Franco Maria do Carmo P, Arruda Robéria Maria M P, Dantas Ana Paula Villela, Kawamoto Elisa Mitiko, Fortes Zuleica B, Scavone Cristoforo, Carvalho Maria Helena C, Tostes Rita C A, Nigro Dorothy
Laboratory of Hypertension, Department of Pharmacology, Institute of Biomedical Science, University of São Paulo, Av. Prof Lineu Prestes, 1524- São Paulo, SP, Brazil.
Cardiovasc Res. 2002 Oct;56(1):145-53. doi: 10.1016/s0008-6363(02)00508-4.
Epidemiological studies suggest that intrauterine undernutrition plays an important role in the development of arterial hypertension in adulthood. In an attempt to define the mechanisms whereby blood pressure may be raised, we have hypothesized that arteries from offspring of nutritionally restricted dams exhibit abnormalities in the endothelial function and in nitric oxide synthesis. In order to investigate the existence of potential gender differences on the effects of intrauterine undernutrition, both male and female offspring of pregnant Wistar rats on normal and restricted diets were studied in adulthood.
Female pregnant Wistar rats were fed either normal or 50% of the normal intake diets, during the whole gestational period. At 14 weeks of age, the rats were used for the study of vascular reactivity, eNOS and iNOS gene expression, eNOS activity and, in the case of females, estrogen levels.
Intrauterine undernutrition induced hypertension in both male and female offspring, but hypertension was more severe in male rats. Endothelium-intact aortic rings from male and female rats in the restricted diet group exhibited increased responses to norepinephrine, decreased vasodilation to acetylcholine and unaltered responses to sodium nitroprusside in comparison to aortic rings from control rats. No gender-related differences were observed in the vascular reactivity studies. Intrauterine undernutrition promoted decreased gene expression for eNOS in aorta isolated from male, but not female, offspring, reduction in eNOS activity in both male and female offspring and impairment in synthesis of estrogen in female offspring.
Our data show that intrauterine undernutrition: (1) induces hypertension both in the male and female offspring, hypertension being more severe in male than in female rats; (2) alters endothelium-dependent responses in aortas from the resulting offspring. The endothelial dysfunction is associated with a decrease in activity/expression of eNOS in aortas from male offspring. The mechanism involved in altered response to ACh in female offspring might be a consequence of reduction in estrogen levels leading to reduced eNOS activity.
流行病学研究表明,子宫内营养不良在成年期动脉高血压的发生发展中起重要作用。为了确定血压升高的机制,我们推测,营养受限母鼠后代的动脉在内皮功能和一氧化氮合成方面存在异常。为了研究子宫内营养不良影响的潜在性别差异,我们对成年期正常饮食和受限饮食的怀孕Wistar大鼠的雄性和雌性后代进行了研究。
雌性怀孕Wistar大鼠在整个妊娠期分别给予正常饮食或正常摄入量50%的饮食。在14周龄时,将大鼠用于血管反应性、内皮型一氧化氮合酶(eNOS)和诱导型一氧化氮合酶(iNOS)基因表达、eNOS活性的研究,对于雌性大鼠,还研究了雌激素水平。
子宫内营养不良在雄性和雌性后代中均诱发高血压,但雄性大鼠的高血压更为严重。与对照组大鼠的主动脉环相比,受限饮食组雄性和雌性大鼠的完整内皮主动脉环对去甲肾上腺素的反应增强,对乙酰胆碱的血管舒张反应减弱,对硝普钠的反应未改变 在血管反应性研究中未观察到性别相关差异。子宫内营养不良促使雄性而非雌性后代分离的主动脉中eNOS基因表达降低,雄性和雌性后代的eNOS活性降低,雌性后代的雌激素合成受损。
我们的数据表明,子宫内营养不良:(1)在雄性和雌性后代中均诱发高血压,雄性大鼠的高血压比雌性大鼠更严重;(2)改变了后代主动脉中内皮依赖性反应。内皮功能障碍与雄性后代主动脉中eNOS活性/表达降低有关。雌性后代对乙酰胆碱反应改变的机制可能是雌激素水平降低导致eNOS活性降低的结果。