Abstract 216P
Background
The association between genetic alterations and benefit of immunotherapy is well documented, but evidence for gastrointestinal cancer (GC) remains limited. Patched1 (PTCH1) mutation, a frequently altered gene in GC, lead to dysregulation of Hedgehog signaling. However, the efficacy of PTCH1 mutations in immunotherapy in patients with GC remains unclear. Herein, we aimed to analyze the association between PTCH1 mutations and immune checkpoint inhibitors (ICIs) efficacy in patients with GC.
Methods
We screened the following 3 cohorts: (1) MSKCC cohort (N=236) of GC (including esophageal, gastric and colorectal cancers) who received ICIs. (2) Peking University Cancer Hospital (PUCH) GC cohort (N=92) who received ICIs. (3) the TCGA cohort (N=914) of GC. The patients were divided into PTCH1 mutant type (PTCH1-MT) group and PTCH1 wild type (PTCH1-WT) group. We analyzed the differences in overall survival (OS) and TMB between the two groups. Tumor immune microenvironment (TIME) was evaluated by calculating the cell infiltration score as the arithmetic mean analysis of the constituent genes.
Results
In MSKCC cohort, PTCH1-MT group (9.3%) had significantly better OS (p=0.017, median OS, 34m vs. 13m) and higher TMB (p<0.01). The results of the multivariate analysis showed that PTCH1 had a significant effect on OS, with the PTCH1-MT group had better OS (p=0.035; HR=0.37; 95%CI: 0.15-0.93). Furthermore, we consistently observed in the PUCH cohort that the PTCH1-MT group (7.6%) significantly prolonged OS (p=0.036). Additionally, in the TCGA cohort, we similarly observed a trend towards longer OS (p=0.63, mOS, 70.2m vs. 61.8m) and higher TMB (p<0.01) in PTCH1-MT group (5.8%). It shows that PTCH1 is a predictor, but not a prognostic factor. Subsequently, we assessed the abundance of 22 predefined immune cells. The score of CD4 T cells, CD8 T cells, NK cells, mast cells, and M1 cells were all significantly higher in the PTCH1-MT group (p<0.05). It shows that the PTCH1-MT group has a higher activation TIME.
Conclusions
Our study demonstrated that PTCH1 mutation could act as a potential predictor for ICIs therapy in GC. In the future, relevant prospective clinical trials need to be designed to verify this conclusion.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
217P - Clinical and molecular features of PTCH1 mutant in solid tumors
Presenter: Xuezheng Li
Session: Poster session 01
218P - Peripheral T cell activation phenotype is associated with clinical outcomes and immune-related adverse events of ipilimumab-nivolumab in advanced hepatocellular carcinoma
Presenter: WON SUK LEE
Session: Poster session 01
219P - Multicentric evaluation of amplicon-based next-generation sequencing solution for local comprehensive molecular tumor profiling
Presenter: Eloisa Jantus Lewintre
Session: Poster session 01
220P - Biomarker of blood age and inflammation in older cancer patients might predict outcome
Presenter: Marcus Vetter
Session: Poster session 01
221P - Peripheral T cell activation phenotype predicts clinical outcomes of atezolizumab-bevacizumab therapy in unresectable hepatocellular carcinoma
Presenter: Chan Kim
Session: Poster session 01
222P - Therapeutic opportunities for porcupine inhibition in gastrointestinal cancer
Presenter: Natalie Cook
Session: Poster session 01
223P - Artificial intelligence-based pathomics biomarker predict primary resistance to first-line treatment in metastatic colorectal cancers
Presenter: Gianluca Mauri
Session: Poster session 01
224P - Germline HLA-I/II is not associated with clinical outcome but the absence of HLA-A01 or the presence of HLA-B27 supertypes were correlated with improved clinical outcome among patients with NSCLC treated with pembrolizumab in combination with chemotherapy
Presenter: Afaf Abed
Session: Poster session 01
225P - Utility of next-generation sequencing (NGS) in patients with advanced cancer in a low-middle income country
Presenter: Milton Lombana Quinonez
Session: Poster session 01
226P - LongiBloodImmunoM: A multi-step analysis pipeline for longitudinal blood-based immunomonitoring for immunotherapy clinical trial
Presenter: Jiangfeng Ye
Session: Poster session 01