Integrative Biology

Biography

Biography: Hila Toledano

Abstract

Highly regenerative tissues are supported by rare populations of tissue-specific stem cells that continuously divide to both self-renew and generate differentiated progeny. Aging is characterized by aberrant tissue regeneration that is attributed to deteriorated function of stem and its surrounding cells; however it is not clear whether this process is genetically regulated. Heterochronic microRNAs (controlling the timing of events) were initially described to control the timing of developmental stages; however their role in the regulation of aging is just beginning to be studied. Previously we have linked the role of the heterochronic miRNA let-7 to the declined function of the germline stem cell in aged Drosophila males. Our recent findings indicate that the expression of the evolutionary conserved miR-9a increases significantly during aging in both stem and progenitor germ cells. We further show that miR-9a directly down regulates the levels of N-cadherin, which is required to enable stem cells detachment from the niche. Thus we conclude that miR-9a promotes differentiation and attenuates tissue degeneration. Characterizing the microRNA based posttranscriptional regulatory network and its temporal modulation is critical towards understanding the role of regulation in driving and responding to aging.