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肽对胃肠运动的调控:旧肽新招——新肽旧法

Control of gastrointestinal motility by peptides: old peptides, new tricks--new peptides, old tricks.

作者信息

Fox J A

机构信息

School of Nursing and Biomedical Sciences, McMaster University Faculty of Health Sciences, Hamilton, Ontario.

出版信息

Gastroenterol Clin North Am. 1989 Jun;18(2):163-77.

PMID:2474497
Abstract

The discovery of new peptides that may or may not be members of existing peptide families is stimulating research in the field of gastrointestinal motility. Before their function in control of human motility can be predicted, both anatomic and functional pathways must be determined in a number of animal models. In many instances this has just begun. In other instances old concepts must be revised. This review examines the recent findings that motor actions attributable to VIP and by extension to its colocalized family member PHI may occur by turning off a tonic release that has held the muscle in a relaxed state. For the opioid family, some of the very complex actions are probably attributable to its action to inhibit the tonic release of VIP. For the tachykinin/neurokinin family, the focus is on the potential role as a sensory transmitter released antidromically from afferent capsaicin-sensitive nerve endings. In summarizing the actions of galanin, the reader is cautioned against any extrapolation to other species, because the actions and structure of the peptides have been found to be different in each species examined. CGRP, again a sensory transmitter found colocalized with substance P, tends to exert an opposite action on the smooth muscle from substance P (that of relaxation), and the interactions between these peptides may well prove to be important in gastrointestinal reflexes. The PP, PYY, and NPY family require much more study in gastrointestinal motor systems but appear to act as presynaptic inhibitory transmitters in a variety of local motor reflexes. One caveat from one who studies these systems is never to predict the action of a new or old peptide in your system of study, because the complexity of the system appears to determine the action expressed.

摘要

新肽的发现,无论其是否属于现有肽家族成员,都推动着胃肠动力领域的研究。在预测它们对人类运动控制的功能之前,必须在多种动物模型中确定其解剖学和功能途径。在许多情况下,这才刚刚开始。在其他情况下,旧观念必须修正。本综述探讨了近期的研究发现,即归因于血管活性肠肽(VIP)以及由此延伸到与其共定位的家族成员肽组氨酸异亮氨酸(PHI)的运动作用,可能是通过关闭使肌肉处于松弛状态的紧张性释放来实现的。对于阿片肽家族,一些非常复杂的作用可能归因于其抑制VIP紧张性释放的作用。对于速激肽/神经激肽家族,重点在于其作为从传入辣椒素敏感神经末梢逆向释放的感觉递质的潜在作用。在总结甘丙肽的作用时,提醒读者不要对其他物种进行任何外推,因为在所研究的每个物种中,肽的作用和结构都有所不同。降钙素基因相关肽(CGRP)也是一种与P物质共定位的感觉递质,它对平滑肌的作用往往与P物质相反(即舒张作用),这些肽之间的相互作用很可能在胃肠反射中发挥重要作用。胰多肽(PP)、酪酪肽(PYY)和神经肽Y(NPY)家族在胃肠运动系统中还需要更多研究,但它们似乎在各种局部运动反射中充当突触前抑制性递质。一位研究这些系统的人员提出的一个告诫是,永远不要预测新的或旧的肽在你所研究的系统中的作用,因为系统的复杂性似乎决定了所表现出的作用。

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