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Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer

Sci Transl Med. 2020-04; 
Subudhi SK, Vence L, Zhao H, Blando J, Yadav SS, Xiong Q, Reuben A, Aparicio A, Corn PG, Chapin BF, Pisters LL, Troncoso P, Tidwell RS, Thall P, Wu CJ, Zhang J, Logothetis CL, Futreal A, Allison JP, Sharma P
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Peptide Synthesis Peptide recognition was considered positive when the spots were two times higher than the negative control (HIV-gag peptide, RS Synthesis). Wild-type peptides (PepMix pool, JPT Peptide Technologies) from proteins tested used in this study were used at a concentration of 10 μM: PSMA 185 peptides 15-mers with 11–amino acid overlap and PAP 94 peptides 15-mers with 11–amino acid overlap. Patient-specific wild-type and mutant peptides were bought from either JPT Peptide Technologies or GenScript Get A Quote

摘要

Tumors with high mutational burden (TMB) tend to be responsive to immune checkpoint blockade (ICB) because there are neoantigens available for targeting by reinvigorated T cells, whereas those with low TMB demonstrate limited clinical responses. To determine whether antigen-specific T cell responses can be elicited after treatment with ICB in cancers that have a low TMB, we conducted a clinical trial with ipilimumab in 30 patients with metastatic castration-resistant prostate cancer. We identified two distinct cohorts by survival and progression times: "favorable" (n = 9) and "unfavorable" (n = 10). Patients in the favorable cohort had high intratumoral CD8 T cell density and IFN-γ response... More

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