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组胺及其他配体偶联大分子与淋巴细胞的结合。

Binding of histamine- and other ligand-conjugated macromolecules to lymphocytes.

作者信息

Matthyssens G E, Hurwitz E, Givol D, Sela M

出版信息

Mol Cell Biochem. 1975 May 30;7(2):119-26. doi: 10.1007/BF01792078.

Abstract

The presence of histamine receptors on lymphocyte membranes was investigated using conjugates of histamine and macromolecules tritiated or iodinated with I-125. Histamine-RSA conjugate binds to lymphocytes and causes patching and capping of the bound conjugate. It was found, however, that free histamine did not inhibit the binding of histamine-rabbit serum albumin to mouse lymphocytes, nor did His-RSA interfere with the binding of free histamine. In addition conjugates between RSA and other small molecules, such as ethylamine, ethanolamine, tyramine and glycine, were found to bind to the same sites on lymphocyte membrane as did His-RSA. Ethylamine-RSA like His-RSA when coupled to Sepharose, was capable of removing antibody producing cells from spleen cells of mice immunized against sheep red blood cells. In addition, when spleen cells from such immunized mice were passed through ethylamine or histamine-RSA-Sepharose and the unbound cells were subsequently injected into X-irradiated mice, a 1.8 fold increase in the immunological response was noted. We conclude that the selective binding to lymphocytes of the various ligand-macromolecular conjugates may be due to some general properties of the cell membrane and not to any specific receptors. Nevertheless, these conjugates can be used as a tool to remove selectively antibody producing cells as well as some regulatory cells.

摘要

利用用氚标记或用碘 - 125碘化的组胺与大分子的结合物,研究了淋巴细胞膜上组胺受体的存在情况。组胺 - 牛血清白蛋白结合物可与淋巴细胞结合,并使结合的结合物出现斑片化和帽化现象。然而,发现游离组胺并不抑制组胺 - 兔血清白蛋白与小鼠淋巴细胞的结合,组胺 - 牛血清白蛋白也不干扰游离组胺的结合。此外,还发现牛血清白蛋白与其他小分子(如乙胺、乙醇胺、酪胺和甘氨酸)之间的结合物与组胺 - 牛血清白蛋白一样,能结合到淋巴细胞膜的相同位点上。与组胺 - 牛血清白蛋白一样,乙胺 - 牛血清白蛋白偶联到琼脂糖上时,能够从小鼠免疫羊红细胞的脾细胞中去除抗体产生细胞。此外,当将这种免疫小鼠的脾细胞通过乙胺或组胺 - 牛血清白蛋白 - 琼脂糖柱,然后将未结合的细胞注射到经X射线照射的小鼠体内时,可观察到免疫反应增加了1.8倍。我们得出结论,各种配体 - 大分子结合物对淋巴细胞的选择性结合可能是由于细胞膜的某些一般特性,而不是由于任何特异性受体。然而,这些结合物可作为一种工具,用于选择性地去除抗体产生细胞以及一些调节细胞。

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