Nucleotides and their receptors in the nervous system, Leipzig, Germany, August 1-2, 1998

L. Köles
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Abstract

This symposium was organized by P. Illes (Univ. Leipzig, Germany), A. Reichenbach (Paul-Flechsig Institute for Brain Research, Leipzig, Germany) and H. Zimmermann (Univ. Frankfurt/Main, Germany). More than 150 experts on purinergic transmission met at a historical building of the University of Leipzig in the center of the town. The symposium consisted of 32 twenty-minute-long lectures by invited speakers from eleven countries. In addition, 50 posters were presented in two poster sessions. After an informal gathering of speakers, participants and guests on Friday evening, the official scientific program of the conference began on Saturday by the opening addresses of T. Butz (Univ. Leipzig) and P. Illes. The first session was chaired by E. A. Barnard (Royal Free Hospital School of Medicine, London, UK) and G. Burnstock (from the same institution). The first speaker of this session was one of the chairmen, G. Burnstock. He gave an outstanding lecture on the current status of purinergic signalling in the nervous system. He reviewed the history of purinergic transmission, from the early 1970s until now. The “purinergic nerve” hypothesis was proposed in 1972, with evidence to suggest that ATP is a neurotransmitter in some non-adrenergic, non-cholinergic nerves. Later it became evident that ATP is a cotransmitter with classical transmitters in autonomic and sensory-motor nerves. In 1978, receptors to purines were shown to belong to two main subtypes: P1 purinoceptors, which are selective for adenosine, and P2 purinoceptors, which are selective for ATP and ADP. Subsequently, subtypes of P1 purinoceptors: A1, A2a, A2b, and A3 were identified. Burnstock and colleagues proposed the subclassification of P2 purinoceptors into P2X and P2Y receptors. Further investigations revealed that the P2X receptors, which are ligand-gated cation channels, can be subclassified to at least seven subtypes, while the P2Y receptor family (G protein-coupled receptors) consists of at least 10 subtypes. G. Burnstock mentioned some new aspects of the purinergic research field at the end of his excellent presentation. P2X and P2Y receptors are present on sensory nerves, and might play an important role in mechanoception and nociception. There is rapidly expanding interest in purinergic signalling in the brain and spinal cord. The plasticity of purinergic cotransmission has a remarkable role in some pathophysiological conditions (e.g., interstitial cystitis, outflow obstruction of the bladder, hypertension). Apart from “fast” purinergic signalling in the nervous system, nucleotides play long-term (trophic) roles in development and degeneration.
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神经系统中的核苷酸及其受体,德国莱比锡,1998年8月1-2日
本次研讨会由P. Illes(德国莱比锡大学)、A. Reichenbach(德国莱比锡paul - flehsig脑研究所)和H. Zimmermann(德国法兰克福大学)共同主办。150多名研究嘌呤能传播的专家在市中心的莱比锡大学的一座历史建筑里会面。专题讨论会由来自11个国家的特邀发言者进行32次20分钟的演讲。此外,在两次海报会议上展出了50幅海报。周五晚上,在演讲者、参与者和嘉宾的非正式聚会之后,会议的正式科学项目于周六开始,由T. Butz(莱比锡大学)和P. Illes的开幕词开始。第一届会议由e.a. Barnard(英国伦敦皇家自由医院医学院)和G. Burnstock(来自同一机构)主持。这次会议的第一位发言人是主席之一G. Burnstock。他就神经系统嘌呤能信号传导的现状作了一次出色的演讲。他回顾了嘌呤能传播的历史,从20世纪70年代早期到现在。“嘌呤能神经”假说于1972年提出,有证据表明ATP是一些非肾上腺素能、非胆碱能神经中的一种神经递质。后来发现ATP在自主神经和感觉运动神经中与经典递质是一种共递质。1978年,嘌呤受体被证明属于两种主要亚型:P1嘌呤受体,对腺苷有选择性,P2嘌呤受体,对ATP和ADP有选择性。随后,鉴定出P1嘌呤受体A1、A2a、A2b和A3亚型。Burnstock等人提出P2嘌呤受体亚分类为P2X和P2Y受体。进一步的研究表明,作为配体门控阳离子通道的P2X受体可以被细分为至少7个亚型,而P2Y受体家族(G蛋白偶联受体)至少包括10个亚型。G. Burnstock在他精彩的演讲结束时提到了嘌呤能研究领域的一些新方面。P2X和P2Y受体存在于感觉神经上,可能在机械感觉和伤害感觉中起重要作用。人们对脑和脊髓中的嘌呤能信号的兴趣正在迅速扩大。嘌呤能共传递的可塑性在一些病理生理条件(如间质性膀胱炎、膀胱流出梗阻、高血压)中具有显著的作用。除了神经系统中的“快速”嘌呤能信号外,核苷酸在发育和退化中起着长期(营养)作用。
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