Alisha A Ziegler, Samuel B R Lawton, Eva M Fekete, Daniel T Brozoski, Valerie A Wagner, Connie C Grobe, Curt D Sigmund, Pablo Nakagawa, Justin L Grobe, Jeffrey L Segar
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C57BL/6J male mice were supplied a low (0.04%) Na or supplemented (0.30%) Na diet from PD21-PD42, before return to standard (0.15%) Na diet. Hemodynamic and autonomic functions were assessed by radiotelemetry and acute administration of autonomic antagonists before and after all animals were switched to a high Na diet (HSD; 1% Na) at 12 weeks of age. Mice were additionally treated with the angiotensin II type 1 receptor (AT<sub>1</sub>R) antagonist, losartan, for two weeks. On standard diet, early-life Na restriction resulted in small but significantly different hemodynamic responses to autonomic blockers without effect on systolic blood pressure (SBP) or heart rate (HR). HSD increased SBP in 0.04% but not 0.30% Na mice, accompanied by increased cardiac sympathetic activity. Losartan had a greater BP lowering effect in early life Na-restricted mice. 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引用次数: 0
摘要
早产会增加成年后罹患心脏代谢疾病的风险。妊娠后三个月是下丘脑发育的关键时期,在此期间出生的婴儿由于肾脏发育不成熟和大量尿钠丢失而面临钠(Na)耗竭的风险。我们以前曾在雄性小鼠身上证实,在小鼠下丘脑发育的同等时期(PD21-PD42),Na 限制会通过增加产热交感神经活动而导致能量平衡的长期变化。因此,我们推测生命早期的钠限制会通过改变自律神经活动来改变心血管控制。从 PD21 到 PD42,给 C57BL/6J 雄性小鼠提供低(0.04%)Na 或补充(0.30%)Na 的饮食,然后再恢复到标准(0.15%)Na 饮食。在所有动物 12 周龄时改用高 Na 食物(HSD;1% Na)之前和之后,通过放射性遥测和急性给予自律神经拮抗剂评估血液动力学和自律神经功能。此外,小鼠还接受了为期两周的血管紧张素II 1型受体(AT1R)拮抗剂洛沙坦治疗。在标准饮食中,早期Na限制会导致对自律神经阻断剂的血液动力学反应出现微小但显著的差异,但不会影响收缩压(SBP)或心率(HR)。HSD 会增加 0.04% Na 小鼠的 SBP,但不会增加 0.30% Na 小鼠的 SBP,同时会增加心脏交感神经活动。洛沙坦对早期Na受限小鼠的降压作用更大。我们的研究结果表明,在下丘脑发育的关键时期,Na限制会导致心血管功能的自主神经控制发生长期变化,这可能有助于了解早产儿罹患心血管疾病风险增加的原因。
Early-Life Sodium Restriction Programs Autonomic Dysfunction and Salt- Sensitivity in Male C57BL/6J Mice.
Preterm birth increases the risk of cardiometabolic disease in adulthood. Infants born during the second trimester of pregnancy, a critical period of hypothalamic development, are at risk of sodium (Na) depletion due to renal immaturity and large urine Na losses. We previously demonstrated in male mice that Na restriction during the equivalent mouse hypothalamic development period (PD21-PD42) programs long-term changes in energy balance via increased thermogenic sympathetic nervous activity. We therefore hypothesized that early-life Na restriction programs changes in cardiovascular control via altered autonomic activity. C57BL/6J male mice were supplied a low (0.04%) Na or supplemented (0.30%) Na diet from PD21-PD42, before return to standard (0.15%) Na diet. Hemodynamic and autonomic functions were assessed by radiotelemetry and acute administration of autonomic antagonists before and after all animals were switched to a high Na diet (HSD; 1% Na) at 12 weeks of age. Mice were additionally treated with the angiotensin II type 1 receptor (AT1R) antagonist, losartan, for two weeks. On standard diet, early-life Na restriction resulted in small but significantly different hemodynamic responses to autonomic blockers without effect on systolic blood pressure (SBP) or heart rate (HR). HSD increased SBP in 0.04% but not 0.30% Na mice, accompanied by increased cardiac sympathetic activity. Losartan had a greater BP lowering effect in early life Na-restricted mice. Our findings suggest Na restriction during a critical hypothalamic developmental period programs long-term changes in autonomic control of cardiovascular functions and may offer insight into the increased risk of cardiovascular disease in former preterm infants.
期刊介绍:
The American Journal of Physiology-Regulatory, Integrative and Comparative Physiology publishes original investigations that illuminate normal or abnormal regulation and integration of physiological mechanisms at all levels of biological organization, ranging from molecules to humans, including clinical investigations. Major areas of emphasis include regulation in genetically modified animals; model organisms; development and tissue plasticity; neurohumoral control of circulation and hypertension; local control of circulation; cardiac and renal integration; thirst and volume, electrolyte homeostasis; glucose homeostasis and energy balance; appetite and obesity; inflammation and cytokines; integrative physiology of pregnancy-parturition-lactation; and thermoregulation and adaptations to exercise and environmental stress.