Hypercholesterolemia Clinical Trial
Official title:
Human Studies On Gender Differences In PCSK9 Function In Lipoprotein Metabolism
This study measures a recently discovered protein named PCSK9 (Proprotein convertase
subtilisin kexin 9) in blood to see if it is influenced by male and female sex hormones.
PCSK9 has recently been shown to control cholesterol and triglyceride levels by diminishing
the ability of liver cells to remove cholesterol from blood leading to high blood
cholesterol levels.
It was found in previous studies that there was a relationship between blood levels of PCSK9
and cholesterol in men but not in women. This gender difference is a new finding and it
raises the question of whether male and female hormones might influence PCSK9's role as a
blood cholesterol regulator.
The study requires a pre-treatment fasting blood sample and another sample 3 months after
starting hormone therapy.
Proprotein convertase subtilisin kexin 9 (PCSK9) is a secreted glycoprotein that was first
demonstrated to play a role in lipoprotein metabolism in 2003 when several gain-of-function
single nucleotide polymorphisms (SNPs) in PCSK9 were shown to associate with autosomal
dominant hypercholesterolemia (ADH). Soon after, loss-of-function nonsense and missense SNPs
in PCSK9 were shown to associate with hypocholesterolemia. Much is still not known about
PCSK9's mechanism of action, its substrate(s), its regulation, and factors affecting its
function, but we do know that PCSK9 decreases LDL clearance through degradation of LDL
receptors. We examined plasma PCSK9 and serum lipids in182 normolipidemic subjects (98 men,
84 women) and found with Spearman analysis a significant correlation between plasma PCSK9
and total cholesterol (TC), LDL-C, and TC/HDL-C in men but not in women, suggesting a gender
difference in PCSK9 regulation and/or function.
Following on our unexpected but novel and exciting observation, we hypothesize: that serum
levels of testosterone and estradiol would be significantly correlated with plasma PCSK9
levels, that testosterone and 17-B estradiol replacement therapies in men and women
respectively would result in changes in the levels of plasma PCSK9, that testosterone and
estradiol modify the effect of PCSK9 on serum lipids in different ways, explaining at least
in part, the gender dichotomy in PCSK9 function, and that a significant percentage of the
effect of hormone replacement therapy on lipids is mediated through PCSK9 function.
Cohort #1 will be 60 hypogonadal men and cohort #2 will be 60 postmenopausal
(hypoestrogenic) women before and after testosterone and estrogen replacement therapy
respectively. They will undergo measurements of plasma PCSK9, serum testosterone in men or
estradiol in women and TC, triglycerides, HDL-C and LDL-C before and 3 months after starting
on replacement therapy. These panel studies will allow us to evaluate whether (a) hormone
replacement therapy has an effect on PCSK9, and (b) whether resulting changes in PCSK9 are
then associated with lipid response.
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Observational Model: Cohort, Time Perspective: Prospective
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