Functional variants of the pentraxin 3 gene are associated with the metastasis and progression of prostate cancer

Author:

Weng Wei‐Chun12,Hsieh Yi‐Hsien34ORCID,Lin Chia‐Yen567,Liu Yu‐Fan8,Su Shih‐Chi910,Wang Shian‐Shiang5611,Yang Shun‐Fa34ORCID

Affiliation:

1. Division of Urology, Department of Surgery Tungs' Taichung Metroharbor Hospital Taichung Taiwan

2. Department of Post‐Baccalaureate Medicine, College of Medicine National Chung Hsing University Taichung Taiwan

3. Institute of Medicine Chung Shan Medical University Taichung Taiwan

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

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

6. School of Medicine Chung Shan Medical University Taichung Taiwan

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

8. Department of Biomedical Sciences Chung Shan Medical University Taichung Taiwan

9. Whole‐Genome Research Core Laboratory of Human Diseases Chang Gung Memorial Hospital Keelung Taiwan

10. Department of Medical Biotechnology and Laboratory Science, College of Medicine Chang Gung University Taoyuan Taiwan

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

Abstract

AbstractAge, ethnic background and genetic components have been identified as the established risks for prostate cancer (PCa). Pentraxin 3 (PTX3), originally identified as a pattern‐recognition molecule for defence against infectious agents, has multiple functions in tissue repair and in the regulation of cancer‐associated inflammation. In this study, we sought to investigate the impact of PTX3 gene variants on the development of PCa. Genotypes of four common single‐nucleotide polymorphisms (SNPs) of PTX3 gene, including rs1840680, rs2305619, rs3816527 and rs2120243, were profiled among 705 PCa patients and 705 ethnicity‐matched controls. In this study, we found that patients who carry at least one minor allele (C) of rs3816527 (AC and CC) tended to develop advanced forms of diseases (clinical large T stage, OR, 1.593, p = 0.032; pathologically‐confirmed nodal spread, OR, 1.987, p = 0.011; metastatic tumour, OR, 3.896, p = 0.032) as compared with those homologous for the major allele (AA). Further stratification analysis showed that such association of rs3816527 with lymphatic and distal metastasis of PCa was accentuated in the younger age group (≤65 at diagnosis) but not seen in the older age group (>65 at diagnosis), suggesting an age‐specific effect of PTX3 variants. Prediction of PTX3 protein structure implied that polymorphism may alter the quaternary organization and oligomerization of PTX3 protein. Moreover, our gene silencing experiments and survey of public datasets revealed that elevation of PTX3 levels in PCa was required for cell migration and associated with tumour metastasis. Our results highlight an association of PTX3 rs3816527 with the progression of PCa.

Publisher

Wiley

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