Constructing a prognostic model for colon cancer patients on basis of coagulation genes enriched in cancer-associated fibroblasts to guide personalized immunotherapy

Author:

Gao Rui12,Zhou Qing345,Hu Shangshang1,Qin Jian1,Xiao Qianni12,Pan Yuqin12,Sun Huiling1,Chen Xiaoxiang6

Affiliation:

1. General Clinical Research Center, Nanjing First Hospital , Nanjing Medical University , Nanjing , Jiangsu , China

2. Department of Basic-Medicine and Clinical Pharmacy, Nanjing First Hospital , China Pharmaceutical University , Nanjing , Jiangsu , China

3. National Health Commission Contraceptives Adverse Reaction Surveillance Center , Nanjing , Jiangsu , China

4. Jiangsu Health Development Research Center , Nanjing , Jiangsu , China

5. Jiangsu Provincial Medical Key Laboratory of Fertility Protection and Health Technology Assessment , Nanjing , Jiangsu , China

6. Department of Medical Oncology, Nanjing First Hospital , 385685 Nanjing Medical University , Nanjing , Jiangsu , China

Abstract

Abstract Objectives Colon cancer is a global health challenge. This research is designed to build a prognostic model that can personalize the guidance of immunotherapy among colon cancer patients. Methods Coagulation-associated prognostic genes which were subsequently integrated into a Least Absolute Shrinkage and Selection Operator algorithm for constructing a prognostic model were identified with the univariate Cox analyses. The potential of coagulation-related risk score (CRRS) in prognosis and immunotherapy outcomes was rigorously assessed. Finally, the cellular origin of genes in the CRRS model was explored with single-cell RNA-seq data, and the biological functions of core genes were further confirmed by cell function experiments. Results Our findings showed the CRRS model usefully classified patients into high-risk and low-risk groups. High-risk patients exhibited worse total survival. A nomogram was subsequently devised, enabling quantitative survival prediction by incorporating CRRS, age, sex, and TNM stage. Moreover, the CRRS model predicted the extent of cancer-associated fibroblasts (CAFs) infiltration. The analysis further indicated diminished immune responsiveness in high-risk patients, and single-cell data analysis pinpointed TIMP1+ CAF as a potential contributor to cancer progression. Conclusions The CRRS model can be adopted as a prognostic device for colon cancer patients and low-risk patients are more suitable for treatment with immune checkpoint inhibitors. TIMP1 secreted by CAF can promote the malignant progression of colon cancer.

Funder

Key Project of Science and Technology Development of Nanjing Medicine

The research project of Jiangsu Health Development Research Center

Jiangsu Provincial Medical Key Discipline Cultivation Unit

Natural Science Foundation of Jiangsu Province

Publisher

Walter de Gruyter GmbH

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