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Inactivation of Hippo pathway characterizes a poor-prognosis subtype of esophageal cancer
Zihang Mai, Jianye Yuan, Hong Yang, Shuogui Fang, Xiuying Xie, Xinye Wang, Jiaxin Xie, Jing Wen, Jianhua Fu
Zihang Mai, Jianye Yuan, Hong Yang, Shuogui Fang, Xiuying Xie, Xinye Wang, Jiaxin Xie, Jing Wen, Jianhua Fu
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Research Article Gastroenterology Oncology

Inactivation of Hippo pathway characterizes a poor-prognosis subtype of esophageal cancer

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Abstract

Identification of molecular subtypes that reflect different prognoses and treatment responses, especially immune checkpoint inhibitors (ICIs) in esophageal squamous cell carcinoma (ESCC), is essential for treatment decisions. We performed targeted sequencing in 201 patients with ESCC to discover genetic subtypes and validate our findings via multiple data sets. We identified 3 driver genes (FCGBP, GRIN2B, and FRY), and recurrent truncating mutations in FRY impaired its tumor-suppressive function and promoted tumor proliferation. A 3-gene mutation signature (FAT1, FAT3, and FRY) recognized a molecular subtype named “FAT/FRY” with frequent Hippo pathway–related mutations. In multiple ESCC cohorts, the patients with the FAT/FRY subtype had poorer prognosis than did patients in the WT group. Transcriptome analysis indicated that the FAT/FRY subtype was characterized by inactivation of the Hippo pathway, hypoxia, chemoresistance, higher infiltration of CD8+ T cells and activated DCs, and a transcriptome similar to that of cancer responders. Furthermore, the 3-gene signature predicted better survival for patients treated with ICIs, partially explained by its positive correlation with the tumor mutation burden and neoantigen burden. The 3-gene signature is a biomarker to recognize the FAT/FRY molecular subtype, evaluate prognosis, and select potential beneficiaries of ICIs in ESCC.

Authors

Zihang Mai, Jianye Yuan, Hong Yang, Shuogui Fang, Xiuying Xie, Xinye Wang, Jiaxin Xie, Jing Wen, Jianhua Fu

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Figure 5

Identification of a 3-gene signature associated with shorter OS for patients with ESCC.

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Identification of a 3-gene signature associated with shorter OS for pati...
(A and B) Kaplan-Meier survival analysis showed that patients with mutation(s) in at least 1 gene of this signature had significantly shorter OS than patients with WT genes in our discovery (A) and validation cohorts (B). (C) Survival curves show a marginal trend in which patients with comutations had worse OS than patients with 1 mutated gene in the 3-gene signature. (D) The FAT/FRY subgroup had worse survival in TCGA-ESCC cohort (n = 96). P values in A–D were calculated by log-rank tests. (E) Forest plot of the HRs of death in different molecular subgroups from 4 cohorts with the random effects model (pooled HR, 2.77 [95% CI, 1.43–5.36]; I2 = 65%; P = 0.03, I2 test). TE, target estimate; GECI, Guangdong Esophageal Cancer Institute; Song’s pN+ cohort, ref. 20.

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