4.5 Article

Strategies for late phase preclinical and early clinical trials of senolytics

Journal

MECHANISMS OF AGEING AND DEVELOPMENT
Volume 200, Issue -, Pages -

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.mad.2021.111591

Keywords

Senolytics; Fisetin; Dasatinib; Quercetin; Unitary Theory of Fundamental Aging; Processes; Translational Geroscience Network

Funding

  1. National Institutes of Health [R37 AG13925, R33 AG61456, R01 AG072301, R01 AG61414, P01 AG62413, UH3 AG56933]
  2. Connor Fund
  3. Noaber Foundation

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Accumulation of senescent cells is associated with various age-related and chronic diseases, making them potential targets for intervention. Preclinical and early clinical trials with senolytics have shown promising results, but more clinical trials are needed to further evaluate their efficacy across different aging and disease models.
Cellular senescence and the hallmarks of aging contribute to age-related disease and dysfunction. The Unitary Theory of Fundamental Aging Mechanisms highlights the interdependence among the hallmarks of aging and suggests that by intervening in one fundamental aging process, most or all of the other processes could be impacted. Accumulation of senescent cells is associated with frailty, cardiovascular disease, obesity, diabetes, cognitive decline, and other age- and/or chronic disease-related disorders, suggesting that senescent cells are a target for intervention. Early preclinical data using senolytics, agents that target senescent cells, show promising results in several aging and disease models. The first in-human trials using the senolytic combination of Dasatinib and Quercetin indicated reduced senescent cell burden in adipose tissue of diabetic kidney disease patients and improved physical function in patients with idiopathic pulmonary fibrosis. Clinical trials with other senolytics, including the flavonoid Fisetin and BCL-xL inhibitors, are underway. These results from preclinical and early clinical trials illustrate the potential of senolytics to alleviate age-related dysfunction and diseases. However, multiple clinical trials across different aging and disease models are desperately needed. Parallel trials across institutions through the Translational Geroscience Network are facilitating testing to determine whether senolytics can be translated into clinical application.

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