Lysine-specific Demethylase-1 Modifies the Age Effect on Blood Pressure Sensitivity to Dietary Salt Intake

Overview

Journal Age (Dordr)

Publisher Springer

Specialty Geriatrics

Date 2012 Oct 12

PMID 23054827

Citations 13

Authors

Alexander W Krug

Eric Tille

Bei Sun

Luminita Pojoga

Jonathan Williams

Bindu Chamarthi

Andrew H Lichtman

Paul N Hopkins

Gail K Adler

Gordon H Williams

Affiliations

Soon will be listed here.

Abstract

How interactions of an individual's genetic background and environmental factors, such as dietary salt intake, result in age-associated blood pressure elevation is largely unknown. Lysine-specific demethylase-1 (LSD1) is a histone demethylase that mediates epigenetic regulation and modification of gene transcription. We have shown previously that hypertensive African-American minor allele carriers of the LSD1 single nucleotide polymorphism (rs587168) display blood pressure salt sensitivity. Our goal was to further examine the effects of LSD1 genotype variants on interactions between dietary salt intake, age, and blood pressure. We found that LSD1 single nucleotide polymorphism (rs7548692) predisposes to increasing salt sensitivity during aging in normotensive Caucasian subjects. Using a LSD1 heterozygous knockout mouse model, we compared blood pressure values on low (0.02 % Na(+)) vs. high (1.6 % Na(+)) salt intake. Our results demonstrate significantly increased blood pressure salt sensitivity in LSD1-deficient compared to wild-type animals with age, confirming our findings of salt sensitivity in humans. Elevated blood pressure in LSD1(+/-) mice is associated with total plasma volume expansion and altered renal Na(+) excretion. In summary, our human and animal studies demonstrate that LSD1 is a genetic factor that interacts with dietary salt intake modifying age-associated blood pressure increases and salt sensitivity through alteration of renal Na(+) handling.

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