Age-Related Changes in Speed and Mechanism of Adult Skeletal Muscle Stem Cell Migration

Author:

Collins-Hooper Henry1,Woolley Thomas E.2,Dyson Louise2,Patel Anand1,Potter Paul3,Baker Ruth E.2,Gaffney Eamonn A.2,Maini Philip K.2,Dash Philip R.1,Patel Ketan1

Affiliation:

1. School of Biological Sciences, University of Reading, Reading, United Kingdom

2. Centre for Mathematical Biology, Mathematical Institute, University of Oxford, Oxford, United Kingdom

3. MRC Harwell, Oxfordshire, United Kingdom

Abstract

Abstract Skeletal muscle undergoes a progressive age-related loss in mass and function. Preservation of muscle mass depends in part on satellite cells, the resident stem cells of skeletal muscle. Reduced satellite cell function may contribute to the age-associated decrease in muscle mass. Here, we focused on characterizing the effect of age on satellite cell migration. We report that aged satellite cells migrate at less than half the speed of young cells. In addition, aged cells show abnormal membrane extension and retraction characteristics required for amoeboid-based cell migration. Aged satellite cells displayed low levels of integrin expression. By deploying a mathematical model approach to investigate mechanism of migration, we have found that young satellite cells move in a random “memoryless” manner, whereas old cells demonstrate superdiffusive tendencies. Most importantly, we show that nitric oxide, a key regulator of cell migration, reversed the loss in migration speed and reinstated the unbiased mechanism of movement in aged satellite cells. Finally, we found that although hepatocyte growth factor increased the rate of aged satellite cell movement, it did not restore the memoryless migration characteristics displayed in young cells. Our study shows that satellite cell migration, a key component of skeletal muscle regeneration, is compromised during aging. However, we propose clinically approved drugs could be used to overcome these detrimental changes. Disclosure of potential conflicts of interest is found at the end of this article.

Funder

BBSRC

Natural Biosciences

Systems Biology Laboratory

Royal Society Wolfson Research Merit Award

EPSRC

British Heart Foundation

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,Molecular Medicine

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