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对铁氧化还原蛋白的免疫反应;无反应状态并非由抑制作用引起。

Immune response to ferredoxin; nonresponder status is not due to suppression.

作者信息

Sikora L K, Levy J G

出版信息

J Immunol. 1984 Dec;133(6):2898-903.

PMID:6208265
Abstract

Ferredoxin (Fd), a small protein from Clostridium pasteurianum, has been selected for immunologic studies because of its limited number (two) of antigenic determinants. Functionally (as determined by antibody binding), monodeterminant fragments of Fd can be generated enzymatically, leaving molecules only a few amino acids smaller than the native protein, with unaltered solid phase binding properties. These fragments were used to assess the immune response to each of the two determinants. Clear differences in immunologic properties can be assigned to sequences within Fd: the amino terminal tripeptide is responsible for inducing a proliferative response and limited antibody production, whereas the carboxy terminal dipeptide accounts for most of the antibody activity, yet little, if any, T-proliferative activity. Studies with the enzyme-generated fragments of Fd have unmasked a sequence proximal to the amino terminal that represents a second determinant for T cell proliferation but does not have any demonstrable antibody-inducing activity. This third determinant is shown to induce responsiveness to Fd in nonresponder animals after the removal of the amino terminal tripeptide. The results indicate that nonresponsiveness to this molecule in H-2d mice is not a direct effect of suppression.

摘要

铁氧化还原蛋白(Fd)是一种来自巴氏梭菌的小蛋白,因其抗原决定簇数量有限(两个)而被选用于免疫学研究。从功能上看(通过抗体结合确定),Fd的单决定簇片段可以通过酶促产生,生成的分子仅比天然蛋白小几个氨基酸,且固相结合特性未改变。这些片段被用于评估对两个决定簇中每一个的免疫反应。Fd内的序列可导致免疫特性存在明显差异:氨基末端三肽负责诱导增殖反应和有限的抗体产生,而羧基末端二肽则占大部分抗体活性,但T细胞增殖活性很小(如果有的话)。对Fd酶促产生的片段进行的研究揭示了氨基末端附近的一个序列,该序列是T细胞增殖的第二个决定簇,但没有任何可证明的抗体诱导活性。在去除氨基末端三肽后,这个第三个决定簇显示可诱导无反应动物对Fd产生反应。结果表明,H-2d小鼠对该分子无反应并非抑制的直接作用。

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