Cancer-associated fibroblasts are associated with neo-adjuvant treatment response in oesophageal adenocarcinoma

Walker, R.C.; Breininger, S.P.; Sharpe, B.P.; Harrington, J.; Reddin, I.; Tse, C.; Rajak, R.; Hayden, A.; Rahman, S.; Grace, B.; Izadi, F.; West, J.; Fitzgerald, R.C.; Edwards, P.A.W.; Grehan, N.; Nutzinger, B.; Hughes, C.; Fidziukiewicz, E.; Macrae, S.; Northrop, A.; Xiaodun, L.; Katz-Summercorn, A.; Abbas, S.; O'Donovan, M.; Miremadi, A.; Malhotra, S.; Tripathi, M.; Smyth, E.; Tavaré, S.; Lynch, A.G.; Eldridge, M.; Secrier, M.; Devonshire, G.; Jammula, S.; Redmond, A.M.; Killcoyne, S.; Grantham, A.; Blasco, A.; Davies, J.; Crichton, C.; Carroll, N.; Safranek, P.; Hindmarsh, A.; Sujendran, V.; O'Neill, J.R.; Hayes, S.J.; Ang, Y.; Sharrocks, A.; Preston, S.R.; Oakes, S.; Bagwan, I.; Save, V.; Skipworth, R.J.E.; Hupp, T.R.; Tucker, O.; Beggs, A.; Taniere, P.; Puig, S.; Contino, G.; Grace, B.L.; Barr, H.; Shepherd, N.; Old, O.; Lagergren, J.; Gossage, J.; Davies, A.; Chang, F.; Zylstra, J.; Mahadeva, U.; Goh, V.; Ciccarelli, F.D.; Sanders, G.; Berrisford, R.; Harden, C.; Lewis, M.; Cheong, E.; Kumar, B.; Parsons, S.L.; Soomro, I.; Kaye, P.; Saunders, J.; Lovat, L.; Haidry, R.; Scott, M.; Sothi, S.; Suortamo, S.; Lishman, S.; Hanna, G.B.; Peters, C.J.; Moorthy, K.; Grabowska, A.; Turkington, R.; Mcmanus, D.; Coleman, H.; Khoo, D.; Fickling, W.; Crosby, T.D.L.; Petty, R.D.; Secrier, M.; Walters, Z.S.; Rose-Zerilli, M.J.J.; Underwood, T.J.

doi:10.1038/s41416-025-03080-8

Background: Neoadjuvant treatment (NAT) in oesophageal adenocarcinoma (EAC) is characterised by differential responses between patients and treatment modalities. The components of the tumour microenvironment (TME) that contribute to this are unknown. We explored this, focusing on cancer-associated fibroblasts (CAF) an abundant TME component. Methods: We performed histopathologic, single-cell RNA sequencing and transcriptomic analysis on 26 patients, stratified by pathological response to NAT, and validated a prognostic model in genomic consortia cohorts. Patient-derived cells were used to model CAF phenotypes in vitro. Results: We observed changes in the TME in response to the NAT received. Specific changes in fibroblasts correlated with treatment response and altered gene expression associated with NAT type. Three myofibroblastic phenotypes dominate the TME, two of which persist in non-responders and could only be partially re-capitulated in vitro using co-culture with cancer cells or TGF-β. A two-gene NAT fibrotic signature was an independent prognostic indicator in chemo/chemoradiotherapy treated patients (HR = 2.47, p = 0.029). Conclusions: This study provides a compendium of cell phenotypes in EAC across the current NAT treatment pathway that provides insights into CAF biology and cancer progression. MyoCAFs represent an axis to repurpose agents to enhance current therapies and immunotherapy. [OCCAMs Consortium]

Cancer-associated fibroblasts are associated with neo-adjuvant treatment response in oesophageal adenocarcinoma / R.C. Walker, S.P. Breininger, B.P. Sharpe, J. Harrington, I. Reddin, C. Tse, R. Rajak, A. Hayden, S. Rahman, B. Grace, F. Izadi, J. West, R.C. Fitzgerald, P.A.W. Edwards, N. Grehan, B. Nutzinger, C. Hughes, E. Fidziukiewicz, S. Macrae, A. Northrop, X. Li, A. Katz-Summercorn, S. Abbas, M. O'Donovan, A. Miremadi, S. Malhotra, M. Tripathi, E. Smyth, S. Tavaré, A.G. Lynch, M. Eldridge, M. Secrier, G. Devonshire, S. Jammula, A.M. Redmond, S. Killcoyne, A. Grantham, A. Blasco, J. Davies, C. Crichton, N. Carroll, P. Safranek, A. Hindmarsh, V. Sujendran, J.R. O'Neill, S.J. Hayes, Y. Ang, A. Sharrocks, S.R. Preston, S. Oakes, I. Bagwan, V. Save, R.J.E. Skipworth, T.R. Hupp, O. Tucker, A. Beggs, P. Taniere, S. Puig, G. Contino, B.L. Grace, H. Barr, N. Shepherd, O. Old, J. Lagergren, J. Gossage, A. Davies, F. Chang, J. Zylstra, U. Mahadeva, V. Goh, F.D. Ciccarelli, G. Sanders, R. Berrisford, C. Harden, M. Lewis, E. Cheong, B. Kumar, S.L. Parsons, I. Soomro, P. Kaye, J. Saunders, L. Lovat, R. Haidry, M. Scott, S. Sothi, S. Suortamo, S. Lishman, G.B. Hanna, C.J. Peters, K. Moorthy, A. Grabowska, R. Turkington, D. Mcmanus, H. Coleman, D. Khoo, W. Fickling, T.D.L. Crosby, R.D. Petty, M. Secrier, Z.S. Walters, M.J.J. Rose-Zerilli, T.J. Underwood. - In: BRITISH JOURNAL OF CANCER. - ISSN 0007-0920. - 133:5(2025 Sep 21), pp. 633-647. [10.1038/s41416-025-03080-8]

