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The functional heterogeneity of eosinophil cationic protein is determined by a gene polymorphism and post-translational modifications.

机译:嗜酸性粒细胞阳离子蛋白的功能异质性由基因多态性和翻译后修饰决定。

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BACKGROUND: The eosinophil is a cytotoxic cell and takes part in parasite killing and tissue-destructive processes by secretion of proteins such as eosinophil cationic protein (ECP). A polymorphism was demonstrated in the ECP gene, giving rise to a substitution of arginine at position 97 with threonine. This polymorphism is related to disease development. OBJECTIVE: To investigate the functional and molecular heterogeneity of native ECP and the functional consequences of the replacement of arginine with a threonine. METHODS: ECP was purified from healthy blood donors by gel filtration, ion-exchange chromatography and reversed-phase chromatography. Recombinant ECPs i.e. rECP 97(arg) and rECP 97(thr) were produced by the pFASTBAC baculovirus expression system. The cytotoxic activity was determined against an erythroleukaemia or a small cell lung cancer cell line. RESULTS: Native ECP was purified to apparent homogeneity and showed a considerable molecular heterogeneity and a corresponding functional heterogeneity with respect to cytotoxic activity. After reduction, the native cytotoxic ECP showed three bands on sodium dodecylsulphate polyacrylamide gel electrophoresis : one major band at 18-20 kDa and two minor bands at about 10 and 5 kDa, respectively. The 5 kDa contained two masses differing with 56.2 Da, which corresponds to the difference in molecular masses of arginine and threonine. rECP 97(arg) was cytotoxic in contrast to rECP97(thr). Deglycosylation with N-glycosidase F did not affect the cytotoxic activity of native ECP to any measurable extent nor the activity of rECP 97(arg), whereas rECP 97(thr) achieved cytotoxic activity. The RNase activities of the recombinant and native ECPs were similar. CONCLUSION: We conclude that ECP is present in several molecular forms with varying biological activities. Some of this functional heterogeneity is based on the genetic polymorphism of the ECP gene and some on post-translational modifications. In subjects carrying the ECP 97(thr) variant, the cytotoxic activity may be disguised by N-linked glycosylation of the active site.
机译:背景:嗜酸性粒细胞是一种细胞毒性细胞,通过分泌诸如嗜酸性粒细胞阳离子蛋白(ECP)之类的蛋白质参与寄生虫杀伤和组织破坏过程。在ECP基因中证实了多态性,导致在97位的精氨酸被苏氨酸取代。这种多态性与疾病的发展有关。目的:研究天然ECP的功能和分子异质性,以及用苏氨酸替代精氨酸的功能后果。方法:通过凝胶过滤,离子交换色谱和反相色谱从健康献血者中纯化ECP。重组ECP,即rECP 97(arg)和rECP 97(thr)是通过pFASTBAC杆状病毒表达系统产生的。确定针对红白血病或小细胞肺癌细胞系的细胞毒性活性。结果:天然ECP纯化到明显的同质性,并表现出相当大的分子异质性和相应的功能异质性的细胞毒活性。还原后,天然的细胞毒性ECP在十二烷基硫酸钠聚丙烯酰胺凝胶电泳上显示三个条带:一个主要条带在18-20 kDa,两个次要条带分别在大约10和5 kDa。 5 kDa包含两个质量相差56.2 Da的质量,这对应于精氨酸和苏氨酸的分子质量差异。与rECP97(thr)相比,rECP 97(arg)具有细胞毒性。用N-糖苷酶F进行的去糖基化不会在任何可测量的程度上影响天然ECP的细胞毒活性,也不会影响rECP 97(arg)的活性,而rECP 97(thr)则具有细胞毒活性。重组和天然ECP的RNase活性相似。结论:我们得出结论,ECP以几种分子形式存在,具有不同的生物活性。这种功能异质性中的某些是基于ECP基因的遗传多态性,而某些则是基于翻译后修饰。在携带ECP 97(thr)变体的受试者中,细胞毒性活性可能被活性位点的N-联糖基化掩盖。

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