Pan-neuronal maturation but not neuronal subtype differentiation of adult neural stem cells is mechanosensitive

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作者
Albert J. Keung
Meimei Dong
David V. Schaffer
Sanjay Kumar
机构
[1] University of California,Department of Chemical and Biomolecular Engineering
[2] University of California,Department of Bioengineering
[3] University of California,Helen Wills Neuroscience Institute
[4] Mannheim University of Applied Sciences,Department of Biomedical Engineering
[5] Boston University,Biophysics Graduate Group
[6] University of California,undefined
[7] University of California,undefined
[8] Berkeley,undefined
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Most past studies of the biophysical regulation of stem cell differentiation have focused on initial lineage commitment or proximal differentiation events. It would be valuable to understand whether biophysical inputs also influence distal endpoints more closely associated with physiological function, such as subtype specification in neuronal differentiation. To explore this question, we cultured adult neural stem cells (NSCs) on variable stiffness ECMs under conditions that promote neuronal fate commitment for extended time periods to allow neuronal subtype differentiation. We find that ECM stiffness does not modulate the expression of NeuroD1 and TrkA/B/C or the percentages of pan-neuronal, GABAergic, or glutamatergic neuronal subtypes. Interestingly, however, an ECM stiffness of 700 Pa maximizes expression of pan-neuronal markers. These results suggest that a wide range of stiffnesses fully permit pan-neuronal NSC differentiation, that an intermediate stiffness optimizes expression of pan-neuronal genes and that stiffness does not impact commitment to particular neuronal subtypes.
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