PATH-12. Pembrolizumab efficacy in recurrent adult-type diffuse gliomas

PATH-12. 帕博利珠单抗治疗复发性成人型弥漫性胶质瘤的疗效

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作者:Calvete,Esther,Cortazar,Nerea,Orue,Izaskun,Roa,Arturo Harker,Lau,Bobo,Ng,Crystal,Chan,Crystal Ying,Fu-Fai Fong,Steve,Fong,Florence,Yu,Doris S F,Choy-Yung,Rebecca,Schrack,Jennifer,Etzkorn,Lacey,Gao,Sunan,Buta,Brian,Davoudi,Anis,Xue,Qian-Li,Bandeen-Roche,Karen,Wanigatunga,Amal,Malhotra,Rahul,Troeung,Lakkhina,Visaria,Abhijit,Koh,Vanessa,Tan,Kok Yang,Lim,Wen Huey,Chan,Angelique,Rayes,T,Ravindran,V,Ser,Merve Hazal,White,Jessica D,Haas,Daniella,Joon,Uhm,Ruff,Micheal,Campian,Jian,Lehrer,Eric,Breen,William G,Kaufmann,Timothy,Brown,Paul,Maciej,Mrugala,Parney,Ian,Burns,Terry,Rosenfeld,Steven,Quinones-Hinojosa,Alfredo,Ida,Cristiane M,Giannini,Caterina,Sener,Ugur,Na,Brian,Shaikh,Farhaz,Mirchia,Kanish,Young,Jacob S,Reddy,Alyssa T,Mueller,Sabine,Morshed,Ramin,Chin,Cynthia T,Perry,Arie,Chang,Susan M,Berger,Mitchel S,de Groot,John F,Monga,Varun,Jacques,Line,Pekmezci,Melike,Vasudevan,Harish N,Zeyen,Thomas,Friker,Lea L,Duffy,Cathrina,Gielen,Gerrit H,Ebrahimi,Azadeh,Schaefer,Niklas,Weller,Johannes,Schneider,Matthias,Potthoff,Anna-Laura,Layer,Julian P,Doerner,Evelyn,Klein,Rebecca,Goschzik,Tobias,Hoelzel,Michael,Pietsch,Torsten,Waha,Andreas,Herrlinger,Ulrich,Maqbool,Muhammad Asad,Shafqat,Shameel,Ida,Cristiane,Vaubel,Rachael,Al-Kateb,Hussam,Burns,Terence,Campian,Jian,Ensign,Shannon Fortin,Galanis,Evanthia,Hammack,Julie,Mrugala,Maciej,Neth,Bryan,Porter,Alyx,Ruff,Michael,Sener,Ugur,Sherman,Wendy,Uhm,Joon,Kizilbash,Sani
期刊:PLoS One影响因子:2.600
时间:2025起止号:2025 Nov;27(Suppl 5):v242
doi:10.1371/journal.pone.0319426疾病类型: 胶质瘤

Abstract

BACKGROUND: Pembrolizumab is FDA approved for solid tumors with high tumor mutation burden (TMB) and may thus have efficacy in hypermutant glioma. This study aimed to identify factors influencing efficacy of pembrolizumab in recurrent glioma. METHODS: This retrospective study at Mayo Clinic included patients with adult-type diffuse gliomas who received pembrolizumab (≥2 cycles) for recurrent disease (01/01/2014–05/01/2025). The Mayo Clinic Solid Tumor Panel (MCSTP), which uses the Illumina TruSight Oncology 500 High-Throughput next-generation sequencing (NGS) assay, was also used to assess the molecular characteristics of the recurrent tumors. Responders to pembrolizumab were defined as patients who did not meet RANO 2.0 criteria for progressive disease on first radiographic response assessment. Progression-free survival (PFS) was analyzed using Kaplan-Meier and Cox-Regression analyses. RESULTS: Sixty-two patients were identified (median age: 46 years; 65% male; 94% white). All patients received pembrolizumab and had prior alkylating chemotherapy. The median PFS from pembrolizumab initiation was 2.3 months. Twenty-five (40%) patients were responders. Patients with IDH-mutant, 1p/19q co-deleted gliomas (OLIGO, n=13) had a longer PFS (4.3 months) than IDH wildtype gliomas (IDH-WT, n=33, 2.2 months, p=0.012) and IDH-mutant, 1p/19q non-co-deleted (IDH-MUT, n=16, 1.7 months, p=0.0006). The proportion of responders was significantly greater in OLIGO patients (IDH-WT, 33%; IDH-MUT, 19%; OLIGO, 85%, p=0.0008). Overall PFS was not impacted by patient age, sex, or extent of initial resection. Twenty-nine percent of patient tumors tested thus far (6/21) had a high TMB (≥10 mut/Mb). Two-thirds (4/6) of high TMB patients were responders, while only one-third (5/15) of low TMB patients were responders. CONCLUSIONS: Patients with recurrent OLIGO may have a longer PFS with pembrolizumab therapy than IDH-WT and IDH-MUT. Furthermore, high TMB may be associated with longer PFS with pembrolizumab therapy in glioma. Additional patients are being assessed using MCSTP (total expected n=43); complete data will be presented.

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