B cell signatures and tertiary lymphoid structures contribute to outcome in head and neck squamous cell carcinoma

Ayana T. Ruffin(University of Pittsburgh), Anthony R. Cillo(University of Pittsburgh), Tracy Tabib(University of Pittsburgh), Angen Liu(University of Pittsburgh), Sayali Onkar(University of Pittsburgh), Sheryl Kunning(University of Pittsburgh), Caleb Lampenfeld(University of Pittsburgh), Huda I. Atiya(UPMC Hillman Cancer Center), Irina Abécassis(University of Pittsburgh), Cornelius Kürten(University of Duisburg-Essen), Zengbiao Qi(University of Pittsburgh), Ryan J. Soose(University of Pittsburgh), Umamaheswar Duvvuri(University of Pittsburgh), Seungwon Kim(University of Pittsburgh), Steffi Oesterrich(University of Pittsburgh), Robert Lafyatis(University of Pittsburgh), Lan Coffman(UPMC Hillman Cancer Center), Robert L. Ferris(University of Pittsburgh), Dario A.A. Vignali(University of Pittsburgh), Tullia C. Bruno(University of Pittsburgh)
Nature Communications
June 7, 2021
Cited by 357Open Access
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Abstract

Abstract Current immunotherapy paradigms aim to reinvigorate CD8 + T cells, but the contribution of humoral immunity to antitumor immunity remains understudied. Here, we demonstrate that in head and neck squamous cell carcinoma (HNSCC) caused by human papillomavirus infection (HPV + ), patients have transcriptional signatures of germinal center (GC) tumor infiltrating B cells (TIL-Bs) and spatial organization of immune cells consistent with tertiary lymphoid structures (TLS) with GCs, both of which correlate with favorable outcome. GC TIL-Bs in HPV + HNSCC are characterized by distinct waves of gene expression consistent with dark zone, light zone and a transitional state of GC B cells. Semaphorin 4a expression is enhanced on GC TIL-Bs present in TLS of HPV + HNSCC and during the differentiation of TIL-Bs. Our study suggests that therapeutics to enhance TIL-B responses in HNSCC should be prioritized in future studies to determine if they can complement current T cell mediated immunotherapies.


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