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速激肽拮抗剂与气道

Tachykinin antagonists and the airways.

作者信息

Joos G F, Kips J C, Peleman R A, Pauwels R A

机构信息

Department of Respiratory Diseases, University Hospital Ghent, Belgium.

出版信息

Arch Int Pharmacodyn Ther. 1995 Jan-Feb;329(1):205-19.

PMID:7543746
Abstract

There is now convincing evidence for the presence of substance P (SP) and neurokinin A (NKA) in human airway nerves. Studies on autopsy tissue, on bronchoalveolar lavage fluid and on sputum suggest that SP may be present in increased amounts in the asthmatic airway. Substance P and NKA are potent bronchoconstrictors of human airways, asthmatics being more sensitive than normal persons. The major enzyme responsible for the degradation of the tachykinins, the neutral endopeptidase, is present in the airways and is involved in the breakdown of exogenously administered SP and NKA, both in normal and asthmatic persons. Other, less well documented airway effects of SP and NKA include mucus secretion, vasodilation and plasma extravasation, as well as the chemoattraction and stimulation of various cells presumed to be involved in asthmatic airway inflammation. NK2 receptors and, to a lesser extent, NK1 receptors have been shown to be involved in bronchoconstriction, whereas NK1 receptors were found to be involved in mucus secretion, microvascular leakage and vasodilatation, and in most of the effects on inflammatory cells. The first clinical trial with FK224, a peptide NK1 and NK2 receptor antagonist, and CP99994, a nonpeptide NK1 receptor antagonist, are negative. However, FK224 failed to block the bronchoconstrictor effect of NKA in asthmatics and the dose of CP99994, needed to antagonize tachykinin effects in man, remains to be determined.

摘要

目前有令人信服的证据表明,人体内气道神经中存在P物质(SP)和神经激肽A(NKA)。对尸检组织、支气管肺泡灌洗液和痰液的研究表明,哮喘气道中SP的含量可能会增加。P物质和NKA是人类气道强力的支气管收缩剂,哮喘患者比正常人更敏感。负责降解速激肽的主要酶——中性内肽酶,存在于气道中,在正常人和哮喘患者体内均参与外源性给予的SP和NKA的分解代谢。SP和NKA的其他尚未得到充分记录的气道效应包括黏液分泌、血管舒张和血浆外渗,以及对各种推测参与哮喘气道炎症的细胞的化学吸引和刺激。已证明NK2受体以及程度较轻的NK1受体参与支气管收缩,而NK1受体参与黏液分泌、微血管渗漏和血管舒张,并参与对炎症细胞的大多数作用。首个使用肽类NK1和NK2受体拮抗剂FK224以及非肽类NK1受体拮抗剂CP99994的临床试验结果为阴性。然而,FK224未能阻断哮喘患者中NKA的支气管收缩作用,而在人体中拮抗速激肽作用所需的CP99994剂量仍有待确定。

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