N-Stearoyl-L-Tyrosine Inhibits the Senescence of Neural Stem/Progenitor Cells Induced by Aβ1–42via the CB2 Receptor

Author:

Li Wen-Qing1,Wang Ze-jian1,Liu Sha2,Hu Yue1,Yin Ming1,Lu Yang2

Affiliation:

1. School of Pharmacy, Shanghai Jiao Tong University, Shanghai 200240, China

2. Shanghai Jiao Tong University School of Medicine, Shanghai 200025, China

Abstract

Alzheimer’s disease, one of the neurodegenerative diseases, shows the progressive senescence of neural progenitor/stem cells. N-Stearoyl-L-tyrosine (NsTyr) showed neuroprotective effect against chronic brain ischemia in previous reports. In the present study, we find the antisenescent effects of NsTyr-2K in NSPCs induced by Aβ142in vitro. Cell viability of NSPCs was evaluated by CCK8 assay; SA-β-gal staining was used to evaluate senescence of NSPCs. CB receptors were detected by immunohistochemistry in NSPCs. AM251 or AM630 was used to offset the anti-senescence effects afforded by NsTyr-2K. The positive rate of SA-β-gal staining was significantly increased in NSPCs after incubation with Aβ142for 9 days. CB receptors were found on the surface of NSPCs. The expression level of CB1 receptors was significantly decreased in NSPCs after incubation with Aβ142. This phenomenon was reversed dose-dependently by NsTyr-2K. NsTyr-2K attenuated Aβ142induced NSPCs senescence dose-dependently, and its antisenescence effect was completely abolished by AM630. Aβ142dose-dependently increased the prosenescence molecules p16 and Rb. Their expression was inhibited by NsTyr-2K dose-dependently and blocked by AM630 in NSPCs. These results suggest that NsTyr-2K can alleviate the senescence of NSPCs induced by Aβ142via CB2 receptor.

Funder

Shanghai Jiao Tong University

Publisher

Hindawi Limited

Subject

Cell Biology,Molecular Biology

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