Circulating tumor DNA serial monitoring of relapse and responses to tislelizumab immunotherapy as second-line monotherapy for metastatic esophageal squamous cell carcinoma: A prospective study

被引:1
|
作者
He, Qiong [1 ]
Shi, Xun [1 ]
Yan, Junrong [2 ]
Wu, Mengmeng [2 ]
Gu, Cuiping [1 ]
Yu, Xinmin [1 ]
机构
[1] Chinese Acad Sci, Zhejiang Canc Hosp, Inst Basic Med & Canc, Dept Oncol, 1 Banshan Rd, Hangzhou 310022, Zhejiang, Peoples R China
[2] Nanjing Geneseeq Technol Inc, Med Dept, Nanjing 210032, Jiangsu, Peoples R China
关键词
tislelizumab; immunotherapy; esophageal squamous cell carcinoma; next-generation sequencing; RATIONALE-302; study; NCT03430843; PD-1; BLOCKADE; CHEMOTHERAPY; NIVOLUMAB; CANCER; PEMBROLIZUMAB; CAMRELIZUMAB; THERAPY; PLACEBO;
D O I
10.3892/mco.2024.2727
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Anti-programmed cell death 1 immuno-monotherapy has become the second-line standard treatment for advanced esophageal squamous cell carcinoma (ESCC) after the failure of first-line chemotherapy. However, new biomarkers are still needed to identify patients at risk of tumor progression and to select patients with advanced ESCC who are likely to benefit from immunotherapy. A total of 12 patients with advanced ESCC treated with tislelizumab were prospectively enrolled and endoscopic biopsy samples were collected. Plasma was obtained prior to and after every 2-3 treatment cycles with tislelizumab and when disease progression occurred. Targeted sequencing of 425 genes from plasma cell-free DNA, DNA from leukocytes and fixed esophageal tumor biopsies was performed. The patients underwent imaging analyses every 6-8 weeks until disease progression. The association between status of circulating tumor DNA (ctDNA) or changes in ctDNA following tislelizumab immunotherapy and response, tumor progression and survival was determined. All patients had evaluable next-generation sequencing results at the time of analysis. The results showed that patients with ESCC with liver metastasis had a significantly shorter median progression-free survival (mPFS: 1.4 vs. 11.7 months; P=0.037). TSC complex subunit 2 [11.7 months vs. not reached (NR); P=0.004] and zinc finger protein 217 (11.7 months vs. NR; P=0.022) gene mutations were the independent and negative prognostic factors for median overall survival (OS), respectively. Of note, ctDNA dynamic changes expressed as increment mutant molecules per milliliter of plasma ( increment MMPM; MMPM detected at the first monitoring time-point after the first infusion of tislelizumab as baseline MMPM) predicted progression-free survival (PFS) and OS more accurately compared to the ctDNA change of an individual gene. increment MMPM <20% was an independent predictor of PFS (2.8 vs. 14.6 months; P=0.029), although there was no significant difference for OS (16.7 vs. 17.6 months; P=0.830). In conclusion, changes in ctDNA levels were associated with anti-tumor effects, progression and disease-specific survival. ctDNA sequencing is promising for predicting response and progression after tislelizumab immunotherapy as second-line monotherapy for advanced ESCC.
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页数:9
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