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化学修饰和片段化对C型逆转录病毒内部蛋白p30和表面糖蛋白gp70抗原决定簇的影响。

Effect of chemical modification and fragmentation on antigenic determinants of internal protein p30 and surface glycoprotein gp70 of type C retroviruses.

作者信息

Versteegen R J, Oroszlan S

出版信息

J Virol. 1980 Mar;33(3):983-92. doi: 10.1128/JVI.33.3.983-992.1980.

Abstract

The effects of protein modification on the antigenic determinants of p30 and gp70 of type C retroviruses were investigated by using solid-phase competition radioimmunoassays. Proteins were modified by reduction with 2-mercaptoethanol and subsequent carboxymethylation of SH groups with iodoacetamide or by amidination of alpha and epsilon amino groups with methylacetimidate. The type-specific determinants of gp70 were found to be conformational in nature, as they were destroyed by these chemical modifications. Group- and interspecies-specific determinants of gp70 antigens, however, appear to be sequential and do not involve residues susceptible to these chemical reagents. Conformation-dependent type-specific determinants of p30 were affected only by methylacetimidate. Group- and interspecies-specific determinants of p30 are similar to those of gp70 in that they also appear to be sequential antigenic sites. Therefore, the broadly reactive group- and interspecies-specific determinants of gp70 and p30 can be followed into small peptides. Accordingly, a cyanogen bromide cleavage fragment derived from the carboxyl-terminal one-third of Rauscher leukemia virus p30 was found to carry group-specific determinants but no detectable interspecies-specific determinants. In contrast, a peptide obtained by limited trypsin cleavage of p30, which was derived from the NH(2)-terminal region of the protein, contained at least one of the interspecies determinants shared with feline leukemia virus p27.

摘要

利用固相竞争放射免疫测定法研究了蛋白质修饰对C型逆转录病毒p30和gp70抗原决定簇的影响。蛋白质通过用2-巯基乙醇还原并随后用碘乙酰胺对SH基团进行羧甲基化修饰,或用甲基乙酰亚胺对α和ε氨基进行脒化修饰。发现gp70的型特异性决定簇本质上是构象性的,因为它们会被这些化学修饰破坏。然而,gp70抗原的组特异性和种间特异性决定簇似乎是序列性的,并且不涉及易受这些化学试剂影响的残基。p30的构象依赖性型特异性决定簇仅受甲基乙酰亚胺影响。p30的组特异性和种间特异性决定簇与gp70的相似,因为它们似乎也是序列性抗原位点。因此,gp70和p30具有广泛反应性的组特异性和种间特异性决定簇可以追踪到小肽中。相应地,发现来自劳氏肉瘤病毒p30羧基末端三分之一的溴化氰裂解片段携带组特异性决定簇,但没有可检测到的种间特异性决定簇。相比之下,通过对p30进行有限胰蛋白酶裂解获得的一种肽,该肽源自该蛋白质的NH(2)-末端区域,含有至少一种与猫白血病病毒p27共有的种间决定簇。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9307/288632/ffd2732000cd/jvirol00171-0067-a.jpg

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