Platelet PD-L1 reflects collective intratumoral PD-L1 expression and predicts immunotherapy response in non-small cell lung cancer

Clemens Hinterleitner(University of Tübingen), Jasmin Strähle(University of Tübingen), Elke Malenke(University of Tübingen), Martina Hinterleitner(University of Tübingen), Melanie Henning(University of Tübingen), Marco Seehawer(University of Tübingen), Tatjana Bilich(German Cancer Research Center), Jonas S. Heitmann(German Cancer Research Center), Martina S. Lutz(German Cancer Research Center), Sven Mattern(University of Tübingen), Sophia Scheuermann(University of Tübingen), Marius Horger(University of Tübingen), Stefanie Maurer(Memorial Sloan Kettering Cancer Center), Juliane S. Walz(German Cancer Research Center), Falko Fend(University of Tübingen), Rupert Handgretinger(University of Tübingen), Christian Seitz(University of Tübingen), Bettina Weigelin(Siemens (Germany)), Stephan Singer(University of Tübingen), Helmut R. Salih(German Cancer Research Center), Oliver Borst(University of Tübingen), Hans‐Georg Kopp(Robert Bosch Hospital), Lars Zender(German Cancer Research Center)
Nature Communications
December 1, 2021
Cited by 164Open Access
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Abstract

Abstract Immune-checkpoint inhibitors (ICI) have transformed oncological therapy. Up to 20% of all non-small cell lung cancers (NSCLCs) show durable responses upon treatment with ICI, however, robust markers to predict therapy response are missing. Here we show that blood platelets interact with lung cancer cells and that PD-L1 protein is transferred from tumor cells to platelets in a fibronectin 1, integrin α5β1 and GPIbα-dependent manner. Platelets from NSCLC patients are found to express PD-L1 and platelet PD-L1 possess the ability to inhibit CD4 and CD8 T-cells. An algorithm is developed to calculate the activation independent adjusted PD-L1 payload of platelets (pPD-L1 Adj. ), which is found to be superior in predicting the response towards ICI as compared to standard histological PD-L1 quantification on tumor biopsies. Our data suggest that platelet PD-L1 reflects the collective tumor PD-L1 expression, plays important roles in tumor immune evasion and overcomes limitations of histological quantification of often heterogeneous intratumoral PD-L1 expression.


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