Integrated epidemiological and molecular data inform the relationship between precancer and cancer states of esophageal adenocarcinoma

Zamani, S.A.; Wu, L.; Black, E.L.; Bartram, A.; A. W. T., N.; Secrier, M.; Perelman, J.D.; Ustaoglu, A.; Ococks, E.; Jacobson, D.; Devonshire, G.; Grehan, N.; Nutzinger, B.; Freeman, A.; Miremadi, A.; O'Donovan, M.; Frankell, A.M.; Killcoyne, S.; Bartlett, F.; Petty, R.D.; Coleman, H.; Mcmanus, D.; Turkington, R.; Grabowska, A.; Moorthy, K.; Peters, C.J.; Hanna, G.B.; Lishman, S.; Sothi, S.; Scott, M.; Haidry, R.; Lovat, L.; Saunders, J.; Kaye, P.; Soomro, I.; Parsons, S.L.; Sreedharan, L.; Kumar, B.; Cheong, E.; Chan, D.; Berrisford, R.; Sanders, G.; Ciccarelli, F.D.; Goh, V.; Mahadeva, U.; Chang, F.; Davies, A.; Gossage, J.; Lagergren, J.; Grace, B.L.; Walker, R.C.; Underwood, T.J.; Contino, G.; Puig, S.; Taniere, P.; Beggs, A.; Tucker, O.; O'Neill, J.R.; Hupp, T.R.; Skipworth, R.J.E.; Save, V.; Bagwan, I.; Preston, S.R.; Sharrocks, A.; Ang, Y.; Hayes, S.J.; Sujendran, V.; Hindmarsh, A.; Safranek, P.; Hardwick, R.H.; Carroll, N.; Crichton, C.; Davies, J.; Jammula, S.; Secrier, M.; Eldridge, M.; Millington, C.; Coles, H.; Cheah, C.; Tripathi, M.; Malhotra, S.; Smyth, E.C.; Abbas, S.; Loreno, C.; Redmond, A.M.; Nutzinger, B.; Edwards, P.A.W.; Coleman, H.G.; Fitzgerald, R.C.

doi:10.1038/s41591-026-04331-8

Cancer generally takes years to evolve, and early diagnosis can prevent life-threatening cancer. Establishing a link between precancerous states and cancer is essential for effective screening and prevention. Esophageal adenocarcinoma (EAC) is an increasingly prevalent, poor-outcome cancer, and its presumed precursor, Barrett’s esophagus (BE), characterized by intestinal metaplasia, is evident in only about half of cases. Here to test whether BE is a prerequisite to EAC, we integrated epidemiological and clinical characteristics in a prospective cohort of 3,100 patients with EAC for any evidence of BE (BE-positive and BE-negative) and compared genomic features using a subset of 710 patients with whole-genome sequencing and 87 patients (380 samples) with multiregional whole-exome sequencing. Demographic and genomic features typically associated with BE were observed across BE-positive and BE-negative EAC cases. Notably, molecular features consistent with early BE evolution were detected in both phenotypes. Advanced tumor stage was the only variable that corresponded with increased likelihood of BE-negative EAC, including in some patients with a previous BE diagnosis. Phylogenetic analyses revealed shared evolutionary trajectories, and spatial transcriptomic and proteomic analyses demonstrated intestinal metaplasia-associated lineage markers in both groups. These findings suggest a single pathway to EAC, with implications for early diagnosis and prevention strategies.

Integrated epidemiological and molecular data inform the relationship between precancer and cancer states of esophageal adenocarcinoma / S.A. Zamani, L. Wu, E.L. Black, A. Bartram, A.W.T. Ng, M. Secrier, J.D. Perelman, A. Ustaoglu, E. Ococks, D. Jacobson, G. Devonshire, N. Grehan, B. Nutzinger, A. Freeman, A. Miremadi, M. O'Donovan, A.M. Frankell, S. Killcoyne, F. Bartlett, R.D. Petty, H. Coleman, D. Mcmanus, R. Turkington, A. Grabowska, K. Moorthy, C.J. Peters, G.B. Hanna, S. Lishman, S. Sothi, M. Scott, R. Haidry, L. Lovat, J. Saunders, P. Kaye, I. Soomro, S.L. Parsons, L. Sreedharan, B. Kumar, E. Cheong, D. Chan, R. Berrisford, G. Sanders, F.D. Ciccarelli, V. Goh, U. Mahadeva, F. Chang, A. Davies, J. Gossage, J. Lagergren, B.L. Grace, R.C. Walker, T.J. Underwood, G. Contino, S. Puig, P. Taniere, A. Beggs, O. Tucker, J.R. O'Neill, T.R. Hupp, R.J.E. Skipworth, V. Save, I. Bagwan, S.R. Preston, A. Sharrocks, Y. Ang, S.J. Hayes, V. Sujendran, A. Hindmarsh, P. Safranek, R.H. Hardwick, N. Carroll, C. Crichton, J. Davies, S. Jammula, M. Secrier, M. Eldridge, C. Millington, H. Coles, C. Cheah, M. Tripathi, S. Malhotra, E.C. Smyth, S. Abbas, C. Loreno, A.M. Redmond, B. Nutzinger, P.A.W. Edwards, H.G. Coleman, R.C. Fitzgerald. - In: NATURE MEDICINE. - ISSN 1078-8956. - 32:5(2026 Apr 16), pp. 1805-1816. [Epub ahead of print] [10.1038/s41591-026-04331-8]

