Tertiary lymphoid structures critical for prognosis in endometrial cancer patients

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作者
Nanda Horeweg
Hagma H. Workel
Dominik Loiero
David N. Church
Lisa Vermij
Alicia Léon-Castillo
Ricki T. Krog
Stephanie M. de Boer
Remi A. Nout
Melanie E. Powell
Linda R. Mileshkin
Helen MacKay
Alexandra Leary
Naveena Singh
Ina M. Jürgenliemk-Schulz
Vincent T. H. B. M. Smit
Carien L. Creutzberg
Viktor H. Koelzer
Hans W. Nijman
Tjalling Bosse
Marco de Bruyn
机构
[1] Leiden University Medical Center,Department of Radiation Oncology
[2] University Medical Center Groningen,Department of Gynaecologic Oncology
[3] University Hospital Zurich,Department of Pathology and Molecular Pathology
[4] University of Zurich,Wellcome Centre for Human Genetics
[5] University of Oxford,Oxford NIHR Comprehensive Biomedical Research Centre
[6] Oxford University Hospitals NHS Foundation Trust,Department of Pathology
[7] Leiden University Medical Center,Department Surgery
[8] Leiden University Medical Center,Department of Radiotherapy
[9] Erasmus MC Cancer Institute,Department of Clinical Oncology
[10] Barts Health NHS Trust,Department of Medical Oncology
[11] Peter MacCallum Cancer Centre,Division of Medical Oncology and Hematology
[12] Sunnybrook Odette Cancer Centre,Department of Medical Oncology
[13] Gustave Roussy,Department of Pathology
[14] Barts Health NHS Trust,Department of Radiation Oncology
[15] University Medical Center Utrecht,Department of Oncology and Nuffield Department of Medicine
[16] University of Oxford,undefined
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摘要
B-cells play a key role in cancer suppression, particularly when aggregated in tertiary lymphoid structures (TLS). Here, we investigate the role of B-cells and TLS in endometrial cancer (EC). Single cell RNA-sequencing of B-cells shows presence of naïve B-cells, cycling/germinal center B-cells and antibody-secreting cells. Differential gene expression analysis shows association of TLS with L1CAM overexpression. Immunohistochemistry and co-immunofluorescence show L1CAM expression in mature TLS, independent of L1CAM expression in the tumor. Using L1CAM as a marker, 378 of the 411 molecularly classified ECs from the PORTEC-3 biobank are evaluated, TLS are found in 19%. L1CAM expressing TLS are most common in mismatch-repair deficient (29/127, 23%) and polymerase-epsilon mutant EC (24/47, 51%). Multivariable Cox regression analysis shows strong favorable prognostic impact of TLS, independent of clinicopathological and molecular factors. Our data suggests a pivotal role of TLS in outcome of EC patients, and establishes L1CAM as a simple biomarker.
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