Inverse correlation between TP53 gene status and PD-L1 protein levels in a melanoma cell model depends on an IRF1/SOX10 regulatory axis.

Lucia MartinkovaPavlina ZatloukalovaMartina KucerikovaNela FriedlovaZuzana TylichovaFilip Zavadil-KokasTed Robert HuppPhilip John CoatesBorivoj Vojtesek

Published in: Cellular & molecular biology letters (2024)

We show that p53 loss influences the level of PD-L1 through IRF1 and SOX10 in an isogenic melanoma cell model, and that p53 loss affects NK-cell cytotoxicity toward tumor cells. Moreover, activation of p53 by MDM2 inhibition has a complex effect on IRF1/PD-L1 activation. These findings indicate that evaluation of p53 status in patients with melanoma will be important for predicting the response to PD-L1 monotherapy and/or dual treatments where p53 pathways participate in the overall response.

Keyphrases

transcription factor
dendritic cells
single cell
stem cells
nk cells
cell therapy
genome wide
clinical trial
immune response
mesenchymal stem cells
bone marrow
small molecule
basal cell carcinoma
binding protein
study protocol
amino acid
double blind