AI Article Synopsis
- Only a small number of cancer patients benefit from immune checkpoint blockade therapy due to complex interactions among immune checkpoint pathways and molecules in circulating small extracellular vesicles (sEVs).
- The study found that PD-1 and CD80 on immunocyte-derived sEVs lead to reduced PD-L1 on tumor cell membranes while increasing PD-L1 secretion, contributing to systemic immunosuppression and making tumors less responsive to immune attacks.
- Analyzing multiple checkpoint molecules on circulating sEVs can help differentiate between patients who will respond well to anti-PD-1 treatments and those who will not, highlighting a potential target for improving cancer therapies.
Article Abstract
Only a minority of cancer patients benefit from immune checkpoint blockade therapy. Sophisticated cross-talk among different immune checkpoint pathways as well as interaction pattern of immune checkpoint molecules carried on circulating small extracellular vesicles (sEV) might contribute to the low response rate. Here we demonstrate that PD-1 and CD80 carried on immunocyte-derived sEVs (I-sEV) induce an adaptive redistribution of PD-L1 in tumour cells. The resulting decreased cell membrane PD-L1 expression and increased sEV PD-L1 secretion into the circulation contribute to systemic immunosuppression. PD-1/CD80 I-sEVs also induce downregulation of adhesion- and antigen presentation-related molecules on tumour cells and impaired immune cell infiltration, thereby converting tumours to an immunologically cold phenotype. Moreover, synchronous analysis of multiple checkpoint molecules, including PD-1, CD80 and PD-L1, on circulating sEVs distinguishes clinical responders from those patients who poorly respond to anti-PD-1 treatment. Altogether, our study shows that sEVs carry multiple inhibitory immune checkpoints proteins, which form a potentially targetable adaptive loop to suppress antitumour immunity.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11079016 | PMC |
| http://dx.doi.org/10.1038/s41467-024-48200-9 | DOI Listing |
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