From the journal:

Chemical Science

Clinically used drug arsenic trioxide targets XIAP and overcomes apoptosis resistance in an organoid-based preclinical cancer model

Liwa Shi,ab   Jing Lu,abc   Xin Xia,ab   Xue Liu,ab   Hongyan Li,d   Xinghua Li,e   Jun Zhu, ORCID logo ab   Xiaofeng Li,*c   Hongzhe Sun ORCID logo *d  and  Xinming Yang ORCID logo *ab  

* Corresponding authors

a Guangdong Provincial Engineering Research Center of Molecular Imaging, The Fifth Affiliated Hospital, Sun Yat-sen University, Zhuhai, China
E-mail: yangxm57@mail.sysu.edu.cn

b Guangdong-Hong Kong-Macao University Joint Laboratory of Interventional Medicine, The Fifth Affiliated Hospital, Sun Yat-sen University, Zhuhai 519000, China

c Department of Gastroenterology, The Fifth Affiliated Hospital, Sun Yat-sen University, Zhuhai, China

d Department of Chemistry, CAS-HKU Joint Laboratory of Metallomics on Health and Environment, The University of Hong Kong, Hong Kong SAR, China
E-mail: hsun@hku.hk

e Department of Infectious Diseases, The Fifth Affiliated Hospital, Sun Yat-sen University, Zhuhai, China
E-mail: lixiaofeng@mail.sysu.edu.cn

Abstract

Drug resistance in tumor cells remains a persistent clinical challenge in the pursuit of effective anticancer therapy. XIAP, a member of the inhibitor of apoptosis protein (IAP) family, suppresses apoptosis via its Baculovirus IAP Repeat (BIR) domains and is responsible for drug resistance in various human cancers. Therefore, XIAP has attracted significant attention as a potential therapeutic target. However, no XIAP inhibitor is available for clinical use to date. In this study, we surprisingly observed that arsenic trioxide (ATO) induced a rapid depletion of XIAP in different cancer cells. Mechanistic studies revealed that arsenic attacked the cysteine residues of BIR domains and directly bound to XIAP, resulting in the release of zinc ions from this protein. Arsenic-XIAP binding suppressed the normal anti-apoptosis functions of BIR domains, and led to the ubiquitination-dependent degradation of XIAP. Importantly, we further demonstrate that arsenic sensitized a variety of apoptosis-resistant cancer cells, including patient-derived colon cancer organoids, to the chemotherapy drug using cisplatin as a showcase. These findings suggest that targeting XIAP with ATO offers an attractive strategy for combating apoptosis-resistant cancers in clinical practice.

Graphical abstract: Clinically used drug arsenic trioxide targets XIAP and overcomes apoptosis resistance in an organoid-based preclinical cancer model

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Article information

DOI
https://doi.org/10.1039/D4SC01294A
Article type
Edge Article
Submitted
24 Feb 2024
Accepted
29 Apr 2024
First published
03 May 2024
This article is Open Access

All publication charges for this article have been paid for by the Royal Society of Chemistry
Creative Commons BY-NC license

Chem. Sci., 2024, Advance Article

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Clinically used drug arsenic trioxide targets XIAP and overcomes apoptosis resistance in an organoid-based preclinical cancer model

L. Shi, J. Lu, X. Xia, X. Liu, H. Li, X. Li, J. Zhu, X. Li, H. Sun and X. Yang, Chem. Sci., 2024, Advance Article , DOI: 10.1039/D4SC01294A

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