American Association for Cancer Research
00085472can123902-sup-fig7.pdf (38.51 kB)

Supplementary Figure 7 from Notch3 Functions as a Tumor Suppressor by Controlling Cellular Senescence

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journal contribution
posted on 2023-03-30, 21:33 authored by Hang Cui, Yahui Kong, Mei Xu, Hong Zhang

PDF file - 38K, Data showing the correlation between Notch3 and p21 expression in human breast cancer and melanoma samples.



Notch signaling regulates a broad spectrum of cell fate decisions and differentiation. Both oncogenic and tumor suppressor functions have been shown for Notch signaling. However, little is known about the underlying mechanisms of its tumor suppressor function. Here, we report that expression of Notch3, a member of Notch family transmembrane receptors, was elevated in human cells during senescence activated by various senescence-inducing stimuli. This upregulation of Notch3 was required for the induction of p21 expression in senescent cells. Downregulation of Notch3 led to a delayed onset of senescence and extended replicative lifespan, whereas adventitious expression of Notch3 was sufficient to activate senescence and p21 expression. The ability of Notch3 to induce senescence and p21 expression was dependent on the canonical Notch singling. Deletion of p21 in cells significantly attenuated Notch3-induced senescence. Furthermore, a significant decrease in Notch3 expression was observed in human tumor cell lines as well as primary human breast cancer and melanoma samples compared with normal tissues. Restoration of Notch3 expression in human tumor cells resulted in inhibition of cell proliferation and activation of senescence. Collectively, our results reveal a novel function of Notch3 in senescence regulation and tumor suppression. Cancer Res; 73(11); 3451–9. ©2013 AACR.

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