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羟基脲在体外诱导正常血红蛋白和镰状细胞血红蛋白变性。

Hydroxyurea-induced denaturation of normal and sickle cell hemoglobins in vitro.

作者信息

Roa D, Kopsombut P, Aguinaga M P, Turner E A

机构信息

Comprehensive Sickle Cell Center, Meharry Medical College, Nashville, Tennessee 37208-3599, USA.

出版信息

J Clin Lab Anal. 1997;11(4):208-13. doi: 10.1002/(sici)1098-2825(1997)11:4<208::aid-jcla6>3.0.co;2-4.

Abstract

Use of hydroxyurea (HU) to treat sickle cell disease is usually associated with increments in fetal hemoglobin (Hb F) production; however, in vitro studies show that HU may also induce hemoglobin denaturation. Whole blood samples from Hb AA, Hb AS, and Hb SS patients were treated in vitro with 100, 150, 200, 250, and 300 micrograms/mL HU, incubated at 30 degrees C for up to 12 days, and analyzed by high-performance liquid chromatography (HPLC). Hb AA levels show decrements of 91 to 14% with 100 micrograms/mL and 89 to 4% with 150 micrograms/mL after 12 days; 86 to 2% with 200 micrograms/mL after 10 days; 86 to 8% with 250 and 300 micrograms/mL after 8 days. Similar treatment and incubation times for Hb AS whole blood demonstrate that HU equally degrades the A and S components of Hb AS. A comparable approach for Hb SS whole blood samples, using a 300 micrograms/mL HU treatment, showed a hemoglobin denaturing pattern that went from 93% to 1% after 12 days. Globin chain analysis of these samples by reverse-phase HPLC showed that the denaturing effects occur mostly on the beta-globin chain.

摘要

使用羟基脲(HU)治疗镰状细胞病通常与胎儿血红蛋白(Hb F)生成增加相关;然而,体外研究表明HU也可能诱导血红蛋白变性。来自Hb AA、Hb AS和Hb SS患者的全血样本在体外分别用100、150、200、250和300微克/毫升的HU进行处理,在30℃下孵育长达12天,然后通过高效液相色谱(HPLC)进行分析。12天后,Hb AA水平在100微克/毫升时下降了91%至14%,在150微克/毫升时下降了89%至4%;10天后,200微克/毫升时下降了86%至2%;8天后,250和300微克/毫升时下降了86%至8%。对Hb AS全血进行类似的处理和孵育时间表明,HU同样会降解Hb AS的A和S成分。对Hb SS全血样本采用类似方法,用300微克/毫升的HU处理,结果显示血红蛋白变性模式在12天后从93%降至1%。通过反相HPLC对这些样本进行珠蛋白链分析表明,变性作用主要发生在β珠蛋白链上。

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