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Potential Interplay Between Tumor Size and Vitamin D Receptor (VDR) Polymorphisms in Breast Cancer Prognosis: a Prospective Cohort Study

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Specialties Oncology
Public Health
Date 2024 Feb 14
PMID 38351438
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Abstract

Purpose: Vitamin D has some anticancer properties that may decrease breast cancer risk and improve prognosis. The aim was to investigate associations between four previously studied VDR SNPs (Taq1, Tru91, Bsm1, and Fok1) and prognosis in different groups of breast cancer patients.

Methods: VDR genotyping of 1,017 breast cancer patients included 2002-2012 in Lund, Sweden, was performed using Oncoarray. Follow-up was until June 30, 2019. Clinical data and patient information were collected from medical records and questionnaires. Cox regression was used for survival analyses.

Results: Genotype frequencies were as follows: Fok1 (AA 15.7%, AG 49.1%, GG 35.1%), Bsm1 (CC 37.2%, CT 46.1%, TT 16.7%), Tru91 (CC 77.8%, CT 20.7%, TT 1.5%), and Taq1 (AA 37.2%, AG 46.2%, GG 16.6%). During follow-up there were 195 breast cancer events. The homozygous variants of Taq1 and Bsm1 were associated with reduced risk of breast cancer events (adjusted HR = 0.59, 95% CI 0.38-0.92 for Taq1 and adjusted HR = 0.61, 95% CI 0.40-0.94 for Bsm1). The G allele of the Fok1 was associated with increased risk of breast cancer events in small tumors (pT1, adjusted HR = 1.83, 95% CI 1.04-3.23) but not in large tumors (pT2/3/4, adjusted HR = 0.80, 95% CI 0.41-1.59) with a borderline interaction (P = 0.058). No interactions between VDR genotypes and adjuvant treatments regarding breast cancer prognosis were detected.

Conclusion: VDR genotypes were associated with breast cancer prognosis and the association might be modified by tumor size. Further research is needed to confirm the findings and elucidate their potential clinical implications.

Citing Articles

The Vitamin D Receptor as a Prognostic Marker in Breast Cancer-A Cohort Study.

Huss L, Gulz-Haake I, Nilsson E, Tryggvadottir H, Nilsson L, Nodin B Nutrients. 2024; 16(7).

PMID: 38612962 PMC: 11013402. DOI: 10.3390/nu16070931.

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