Loss of ATG4B and ATG4A results in two-stage cell cycle defects in pancreatic ductal adenocarcinoma cells-Reference-Cited by-同舟云学术

Loss of ATG4B and ATG4A results in two-stage cell cycle defects in pancreatic ductal adenocarcinoma cells

Published:2023-10-01 Issue:19 Volume:136 Page:
ISSN:0021-9533
Container-title:Journal of Cell Science
language:en
Short-container-title:

Author:

Sathiyaseelan Paalini¹²,Chittaranjan Suganthi¹,Kalloger Steve E.³⁴⁵^ORCID,Chan Jennifer¹²,Go Nancy E.¹,Jardon Mario A.¹,Ho Cally J.¹²,Hui Theodore¹²,Xu Jing¹^ORCID,Chow Christine⁶^ORCID,Gao Dongxia⁶,Johnson Fraser D.¹⁷,Lockwood William W.³⁷,Morin Gregg B.¹⁸^ORCID,Renouf Daniel J.⁵⁹,Schaeffer David F.³⁵¹⁰,Gorski Sharon M.¹²⁸¹¹^ORCID

Affiliation:

1. , BC Cancer 1 Canada's Michael Smith Genome Sciences Centre , Vancouver, BC, V5Z 1L3 , Canada

2. Simon Fraser University 2 Department of Molecular Biology and Biochemistry , , Burnaby, BC, V5A 1S6 , Canada

3. University of British Columbia 3 Department of Pathology and Laboratory Medicine , , Vancouver, BC, V6T 2B5 , Canada

4. , University of British Columbia 4 School of Population and Public Health , Vancouver, BC V6T 1Z3 , Canada

5. Pancreas Centre BC 5 , Vancouver, BC, V5Z 1L8 , Canada

6. Genetic Pathology Evaluation Centre 6 , Vancouver, BC, V6H 3Z6 , Canada

7. BC Cancer 7 Department of Integrative Oncology , , Vancouver, BC, V5Z 1L3 , Canada

8. University of British Columbia 8 Department of Medical Genetics , , Vancouver, BC, V6H 3N1 , Canada

9. BC Cancer 9 Division of Medical Oncology , , Vancouver, BC, V5Z 4E6 , Canada

10. Vancouver General Hospital 10 Division of Anatomical Pathology , , Vancouver, BC, V5Z 1M9 , Canada

11. , Simon Fraser University 11 Centre for Cell Biology, Development and Disease , Burnaby, BC, V5A 1S6 , Canada

Abstract

ABSTRACT Pancreatic ductal adenocarcinoma (PDAC) exhibits elevated levels of autophagy, which promote tumor progression and treatment resistance. ATG4B is an autophagy-related cysteine protease under consideration as a potential therapeutic target, but it is largely unexplored in PDAC. Here, we investigated the clinical and functional relevance of ATG4B expression in PDAC. Using two PDAC patient cohorts, we found that low ATG4B mRNA or protein expression is associated with worse patient survival outcomes, poorly differentiated PDAC tumors and a lack of survival benefit from adjuvant chemotherapy. In PDAC cell lines, ATG4B knockout reduced proliferation, abolished processing of LC3B (also known as MAP1LC3B), and reduced GABARAP and GABARAPL1 levels, but increased ATG4A levels. ATG4B and ATG4A double knockout lines displayed a further reduction in proliferation, characterized by delays in G1-S phase transition and mitosis. Pro-LC3B accumulated aberrantly at the centrosome with a concomitant increase in centrosomal proteins PCM1 and CEP131, which was rescued by exogenous ATG4B. The two-stage cell cycle defects following ATG4B and ATG4A loss have important therapeutic implications for PDAC.

Funder

Pancreas Centre BC

Pancreatic Cancer Action Network

BC Cancer Foundation

Canadian Institutes of Health Research

Publisher

The Company of Biologists

Subject

Cell Biology

Link

https://journals.biologists.com/jcs/article-pdf/doi/10.1242/jcs.260644/3144773/jcs260644.pdf

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