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Poster session 11

633P - Genomic alterations in SPEN predict outcome of immune checkpoint therapy in gastrointestinal cancer

Date

21 Oct 2023

Session

Poster session 11

Topics

Tumour Site

Gastric Cancer;  Colon and Rectal Cancer

Presenters

Changxiong Wu

Citation

Annals of Oncology (2023) 34 (suppl_2): S410-S457. 10.1016/S0923-7534(23)01935-X

Authors

C. Wu1, X. Qiao1, D. Gong1, S. Li1, Z. Yu1, Y. Liu2, Q. Zhang2, D. Chen2

Author affiliations

  • 1 Hepatic-biliary-pancreatic Surgery, Hainan General Hospital, 570311 - Haikou/CN
  • 2 The Medical Department, Jiangsu Simcere Diagnostics Co., Ltd., 210042 - Nanjing/CN

Resources

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Abstract 633P

Background

Application of Immune Checkpoint Inhibitors (ICIs) has become important therapy for gastrointestinal cancer (GC). SPEN gene encodes Msx2-interacting protein which can block the differentiation of precursor B-cells into marginal zone B-cells and represses transcription. However, the correlation between SPEN mutation and immune efficacy is unclear.

Methods

We retrospectively analyzed the genomic and survival data from 236 patients with GC derived from MSKCC cohort ( Nat Genet 2019 ) to evaluate the relationship between SPEN mutation status and efficacy of immunotherapy. Then we explored the prognostic value of SPEN mutation in 914 GC patients from The Cancer Genome Atlas (TCGA) database. TMB was calculated as the total count of nonsynonymous mutations in coding sequence. The CIBERSORT analysis relied on RNA-seq data in TCGA database to evaluate 22 types immune cell infiltration status.

Results

The TMB level of SPEN-mutant patients was higher than SPEN-wildtype patients in both MSKCC (Median [IQR]: 64.94[2.63-203.64] vs 6.14[0.00-153.47], P < 0.001) and TCGA (Median [IQR]: 31.20[0.96-296.91] vs 2.70[0.05-194.70], P < 0.001) cohort. In MSKCC cohort, compared to SPEN-wildtype patients, SPEN-mutant patients achieved prolonged OS (median OS: 34 vs 13 months, P=0.009). Moreover, a multivariable analysis across the MSKCC cohort demonstrated that SPEN-mutant was associated with better OS (HR=0.30; 95%CI, 0.11-0.82; P=0.019), after adjusting for age, gender, metastasis and treatment. In TCGA cohort, there was no significant difference in OS between SPEN-wildtype group and SPEN-mutant group (median OS: 67.3 vs 60.8 months, P = 0.33). The CIBERSORT analysis revealed that CD8+ T cell infiltration and activated CD4 memory T cell were significantly higher in SPEN-mutant group than SPEN-wildtype group (p < 0.05).

Conclusions

SPEN mutation is associated with higher TMB in ICI-treated gastrointestinal cancer patients. Survival analysis suggests that SPEN mutation may serve as a novel predictive biomarker in GC patients with ICIs, but not a prognostic factor. The significantly higher CD8+ T cell infiltration and activated CD4 memory T cell in SPEN-mutant group may be the potential mechanism.

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.

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