ISG20L1 acts as a co-activator of DAPK1 in the activation of the p53-dependent cell death pathway

Author:

Zou Shuxian12ORCID,Zhang Chongchong13ORCID,Xu Huan14ORCID,Liu Zhihui15ORCID,Hu Yongliang16ORCID,Wang Wei17ORCID,Liu Kun1,Wen Qing1ORCID,Song Lun1547ORCID

Affiliation:

1. Beijing Institute of Basic Medical Sciences 1 , 27 Taiping Road, Beijing 100850 , P. R. China

2. Guangxi Medical University 2 , 22 Shuangyong Road, Nanning 530021 , P. R. China

3. Henan University Joint National Laboratory for Antibody Drug Engineering, School of Medicine, Henan University 3 , 357 Ximen Road, Kaifeng 475004 , P. R. China

4. Anhui Medical University 4 , 81 Meishan Road, Hefei 230032 , P. R. China

5. College of Life Science, Henan Normal University 5 , 46 Jianshe Road, Xinxiang 473007 , P. R. China

6. The 309 Hospital of PLA 6 Department of Dermatology , , 17 Heishanhu Street, Beijing 100091 , P. R. China

7. School of Pharmacy, Jiamusi University 7 , Jiamusi 154007 , P. R. China

Abstract

ABSTRACT Our previous studies have revealed that GADD45α is a liable proapoptotic protein, which undergoes MDM2-dependent constitutive ubiquitylation and degradation in resting cancer cells. Under chemotherapeutic agent (such as arsenite, 5-Fu and VP-16) exposure, DAPK1 functions as a novel p53 (also known as TP53) kinase, which induces phosphorylation of p53 at Ser15 and transactivates the p53 target Ets-1, to synergistically repress IKKβ-dependent MDM2 stability, and ultimately removes the inhibitory effect of MDM2 on GADD45α, resulting in GADD45α accumulation and cell apoptosis. In the current study, we show that there is a strong induction of ISG20L1 (also known as AEN) expression in several cancer cell lines under exposure of arsenite and other chemotherapeutic agents. Surprisingly, although originally identified as a transcriptional target of p53, ISG20L1 induction was not controlled by p53. Instead, ISG20L1 functioned as upstream activator of p53 by interacting with DAPK1, and plays an essential role in promoting DAPK1–p53 complex formation and the subsequent activation of Ets-1/IKKβ/MDM2/GADD45α cascade. Therefore, our findings have revealed novel function of ISG20L1 in mediating cancer cell apoptosis induced by chemotherapeutic agents via modulating activation of the DAPK1- and p53-dependent cell death pathway.

Funder

Natural Science Foundation of Beijing Municipality

National Natural Science Foundation of China

Publisher

The Company of Biologists

Subject

Cell Biology

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