle Pohl1, Jeremy Tuler1, Mingyi Wang6, Edward G Lakatta6, Karen Ocorr7, Rolf Bodmer7, Sanford I Bernstein3, Jennifer E Van Eyk8, Anthony Cammarato9, Adam J Engler10.
Abstract
The human heart is capable of functioning for decades despite minimal cell turnover or regeneration, suggesting that molecular alterations help sustain heart function with age. However, identification of compensatory remodeling events in the aging heart remains elusive. We present the cardiac proteomes of young and old rhesus monkeys and rats, from which we show that certain age-associated remodeling events within the cardiomyocyte cytoskeleton are highly conserved and beneficial rather than deleterious. Targeted transcriptomic analysis in Drosophila confirmed conservation and implicated vinculin as a unique molecular regulator of cardiac function during aging. Cardiac-restricted vinculin overexpression reinforced the cortical cytoskeleton and enhanced myofilament organization, leading to improved contractility and hemodynamic stress tolerance in healthy and myosin-deficient fly hearts. Moreover, cardiac-specific vinculin overexpression increased median life span by more than 150% in flies. A broad array of potential therapeutic targets and regulators of age-associated modifications, specifically for vinculin, are presented. These findings suggest that the heart has molecular mechanisms to sustain performance and promote longevity, which may be assisted by therapeutic intervention to ameliorate the decline of function in aging patient hearts.Entities:
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Year: 2015 PMID: 26084806 PMCID: PMC4507505 DOI: 10.1126/scitranslmed.aaa5843
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956