The accumulation of damaged/senescent cells in the body with time is a hallmark of aging. Since these cells produce pro-inflammatory and pro-fibrotic molecules, they are believed to contribute to the onset and/or the severity of the chronic diseases that accompany old age. Based on this, the development of strategies to eliminate senescent cells for instance by using senolytics has opened new possibilities for anti-aging therapeutic development. Prior to the discovery of senolytic agents, evidence was provided that local or systemic transplantation of mesenchymal stem cells improve the outcome of various aging associated diseases. Although the underlying mechanism of their action is still not well defined, it is believed to be mediated by paracrine and immunomodulatory effects.

Here we set out to test the hypothesis that the combination of senolytics with mesenchymal stem cell transplantation will have a synergistic effect in extending mouse health span. In vitro and in vivo studies are underway to identify adequate biomarkers and imaging techniques to monitor response to the anti-aging interventions to be tested. We are also conducting cell-based analyses to select a senolytic candidate and to assess the quality and suitability of the MSC cells to be used in in vivo. Finding from this study will allow for evaluating the efficacy of candidate senolytics in reducing senescent cell burden in mice and whether their combination with stem cells will enhance health span of the treated animals.