| Literature DB >> 30400034 |
Yuefei Huang1, Pei Yee Ting1, Tham M Yao1, Tsuyoshi Homma1, Danielle Brooks1, Isis Katayama Rangel1, Gail K Adler1, Jose R Romero1, Jonathan S Williams1, Luminita H Pojoga1, Gordon H Williams1.
Abstract
Human risk allele carriers of lysine-specific demethylase 1 (LSD1) and LSD1-deficient mice have salt-sensitive hypertension for unclear reasons. We hypothesized that LSD1 deficiency causes dysregulation of aldosterone's response to salt intake resulting in increased cardiovascular risk factors (blood pressure and microalbumin). Furthermore, we determined the effect of biological sex on these potential abnormalities. To test our hypotheses, LSD1 male and female heterozygote-knockout (LSD1+/-) and WT mice were assigned to two age groups: 18 weeks and 36 weeks. Plasma aldosterone levels and aldosterone production from zona glomerulosa cells studied ex vivo were greater in both male and female LSD1+/- mice consuming a liberal salt diet as compared to WT mice consuming the same diet. However, salt-sensitive blood pressure elevation and increased microalbuminuria were only observed in male LSD1+/- mice. These data suggest that LSD1 interacts with aldosterone's secretory response to salt intake. Lack of LSD1 causes inappropriate aldosterone production on a liberal salt diet; males appear to be more sensitive to this aldosterone increase as males, but not females, develop salt sensitivity of blood pressure and increased microalbuminuria. The mechanism responsible for the cardiovascular protective effect in females is uncertain but may be related to estrogen modulating the effect of mineralocorticoid receptor activation.Entities:
Keywords: aldosterone; blood pressure; lysine-specific demethylase 1; sex
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Year: 2019 PMID: 30400034 PMCID: PMC6824586 DOI: 10.1530/JOE-18-0247
Source DB: PubMed Journal: J Endocrinol ISSN: 0022-0795 Impact factor: 4.286