The predicting role of circulating tumor DNA landscape in gastric cancer patients treated with immune checkpoint inhibitors

The predicting role of circulating tumor DNA landscape in gastric cancer patients treated with immune checkpoint inhibitors

A more common and noninvasive predicting biomarker for programmed cell death 1 (PD-1) antibody remains to be explored. We assessed 46 patients with advanced gastric cancer who received PD-1 antibody immunotherapy and 425-genes next-generation sequencing (NGS) testing. Patients who had a > 25% dec...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:Molecular cancer 2020-10, Vol.19 (1), p.1-154, Article 154
Hauptverfasser: Jin, Ying, Chen, Dong-Liang, Wang, Feng, Yang, Chao-pin, Chen, Xu-Xian, You, Jin-qi, Huang, Jin-Sheng, Shao, Yang, Zhu, Dong-Qin, Ouyang, Yu-Ming, Luo, Hui-Yan, Wang, Zhi-Qiang, Wang, Feng-Hua, Li, Yu-Hong, Xu, Rui-Hua, Zhang, Dong-Sheng
Format: Artikel
Sprache:eng
Schlagworte:
Advanced
Apoptosis
Atezolizumab
Biomarkers
Biopsy
Cancer genetics
Cancer patients
Cancer therapies
Cell death
Chemotherapy
Circulating tumor DNA
Clinical trials
Deoxyribonucleic acid
DNA
Drug therapy
Fibroblast growth factor receptor 4
Gastric cancer
Gastrointestinal cancer
Immune checkpoint
Immune checkpoint inhibitors
Immunotherapy
Letter to the Editor
Medical prognosis
Medical research
Melanoma
Metastasis
Mutation
Next-generation sequencing
Nivolumab
Patients
PD-1 protein
Pembrolizumab
Plasma
Prognosis
RhoA protein
Stomach cancer
Tumors
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
Beschreibung
Zusammenfassung:A more common and noninvasive predicting biomarker for programmed cell death 1 (PD-1) antibody remains to be explored. We assessed 46 patients with advanced gastric cancer who received PD-1 antibody immunotherapy and 425-genes next-generation sequencing (NGS) testing. Patients who had a > 25% decline in maximal somatic variant allelic frequency (maxVAF) had a longer progression free survival (PFS) and higher response rate than those who did not (7.3 months vs 3.6 months, p  = 0.0011; 53.3% vs 13.3%, p  = 0.06). The median PFS of patients with undetectable and detectable post-treatment circulating tumor DNA (ctDNA) was 7.4 months vs. 4.9 months ( p  = 0.025). Mutation status of TGFBR2, RHOA, and PREX2 in baseline ctDNA influenced the PFS of immunotherapy ( p  
ISSN:1476-4598
1476-4598
DOI:10.1186/s12943-020-01274-7