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致敏的、IgD 阴性小鼠脾细胞的体外耐受诱导

In vitro tolerance induction of primed, IgD-negative murine spleen cells.

作者信息

Walker S M, Weigle W O

出版信息

J Exp Med. 1981 Mar 1;153(3):653-64. doi: 10.1084/jem.153.3.653.

Abstract

The above observations demonstrated induction of immunological tolerance in vitro in primed IgD-, IgG+ B cells. In these studies, addition of trinitrophenylated (TNP) turkey gammaglobulin (TGG) or TNP ovalbumin conjugates suppressed the secondary in vitro response in mice primed with TNP keyhole limpet hemocyanin (TNP-KLH). Suppression was not a reflection of a shift in kinetics of the antibody response, was not dependent on suppressor T cells, and could only be eliciate when conjugate was added within 4 h of addition of TNP-KLH moreover, preincubation of the primed spleen cells with TNP-TGG for 20 h at 37 degrees C, followed by extensive washing, was as effective in inhibiting the response to TNP-KLH as when TNP-TGG was present throughout the 5 d of culture, reflecting induction of a tolerant state. Amounts of conjugate in the concentration range that have been shown by others to tolerize immature or neonatal B cells or mature B cells that have been stripped of surface IgD were sufficient to induce tolerance. The target cells being tolerized did not bear IgD, as determined by B cell depletion and blocking procedures with anti IgD. Whether the lack of surface IgD on the primed cells contributed to the relative ease of tolerance induction was not established by these studies, but the advantages of using primed B cells to examine further the role of surface IgD in tolerance susceptibility was discussed.

摘要

上述观察结果表明,在体外已致敏的IgD-、IgG+B细胞中可诱导免疫耐受。在这些研究中,添加三硝基苯基化(TNP)的火鸡γ球蛋白(TGG)或TNP卵清蛋白偶联物可抑制用TNP钥孔戚血蓝蛋白(TNP-KLH)致敏的小鼠的体外二次应答。抑制作用并非抗体应答动力学变化的反映,不依赖于抑制性T细胞,且只有在添加TNP-KLH后4小时内添加偶联物才能引发。此外,将致敏的脾细胞与TNP-TGG在37℃预孵育20小时,然后充分洗涤,在抑制对TNP-KLH的应答方面与在整个5天培养过程中都存在TNP-TGG时一样有效,这反映出诱导了耐受状态。其他研究表明,能够使未成熟或新生B细胞或已去除表面IgD的成熟B细胞产生耐受的偶联物浓度范围内的量,足以诱导耐受。通过B细胞清除和抗IgD阻断程序确定,被诱导耐受的靶细胞不表达IgD。这些研究未确定致敏细胞表面缺乏IgD是否导致相对容易诱导耐受,但讨论了使用致敏B细胞进一步研究表面IgD在耐受易感性中的作用的优势。

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Immunological unresponsiveness in primed B lymphocytes.致敏B淋巴细胞中的免疫无反应性。
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