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活化的B细胞对多种次要组织相容性细胞的耐受诱导与Th2细胞的优先活化相关。

Tolerance induction to multiple minor histoincompatible cells by activated B cells is associated with preferential activation of Th2 cells.

作者信息

Gorczynski R M, Kiziroglu F

机构信息

Department of Surgery, University of Toronto, Ontario, Canada.

出版信息

Transplantation. 1994 Jul 15;58(1):51-8.

PMID:8036708
Abstract

C3H/HeH or C57BL/6 mice were injected with resting or Escherichia coli lipopolysaccharide (LPS)-stimulated splenic B cells from adult B10.BR mice. Animals were grafted with tail skin grafts from B10.BR mice 36 hr later. Spleen cells were removed from these mice 7 days after grafting and challenged in tissue culture with irradiated B10.BR spleen cells or BALB/c cells. LPS blasts, but not naive B cells, induced an antigen-specific reduction in proliferation and IL-2 production from stimulated C3H/HeJ cells. The response obtained from C57BL/6 spleen responder cells was increased by this treatment. IL-4 production was either unchanged (C57BL/6) or enhanced (C3H/HeJ). Modification of the C3H/HeJ anti-B10.BR response by B blasts was not blocked by CTLA-4 Ig, although the increased response seen using MHC-incompatible (C57BL/6) spleen cells was inhibited by CTLA-4 Ig. B10.BR, but not BALB/c, skin graft survival in vivo was enhanced in C3H/HeJ recipients of B10.BR B blasts. In addition, in lymph nodes draining the graft site of C3H/HeJ mice injected with B10.BR LPS blasts, mRNA for IL-4 was detected by polymerase chain reaction. When similar studies were performed with B10.BR immune C3H/HeJ or C57BL/6 mice, no enhancement of graft survival in vivo, or decrease in proliferation/IL-2 production in vitro, was seen following prechallenge with B10.BR LPS blasts.

摘要

将成年B10.BR小鼠静止或经大肠杆菌脂多糖(LPS)刺激的脾B细胞注射到C3H/HeH或C57BL/6小鼠体内。36小时后,给这些动物移植来自B10.BR小鼠的尾部皮肤移植物。移植7天后,从这些小鼠体内取出脾细胞,并用经辐照的B10.BR脾细胞或BALB/c细胞在组织培养中进行刺激。LPS活化的B细胞(而非未活化的B细胞)可诱导受刺激的C3H/HeJ细胞增殖和IL-2产生出现抗原特异性降低。这种处理可增强C57BL/6脾反应细胞的反应。IL-4产生要么未改变(C57BL/6),要么增强(C3H/HeJ)。B细胞活化的C3H/HeJ抗B10.BR反应的改变未被CTLA-4 Ig阻断,尽管使用MHC不相容(C57BL/6)脾细胞时观察到的反应增强被CTLA-4 Ig抑制。在接受B10.BR B细胞活化的C3H/HeJ受体中,B10.BR而非BALB/c的皮肤移植物在体内的存活得到增强。此外,在注射了B10.BR LPS活化的B细胞的C3H/HeJ小鼠移植物部位引流的淋巴结中,通过聚合酶链反应检测到IL-4的mRNA。当用B10.BR免疫的C3H/HeJ或C57BL/6小鼠进行类似研究时,在预先用B10.BR LPS活化的B细胞刺激后,未观察到体内移植物存活增强或体外增殖/IL-2产生减少。

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