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Merck
  • Relationship between testosterone, estradiol and circulating PCSK9: Cross-sectional and interventional studies in humans.

Relationship between testosterone, estradiol and circulating PCSK9: Cross-sectional and interventional studies in humans.

Clinica chimica acta; international journal of clinical chemistry (2015-04-11)
T C Ooi, A Raymond, M Cousins, C Favreau, M Taljaard, C Gavin, E E Jolly, S Malone, L Eapen, M Chretien, M Mbikay, J Mayne
摘要

Circulating PCSK9 levels are higher in women than men, in postmenopausal than premenopausal women, and in pregnant than non-pregnant women, suggesting that sex hormones may be related to PCSK9 levels. We have examined the relationship between serum estradiol (E2) and testosterone (T) and PCSK9, and the impact of E2 replacement therapy in women and T replacement and ablation therapy in men on circulating PCSK9. We conducted a cross-sectional study to examine the correlation between serum T (in males) and E2 (in females) and serum PCSK9. We also conducted interventional studies to examine the effect of hormonal therapy on serum PCSK9 levels. In men, (1) serum T does not correlate with circulating PCSK9 or with LDLC in the basal state, (2) T replacement therapy does not have any effect on circulating PCSK9, and (3) T ablation therapy has mixed results. In women, (1) E2 correlates inversely with circulating PCSK9 and directly with serum LDLC, but (2) E2 replacement therapy does not have any effect on circulating PCSK9. We demonstrate differences between men and women in the relationship of their major sex hormones with circulating PCSK9. In men, circulating PCSK9 is not related to or affected by T except for a possible effect during T ablation therapy. In women, E2 is inversely related to circulating PCSK9 but the lack of effect of E2 therapy on circulating PCSK9 suggests that the E2-related differences in PCSK9 levels may be the result of differences in receptor-mediated PCSK9 clearance through E2-induced changes rather than production of PCSK9. The studies were registered with ClinicalTrials.gov NCT00848276.

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Sigma-Aldrich
碳负载钌, extent of labeling: 5 wt. % loading
Sigma-Aldrich
钌, powder
Sigma-Aldrich
钌黑
Sigma-Aldrich
钌, powder, −200 mesh, 99.9% trace metals basis
钌, Ruthenium, foil, 6x6mm, thickness 1.0mm, 99.9%
钌, Ruthenium, pellets, 5g, max. size 10mm, 99.9%
钌, Ruthenium, foil, 25x25mm, thickness 1.0mm, 99.9%
钌, Ruthenium, bar, 50mm x 2mm x 2mm, 99.9%
钌, Ruthenium, bar, 25mm x 2mm x 2mm, 99.9%
钌, Ruthenium, foil, 10x10mm, thickness 1.0mm, 99.9%
钌, Ruthenium, rod, 12.7mm, diameter 12.7mm, 99.9%
钌, Ruthenium, microfoil, disks, 10mm, thinness 0.1μm, specific density 122μg/cm2, permanent mylar 3.5μm support, 99.9%
钌, Ruthenium, microfoil, disks, 10mm, thinness 0.025μm, specific density 30.5μg/cm2, permanent mylar 3.5μm support, 99.9%
钌, Ruthenium, pellets, 2.5g, max. size 10mm, 99.9%