Integrated epidemiological and molecular data inform the relationship between precancer and cancer states of esophageal adenocarcinoma

Wu L.^Secondo;Black E. L.;Bartram A.;Ng A. W. T.;Secrier M.;Perelman J. D.;Ustaoglu A.;Ococks E.;Jacobson D.;Devonshire G.;Grehan N.;Nutzinger B.;Freeman A.;Miremadi A.;O'Donovan M.;Frankell A. M.;Killcoyne S.;Bartlett F.;Petty R. D.;Coleman H.;McManus D.;Turkington R.;Grabowska A.;Moorthy K.;Peters C. J.;Hanna G. B.;Lishman S.;Sothi S.;Scott M.;Haidry R.;Lovat L.;Saunders J.;Kaye P.;Soomro I.;Parsons S. L.;Sreedharan L.;Kumar B.;Cheong E.;Chan D.;Berrisford R.;Sanders G.;F.D. Ciccarelli^{Membro del Collaboration Group};Goh V.;Mahadeva U.;Chang F.;Davies A.;Gossage J.;Lagergren J.;Grace B. L.;Walker R. C.;Underwood T. J.;G. Contino;Puig S.;Taniere P.;Beggs A.;Tucker O.;O'Neill J. R.;Hupp T. R.;Skipworth R. J. E.;Save V.;Bagwan I.;Preston S. R.;Sharrocks A.;Ang Y.;Hayes S. J.;Sujendran V.;Hindmarsh A.;Safranek P.;Hardwick R. H.;Carroll N.;Crichton C.;Davies J.;Jammula S.;Secrier M.;Eldridge M.;Millington C.;Coles H.;Cheah C.;Tripathi M.;Malhotra S.;Smyth E. C.;Abbas S.;Loreno C.;Redmond A. M.;Nutzinger B.;Edwards P. A. W.;Coleman H. G.^Penultimo;

2026

Abstract

Cancer generally takes years to evolve, and early diagnosis can prevent life-threatening cancer. Establishing a link between precancerous states and cancer is essential for effective screening and prevention. Esophageal adenocarcinoma (EAC) is an increasingly prevalent, poor-outcome cancer, and its presumed precursor, Barrett’s esophagus (BE), characterized by intestinal metaplasia, is evident in only about half of cases. Here to test whether BE is a prerequisite to EAC, we integrated epidemiological and clinical characteristics in a prospective cohort of 3,100 patients with EAC for any evidence of BE (BE-positive and BE-negative) and compared genomic features using a subset of 710 patients with whole-genome sequencing and 87 patients (380 samples) with multiregional whole-exome sequencing. Demographic and genomic features typically associated with BE were observed across BE-positive and BE-negative EAC cases. Notably, molecular features consistent with early BE evolution were detected in both phenotypes. Advanced tumor stage was the only variable that corresponded with increased likelihood of BE-negative EAC, including in some patients with a previous BE diagnosis. Phylogenetic analyses revealed shared evolutionary trajectories, and spatial transcriptomic and proteomic analyses demonstrated intestinal metaplasia-associated lineage markers in both groups. These findings suggest a single pathway to EAC, with implications for early diagnosis and prevention strategies.

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	Settori scientifico-disciplinari dell'articolo (validi dal 09/05/2024)
	
				Settore BIOS-08/A - Biologia molecolare
			
	Data di pubblicazione
	
				16-apr-2026
			
	Rivista in ANCE
	
				NATURE MEDICINE
			
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				https://dx.doi.org/10.1038/s41591-026-04331-8
			
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