Pharmaceutical Preconditioning With Nitric Oxide Synthase and l-Arginine in Ischemic Tissues

医学 一氧化氮合酶 一氧化氮 缺血预处理 精氨酸 药理学 内科学 缺血 生物化学 化学 氨基酸
作者
Emre Gazyakan,Christoph Hirche,Matthias A. Reichenberger,Günter Germann,Holger Engel
出处
期刊:Annals of Plastic Surgery [Ovid Technologies (Wolters Kluwer)]
卷期号:84 (6): 705-710 被引量:2
标识
DOI:10.1097/sap.0000000000002117
摘要

Background Nitric oxide (NO) is a multifunctional signaling molecule involved in regulating vascular tone and tissue oxygenation. It is also an important cytoprotective agent against ischemia-reperfusion injury (IRI). Enhancing NO bioavailability via exogenous NO synthases (NOSs) and L-arginine promotes conversation to NO, circumventing the problem of nonfunctioning NOSs under hypoxic and acidic conditions. In this study, the authors evaluated the therapeutic efficacy of neuronal, inducible, and endothelial NOS and L-arginine on reperfusion-induced skin flap alterations. Methods The vascular pedicle isolated rat skin flap model was used and underwent 3 hours of ischemia. At 30 minutes before ischemia, normal saline, endothelial-, inducible-, and neuronal NOSs (1/2 IU) and L-arginine (100 mg/kg body weight) were administered by means of intravenous infusion. The IRI-induced alterations were measured 5 days after the operation. Results The 3 isoforms of NOS increased the flap vitality rate (VR) from 10% to 23% compared with the control group. L-Arginine treatment also increased the VR by approximately 15%. The combination of L-arginine with NOS resulted in even higher flap VRs. The best results could be achieved with the combination of endothelial NOS (2 IU) and L-arginine. Conclusions Modulation of NO bioavailability via exogenous application of NOSs and L-arginine significantly improved VRs in a skin flap rat model. This pharmacologic preconditioning has the potential to attenuate IRI-induced alterations in skin flaps.
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