Mature tertiary lymphoid structures are key niches of tumour-specific immune responses in pancreatic ductal adenocarcinomas

Gabriela Sarti Kinker(AC Camargo Hospital), Glauco Akelinghton Freire Vitiello(AC Camargo Hospital), Ariane Barros Diniz(Hospital Israelita Albert Einstein), Mariela P. Cabral-Piccin(AC Camargo Hospital), Pedro Henrique Barbosa Pereira(AC Camargo Hospital), Maria Letícia Rodrigues Carvalho(AC Camargo Hospital), Wallax Augusto Silva Ferreira(AC Camargo Hospital), Alexandre Silva Chaves(AC Camargo Hospital), Amanda Rondinelli(AC Camargo Hospital), Arianne Fagotti Gusmão(AC Camargo Hospital), Alexandre Defelicibus(AC Camargo Hospital), Gabriel Oliveira dos Santos(AC Camargo Hospital), Warley Abreu Nunes(AC Camargo Hospital), Laura Carolina López Claro(Irmandade da Santa Casa de Misericórdia de São Paulo), Talita Magalhães Bernardo(Irmandade da Santa Casa de Misericórdia de São Paulo), Ricardo Tadashi Nishio(Irmandade da Santa Casa de Misericórdia de São Paulo), Adhemar Monteiro Pacheco(Irmandade da Santa Casa de Misericórdia de São Paulo), Ana Carolina Laus(Hospital de Câncer de Barretos), Lídia Maria Rebolho Batista Arantes(Hospital de Câncer de Barretos), Julia L. Fleck(Centre National de la Recherche Scientifique), Victor Hugo Fonseca de Jesus(AC Camargo Hospital), André de Moricz(Irmandade da Santa Casa de Misericórdia de São Paulo), Ricardo Weinlich(Hospital Israelita Albert Einstein), Felipe José Fernández Coimbra(AC Camargo Hospital), Vladmir Cláudio Cordeiro de Lima(AC Camargo Hospital), Tiago da Silva Medina(AC Camargo Hospital)
Gut
May 25, 2023
10.1136/gutjnl-2022-328697
Cited by 105

Abstract

Objective To better understand the immune microenvironment of pancreatic ductal adenocarcinomas (PDACs), here we explored the relevance of T and B cell compartmentalisation into tertiary lymphoid structures (TLSs) for the generation of local antitumour immunity. Design We characterised the functional states and spatial organisation of PDAC-infiltrating T and B cells using single-cell RNA sequencing (scRNA-seq), flow cytometry, multicolour immunofluorescence, gene expression profiling of microdissected TLSs, as well as in vitro assays. In addition, we performed a pan-cancer analysis of tumour-infiltrating T cells using scRNA-seq and sc T cell receptor sequencing datasets from eight cancer types. To evaluate the clinical relevance of our findings, we used PDAC bulk RNA-seq data from The Cancer Genome Atlas and the PRINCE chemoimmunotherapy trial. Results We found that a subset of PDACs harbours fully developed TLSs where B cells proliferate and differentiate into plasma cells. These mature TLSs also support T cell activity and are enriched with tumour-reactive T cells. Importantly, we showed that chronically activated, tumour-reactive T cells exposed to fibroblast-derived TGF-β may act as TLS organisers by producing the B cell chemoattractant CXCL13. Identification of highly similar subsets of clonally expanded CXCL13 + tumour-infiltrating T cells across multiple cancer types further indicated a conserved link between tumour-antigen recognition and the allocation of B cells within sheltered hubs in the tumour microenvironment. Finally, we showed that the expression of a gene signature reflecting mature TLSs was enriched in pretreatment biopsies from PDAC patients with longer survival after receiving different chemoimmunotherapy regimens. Conclusion We provided a framework for understanding the biological role of PDAC-associated TLSs and revealed their potential to guide the selection of patients for future immunotherapy trials.

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