Tissue-resident memory T cells from a metastatic vaginal melanoma patient are tumor-responsive T cells and increase after anti-PD-1 treatment.

Angela Pizzolla Simon Paul KeamIsmael A VergaraFranco CaramiaNiko ThioMinyu WangNikolce KocovskiDaniela TantaloJafar JabbariGeorge Au-YeungShahneen SandhuDavid E GyorkiAlison WepplerMaurizio PerdicchioGrant A McArthurAnthony T PapenfussPaul Joseph Neeson

Published in: Journal for immunotherapy of cancer (2022)

TRM exhibited the highest tumor-responsive potential and shared their TCR with tumor-infiltrating effector memory T cells. This suggests VM metastases from this patient retain strong antitumor T cell functional responses; however, this response is suppressed in vivo. The loss of VG MHC-I expression is a common immune escape mechanism which was not addressed by anti-PD-1 monotherapy; rather an additional targeted approach to upregulate MHC-I expression is required.

Keyphrases

poor prognosis
cancer therapy
case report
regulatory t cells
working memory
small cell lung cancer
squamous cell carcinoma
combination therapy
binding protein
long non coding rna
patient safety
open label
clinical trial
quality improvement
risk assessment
human health
study protocol
replacement therapy