Cancer-associated fibroblasts are associated with neo-adjuvant treatment response in oesophageal adenocarcinoma

Walker, Robert C.;Breininger, Stella P.;Sharpe, Benjamin P.;Harrington, Jack;Reddin, Ian;Tse, Carmen;Rajak, Rushda;Hayden, Annette;Rahman, Saqib;Grace, Ben;Izadi, Fereshteh;West, Jonathan;Fitzgerald, Rebecca C.;Edwards, Paul A. W.;Grehan, Nicola;Nutzinger, Barbara;Hughes, Caitriona;Fidziukiewicz, Elwira;MacRae, Shona;Northrop, Alex;Li, Xiaodun;Katz-Summercorn, Annalise;Abbas, Sujath;O'Donovan, Maria;Miremadi, Ahmad;Malhotra, Shalini;Tripathi, Monika;Smyth, EC;Tavaré, Simon;Lynch, Andy G.;Eldridge, Matthew;Secrier, Maria;Devonshire, Ginny;Jammula, Sriganesh;Redmond, Aisling M.;Killcoyne, Sarah;Grantham, Amber;Blasco, Adrienn;Davies, Jim;Crichton, Charles;Carroll, Nick;Safranek, Peter;Hindmarsh, Andrew;Sujendran, Vijayendran;O'Neill, J. Robert;Hayes, Stephen J.;Ang, Yeng;Sharrocks, Andrew;Preston, Shaun R.;Oakes, Sarah;Bagwan, Izhar;Save, Vicki;Skipworth, Richard J. E.;Hupp, Ted R.;Tucker, Olga;Beggs, Andrew;Taniere, Philippe;Puig, Sonia;G. Contino;Grace, Ben L.;Barr, Hugh;Shepherd, Neil;Old, Oliver;Lagergren, Jesper;Gossage, James;Davies, Andrew;Chang, Fuju;Zylstra, Janine;Mahadeva, Ula;Goh, Vicky;F.D. Ciccarelli;Sanders, Grant;Berrisford, Richard;Harden, Catherine;Lewis, Mike;Cheong, Ed;Kumar, Bhaskar;Parsons, Simon L.;Soomro, Irshad;Kaye, Philip;Saunders, John;Lovat, Laurence;Haidry, Rehan;Scott, Michael;Sothi, Sharmila;Suortamo, Sari;Lishman, Suzy;Hanna, George B.;Peters, Christopher J.;Moorthy, Krishna;Grabowska, Anna;Turkington, Richard;McManus, Damian;Coleman, Helen;Khoo, David;Fickling, Will;Crosby, Tom D. L.;Petty, Russell D.;Secrier, Maria;Walters, Zoë S.;Rose-Zerilli, Matthew J. J.;Underwood, Timothy J.

2025

Abstract

Background: Neoadjuvant treatment (NAT) in oesophageal adenocarcinoma (EAC) is characterised by differential responses between patients and treatment modalities. The components of the tumour microenvironment (TME) that contribute to this are unknown. We explored this, focusing on cancer-associated fibroblasts (CAF) an abundant TME component. Methods: We performed histopathologic, single-cell RNA sequencing and transcriptomic analysis on 26 patients, stratified by pathological response to NAT, and validated a prognostic model in genomic consortia cohorts. Patient-derived cells were used to model CAF phenotypes in vitro. Results: We observed changes in the TME in response to the NAT received. Specific changes in fibroblasts correlated with treatment response and altered gene expression associated with NAT type. Three myofibroblastic phenotypes dominate the TME, two of which persist in non-responders and could only be partially re-capitulated in vitro using co-culture with cancer cells or TGF-β. A two-gene NAT fibrotic signature was an independent prognostic indicator in chemo/chemoradiotherapy treated patients (HR = 2.47, p = 0.029). Conclusions: This study provides a compendium of cell phenotypes in EAC across the current NAT treatment pathway that provides insights into CAF biology and cancer progression. MyoCAFs represent an axis to repurpose agents to enhance current therapies and immunotherapy. [OCCAMs Consortium]

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	Settori scientifico-disciplinari dell'articolo (validi dal 09/05/2024)
	
				Settore BIOS-08/A - Biologia molecolare
			
	Data di pubblicazione
	
				21-set-2025
			
	Data ahead of print o data di stampa
	
				10-lug-2025
			
	Rivista in ANCE
	
				BRITISH JOURNAL OF CANCER
			
	DOI
	
				https://dx.doi.org/10.1038/s41416-025-03080-8
			
	Tipologia
	
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				01 - Articolo su periodico

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