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基于亚氯酸盐的药物WF10对血红素诱导的红细胞溶血的抑制作用。

Inhibition of the heme-induced hemolysis of red blood cells by thechlorite-based drug WF10.

作者信息

Flemmig J, Schlorke D, Kühne F-W, Arnhold J

机构信息

a Institute for Medical Physics and Biophysics, University of Leipzig , Leipzig , Germany.

b OXO Chemie (Thailand) Co., Ltd , Bangkok , Thailand.

出版信息

Free Radic Res. 2016 Dec;50(12):1386-1395. doi: 10.1080/10715762.2016.1252838. Epub 2016 Nov 23.

Abstract

Excessive release of hemoglobin from red blood cells markedly disturbs the health status of patients due to cytotoxic effects of free hemoglobin and heme. The latter component is able to initiate novel hemolytic events in unperturbed red blood cells. We modeled this process by incubation of ferric protoporphyrin IX with freshly isolated red blood cells from healthy volunteers. The heme-induced hemolysis was inhibited in a concentration-dependent manner by the chlorite-based drug WF10, whereby the hemolysis degree was totally abolished at a molar ratio of 1:2 between chlorite and heme. Upon incubation of heme with WF10, the ultraviolet-visible spectrum changed, whereas the release of iron from heme and the appearance of fluorescent breakdown products of the porphyrin ring were negligible at this ratio, but increased with increasing excess of chlorite over heme. Thus, inhibition of hemolysis by WF10 takes already place at those chlorite concentrations, where no degradation of the porphyrin ring occurs. As WF10 is applied in form of an intravenous infusion to patients with severe inflammatory states, these data support the hypothesis that the beneficial WF10 effects are closely associated with inactivation of free heme.

摘要

红细胞中血红蛋白的过度释放会因游离血红蛋白和血红素的细胞毒性作用而显著扰乱患者的健康状况。后者能够在未受干扰的红细胞中引发新的溶血事件。我们通过将铁卟啉IX与从健康志愿者新鲜分离的红细胞孵育来模拟这一过程。基于亚氯酸盐的药物WF10以浓度依赖的方式抑制血红素诱导的溶血,在亚氯酸盐与血红素的摩尔比为1:2时溶血程度完全消除。将血红素与WF10孵育后,紫外可见光谱发生变化,而在此比例下,血红素中铁的释放和卟啉环荧光分解产物的出现可忽略不计,但随着亚氯酸盐相对于血红素过量增加而增加。因此,WF10对溶血的抑制作用在卟啉环未发生降解的亚氯酸盐浓度下就已发生。由于WF10以静脉输注的形式应用于重症炎症状态的患者,这些数据支持了有益的WF10效应与游离血红素失活密切相关的假说。

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