Immune checkpoints are predominantly co-expressed by clonally expanded CD4 + FoxP3 + intratumoral T-cells in primary human cancers.
Delphine BredelEdi TihicSéverine MouraudFrançois-Xavier DanlosSandrine SusiniMarine AglaveAlexia AlfaroChifaou Mohamed-DjalimMathieu RouanneHéloise HalseAmélie BigorgneLambros TselikasStéphane DalleDana M HartlEric BaudinCatherine GuettierEric VibertOlivier RosmorducCaroline RobertSophie FerlicotBastien ParierLaurence AlbigesVincent Thomas de MontprevilleBenjamin BesseOlaf MercierCaroline EvenIngrid BreuskinMarion ClasseCamélia RadulescuThierry LebretPatricia PautierSébastien GouyJean-Yves ScoazecLaurence ZitvogelAurélien MarabelleMélodie BonvaletPublished in: Journal of experimental & clinical cancer research : CR (2023)
Tumor histology alone does not reveal the complete picture of the tumor immune contexture. In clinical trials, assumptions regarding target expression should rely on more sensitive and specific techniques than conventional IHC or transcriptomics. Flow cytometry and scRNAseq accurately characterize ICP expression within immune cell subsets. Much like in hematology, flow cytometry can better describe the immune contexture of solid tumors, offering the opportunity to guide patient treatment according to drug target expression rather than tumor histological type.