速激肽NK3和NK1受体激活引发猪气道黏膜下腺的分泌。
Tachykinin NK3 and NK1 receptor activation elicits secretion from porcine airway submucosal glands.
作者信息
Phillips Jonathan E, Hey John A, Corboz Michel R
机构信息
Allergy, Schering-Plough Research Institute, 2015 Galloping Hill Road, Kenilworth, NJ 07033, U.S.A.
出版信息
Br J Pharmacol. 2003 Jan;138(1):254-60. doi: 10.1038/sj.bjp.0705029.
1 We presently characterized the tachykinin receptor subtypes, using tachykinin receptor agonists and selective antagonists, that induce submucosal gland fluid flux (J(G)) from porcine tracheal explants with the hillocks technique. We also investigated the effects of the tachykinin receptor agonists on the electrophysiologic parameters of the tracheal epithelium in Ussing chambers. 2 The NK(1) tachykinin receptor agonist substance P (SP, 1 microM) and the NK(3) tachykinin receptor agonist [MePhe(7)]neurokinin B ([MePhe(7)]NKB, 1 microM) induced gland fluid fluxes of 0.29+/-0.03 microl min(-1) cm(-2) (n=26) and 0.36+/-0.05 microl min(-1) cm(-2) (n=24), respectively; while the NK(2) tachykinin receptor agonist [betaAla(8)]neurokinin A (4-10) ([betaAla(8)]NKA (4-10), 1 microM) had no effect on J(G) (n=10). 3 The NK(1) receptor antagonist CP99994 (1 microM, n=9) blocked 93% of the SP-induced J(G), whereas the NK(3) receptor antagonist SB223412 (1 microM, n=12) had no effect on the SP-induced J(G). However, SB223412 (1 microM, n=9) blocked 89% of the [MePhe(7)]NKB-induced J(G) while CP99994 (1 microM, n=10) did not affect the [MePhe(7)]NKB-induced J(G). The NK(2) receptor antagonist SR48968 (1 microM) did not block the J(G) induced by either the NK(1) (n=4) or NK(3) (n=13) receptor agonists. 4 The nicotinic ganglionic acetylcholine receptor antagonist hexamethonium (1 microM) and the muscarinic acetylcholine receptor antagonist atropine (1 microM) also decreased the NK(3) receptor agonist-induced J(G) by 67% (n=10) and 71% (n=12), respectively. 5 The potential difference (PD), short-circuit current (I(SC)), and membrane resistance (R(M)) of the porcine tracheal epithelial membranes were not significantly affected by any of the neurokinin agonists or antagonists (1 microM, basolateral) used in this study, although SP and [betaAla(8)]NKA (4-10) induced a slight transient epithelial hyperpolarization. 6 These data suggest that NK(1) and NK(3) receptors induce porcine airway gland secretion by different mechanisms and that the NK(3) receptor agonists induced secretion is likely due to activation of prejunctional NK(3) receptors on parasympathetic nerves, resulting in acetylcholine-release. We conclude that tachykinin receptor antagonists may have therapeutic potential in diseases with pathophysiological mucus hypersecretion such as asthma and chronic bronchitis.
- 我们目前使用速激肽受体激动剂和选择性拮抗剂,通过小丘技术对猪气管外植体的黏膜下腺液通量(J(G))进行了速激肽受体亚型的鉴定。我们还研究了速激肽受体激动剂对Ussing室中气管上皮电生理参数的影响。2. NK(1)速激肽受体激动剂P物质(SP,1微摩尔)和NK(3)速激肽受体激动剂[MePhe(7)]神经激肽B([MePhe(7)]NKB,1微摩尔)分别诱导的腺液通量为0.29±0.03微升·分钟(-1)·厘米(-2)(n = 26)和0.36±0.05微升·分钟(-1)·厘米(-2)(n = 24);而NK(2)速激肽受体激动剂[βAla(8)]神经激肽A(4 - 10)([βAla(8)]NKA (4 - 10),1微摩尔)对J(G)无影响(n = 10)。3. NK(1)受体拮抗剂CP99994(1微摩尔,n = 9)阻断了93%的SP诱导的J(G),而NK(3)受体拮抗剂SB223412(1微摩尔,n = 12)对SP诱导的J(G)无影响。然而,SB223412(1微摩尔,n = 9)阻断了89%的[MePhe(7)]NKB诱导的J(G),而CP99994(1微摩尔,n = 10)不影响[MePhe(7)]NKB诱导的J(G)。NK(2)受体拮抗剂SR48968(1微摩尔)不阻断NK(1)(n = 4)或NK(3)(n = 13)受体激动剂诱导的J(G)。4. 烟碱型神经节乙酰胆碱受体拮抗剂六甲铵(1微摩尔)和毒蕈碱型乙酰胆碱受体拮抗剂阿托品(1微摩尔)也分别使NK(3)受体激动剂诱导的J(G)降低了67%(n = 10)和71%(n = 12)。5. 本研究中使用的任何神经激肽激动剂或拮抗剂(1微摩尔,基底外侧)对猪气管上皮膜的电位差(PD)、短路电流(I(SC))和膜电阻(R(M))均无显著影响,尽管SP和[βAla(8)]NKA (4 - 10)诱导了轻微的短暂上皮超极化。6. 这些数据表明,NK(1)和NK(3)受体通过不同机制诱导猪气道腺分泌,并且NK(3)受体激动剂诱导的分泌可能是由于副交感神经上的节前NK(3)受体激活,导致乙酰胆碱释放。我们得出结论,速激肽受体拮抗剂在哮喘和慢性支气管炎等具有病理生理性黏液分泌过多的疾病中可能具有治疗潜力。
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