1. Academic Validation
  2. Targeted Degradation of XIAP is Sufficient and Specific to Induce Apoptosis in MYCN-overexpressing High-risk Neuroblastoma

Targeted Degradation of XIAP is Sufficient and Specific to Induce Apoptosis in MYCN-overexpressing High-risk Neuroblastoma

  • Cancer Res Commun. 2023 Nov 22;3(11):2386-2399. doi: 10.1158/2767-9764.CRC-23-0082.
Zhang'E Choo 1 2 Xiaoying Koh 3 Megan Rui En Wong 4 Ruth Minothini Ashokan 1 2 Nurul Suhana Binte Ali Ahamed 1 2 CongBao Kang 3 Chik Hong Kuick 5 Kenneth Tou En Chang 4 5 6 Sarit Larisch 7 Amos Hong Pheng Loh 4 6 7 8 Zhi Xiong Chen 1 2 4 9
Affiliations

Affiliations

  • 1 Department of Physiology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
  • 2 NUS Centre for Cancer Research, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
  • 3 Experimental Drug Development Centre, A*STAR, Singapore.
  • 4 VIVA-KKH Paediatric Brain and Solid Tumour Programme, Children's Blood and Cancer Centre, KK Women's and Children's Hospital, Singapore.
  • 5 Department of Pathology and Laboratory Medicine, KK Women's and Children's Hospital, Singapore.
  • 6 Duke NUS Medical School, Singapore.
  • 7 Cell Death and Cancer Research Laboratory, Department of Human Biology and Medical Sciences, University of Haifa, Haifa, Israel.
  • 8 Department of Paediatric Surgery, KK Women's and Children's Hospital, Singapore.
  • 9 National University Cancer Institute, Singapore, National University Health System, Singapore.
Abstract

XIAP, the most potent mammalian inhibitor of Apoptosis protein (IAP), critically restricts developmental culling of sympathetic neuronal progenitors, and is correspondingly overexpressed in most MYCN-amplified neuroblastoma tumors. Because apoptosis-related protein in the TGFβ signaling pathway (ARTS) is the only XIAP Antagonist that directly binds and degrades XIAP, we evaluated the preclinical effectiveness and tolerability of XIAP antagonism as a novel targeting strategy for neuroblastoma. We found that antagonism of XIAP, but not Other IAPs, triggered apoptotic death in neuroblastoma cells. XIAP silencing induced Apoptosis while overexpression conferred protection from drug-induced Apoptosis. From a screen of IAP inhibitors, first-in-class ARTS mimetic A4 was most effective against high-risk and high XIAP-expressing neuroblastoma cells, and least toxic toward normal liver- and bone marrow-derived cells, compared with pan-IAP antagonists. On target engagement assays and nuclear magnetic resonance spectroscopy, A4 was observed to degrade rather than inhibit XIAP, catalyzing rapid degradation of XIAP through the ubiquitin-proteasome pathway. In MYCN-amplified neuroblastoma patient-derived xenografts, A4 significantly prolonged survival as a single agent, and demonstrated synergism with standard-of-care agents to reduce their effective required doses 3- to 6-fold. Engagement and degradation of XIAP by ARTS mimetics is a novel targeting strategy for neuroblastoma that may be especially effective against MYCN-amplified disease with intrinsically high XIAP expression. First-in-class ARTS mimetic A4 demonstrates preclinical efficacy and warrants further development and study.

Significance: XIAP degradation is sufficient to kill MYCN-amplified neuroblastoma which overexpresses and relies on XIAP as a brake against cell death, without affecting normal cells.

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