N-cadherin adhesive interactions modulate matrix mechanosensing and fate commitment of mesenchymal stem cells

被引:0
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作者
Brian D. Cosgrove
Keeley L. Mui
Tristan P. Driscoll
Steven R. Caliari
Kush D. Mehta
Richard K. Assoian
Jason A. Burdick
Robert L. Mauck
机构
[1] McKay Orthopaedic Research Laboratory,Department of Orthopaedic Surgery
[2] Perelman School of Medicine,Department of Bioengineering
[3] University of Pennsylvania,Department of Pharmacology
[4] University of Pennsylvania,undefined
[5] Translational Musculoskeletal Research Center,undefined
[6] Philadelphia VA Medical Center,undefined
[7] Perelman School of Medicine,undefined
[8] University of Pennsylvania,undefined
来源
Nature Materials | 2016年 / 15卷
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摘要
During mesenchymal development, the microenvironment gradually transitions from one that is rich in cell–cell interactions to one that is dominated by cell–ECM (extracellular matrix) interactions. Because these cues cannot readily be decoupled in vitro or in vivo, how they converge to regulate mesenchymal stem cell (MSC) mechanosensing is not fully understood. Here, we show that a hyaluronic acid hydrogel system enables, across a physiological range of ECM stiffness, the independent co-presentation of the HAVDI adhesive motif from the EC1 domain of N-cadherin and the RGD adhesive motif from fibronectin. Decoupled presentation of these cues revealed that HAVDI ligation (at constant RGD ligation) reduced the contractile state and thereby nuclear YAP/TAZ localization in MSCs, resulting in altered interpretation of ECM stiffness and subsequent changes in downstream cell proliferation and differentiation. Our findings reveal that, in an evolving developmental context, HAVDI/N-cadherin interactions can alter stem cell perception of the stiffening extracellular microenvironment.
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页码:1297 / 1306
页数:9
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