CAF hierarchy driven by pancreatic cancer cell p53-status creates a pro-metastatic and chemoresistant environment via perlecan

Claire Vennin; Pauline Mélénec; Romain Rouet; Max Nobis; Aurélie S Cazet; Kendelle J Murphy; David Herrmann; Daniel A Reed; Morghan C Lucas; Sean C Warren; Zehra Elgundi; Mark Pinese; Gabriella Kalna; Daniel Roden; Monisha Samuel; Anaiis Zaratzian; Shane T Grey; Andrew Da Silva; Wilfred Leung; Australian Pancreatic Genome Initiative (APGI); Suresh Mathivanan; Yingxiao Wang; Anthony W Braithwaite; Daniel Christ; Ales Benda; Ashleigh Parkin; Phoebe A Phillips; John M Whitelock; Anthony J Gill; Owen J Sansom; David R Croucher; Benjamin L Parker; Marina Pajic; Jennifer P Morton; Thomas R Cox; Paul Timpson

doi:10.1038/s41467-019-10968-6

CAF hierarchy driven by pancreatic cancer cell p53-status creates a pro-metastatic and chemoresistant environment via perlecan

Nat Commun. 2019 Aug 12;10(1):3637. doi: 10.1038/s41467-019-10968-6.

Authors

Claire Vennin^{1

2

3}, Pauline Mélénec^{1

2}, Romain Rouet^{1

2}, Max Nobis^{1

2}, Aurélie S Cazet^{1

2}, Kendelle J Murphy^{1

2}, David Herrmann^{1

2}, Daniel A Reed^{1

2}, Morghan C Lucas^{1

2}, Sean C Warren^{1

2}, Zehra Elgundi⁴, Mark Pinese^{1

2}, Gabriella Kalna⁵, Daniel Roden^{1

2}, Monisha Samuel⁶, Anaiis Zaratzian¹, Shane T Grey^{1

2}, Andrew Da Silva¹, Wilfred Leung^{1

2

7}; Australian Pancreatic Genome Initiative (APGI); Suresh Mathivanan⁶, Yingxiao Wang⁸, Anthony W Braithwaite^{9

10

11}, Daniel Christ^{1

2}, Ales Benda¹², Ashleigh Parkin^{1

2}, Phoebe A Phillips^{13

14}, John M Whitelock⁴, Anthony J Gill^{1

15

16

17}, Owen J Sansom⁵, David R Croucher^{1

2}, Benjamin L Parker¹⁸, Marina Pajic^{1

2}, Jennifer P Morton⁵, Thomas R Cox^{19

20}, Paul Timpson^{21

22}

Collaborators

Australian Pancreatic Genome Initiative (APGI):
Amber L Johns, Lorraine A Chantrill, Angela Chou, Angela Steinmann, Mehreen Arshi, Tanya Dwarte, Danielle Froio, Brooke Pereira, Shona Ritchie, Cecilia R Chambers, Xanthe Metcalf, Nicola Waddell, John V Pearson, Ann-Marie Patch, Katia Nones, Felicity Newell, Pamela Mukhopadhyay, Venkateswar Addala, Stephen Kazakoff, Oliver Holmes, Conrad Leonard, Scott Wood, Sean M Grimmond, Oliver Hofmann, Angelika Christ, Tim Bruxner, Jaswinder S Samra, Nick Pavlakis, Hilda A High, Ray Asghari, Neil D Merrett, Darren Pavey, Amitabha Das, Peter H Cosman, Kasim Ismail, Chelsie O'Connnor, Alina Stoita, David Williams, Allan Spigellman, Vincent W Lam, Duncan McLeod, Judy Kirk, James G Kench, Peter Grimison, Caroline L Cooper, Charbel Sandroussi, Annabel Goodwin, R Scott Mead, Katherine Tucker, Lesley Andrews, Michael Texler, Cindy Forest, Krishna P Epari, Mo Ballal, David R Fletcher, Sanjay Mukhedkar, Nikolajs Zeps, Maria Beilin, Kynan Feeney, Nan Q Nguyen, Andrew R Ruszkiewicz, Chris Worthley, John Chen, Mark E Brooke-Smith, Virginia Papangelis, Andrew D Clouston, Andrew P Barbour, Thomas J O'Rourke, Jonathan W Fawcett, Kellee Slater, Michael Hatzifotis, Peter Hodgkinson, Mehrdad Nikfarjam, James R Eshleman, Ralph H Hruban, Christopher L Wolfgang, Rita T Lawlor, Stefania Beghelli, Vincenzo Corbo, Maria Scardoni, Claudio Bassi, Andrew V Biankin, Judith Dixon, Nigel B Jamieson, David K Chang

