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WT1 Trio Peptide-Based Cancer Vaccine for Rare Cancers Expressing Shared Target WT1.

Yusuke OjiNaoki KagawaHideyuki AritaNorifumi NakaKen-Ichiro HamadaHidetatsu OutaniYasushi ShintaniYoshito TakedaEiichi MoriiKenzo ShimazuMotoyuki SuzukiSumiyuki NishidaJun NakataAkihiro TsuboiMiki IwaiSae HayashiRin ImanishiSayaka IkejimaMizuki KanegaeMasahiro IwamotoMayu IkedaKento YagiHaruka ShimokadoHiroko NakajimaKana HasegawaSoyoko MorimotoFumihiro FujikiAkira NagaharaAtsushi TanemuraYutaka UedaTsunekazu MizushimaMasato OhmiTakayuki IshidaManabu FujimotoNorio NonomuraTadashi KimuraHidenori InoharaSeiji OkadaHaruhiko KishimaNaoki HosenAtsushi KumanogohYoshihiro OkaHaruo Sugiyama
Published in: Cancers (2023)
No standard treatment has been established for most rare cancers. Here, we report a clinical trial of a biweekly WT1 tri-peptide-based vaccine for recurrent or advanced rare cancers. Due to the insufficient number of patients available for a traditional clinical trial, the trial was designed for rare cancers expressing shared target molecule WT1. The recruitment criteria included WT1-expressing tumors as well as HLA-A*24:02 or 02:01. The primary endpoints were immunoglobulin G (IgG) antibody (Ab) production against the WT1-235 cytotoxic T lymphocyte (CTL) epitope and delayed-type hypersensitivity (DTH) skin reactions to targeted WT1 CTL epitopes. The secondary endpoints were safety and clinical efficacy. Forty-five patients received WT1 Trio, and 25 (55.6%) completed the 3-month protocol treatment. WT1-235 IgG Ab was positive in 88.0% of patients treated with WT1 Trio at 3 months, significantly higher than 62.5% of the weekly WT1-235 CTL peptide vaccine. The DTH positivity rate in WT1 Trio was 62.9%, which was not significantly different from 60.7% in the WT1-235 CTL peptide vaccine. The WT1 Trio safety was confirmed without severe treatment-related adverse events, except grade 3 myasthenia gravis-like symptoms observed in a patient with thymic cancer. Fifteen (33.3%) patients achieved stable disease after 3 months of treatment. In conclusion, the biweekly WT1 Trio vaccine containing the WT1-332 helper T lymphocyte peptide induced more robust immune responses targeting WT1 than the weekly WT1-235 CTL peptide vaccine. Therefore, WT1-targeted immunotherapy may be a potential therapeutic strategy for rare cancers.
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