Functional variants of the chitinase 3‐like 1 gene are associated with clinicopathologic outcomes and progression of prostate cancer

Author:

Wen Yu‐Ching12,Lin Chia‐Yen345,Ho Kuo‐Hao6,Lin Yung‐Wei127,Hsiao Chi‐Hao12,Wang Shian‐Shiang348,Chang Lun‐Ching9,Yang Shun‐Fa1011ORCID,Chien Ming‐Hsien6121314ORCID

Affiliation:

1. Department of Urology, School of Medicine, College of Medicine and TMU Research Center of Urology and Kidney (TMU‐RCUK) Taipei Medical University Taipei Taiwan

2. Department of Urology, Wan Fang Hospital Taipei Medical University Taipei Taiwan

3. Division of Urology, Department of Surgery Taichung Veterans General Hospital Taichung Taiwan

4. School of Medicine Chung Shan Medical University Taichung Taiwan

5. School of Medicine National Yang Ming Chiao Tung University Taipei Taiwan

6. Graduate Institute of Clinical Medicine, College of Medicine Taipei Medical University Taipei Taiwan

7. International Master/PhD Program in Medicine, College of Medicine Taipei Medical University Taipei Taiwan

8. Department of Applied Chemistry National Chi Nan University Nantou Taiwan

9. Department of Mathematical Sciences Florida Atlantic University Boca Raton Florida USA

10. Institute of Medicine Chung Shan Medical University Taichung Taiwan

11. Department of Medical Research Chung Shan Medical University Hospital Taichung Taiwan

12. Pulmonary Research Center, Wan Fang Hospital Taipei Medical University Taipei Taiwan

13. Traditional Herbal Medicine Research Center Taipei Medical University Hospital Taipei Taiwan

14. TMU Research Center of Cancer Translational Medicine Taipei Medical University Taipei Taiwan

Abstract

AbstractChitinase 3‐like 1 (CHI3L1 or YKL40) is a secreted glycoprotein highly expressed in advanced stages of several cancer types, including prostate cancer (PCa). Impacts of genetic variants of CHI3L1 on PCa development have not yet been investigated. The most common well‐studied genetic variations are single‐nucleotide polymorphisms (SNPs). Therefore, the objective of this study was to explore associations of CHI3L1 SNPs with both the susceptibility to PCa and its clinicopathological development. Three promoter SNPs, rs6691378 (−1371, G>A), rs10399805 (−247, G>A) and rs4950928 (−131, C>G), and one non‐synonymous SNP, rs880633 (+2950, T>C), were analysed using a TaqMan allelic discrimination assay for genotyping in a cohort of 701 PCa patients and 701 healthy controls. Results indicated that there were no significant associations of PCa susceptibility with these four CHI3L1 SNPs. However, among elderly PCa patients (aged >65 years), it was observed that polymorphic variants (GA + AA) of CHI3L1 rs6691378 and 10399805 were significantly linked to reduced risks of several clinicopathological characteristics, including a high Gleason grade, advanced pathologic T stage and tumour cell invasion. Moreover, analyses of The Cancer Genome Atlas database revealed that CHI3L1 expression levels were elevated in PCa tissues compared with normal tissues. Interestingly, higher CHI3L1 expression levels were found to be associated with longer progression‐free survival rates in PCa patients. Our findings indicated that levels of CHI3L1 may influence the progression of PCa, and the rs6691378 and 10399805 SNP genetic variants of CHI3L1 are linked to the clinicopathological development of PCa within a Taiwanese population.

Funder

Wan Fang Hospital

Publisher

Wiley

Subject

Cell Biology,Molecular Medicine

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