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用修饰变应原抑制反应素抗体。IV. 聚乙二醇(PEG)和单甲氧基PEG与卵清蛋白的缀合物诱导抑制性T细胞

Suppression of reaginic antibodies with modified allergens. IV. Induction of suppressor T cells by conjugates of polyethylene glycol (PEG) and monomethoxy PEG with ovalbumin.

作者信息

Lee W Y, Sehon A H, Akerblom E

出版信息

Int Arch Allergy Appl Immunol. 1981;64(1):100-14.

PMID:6450171
Abstract

Administration of multiple injections of conjugates of ovalbumin (OA) and polyethylene glycol (PEG) or its monomethoxy derivative (mPEG) into mice which had been sensitized with 2,4-dinitrophenylated OA (DNP3-OA) abrogated both the anti-OA and anti-DNP IgE responses, in spite of additional injections of the sensitizing dose of DNP3-OA in the presence of A1(OH)3. Treatment of mice with OA-PEG in A1(OH)3 stimulated preferentially helper T cells, whereas injection of mice with OA-PEG in the absence of adjuvant elicited predominantly suppressor T cells. The unresponsive state of mice which had been treated 21 days earlier with OA-PEG could not be broken by the transfer of normal spleen cells and an additional sensitizing dose of DNP3-OA. Transfer of spleen cells from tolerized animals to normal mice dampened the capacity of the latter to mount both anti-DNP and anti-OA IgE responses; however, the suppressive effect of these cells was eliminated by treatment of the normal recipients with cyclophosphamide, which is a procedure known to inactive suppressor T cells, and hence it may be concluded that this effect was not due to the carryover of the tolerogen with the transferred cells. All these results provide strong support for the conclusion that the suppressor cells induced by the treatment of mice with OA-PEG and OA-mPEG conjugates belonged to a T cell subpopulation, and that the B cells of these mice were devoid of suppressive activity.

摘要

向已用2,4 - 二硝基苯化卵清蛋白(DNP3 - OA)致敏的小鼠多次注射卵清蛋白(OA)与聚乙二醇(PEG)或其单甲氧基衍生物(mPEG)的缀合物,尽管在存在氢氧化铝(Al(OH)3)的情况下额外注射了致敏剂量的DNP3 - OA,但仍消除了抗OA和抗DNP IgE反应。在Al(OH)3中用OA - PEG处理小鼠优先刺激辅助性T细胞,而在无佐剂的情况下向小鼠注射OA - PEG主要诱导抑制性T细胞。21天前用OA - PEG处理的小鼠的无反应状态不能通过转移正常脾细胞和额外的致敏剂量的DNP3 - OA来打破。将耐受动物的脾细胞转移到正常小鼠中会减弱后者产生抗DNP和抗OA IgE反应的能力;然而,用环磷酰胺处理正常受体可消除这些细胞的抑制作用,环磷酰胺是一种已知能使抑制性T细胞失活的程序,因此可以得出结论,这种作用不是由于转移细胞携带耐受原所致。所有这些结果都有力地支持了以下结论:用OA - PEG和OA - mPEG缀合物处理小鼠所诱导的抑制细胞属于T细胞亚群,并且这些小鼠的B细胞没有抑制活性。

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