Abstract

BackgroundEstrogen and androgen have been linked to the regulation of circulating hepatocyte growth factor (HGF), an adipose tissue-derived cytokine. It is possible that the CYP19A1 gene which alters sex hormones production may influence HGF levels. We examined the association between the CYP19A1 gene variants and plasma HGF concentrations.DesignWe evaluated 45 common and putative functional variants of CYP19A1 and circulating levels of HGF among 260 postmenopausal women who later developed colorectal cancer from the Women's Health Initiative Observational Cohort. As the distribution of HGF levels was highly skewed, we transformed HGF concentrations for all women into a log-, ranked-, or normal score-scale value. Multiple linear regression with adjustment for age was used to evaluate the associations.ResultsWe observed an association between the rs7172156, rs1008805, rs6493494, rs749292, and rs11636639 variants and HGF levels in ranked and normal score scales (corrected p values ≤0.02), although the association of these 5 SNPs with log-scale HGF was not significant (corrected p values ≥0.16). The associations remained unchanged after additional adjustment for hormone therapy use and estradiol levels. These 5 SNPs, which were in linkage disequilibrium (pairwise D′≥97%, r2≥56%), constituted a block with 2 common haplotypes accounting for 82% frequency. The most common haplotype, TCCCA, was associated with lower ranked- or normal score-transformed HGF levels (corrected p values ≤0.001), whereas the second most common haplotype, CTTCA, was associated with higher ranked- or normal score-transformed HGF levels (corrected p values ≤0.02).ConclusionOur findings of a potential association between the CYP19A1 variants and circulating HGF levels warrant confirmation in studies with larger sample size.

Highlights

  • Obesity contributes to the development of a variety of common chronic diseases among postmenopausal women, including cardiometabolic diseases and several cancers

  • We observed an association between the rs7172156, rs1008805, rs6493494, rs749292, and rs11636639 variants and hepatocyte growth factor (HGF) levels in ranked and normal score scales, the association of these 5 single nucleotide polymorphism (SNP) with logscale HGF was not significant

  • These 5 SNPs, which were in linkage disequilibrium, constituted a block with 2 common haplotypes accounting for 82% frequency

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Summary

Introduction

Obesity contributes to the development of a variety of common chronic diseases among postmenopausal women, including cardiometabolic diseases and several cancers. Circulating hepatocyte growth factor (HGF), a less-studied adipokine to date, has been found to be elevated .3-fold in obese individuals than in those of normal body size [4]. Experimental studies in animals and cell lines have shown that HGF expression are elevated by sex steroids including estradiol and testosterone [9,10,11] and the activation of HGF pathway is regulated by estrogen and androgen signaling [12,13]. Excess adiposity has been linked to increased aromatase activity, and, increased estrogen production among postmenopausal women [15]. It is further possible that elevated aromatase activity, resulting from excess adiposity, alters sex steroids production which leads to changes in HGF levels. Estrogen and androgen have been linked to the regulation of circulating hepatocyte growth factor (HGF), an adipose tissue-derived cytokine. We examined the association between the CYP19A1 gene variants and plasma HGF concentrations

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