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S-亚硝基化聚乙二醇化血红蛋白可减小大鼠脑梗死体积。

S-nitrosylated pegylated hemoglobin reduces the size of cerebral infarction in rats.

作者信息

Kawaguchi Akira T, Nakai Kunihiko, Fukumoto Dai, Yamano Mariko, Haida Munetaka, Tsukada Hideo

机构信息

Tokai University School of Medicine, Isehara, Kanagawa, Japan.

出版信息

Artif Organs. 2009 Feb;33(2):183-8. doi: 10.1111/j.1525-1594.2008.00705.x.

Abstract

Cell-free hemoglobin-based oxygen carriers have well-documented safety and efficacy problems such as nitric oxide (NO) scavenging and extravasation that preclude clinical use. To counteract these effects, we developed S-nitrosylated pegylated hemoglobin (SNO-PEG-Hb, P(50) = 12 mm Hg) and tested it in a brain ischemia and reperfusion model. Neurological function and extent of cerebral infarction was determined 24 h after photochemically induced thrombosis of the middle cerebral artery in the rat. Infarction extent was determined from the integrated area in the cortex and basal ganglia detected by triphenyltetrazolium chloride staining in rats receiving various doses of SNO-PEG-Hb (2, 0.4, and 0.08 mL/kg) and compared with rats receiving pegylated hemoglobin without S-nitrosylation (PEG-Hb) or saline of the same dosage. Results indicated that successive dilution revealed SNO-PEG-Hb but not PEG-Hb to be effective in reducing the size of cortical infarction but not neurological function at a dose of 0.4 mL/kg. In conclusion, SNO-PEG-Hb in a dose of 0.4 mL/kg (Hb 24 mg/kg) showed to be most effective in reducing the size of cortical infarction, however, without functional improvement.

摘要

无细胞血红蛋白基氧载体存在诸如一氧化氮(NO)清除和血管外渗等有充分文献记载的安全性和有效性问题,这使得其无法用于临床。为抵消这些影响,我们研发了S-亚硝基化聚乙二醇化血红蛋白(SNO-PEG-Hb,P(50)=12mmHg),并在脑缺血再灌注模型中对其进行了测试。在大鼠大脑中动脉光化学诱导血栓形成24小时后,测定神经功能和脑梗死范围。通过对接受不同剂量SNO-PEG-Hb(2、0.4和0.08mL/kg)的大鼠进行氯化三苯基四氮唑染色,测定皮质和基底神经节的积分面积,从而确定梗死范围,并与接受未进行S-亚硝基化的聚乙二醇化血红蛋白(PEG-Hb)或相同剂量生理盐水的大鼠进行比较。结果表明,连续稀释显示,在0.4mL/kg的剂量下,SNO-PEG-Hb而非PEG-Hb可有效减小皮质梗死面积,但对神经功能无影响。总之,0.4mL/kg(血红蛋白24mg/kg)剂量的SNO-PEG-Hb在减小皮质梗死面积方面显示出最有效的效果,然而,并未改善功能。

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