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心血管系统对早期缓激肽受体阻断反应的性别差异。

Sexual dimorphism of cardiovascular responses to early blockade of bradykinin receptors.

作者信息

Madeddu P, Pinna Parpaglia P, Anania V, Glorioso N, Chao C, Wang C, Chao J

机构信息

Clinica Medica, University of Sassari, Italy.

出版信息

Hypertension. 1996 Mar;27(3 Pt 2):746-51. doi: 10.1161/01.hyp.27.3.746.

Abstract

To assess whether the cardiovascular effects induced by early blockade of bradykinin B2-receptors with Hoe 140 (D-Arg[Hyp3,Thi5,D-Tic7,Oic8]-bradykinin) are influenced by sex, Wistar rats of both sexes received the antagonist (300 nmol/d per kilogram body wt) or vehicle from 2 days to 7 weeks of age by subcutaneous injection and then by intraperitoneal infusion. Compared with control rats, Hoe 140-treated female rats showed higher systolic blood pressure levels at 7 and 9 weeks of age (125 +/- 2 versus 111 +/- 2 mm Hg and 132 +/- 3 versus 116 +/- 2 mm Hg, respectively, P < .05), whereas in male rats a difference was found at 7 weeks (122 +/- 4 versus 108 +/- 4 mm Hg, P < .05) but not at 9 weeks. At this stage, the mean blood pressure of Hoe 140-treated rats was higher than that of control animals, and this difference was more pronounced at 12 weeks in female rats (121 +/- 2 versus 100 +/- 3 mm Hg in control animals, P < .01) compared with males (116 +/- 3 versus 104 +/- 2 mm Hg in control animals, P < .05). After the first week of life, body weight gain was greater in Hoe 140-treated female rats than in control rats, whereas a group-difference was detected in male rats only after weaning. In Hoe 140-treated female rats, heart weight was already increased at 9 weeks (330 +/- 6 versus 305 +/- 5 mg/100 g body wt in control rats, P < .05), whereas it was necessary to prolong Hoe 140 administration in male rats to develop heart hypertrophy (300 +/- 4 versus 275 +/- 4 mg/100 g body wt in control rats at 12 weeks, P < .05). Tissue kallikrein mRNA levels were higher in the kidney of adult female rats, whereas no sex difference was detected in the heart. The finding of a sexual dimorphism in the cardiovascular response to early blockade of bradykinin receptor suggests that endogenous kinins play a role in the regulation of cardiovascular function in both sexes, but they may be functionally more important in the female rat.

摘要

为了评估用Hoe 140(D-精氨酸[Hyp3,Thi5,D- Tic7,Oic8]-缓激肽)早期阻断缓激肽B2受体所诱导的心血管效应是否受性别影响,雌雄Wistar大鼠从2日龄至7周龄通过皮下注射,然后通过腹腔输注接受拮抗剂(300 nmol/(d·kg体重))或赋形剂。与对照大鼠相比,经Hoe 140处理的雌性大鼠在7周龄和9周龄时收缩压水平更高(分别为125±2与111±2 mmHg和132±3与116±2 mmHg,P<0.05),而雄性大鼠仅在7周龄时发现差异(122±4与108±4 mmHg,P<0.05),9周龄时未发现差异。在此阶段,经Hoe 140处理的大鼠的平均血压高于对照动物,且这种差异在雌性大鼠12周龄时比雄性大鼠更明显(对照动物分别为121±2与100±3 mmHg,P<0.01)(对照动物分别为116±3与104±2 mmHg,P<0.05)。出生后第一周后,经Hoe 140处理的雌性大鼠体重增加大于对照大鼠,而雄性大鼠仅在断奶后检测到组间差异。在经Hoe 140处理的雌性大鼠中,9周龄时心脏重量已增加(330±6与对照大鼠305±5 mg/100 g体重,P<0.05),而雄性大鼠则需要延长Hoe 140给药时间才能出现心脏肥大(12周龄时对照大鼠为300±4与275±4 mg/100 g体重,P<0.05)。成年雌性大鼠肾脏中组织激肽释放酶mRNA水平较高,而心脏中未检测到性别差异。缓激肽受体早期阻断的心血管反应中存在性二态性这一发现表明,内源性激肽在两性心血管功能调节中均起作用,但它们在雌性大鼠中可能在功能上更重要。

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