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ATP和去氧肾上腺素对血管加压素和催产素释放的持续刺激需要募集脱敏抗性P2X嘌呤能受体。

Sustained stimulation of vasopressin and oxytocin release by ATP and phenylephrine requires recruitment of desensitization-resistant P2X purinergic receptors.

作者信息

Gomes Dayane A, Song Zhilin, Stevens Wanida, Sladek Celia D

机构信息

Department of Physiology and Biophysics, University of Colorado Denver School of Medicine, Denver, Colorado 80045, USA.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2009 Oct;297(4):R940-9. doi: 10.1152/ajpregu.00358.2009. Epub 2009 Jul 22.

Abstract

Coexposure of hypothalamo-neurohypophyseal system explants to ATP and phenylephrine [PE; an alpha1-adrenergic receptor (alpha1-AR) agonist] induces an extended elevation in vasopressin and oxytocin (VP/OT) release. New evidence is presented that this extended response is mediated by recruitment of desensitization-resistant ionotropic purinergic receptor subtypes (P2X-Rs): 1) Antagonists of the P2X2/3 and P2X7-Rs truncated the sustained VP/OT release induced by ATP+PE but did not alter the transient response to ATP alone. 2) The P2X2/3 and P2X7-R antagonists did not alter either ATP or ATP+PE-induced increases in Ca(2+). 3) P2X2/3 and P2X7-R agonists failed to elevate Ca(2+), while ATP-gamma-S, an agonist for P2X2-Rs increased Ca(2+) and induced a transient increase in VP/OT release. 4) A P2Y1-R antagonist did not prevent initiation of the synergistic, sustained stimulation of VP/OT release by ATP+PE but did reduce its duration. Thus, the desensitization-resistant P2X2/3 and P2X7-R subtypes are required for the sustained, synergistic hormone response to ATP+PE, while P2X2-Rs are responsible for the initial activation of Ca(2+)-influx by ATP and ATP stimulation of VP/OT release. Immunohistochemistry, coimmunoprecipitation, and Western blot analysis confirmed the presence of P2X2 and P2X3, P2X2/3, and P2X7-R protein, respectively in SON. These findings support the hypothesis that concurrent activation of P2X2-R and alpha1-AR induces calcium-driven recruitment of P2X2/3 and 7-Rs, allowing sustained activation of a homeostatic circuit. Recruitment of these receptors may provide sustained release of VP during dehydration and may be important for preventing hemorrhagic and septic shock.

摘要

下丘脑 - 神经垂体系统外植体同时暴露于ATP和去氧肾上腺素[PE;一种α1 - 肾上腺素能受体(α1 - AR)激动剂]会导致血管加压素和催产素(VP/OT)释放出现长时间升高。新证据表明,这种延长反应是由脱敏抗性离子型嘌呤能受体亚型(P2X - Rs)的募集介导的:1)P2X2/3和P2X7 - Rs的拮抗剂可缩短由ATP + PE诱导的持续VP/OT释放,但不会改变对单独ATP的瞬时反应。2)P2X2/3和P2X7 - R拮抗剂既不会改变ATP或ATP + PE诱导的细胞内钙离子浓度(Ca(2 +))升高。3)P2X2/3和P2X7 - R激动剂未能升高Ca(2 +),而P2X2 - Rs的激动剂ATP - γ - S可增加Ca(2 +)并诱导VP/OT释放出现瞬时增加。4)P2Y1 - R拮抗剂不能阻止ATP + PE对VP/OT释放的协同、持续刺激的起始,但会缩短其持续时间。因此,脱敏抗性P2X2/3和P2X7 - R亚型是对ATP + PE产生持续、协同激素反应所必需的,而P2X2 - Rs负责ATP对Ca(2 +)内流的初始激活以及ATP对VP/OT释放的刺激。免疫组织化学、免疫共沉淀和蛋白质印迹分析分别证实了视上核中存在P2X2和P2X3、P2X2/3以及P2X7 - R蛋白。这些发现支持了以下假设:P2X2 - R和α1 - AR的同时激活会诱导钙驱动的P2X2/3和7 - Rs募集,从而使稳态回路持续激活。这些受体的募集可能在脱水过程中提供VP的持续释放,并且对于预防出血性和败血性休克可能很重要。

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