Deciphering the maturation of tertiary lymphoid structures in cancer and inflammatory diseases of the digestive tract using imaging mass cytometry

被引:18
作者
Le Rochais, Marion [1 ]
Hemon, Patrice [1 ]
Ben-guigui, Danivanh [1 ]
Garaud, Soizic [1 ]
Le Dantec, Christelle [1 ]
Pers, Jacques-Olivier [1 ,2 ]
Cornec, Divi [1 ,2 ]
Uguen, Arnaud [1 ,2 ]
机构
[1] Univ Brest, Unite Mixte Rech, Lymphocytes B Autoimmun & Immunotherapies LBAI, Inserm,UMR 51227, F-51227 Brest, France
[2] CHU Brest, Brest, France
来源
FRONTIERS IN IMMUNOLOGY | 2023年 / 14卷
关键词
tertiary lymphoid structures; imaging mass cytometry; Hyperion; cancer; inflammation; B-CELLS; IMMUNOTHERAPY; SURVIVAL; ORGAN;
D O I
10.3389/fimmu.2023.1147480
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Persistent inflammation can promote the development of tertiary lymphoid structures (TLS) within tissues resembling secondary lymphoid organs (SLO) such as lymph nodes (LN). The composition of TLS across different organs and diseases could be of pathophysiological and medical interest. In this work, we compared TLS to SLO in cancers of the digestive tract and in inflammatory bowel diseases. Colorectal and gastric tissues with different inflammatory diseases and cancers from the department of pathology of CHU Brest were analyzed based on 39 markers using imaging mass cytometry (IMC). Unsupervised and supervised clustering analyses of IMC images were used to compare SLO and TLS. Unsupervised analyses tended to group TLS per patient but not per disease. Supervised analyses of IMC images revealed that LN had a more organized structure than TLS and non-encapsulated SLO Peyer's patches. TLS followed a maturation spectrum with close correlations between germinal center (GC) markers' evolution. The correlations between organizational and functional markers made relevant the previously proposed TLS division into three stages: lymphoid-aggregates (LA) (CD20+CD21-CD23-) had neither organization nor GC functionality, non-GC TLS (CD20+CD21+CD23-) were organized but lacked GC's functionality and GC-like TLS (CD20+CD21+CD23+) had GC's organization and functionality. This architectural and functional maturation grading of TLS pointed to differences across diseases. TLS architectural and functional maturation grading is accessible with few markers allowing future diagnostic, prognostic, and predictive studies on the value of TLS grading, quantification and location within pathological tissues in cancers and inflammatory diseases.
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页数:12
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