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Comprehensive identification of NRG1 fusions in 25,203 patients with solid tumors.

NPJ precision oncology 2025 Vol.9(1) p. 262

Xiang S, Zheng Y, Wang M, Liu X, Zhang X, Chen D, Meng G, Xu H, Wang X

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NRG1 fusion is an emerging oncogenic driver, and the FDA has approved drugs for the treatment of non-small cell lung cancer and pancreatic cancer associated with NRG1 fusions.

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APA Xiang S, Zheng Y, et al. (2025). Comprehensive identification of NRG1 fusions in 25,203 patients with solid tumors.. NPJ precision oncology, 9(1), 262. https://doi.org/10.1038/s41698-025-01044-y
MLA Xiang S, et al.. "Comprehensive identification of NRG1 fusions in 25,203 patients with solid tumors.." NPJ precision oncology, vol. 9, no. 1, 2025, pp. 262.
PMID 40730881

Abstract

NRG1 fusion is an emerging oncogenic driver, and the FDA has approved drugs for the treatment of non-small cell lung cancer and pancreatic cancer associated with NRG1 fusions. This study retrospectively analyzed data from 25,203 patients with solid tumors who underwent next-generation sequencing (NGS) and identified 49 patients with NRG1 fusions. The mutation profiles and actionable therapeutic targets were analyzed among patients with fusions. In this study, 0.2% (49/25,203) of patients harbored NRG1 fusions. The frequencies of NRG1 fusions across various cancer types were as follows: prostate cancer, 0.65%; breast cancer, 0.47%; lung cancer, 0.29%; esophageal cancer, 0.25%; colorectal cancer, 0.17%; gastric cancer, 0.13%; pancreatic cancer, 0.11%; and hepatocellular carcinoma, 0.05%). A total of 36 fusion partners were detected, among which CD74 was predominant, accounting for 29.3% of cases. Patients with NRG1 fusions presented a greater frequency of FGFR1 mutations and RET fusions, compared with non-NRG1 fusion patients. Most lung cancer and colorectal cancer patients with NRG1 fusions harbored FDA-approved or potential drug targets, whereas those diagnosed with breast cancer harbored fewer such targets. NRG1 fusion-related drugs can provide additional treatment options. Our study expands the NRG1 fusion gene landscape and provides a valuable reference for the comprehensive treatment of patients with NRG1 fusions.

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