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来自胸腺衍生淋巴细胞的、与人免疫球蛋白Fab片段相关的受体的抗原性多肽片段。

Antigenic polypeptide fragments of a receptor related to the Fab fragment of human immunoglobulin from thymus-derived lymphocytes.

作者信息

Marchalonis J J, Hunt J C, Maxwell J, Wang A C

出版信息

Proc Natl Acad Sci U S A. 1982 Aug;79(15):4733-6. doi: 10.1073/pnas.79.15.4733.

Abstract

Certain thymus-derived lymphocytes of man and other primates express surface components related to the variable region of immunoglobulin heavy chains but lack constant region determinants defining any known immunoglobulin class. To obtain structural information on this molecule that can be used for comparison with known immunoglobulins and other surface molecules, we isolated the T cell-derived molecule by affinity chromatography using an antiserum raised against the monomeric Fab fragment of a human Waldenström macroglobulin and subjected the isolated molecule to either proteolysis using enzymes or cleavage with cyanogen bromide, followed by isolation of polypeptides which bore the Fab- or heavy chain variable region (VH)-related antigenic markers. The intact T cell molecule had an apparent mass of 68,000 daltons and no evidence was found for covalent or noncovalent association with polypeptides resembling light chains in apparent mass. The pattern of fragments obtained by cleavage of the T cell heavy chain suggests that the molecule is comprised of domains of approximate mass 12,000 daltons. Isolation of fragments from the digests that bear Fab-related serological markers shows that the molecule can be degraded into fragments resembling the Fd and VH of standard immunoglobulin heavy chains. A procedure was developed enabling the isolation of milligram quantities of VH-related T cell products. These results support the concept of a sharing of combining site determinants between T cell receptors and immunoglobulin heavy chains and show a general formal similarity between the two classes of molecules, even though they lack shared constant region determinants. The susceptibility of the T cell molecule to be cleaved into discrete antigenic fragments by controlled proteolysis might help to explain the plethora of sizes observed for antigen-specific T cell factors.

摘要

人类和其他灵长类动物的某些胸腺衍生淋巴细胞表达与免疫球蛋白重链可变区相关的表面成分,但缺乏定义任何已知免疫球蛋白类别的恒定区决定簇。为了获得可用于与已知免疫球蛋白和其他表面分子进行比较的该分子的结构信息,我们使用针对人瓦尔登斯特伦巨球蛋白单体Fab片段产生的抗血清,通过亲和层析分离了T细胞衍生分子,并将分离出的分子用酶进行蛋白水解或用溴化氰裂解,随后分离出带有Fab或重链可变区(VH)相关抗原标记的多肽。完整的T细胞分子表观质量为68,000道尔顿,未发现与表观质量类似轻链的多肽有共价或非共价结合的证据。通过裂解T细胞重链获得的片段模式表明该分子由表观质量约为12,000道尔顿的结构域组成。从带有Fab相关血清学标记的消化物中分离片段表明,该分子可降解为类似于标准免疫球蛋白重链Fd和VH的片段。开发了一种方法,能够分离出毫克量的VH相关T细胞产物。这些结果支持T细胞受体和免疫球蛋白重链之间存在结合位点决定簇共享的概念,并表明这两类分子在总体形式上具有相似性,尽管它们缺乏共享的恒定区决定簇。T细胞分子通过可控蛋白水解裂解为离散抗原片段的敏感性可能有助于解释观察到的抗原特异性T细胞因子的多种大小。

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