AI Article Synopsis
- Type 1 diabetes (T1D) negatively impacts skeletal muscle health, particularly affecting muscle satellite cells (SCs), crucial for muscle growth and repair.
- Research on SCs from rodent (Akita) models and human subjects with T1D shows decreased SC density and functionality compared to healthy controls, along with increased muscle damage post-exercise.
- Persistent activation of the Notch signaling pathway in SCs from T1D samples contributes to these impairments and could be mitigated using a Notch inhibitor, highlighting the need for further study on SC function in T1D-induced muscle myopathy.
Article Abstract
Type 1 diabetes (T1D) negatively influences skeletal muscle health; however, its effect on muscle satellite cells (SCs) remains largely unknown. SCs from samples from rodents (Akita) and human subjects with T1D were examined to discern differences in SC density and functionality compared with samples from their respective control subjects. Examination of the Notch pathway was undertaken to investigate its role in changes to SC functionality. Compared with controls, Akita mice demonstrated increased muscle damage after eccentric exercise along with a decline in SC density and myogenic capacity. Quantification of components of the Notch signaling pathway revealed a persistent activation of Notch signaling in Akita SCs, which could be reversed with the Notch inhibitor DAPT. Similar to Akita samples, skeletal muscle from human subjects with T1D displayed a significant reduction in SC content, and the Notch ligand, DLL1, was significantly increased compared with control subjects, supporting the dysregulated Notch pathway observed in Akita muscles. These data indicate that persistent activation in Notch signaling impairs SC functionality in the T1D muscle, resulting in a decline in SC content. Given the vital role played by the SC in muscle growth and maintenance, these findings suggest that impairments in SC capacities play a primary role in the skeletal muscle myopathy that characterizes T1D.
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| http://dx.doi.org/10.2337/db15-1577 | DOI Listing |
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