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内皮素-1对清醒大鼠血管通透性的影响:与血小板活化因子的相互作用。

Effects of endothelin-1 on vascular permeability in the conscious rat: interactions with platelet-activating factor.

作者信息

Filep J G, Sirois M G, Rousseau A, Fournier A, Sirois P

机构信息

Department of Pharmacology, Faculty of Medicine, University of Sherbrooke, Canada.

出版信息

Br J Pharmacol. 1991 Dec;104(4):797-804. doi: 10.1111/j.1476-5381.1991.tb12509.x.

Abstract
  1. The objectives of the present experiments were to assess the effects of endothelin-1 on the macrovascular permeability in selected vascular beds, to study the involvement of platelet-activating factor (PAF) in vascular responses to endothelin-1 and to examine the vascular effects of combined administration of endothelin-1 and PAF in conscious rats. 2. Intravenous bolus injection of endothelin-1 (0.1-2 nmol kg-1) resulted in a dose-dependent biphasic change in mean arterial blood pressure (MABP) with initial transient hypotension followed by a prolonged pressor action. These changes were accompanied by a dose-dependent increase in haematocrit values. 3. Endothelin-1 (0.1 and 1 nmol kg-1) increased dose-dependently the vascular permeability of the trachea, upper and lower bronchi, stomach, duodenum, spleen and kidney (up to 240%) as measured by the extravasation of Evans blue dye. The permeability of pulmonary parenchyma, liver and pancreas was not affected significantly by endothelin-1 treatment. 4. Pretreatment of animals with the specific PAF receptor antagonist, WEB 2086 (1 mg kg-1, i.v.) or BN 52021 (10 mg kg-1, i.v.) reduced the endothelin-1 (1 nmol kg-1)-induced rise in haematocrit by about 50 and 30%, respectively. Both antagonists were highly effective at inhibiting protein extravasation in the stomach, duodenum and kidney. On the other hand, BN 52021, but not WEB 2086, significantly attenuated the effect of endothelin-1 on permeability in the lower bronchi and spleen. Neither WEB 2086 nor BN 52021 modified the changes in MABP evoked by endothelin-1.5. When low doses of endothelin-1 (0.1 nmolkg-')and PAF (0.19nmolkg-')were administered simultaneously, enhanced protein extravasation was detected in the upper and lower bronchi, whereas neither endothelin-1 nor PAF by themselves affected vascular permeability in these tissues. These changes occurred in the absence of significant changes in MABP.6. Combined administration of higher doses of endothelin-1 (1nmolkg-') and PAF (1.9nmolkg-') resulted in marked increases (up to 530%) in protein extravasation in the airways, pancreas, stomach and duodenum. The effect of endothelin-1 on permeability was not affected by PAF in the spleen, whereas it was completely inhibited by PAF in the kidney. Combined injection of endothelin-1 and PAF resulted in a slight, but significant increase in MABP.7. The present findings show that endothelin-1 is capable of increasing vascular permeability in selected vascular beds including the airways, gastrointestinal tract and kidney, and suggest that PAF may mediate, in part, its action on permeability, but not its hypotensive action. The present data also suggest that endothelin-1 and PAF can act in concert to increase vascular permeability in rat airways and gastrointestinal tract.
摘要
  1. 本实验的目的是评估内皮素 -1 对特定血管床大血管通透性的影响,研究血小板活化因子(PAF)在血管对内皮素 -1 反应中的作用,并检测内皮素 -1 与 PAF 联合给药对清醒大鼠的血管效应。2. 静脉推注内皮素 -1(0.1 - 2 nmol·kg⁻¹)导致平均动脉血压(MABP)出现剂量依赖性双相变化,起初短暂低血压,随后是持续的升压作用。这些变化伴随着血细胞比容值的剂量依赖性增加。3. 内皮素 -1(0.1 和 1 nmol·kg⁻¹)通过伊文思蓝染料外渗测定,剂量依赖性地增加气管、上下支气管、胃、十二指肠、脾脏和肾脏的血管通透性(高达 240%)。内皮素 -1 处理对肺实质、肝脏和胰腺的通透性无显著影响。4. 用特异性 PAF 受体拮抗剂 WEB 2086(1 mg·kg⁻¹,静脉注射)或 BN 52021(10 mg·kg⁻¹,静脉注射)预处理动物,分别使内皮素 -1(1 nmol·kg⁻¹)诱导的血细胞比容升高降低约 50%和 30%。两种拮抗剂在抑制胃、十二指肠和肾脏中的蛋白质外渗方面都非常有效。另一方面,BN 52021 而非 WEB 2086 显著减弱了内皮素 -1 对下支气管和脾脏通透性的影响。WEB 2086 和 BN 52021 均未改变内皮素 -1 引起的 MABP 变化。5. 当同时给予低剂量的内皮素 -1(0.1 nmol·kg⁻¹)和 PAF(0.19 nmol·kg⁻¹)时,在上、下支气管中检测到蛋白质外渗增强,而单独的内皮素 -1 或 PAF 均不影响这些组织的血管通透性。这些变化发生时 MABP 无显著变化。6. 联合给予高剂量的内皮素 -1(1 nmol·kg⁻¹)和 PAF(1.9 nmol·kg⁻¹)导致气道、胰腺、胃和十二指肠中的蛋白质外渗显著增加(高达 530%)。在脾脏中,PAF 不影响内皮素 -1 对通透性的作用,而在肾脏中,PAF 完全抑制了内皮素 -1 的作用。内皮素 -1 和 PAF 联合注射导致 MABP 轻微但显著升高。7. 目前的研究结果表明,内皮素 -1 能够增加包括气道、胃肠道和肾脏在内的特定血管床的血管通透性,并提示 PAF 可能部分介导其对通透性的作用,但不介导其降压作用。目前的数据还表明,内皮素 -1 和 PAF 可协同作用增加大鼠气道和胃肠道的血管通透性。

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