首页> 外文期刊>Cryobiology: International Journal of Low Temperature Biology and Medicine >Cold storage of rabbit thoracic aorta in University of Wisconsin solution attenuates P2Y(2) purine receptors.
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Cold storage of rabbit thoracic aorta in University of Wisconsin solution attenuates P2Y(2) purine receptors.

机译:威斯康星大学溶液中的兔胸主动脉的冷存储减弱P2Y(2)嘌呤受体。

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Post-transplantation thrombosis may occur in donor segments of iliac arteries and livers following surgical removal and storage in University of Wisconsin (UW) solution for transplantation. We have previously suggested that purine receptors are vulnerable to denaturation after UW storage. The aims of the present study were to determine what particular subtypes of purine P2Y receptors in rabbit thoracic aorta deteriorate after 8 days of UW storage by studying vascular reactivity to acetylcholine, ATP, 2MeSATP and UTP. Ring segments of aortae from male New Zealand White rabbits were mounted upon fine-wire myographs and vasodilatation to the above agents tested on fresh tissue, and after 8 days of UW storage. Vasodilatation to ATP was attenuated by 100&mgr;M L-NAME in fresh tissue suggesting that the relaxant response was, in part, due to nitric oxide (NO). P2Y-mediated relaxation to ATP was significantly attenuated by UW storage and cholinergic responses were not. This attenuated relaxation to ATP was not further attenuated by L-NAME, suggesting a loss of the NO-dependent mechanism. De-endothelialisation indicated that UTP-mediated vasorelaxation, via P2Y(2) receptors, was endothelium-dependent. Any residual endothelium-independent relaxation to UTP was abolished by UW storage and endothelium-dependent UTP relaxation was reduced to the same level as that seen in fresh, de-endothelialised tissue. In contrast responses to 2MeSATP, via P2Y(1) receptors, were predominantly endothelium-independent and were only partially attenuated by UW storage. Responses to pyridoxalphosphate-6-azophenyl-2('),4(')-disulphonic acid (PPADS) and L-NAME suggested that vasorelaxation to 2MeSATP and UTP was mediated by P2Y(1) and P2Y(2) receptors, respectively. It is therefore concluded that UW storage predominantly decreases P2Y(2) receptor-mediated vascular reactivity.
机译:在威斯康星大学(UW)解决方案中进行外科手术切除和储存后,在动脉和肝脏的供体段中可能发生移植后血栓形成。我们以前曾提出,嘌呤受体在UW储存后容易变性。本研究的目的是通过研究血管对乙酰胆碱,ATP,2MeSATP和UTP的反应性,确定UW储存8天后胸主动脉中嘌呤P2Y受体的哪些特定亚型恶化。在UW储存8天后,将来自雄性新西兰白兔的主动脉的环段通过细线肌电图仪和血管舒张术安装到在新鲜组织上测试的上述试剂上。在新鲜组织中,ATP的血管舒张作用减弱了100 mg L-NAME,这表明松弛反应部分是由于一氧化氮(NO)引起的。 P2Y介导的ATP松弛通过UW储存显着减弱,而胆碱能反应则没有。 L-NAME并没有进一步减弱这种减弱的对ATP的弛豫,表明失去了NO依赖性机制。去内皮化表明UTP介导的血管舒张,通过P2Y(2)受体,是内皮依赖性的。 UW储存消除了任何残留的非内皮依赖性UTP松弛,并且内皮依赖性UTP松弛降低至与新鲜,去内皮化组织中相同的水平。相比之下,通过P2Y(1)受体对2MeSATP的反应主要是内皮依赖性的,并且仅被UW储存部分减弱。对吡ido醛磷酸-6-偶氮苯基-2('),4(')-二磺酸(PPADS)和L-NAME的反应表明,向2MeSATP和UTP的血管舒张作用分别由P2Y(1)和P2Y(2)受体介导。因此得出的结论是,UW存储主要降低P2Y(2)受体介导的血管反应性。

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