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Open AccessJournal ArticleDOI

Increased Stiffness in Aged Skeletal Muscle Impairs Muscle Progenitor Cell Proliferative Activity

TLDR
Findings provide novel evidence that the low regenerative potential of aged skeletal muscle is independent of intrinsic MPC properties but is related to the increase in the stiffness of the MPC microenvironment.
Abstract
Background Skeletal muscle aging is associated with a decreased regenerative potential due to the loss of function of endogenous stem cells or myogenic progenitor cells (MPCs). Aged skeletal muscle is characterized by the deposition of extracellular matrix (ECM), which in turn influences the biomechanical properties of myofibers by increasing their stiffness. Since the stiffness of the MPC microenvironment directly impacts MPC function, we hypothesized that the increase in muscle stiffness that occurs with aging impairs the behavior of MPCs, ultimately leading to a decrease in regenerative potential. Results We showed that freshly isolated individual myofibers from aged mouse muscles contain fewer MPCs overall than myofibers from adult muscles, with fewer quiescent MPCs and more proliferative and differentiating MPCs. We observed alterations in cultured MPC behavior in aged animals, where the proliferation and differentiation of MPCs were lower and higher, respectively. These alterations were not linked to the intrinsic properties of aged myofibers, as shown by the similar values for the cumulative population-doubling values and fusion indexes. However, atomic force microscopy (AFM) indentation experiments revealed a nearly 4-fold increase in the stiffness of the MPC microenvironment. We further showed that the increase in stiffness is associated with alterations to muscle ECM, including the accumulation of collagen, which was correlated with higher hydroxyproline and advanced glycation end-product content. Lastly, we recapitulated the impaired MPC behavior observed in aging using a hydrogel substrate that mimics the stiffness of myofibers. Conclusions These findings provide novel evidence that the low regenerative potential of aged skeletal muscle is independent of intrinsic MPC properties but is related to the increase in the stiffness of the MPC microenvironment.

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Journal ArticleDOI

Changes in Regenerative Capacity through Lifespan.

TL;DR: A review of how regenerative abilities change through lifespan in various organisms, the factors that underlie such changes and the avenues for therapeutic intervention is provided in this article. But the review focuses on established models of mammalian regeneration as well as on models in which regenerative ability do not decline with age, as these can deliver valuable insights for our understanding of the interplay between regeneration and aging.
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Microcarriers for Upscaling Cultured Meat Production.

TL;DR: This paper aims to discuss the MCs' design criteria for skeletal muscle cell proliferation and subsequently for meat production based on three scenarios: one of which appears to be the most promising one for a production process, using an edible material can limit or completely eliminate dissociation/degradation/separation steps and even promote organoleptic qualities when embedded in the final product.
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Control of satellite cell function in muscle regeneration and its disruption in ageing.

TL;DR: The role and regulation of satellite cells in skeletal muscle homeostasis and regeneration is discussed in this paper, highlighting the cell-intrinsic control of quiescence versus activation, the importance of satellite cell-niche communication, and deregulation of these mechanisms associated with ageing.
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Mechanosensing of matrix by stem cells: From matrix heterogeneity, contractility, and the nucleus in pore-migration to cardiogenesis and muscle stem cells in vivo

TL;DR: This seminar-style review focuses on mechanosensing of matrix elasticity in the differentiation or early maturation of a few illustrative stem cell types, with an intended audience of biologists and physical scientists.
Journal ArticleDOI

Secondary Photocrosslinking of Click Hydrogels To Probe Myoblast Mechanotransduction in Three Dimensions

TL;DR: The ability of azadibenzocyclooctyne to undergo a cytocompatible, photoinitiated crosslinking reaction is reported, exploited as a strategy for on-demand stiffening of three-dimensional cell scaffolds formed through an initial strain-promoted azide-alkyne cycloaddition.
References
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Journal ArticleDOI

Tissue Cells Feel and Respond to the Stiffness of Their Substrate

TL;DR: An understanding of how tissue cells—including fibroblasts, myocytes, neurons, and other cell types—sense matrix stiffness is just emerging with quantitative studies of cells adhering to gels with which elasticity can be tuned to approximate that of tissues.
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Control of stem cell fate by physical interactions with the extracellular matrix.

TL;DR: Some of the physical processes by which cues from the ECM can influence stem cell fate are reviewed, with particular relevance to the use of stem cells in tissue engineering and regenerative medicine.
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Satellite Cells and the Muscle Stem Cell Niche

TL;DR: For the last half century, the advance of molecular biology, cell biology, and genetics has greatly improved the understanding of skeletal muscle biology, with focuses on functions of satellite cells and their niche during the process ofletal muscle regeneration.
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Substrate Elasticity Regulates Skeletal Muscle Stem Cell Self-Renewal in Culture

TL;DR: Using a bioengineered substrate to recapitulate key biophysical and biochemical niche features in conjunction with a highly automated single-cell tracking algorithm, it is shown that substrate elasticity is a potent regulator of MuSC fate in culture.
Journal ArticleDOI

Notch-Mediated Restoration of Regenerative Potential to Aged Muscle

TL;DR: Analysis of injured muscle revealed that, with age, resident precursor cells had a markedly impaired propensity to proliferate and to produce myoblasts necessary for muscle regeneration, and Notch signaling is a key determinant of muscle regenerative potential that declines with age.
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