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内皮素-1和一氧化氮生物利用度在移植相关血管损伤中的作用:雷帕霉素和环孢素的比较效应

Role of endothelin-1 and nitric oxide bioavailability in transplant-related vascular injury: comparative effects of rapamycin and cyclosporine.

作者信息

Ramzy Danny, Rao Vivek, Tumiati Laura C, Xu Ning, Miriuka Santiago, Delgado Diego, Ross Heather J

机构信息

Heart Transplant Program, Toronto General Hospital, University Health Network, University of Toronto, Toronto, Ontario, Canada.

出版信息

Circulation. 2006 Jul 4;114(1 Suppl):I214-9. doi: 10.1161/CIRCULATIONAHA.105.000471.

Abstract

BACKGROUND

Cyclosporine (CyA) is associated with many side effects, including endothelial dysfunction and transplant vasculopathy (TxV). We previously demonstrated that CyA results in impairment of nitric oxide bioavailability and enhanced sensitivity to endothelin-1 (ET-1). In this study, we evaluated rapamycin (SRL) for its effects on the endothelium.

METHODS AND RESULTS

Lewis rats (n = 8) were injected with SRL (1.5 mg/kg), CyA (5 mg/Kg), or saline (Con) intraperitoneally daily for 2-weeks. Thoracic aortic segments were assessed for endothelial-dependent (Edep) and independent (Eind) relaxation after exposure to acetylcholine and sodium nitroprusside by deriving the percent maximum relaxation (Emax). ET-1 plasma levels were also measured. Thoracic aortic expression of endothelial nitric oxide synthase (eNOS), ET(A) and ET(B) receptors (Rc), were determined. Oxidative injury was assessed by changes in 8-isoprostane levels. CyA exposure resulted in lower Edep vasorelaxation compared with control and SRL (Emax: SRL, 58+/-4%; CyA, 24+/-7%; Con, 52+/-8%; P=0.001). No differences in Eind vasorelaxation were seen. CyA exposure also increased sensitivity to ET-1 (% maximum contraction [Cmax]: Con, 211+/-8%; SRL, 230+/-5%; CyA, 259+/-3%; P=0.04). Only SRL treatment reduced ET-1 plasma levels. CyA reduced eNOS expression by 30% and increased ETA Rc expression by 34% compared with both Con and SRL (P=0.02). CyA resulted in higher 8-isoprostane levels (CyA, 50+/-2%; SRL, 3+/-3%; Con, 2+/-5%; P=0.02).

CONCLUSIONS

CyA results in vascular dysfunction characterized by impairment of Edep vasorelaxation and enhanced sensitivity to vasospasm. SRL did not impair Edep vasorelaxation or increase sensitivity to vasospasm while lowering ET-1 levels and preserving eNOS protein expression. We conclude that SRL is less deleterious to the vasculature than CyA and may prevent TxV by these mechanisms.

摘要

背景

环孢素(CyA)与许多副作用相关,包括内皮功能障碍和移植血管病变(TxV)。我们之前证明,CyA会导致一氧化氮生物利用度受损,并增强对内皮素-1(ET-1)的敏感性。在本研究中,我们评估了雷帕霉素(SRL)对内皮的影响。

方法与结果

将Lewis大鼠(n = 8)每天腹腔注射SRL(1.5 mg/kg)、CyA(5 mg/Kg)或生理盐水(对照),持续2周。通过计算最大舒张百分比(Emax),评估胸主动脉段在暴露于乙酰胆碱和硝普钠后的内皮依赖性(Edep)和非内皮依赖性(Eind)舒张。还测量了ET-1血浆水平。测定胸主动脉中内皮型一氧化氮合酶(eNOS)、ET(A)和ET(B)受体(Rc)的表达。通过8-异前列腺素水平的变化评估氧化损伤。与对照组和SRL相比,CyA暴露导致Edep血管舒张降低(Emax:SRL,58±4%;CyA,24±7%;对照,52±8%;P = 0.001)。Eind血管舒张未见差异。CyA暴露还增加了对ET-1的敏感性(最大收缩百分比[Cmax]:对照,211±8%;SRL,230±5%;CyA,259±3%;P = 0.04)。只有SRL治疗降低了ET-1血浆水平。与对照组和SRL相比,CyA使eNOS表达降低30%,并使ETA Rc表达增加34%(P = 0.02)。CyA导致8-异前列腺素水平升高(CyA,50±2%;SRL,3±3%;对照,2±5%;P = 0.02)。

结论

CyA导致血管功能障碍,其特征为Edep血管舒张受损和对血管痉挛的敏感性增强。SRL不会损害Edep血管舒张或增加对血管痉挛的敏感性,同时降低ET-1水平并保留eNOS蛋白表达。我们得出结论,SRL对血管系统的损害小于CyA,并且可能通过这些机制预防TxV。

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