Microphysiological systems for human aging research

Author:

Park Seungman1ORCID,Laskow Thomas C.2ORCID,Chen Jingchun3ORCID,Guha Prasun34ORCID,Dawn Buddhadeb5,Kim Deok‐Ho267ORCID

Affiliation:

1. Department of Mechanical Engineering University of Nevada, Las Vegas Las Vegas Nevada USA

2. Department of Medicine Johns Hopkins University School of Medicine Baltimore Maryland USA

3. Nevada Institute of Personalized Medicine University of Nevada, Las Vegas Las Vegas Nevada USA

4. School of Life Sciences University of Nevada, Las Vegas Las Vegas Nevada USA

5. Department of Internal Medicine, Kirk Kerkorian School of Medicine University of Nevada, Las Vegas Las Vegas Nevada USA

6. Department of Biomedical Engineering Johns Hopkins University Baltimore Maryland USA

7. Center for Microphysiological Systems Johns Hopkins University Baltimore Maryland USA

Abstract

AbstractRecent advances in microphysiological systems (MPS), also known as organs‐on‐a‐chip (OoC), enable the recapitulation of more complex organ and tissue functions on a smaller scale in vitro. MPS therefore provide the potential to better understand human diseases and physiology. To date, numerous MPS platforms have been developed for various tissues and organs, including the heart, liver, kidney, blood vessels, muscle, and adipose tissue. However, only a few studies have explored using MPS platforms to unravel the effects of aging on human physiology and the pathogenesis of age‐related diseases. Age is one of the risk factors for many diseases, and enormous interest has been devoted to aging research. As such, a human MPS aging model could provide a more predictive tool to understand the molecular and cellular mechanisms underlying human aging and age‐related diseases. These models can also be used to evaluate preclinical drugs for age‐related diseases and translate them into clinical settings. Here, we provide a review on the application of MPS in aging research. First, we offer an overview of the molecular, cellular, and physiological changes with age in several tissues or organs. Next, we discuss previous aging models and the current state of MPS for studying human aging and age‐related conditions. Lastly, we address the limitations of current MPS and present future directions on the potential of MPS platforms for human aging research.

Funder

National Institutes of Health

Publisher

Wiley

Subject

Cell Biology,Aging

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