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  2. An autophagy-inducing stapled peptide induces mitochondria dysfunction and triggers autotic cell death in triple-negative breast cancer

An autophagy-inducing stapled peptide induces mitochondria dysfunction and triggers autotic cell death in triple-negative breast cancer

  • Cell Death Discov. 2023 Aug 19;9(1):303. doi: 10.1038/s41420-023-01600-0.
Xiaozhe Zhang 1 Gao Shan 1 Na Li 2 Jingyi Chen 1 Changyang Ji 3 Xiaoxiao Li 2 Liwen Jiang 3 Terence Kin Wah Lee 1 Vincent W Keng 1 Yanxiang Zhao 4 5
Affiliations

Affiliations

  • 1 Department of Applied Biology and Chemical Technology, State Key Laboratory of Chemical Biology and Drug Discovery, The Hong Kong Polytechnic University, Hung Hom, Kowloon, 999077, Hong Kong, P. R. China.
  • 2 The Hong Kong Polytechnic University Shenzhen Research Institute, 518057, Shenzhen, P. R. China.
  • 3 School of Life Sciences, Centre for Cell & Developmental Biology, State Key Laboratory of Agrobiotechnology, The Chinese University of Hong Kong, Shatin, New Territories, Hong Kong, China.
  • 4 Department of Applied Biology and Chemical Technology, State Key Laboratory of Chemical Biology and Drug Discovery, The Hong Kong Polytechnic University, Hung Hom, Kowloon, 999077, Hong Kong, P. R. China. yanxiang.zhao@polyu.edu.hk.
  • 5 The Hong Kong Polytechnic University Shenzhen Research Institute, 518057, Shenzhen, P. R. China. yanxiang.zhao@polyu.edu.hk.
Abstract

Autophagy is a lysosome-dependent bulk degradation process essential for cell viability but excessive Autophagy leads to a unique form of cell death termed autosis. Triple-negative breast Cancer (TNBC) is a highly aggressive subtype of breast Cancer with notable defect in its Autophagy process. In previous studies, we developed stapled Peptides that specifically targeted the essential Autophagy protein Beclin 1 to induce Autophagy and promote endolysosomal trafficking. Here we show that one lead peptide Tat-SP4 induced mild increase of Autophagy in TNBC cells but showed potent anti-proliferative effect that could not be rescued by inhibitors of programmed cell death pathways. The cell death induced by Tat-SP4 showed typical features of autosis including sustained adherence to the substrate surface, rupture of plasma membrane and effective rescue by digoxin, a cardioglycoside that blocks the Na+/K+ ATPase. Tat-SP4 also induced prominent mitochondria dysfunction including loss of mitochondria membrane potential, elevated mitochondria Reactive Oxygen Species and reduced Oxidative Phosphorylation. The anti-proliferative effect of Tat-SP4 was confirmed in a TNBC xenograft model. Our study uncovers three notable aspects of autosis. Firstly, autosis can be triggered by moderate increase in Autophagy if such increase exceeds the endogenous capacity of the host cells. Secondly, mitochondria may play an essential role in autosis with dysregulated Autophagy leading to mitochondria dysfunction to trigger autosis. Lastly, intrinsic Autophagy deficiency and quiescent mitochondria bioenergetic profile likely render TNBC cells particularly susceptible to autosis. Our designed Peptides like Tat-SP4 may serve as potential therapeutic candidates against TNBC by targeting this vulnerability.

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