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肾上腺髓质素通过激活ATP依赖性钾通道,减少新生儿脑损伤后性别依赖性的降压性脑血管舒张功能丧失。

Adrenomedullin reduces gender-dependent loss of hypotensive cerebrovasodilation after newborn brain injury through activation of ATP-dependent K channels.

作者信息

Armstead William M, Vavilala Monica S

机构信息

Departments of Anesthesiology and Critical Care and Pharmacology, University of Pennsylvania, Philadelphia, Pennsylvania, USA.

出版信息

J Cereb Blood Flow Metab. 2007 Oct;27(10):1702-9. doi: 10.1038/sj.jcbfm.9600473. Epub 2007 Mar 21.

Abstract

Cerebrovascular dysregulation during hypotension occurs after fluid percussion brain injury (FPI) in the newborn pig owing to impaired K channel function. This study was designed to (1) determine the role of gender and K channel activation in adrenomedullin (ADM) cerebrovasodilation, (2) characterize the role of gender in the loss of hypotensive cerebrovasodilation after FPI, and (3) determine the role of gender in the ability of exogenous ADM to modulate hypotensive dysregulation after FPI. Lateral FPI (2 atm) was induced in newborn male and female newborn pigs (1 to 5 days old) equipped with a closed cranial window, n=6 for each protocol. Adrenomedullin-induced pial artery dilation was significantly greater in female than male piglets and blocked by the K(ATP) channel antagonist glibenclamide, but not by the K(ca) channel antagonist iberiotoxin. Cerebrospinal fluid ADM was increased from 3.8+/-0.7 to 14.6+/-3.0 fmol/mL after FPI in female but was unchanged in male piglets. Hypotensive pial artery dilation was blunted to a significantly greater degree in male versus female piglets after FPI. Topical pretreatment with a subthreshold vascular concentration of ADM (10(-10) mol/L) before FPI reduced the loss of hypotensive pial artery dilation in both genders, but protection was significantly greater in male versus female piglets. These data show that hypotensive pial artery dilation is impaired after FPI in a gender-dependent manner. By unmasking a gender-dependent endogenous protectant, these data suggest novel gender-dependent approaches for clinical intervention in the treatment of perinatal traumatic brain injury.

摘要

新生猪在液体冲击脑损伤(FPI)后,由于钾通道功能受损,会在低血压期间出现脑血管调节异常。本研究旨在:(1)确定性别和钾通道激活在肾上腺髓质素(ADM)介导的脑血管舒张中的作用;(2)明确性别在FPI后低血压性脑血管舒张功能丧失中的作用;(3)确定性别在外源性ADM调节FPI后低血压性调节异常能力中的作用。对配备封闭颅骨视窗的1至5日龄新生雄性和雌性仔猪诱导侧方FPI(2个大气压),每个方案n = 6。肾上腺髓质素诱导的软脑膜动脉舒张在雌性仔猪中显著大于雄性仔猪,并被K(ATP)通道拮抗剂格列本脲阻断,但未被K(ca)通道拮抗剂iberiotoxin阻断。FPI后,雌性仔猪脑脊液ADM从3.8±0.7增加到14.6±3.0 fmol/mL,而雄性仔猪则无变化。FPI后,雄性仔猪低血压性软脑膜动脉舒张的减弱程度明显大于雌性仔猪。FPI前用亚阈值血管浓度的ADM(10(-10)mol/L)进行局部预处理,可减少两性低血压性软脑膜动脉舒张的丧失,但雄性仔猪的保护作用明显大于雌性仔猪。这些数据表明,FPI后低血压性软脑膜动脉舒张以性别依赖的方式受损。通过揭示一种性别依赖的内源性保护剂,这些数据提示了围产期创伤性脑损伤治疗中性别依赖的新型临床干预方法。

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