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Book ChapterDOI

Methods for Observing and Quantifying Muscle Satellite Cell Motility and Invasion In Vitro.

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TLDR
Three protocols developed in the group for quantitatively analyzing satellite cell motility over time are described, which allow identification and longitudinal evaluation of individual cells over time and quantification of variations in motility due to intrinsic or extrinsic factors.
Abstract
Motility and/or chemotaxis of satellite cells has been suggested or observed in multiple in vitro and in vivo contexts. Satellite cell motility also affects the efficiency of muscle regeneration, particularly in the context of engrafted exogenous cells. Consequently, there is keen interest in determining what cell-autonomous and environmental factors influence satellite cell motility and chemotaxis in vitro and in vivo. In addition, the ability of activated satellite cells to relocate in vivo would suggest that they must be able to invade and transit through the extracellular matrix (ECM), which is supported by studies in which alteration or addition of matrix metalloprotease (MMP) activity enhanced the spread of engrafted satellite cells. However, despite its potential importance, analysis of satellite cell motility or invasion quantitatively even in an in vitro setting can be difficult; one of the most powerful techniques for overcoming these difficulties is timelapse microscopy. Identification and longitudinal evaluation of individual cells over time permits not only quantification of variations in motility due to intrinsic or extrinsic factors, it permits observation and analysis of other (frequently unsuspected) cellular activities as well. We describe here three protocols developed in our group for quantitatively analyzing satellite cell motility over time in two dimensions on purified ECM substrates, in three dimensions on a living myofiber, and in three dimensions through an artificial matrix.

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Book ChapterDOI

Muscle Stem Cells: A Model System for Adult Stem Cell Biology.

TL;DR: Background in the field is provided and recent advances in the understanding of muscle stem cell function and dysfunction are discussed, particularly in the case of aging, and the potential involvement of Muscle stem cells in genetic diseases such as the muscular dystrophies are discussed.
References
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Journal ArticleDOI

Migration of myoblasts across basal lamina during skeletal muscle development.

TL;DR: The results show that myoblasts from healthy fibres migrate across basal lamina during normal development and could contribute to the repair of fibres damaged by injury or disease.
Journal ArticleDOI

MOR23 promotes muscle regeneration and regulates cell adhesion and migration

TL;DR: A functional role for an OR outside of the nose is identified and a larger role for ORs during tissue repair is suggested, both during myogenesis and muscle regeneration.
Journal Article

Remodeling of Collagen Matrix by Human Tumor Cells Requires Activation and Cell Surface Association of Matrix Metalloproteinase-2

TL;DR: In this paper, the authors assessed the functional significance of tumor cell-associated matrix metalloproteinase (MMP)-2 in extracellular matrix remodeling compared with that of the soluble enzyme by evaluating the contraction of three-dimensional collagen lattices by human glioma U251.3 and fibrosarcoma HT-1080 cell lines.
Journal ArticleDOI

3D Timelapse Analysis of Muscle Satellite Cell Motility

TL;DR: Primary satellite cells are significantly more motile than myoblast cell lines, and that adhesion to laminin promotes primary cell motility more than fourfold over other substrates, suggesting that satellite cell migration in vivo may be more extensive than currently thought, and could be regulated by combinations of signals.
Journal ArticleDOI

Absence of exogenous satellite cell contribution to regeneration of frozen skeletal muscle.

TL;DR: This study demonstrates that regeneration of a muscle is primarily dependent upon the intrinsic satellite cell population, although under some circumstances recruitment of extrinsic cells is possible.
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