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三磷酸尿苷腺苷影响小鼠主动脉的收缩性,并降低清醒大鼠和小鼠的血压。

Uridine adenosine tetraphosphate affects contractility of mouse aorta and decreases blood pressure in conscious rats and mice.

机构信息

Cardiovascular and Renal Research, Institute of Medical Biology, University of Southern Denmark, Odense, Denmark.

出版信息

Acta Physiol (Oxf). 2010 Oct;200(2):171-9. doi: 10.1111/j.1748-1716.2010.02135.x.

Abstract

AIM

in the anaesthetized rat, uridine adenosine tetraphosphate (Up(4) A) is a circulating, endothelium-derived vasoconstrictor presumably operating as such in un-anaesthetized animals. The present study investigated the in vivo effects of Up(4) A in conscious mice and rats, and its direct vascular effects in the mouse aorta in vitro.

METHODS

in vivo, Up(4) A was given as step-up infusion at rates of 8-512 nmol min(-1) kg(-1) for 30 min periods in chronically catheterized rodents. In vitro, the effect of Up(4) A on rings of mouse aortae mounted in a myograph was tested.

RESULTS

high doses of Up(4) A (mice: 512 nmol min(-1) kg(-1) ; rats: 128 nmol min(-1) kg(-1) ) caused hypotension (99 (+/-)4 to 64 7(+/-) mmHg and 114 (+/-) 3 to 108 (+/-) 3 mmHg, respectively, both P < 0.01). In rats, Up(4) A significantly decreased sodium excretion by >75% and potassium excretion by approximately 60% without significant changes in urine flow. Exposure of phenylephrine-contracted rings to increasing concentrations of Up(4) A elicited contraction at 10(-7) and 10(-6) molL(-1) (18 ± 2% and 76 (+/-) 16% respectively); unexpectedly, 10(-5) molL(-1) caused a biphasic response with a contraction (19 6(+/-)2%) followed by a relaxation (-46 (+/-) 6%). No relaxation was observed when the concentration was increased further. Bolus exposure to 10(-5) molL(-1) of Up(4) A caused contraction (+80 (+/-) 2%). Added successively to untreated vessels, increasing concentrations of Up(4) A (10(-7) -10(-5) molL(-1) ) induced a biphasic response of contraction followed by relaxation.

CONCLUSION

up(4) A has direct biphasic effects on vascular smooth muscle of the mouse aorta but vasoconstriction dominates at low concentrations. In conscious rodents, step-up infusions of Up(4) A elicit hypotension and electrolyte retention.

摘要

目的

在麻醉大鼠中,尿苷腺苷四磷酸(Up4A)是一种循环的内皮衍生的血管收缩剂,在未麻醉动物中可能以此方式发挥作用。本研究旨在研究 Up4A 在清醒小鼠和大鼠体内的作用及其在体外对小鼠主动脉的直接血管作用。

方法

在体内,慢性导管化啮齿动物以 8-512nmolmin-1kg-1 的速度进行 Up4A 递增输注 30 分钟。在体外,测试 Up4A 对置于肌动描记器中的小鼠主动脉环的影响。

结果

高剂量 Up4A(小鼠:512nmolmin-1kg-1;大鼠:128nmolmin-1kg-1)导致低血压(分别为 99(+/-)4 至 647(+/-)mmHg 和 114(+/-)3 至 108(+/-)3mmHg,均 P<0.01)。在大鼠中,Up4A 显著降低钠排泄>75%,钾排泄约 60%,而尿液流量无明显变化。用苯肾上腺素收缩的环暴露于递增浓度的 Up4A 时,在 10-7 和 10-6molL-1 时引起收缩(分别为 18(+/-)2%和 76(+/-)16%);出乎意料的是,10-5molL-1 引起双相反应,收缩(196(+/-)2%)后松弛(-46(+/-)6%)。进一步增加浓度时,未观察到松弛。将 10-5molL-1 的 Up4A 单次暴露于血管时引起收缩(+80(+/-)2%)。连续加入未处理的血管时,递增浓度的 Up4A(10-7-10-5molL-1)引起收缩后松弛的双相反应。

结论

Up4A 对小鼠主动脉血管平滑肌有直接的双相作用,但低浓度时以血管收缩为主。在清醒的啮齿动物中,递增输注 Up4A 可引起低血压和电解质潴留。

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