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Marinobufagenin is related to elevated central and 24-h systolic blood pressures in young black women: the African-PREDICT Study

机译:Marinobufagenin与年轻黑人女性的中枢和24小时收缩压升高有关:Africa-PREDICT研究

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摘要

Marinobufagenin (MBG) is an endogenous steroidal α1-Na+K+-ATPase inhibitor. Because of its role in sodium handling, MBG has been associated with both antihypertensive and prohypertensive effects in normal physiology and pathology. MBG is positively associated with blood pressure in Dahl salt-sensitive rats exhibiting a similar hypertensive phenotype to black populations, characterized by impaired urinary Na+ excretion. However, clinical studies exploring blood pressure (BP)-related effects of MBG in black populations are scant. We determined whether the MBG/Na+ ratio (assessing the effectiveness of Na+ excretion resistance to MBG) is related to systolic BP (SBP) in young black men and women, compared to whites. We included 331 apparently healthy participants (20–30 years) (42.9% black, 43.8% men) on a habitual diet. We obtained 24-h and central SBP, and 24-h urinary Na+ and MBG levels. We found no ethnic differences in MBG, Na+ or MBG/Na+. MBG excretion correlated positively with Na+ excretion in all groups and to SBP in white men and black women (p ≤ 0.011). In black women only SBP related positively to MBG/Na+ in single and multi-variable adjusted regression models: central SBP (R2 = 0.26; ß = 0.28; p = 0.039), 24-h SBP (R2 = 0.46; ß = 0.30; p = 0.011), daytime (R2 = 0.38; ß = 0.28; p = 0.023) and nighttime SBP (R2 = 0.38; ß = 0.33; p = 0.009). In contrast, inverse associations of MBG/Na+ with nighttime SBP were evident in white women (r = −0.20; p = 0.038) but lost significance after multiple adjustments (R2 = 0.36; ß = −0.13; p = 0.12). We found independent positive associations of SBP with MBG/Na+ in black women. This data supports the concept that reduced MBG-mediated Na+ excretion can contribute to adverse hemodynamics.
机译:Marinobufagenin(MBG)是内源性甾体α1-Na + K + -ATPase抑制剂。由于其在钠处理中的作用,MBG与正常生理和病理学中的降压和降压作用相关。 MBG与Dahl盐敏感性大鼠的血压呈正相关,表现出与黑人人群相似的高血压表型,其特征是尿Na + 排泄受损。然而,很少有临床研究探索MBG对黑人人群的血压(BP)相关作用。我们确定了黑人男性和女性的MBG / Na + 比(评估Na + 排泄对MBG的有效性)是否与收缩压(SBP)有关,与白人相比。我们纳入了331名看似健康的参与者(20至30岁)(习惯饮食为黑人,占42.9%,男性为43.8%)。我们获得了24小时和中央SBP,以及24小时尿Na + 和MBG水平。我们发现MBG,Na + 或MBG / Na + 中没有种族差异。在所有组中,MBG排泄与Na + 排泄呈正相关,在白人和黑人妇女中,其与SBP呈正相关(p≤0.011)。在单变量和多变量校正回归模型中,只有黑人女性的SBP与MBG / Na + 正相关:中央SBP(R 2 = 0.26;ß= 0.28; p = 0.039),24小时SBP(R 2 = 0.46;ß= 0.30; p = 0.011),白天(R 2 = 0.38;ß= 0.28; p = 0.023) )和夜间SBP(R 2 = 0.38;ß= 0.33; p = 0.009)。相反,在白人女性中,MBG / Na + 与夜间SBP呈负相关(r = −0.20; p = 0.038),但在多次调整后(R 2 = 0.36; ß = −0.13; p = 0.12)。我们在黑人女性中发现SBP与MBG / Na + 具有独立的正相关性。该数据支持这样的概念,即减少的MBG介导的Na + 排泄可以导致不良的血液动力学。

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