Affiliations

¹ The Garvan Institute of Medical Research & The Kinghorn Cancer Centre, Sydney, NSW, 2010, Australia.
² St Vincent's Clinical School, Faculty of Medicine, University of New South Wales Sydney, Sydney, NSW, 2010, Australia.
³ Molecular Pathology department, the Netherlands Cancer Institute, Amsterdam, 1066CX, the Netherlands.
⁴ Graduate school of Biomedical Engineering, University of New South Wales Sydney, Sydney, NSW, 2052, Australia.
⁵ Cancer Research UK Beatson Institute, Glasgow Scotland, G61 BD, UK.
⁶ Department of Physiology, Anatomy and Microbiology, School of Life Sciences, La Trobe University, Bundoora, VIC, 3086, Australia.
⁷ Department of Biomedical Sciences, College of Veterinary Medicine, Cornell University, Ithaca, NY, 14853, USA.
⁸ Department of Bioengineering, Institute of Engineering in Medicine, University of California, San Diego, CA, 92121, USA.
⁹ Children's Medical Research Institute, University of Sydney, Sydney, NSW, 2006, Australia.
¹⁰ Department of Pathology, Dunedin School of Medicine, University of Otago, Dunedin, 9054, New Zealand.
¹¹ Maurice Wilkins Centre, University of Otago, Dunedin, 9054, New Zealand.
¹² Biomedical imaging facility, Lowy Cancer Research Centre, University of New South Wales, Sydney, NSW, Australia.
¹³ Pancreatic Cancer Translational Research Group, Lowy Cancer Research Centre, School of Medical Sciences, University of New South Wales, Sydney, NSW, 2052, Australia.
¹⁴ Australian Centre for Nanomedicine, University of New South Wales, Sydney, NSW, 2052, Australia.
¹⁵ Sydney Medical School, University of Sydney, Sydney, NSW, 2006, Australia.
¹⁶ NSW Health Pathology, Department of Anatomical Pathology, Royal North Shore Hospital, St Leonards, Sydney, NSW, 2065, Australia.
¹⁷ Cancer Diagnosis and Pathology Research Group, Kolling Institute of Medical Research, St Leonards, NSW, 2065, Australia.
¹⁸ Schools of Life and Environmental Sciences, the Charles Perkin Centre, the University of Sydney, Sydney, NSW, 2006, Australia.
¹⁹ The Garvan Institute of Medical Research & The Kinghorn Cancer Centre, Sydney, NSW, 2010, Australia. t.cox@garvan.org.au.
²⁰ St Vincent's Clinical School, Faculty of Medicine, University of New South Wales Sydney, Sydney, NSW, 2010, Australia. t.cox@garvan.org.au.
²¹ The Garvan Institute of Medical Research & The Kinghorn Cancer Centre, Sydney, NSW, 2010, Australia. p.timpson@garvan.org.au.
²² St Vincent's Clinical School, Faculty of Medicine, University of New South Wales Sydney, Sydney, NSW, 2010, Australia. p.timpson@garvan.org.au.

Abstract

Heterogeneous subtypes of cancer-associated fibroblasts (CAFs) coexist within pancreatic cancer tissues and can both promote and restrain disease progression. Here, we interrogate how cancer cells harboring distinct alterations in p53 manipulate CAFs. We reveal the existence of a p53-driven hierarchy, where cancer cells with a gain-of-function (GOF) mutant p53 educate a dominant population of CAFs that establish a pro-metastatic environment for GOF and null p53 cancer cells alike. We also demonstrate that CAFs educated by null p53 cancer cells may be reprogrammed by either GOF mutant p53 cells or their CAFs. We identify perlecan as a key component of this pro-metastatic environment. Using intravital imaging, we observe that these dominant CAFs delay cancer cell response to chemotherapy. Lastly, we reveal that depleting perlecan in the stroma combined with chemotherapy prolongs mouse survival, supporting it as a potential target for anti-stromal therapies in pancreatic cancer.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cancer-Associated Fibroblasts / pathology*
Cell Line, Tumor
Cell Movement
Cell Proliferation
Drug Resistance, Neoplasm / genetics*
Gene Expression Regulation, Neoplastic / genetics
Heparan Sulfate Proteoglycans / metabolism*
Mice
Mice, Inbred BALB C
Neoplasm Invasiveness / pathology
Pancreas / pathology
Pancreatic Neoplasms / genetics
Pancreatic Neoplasms / pathology*
Signal Transduction / physiology
Tumor Suppressor Protein p53 / genetics
Tumor Suppressor Protein p53 / metabolism*

Substances

Heparan Sulfate Proteoglycans
Trp53 protein, mouse
Tumor Suppressor Protein p53
perlecan

Abstract

Publication types

MeSH terms

Substances

Grants and funding