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T-helper subset function in the gut of rats: differential stimulation of eosinophils mucosal mast cells and antibody-forming cells by OX8- OX22- and OX8- OX22+ cells.

机译：大鼠肠道中的T辅助亚群功能：OX8-OX22-和OX8-OX22 +细胞对嗜酸性粒细胞粘膜肥大细胞和抗体形成细胞的差异刺激。

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Thoracic duct lymphocytes (TDL) collected 3 days after infection of rats with Trichinella spiralis (TS) and adoptively transferred into normal, uninfected recipients, increased the numbers of both mucosal mast cells (MMC) and eosinophils (EOS) in the intestine. The CD4+ T-helper cell population was separated into two subsets (OX22+ and OX22-) using OX22 monoclonal antibody (mAb) and panning techniques. After adoptive transfer of these T-helper subsets i.v., rats were challenged with TS 24 hr later. The intestine of recipient rats was examined histologically at intervals from Day 3 to Day 21. On Day 9 after transfer, OX22+ T helpers induced a substantial mastocytosis [94 +/- 3, mean +/- SE/villus crypt unit (VCU)], whereas the OX22- T-helper subset increased resident EOS numbers (60 +/- 2/VCU) compared to the challenge control (18 +/- 1 MMC, 27 +/- 1 EOS/VCU). The time of peak eosinophilia was advanced by 3-6 days for recipients of OX22- cells and that of mast cells by 9-12 days for recipients of OX22+ cells. The recipients of OX22-, but not OX22+, cells also showed a large increase in the numbers of B cells in the spleen and mesenteric lymph node (MLN) secreting antibody against adult TS. Recipients of OX22- cells displayed an even increase in EOS throughout the villi, lamina propria (LP) and muscularis, whereas in OX22+ cell recipients mast cells were only present in the lower villus and the epithelium just above the crypt as well as the muscularis layer. Only the CD4+ OX22- cell subset conferred protection against TS in the intestine. We conclude that the OX22+ and OX22- T-helper cells exert distinctive effects in the intestine on MMC and EOS. Because protection was established in the presence of an OX22- T-helper-induced eosinophilia but without a concurrent mastocytosis, the results suggest that MMC are probably not involved in expulsion of TS to terminate the primary infection.

机译：感染旋毛虫（TS）的大鼠感染3天后收集胸导管淋巴细胞（TDL），并过继转移到未感染的正常受体中，增加了肠道粘膜肥大细胞（MMC）和嗜酸性粒细胞（EOS）的数量。使用OX22单克隆抗体（mAb）和淘选技术，将CD4 + T辅助细胞群分为两个子集（OX22 +和OX22-）。静脉内转移这些T辅助细胞亚群后，在24小时后用TS攻击大鼠。从第3天到第21天的时间间隔，组织学检查受体大鼠的肠道。在转移后第9天，OX22 + T辅助物引起实质性肥大细胞增多[94 +/- 3，平均+/- SE /绒毛隐窝单位（VCU）] ，而OX22- T-helper子集比挑战对照（18 +/- 1 MMC，27 +/- 1 EOS / VCU）增加了常驻EOS数量（60 +/- 2 / VCU）。对于OX22-细胞的接受者，嗜酸性粒细胞高峰时间延长了3-6天，对于OX22 +细胞的接受者，肥大细胞的嗜酸性粒细胞时间延长了9-12天。 OX22-而不是OX22 +细胞的受体在脾脏和肠系膜淋巴结（MLN）分泌针对成年TS的抗体中也显示出B细胞数量的大幅增加。 OX22细胞的接受者在整个绒毛，固有层（LP）和肌层中的EOS均匀增加，而在OX22 +细胞接受者中，肥大细胞仅存在于绒毛下部和上皮以及隐窝以及肌层中。只有CD4 + OX22-细胞亚群才赋予了肠道抗TS的保护。我们得出结论，OX22 +和OX22- T辅助细胞在肠道中对MMC和EOS发挥独特的作用。由于在存在OX22-T辅助细胞诱导的嗜酸性粒细胞增多的情况下建立了保护作用，但没有同时发生肥大细胞增多症，因此结果表明MMC可能不参与TS的排出以终止原发感染。

著录项

期刊名称 Immunology
作者
C H Wang; M Korenaga; A Greenwood; R G Bell;
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年(卷),期 1990(71),2
年度 1990
页码 166–175
总页数 10
原文格式 PDF
正文语种
中图分类免疫学;
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专利

1. Antiidiotypic immunity in interstitial nephritis. II. Rats developing anti-tubular basement membrane disease fail to make an antiidiotypic regulatory response: the modulatory role of an RT7.1+, OX8- suppressor T cell mechanism. [J] . E G Neilson, E McCafferty, S M Phillips, The Journal of Experomental Medicine . 1984,第4期

机译：间质性肾炎的抗独特型免疫。二。发生抗肾小管基底膜疾病的大鼠无法做出抗独特型调节反应：RT7.1 +，OX8-抑制性T细胞机制的调节作用。
2. Phenotypic and functional analyses of KIR3DL1+ and KIR3DS1+ NK cell subsets demonstrate differential regulation by Bw4 molecules and induced KIR3DS1 expression on stimulated NK cells. [J] . Morvan M, Willem C, Gagne K, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2009,第11期

机译：对KIR3DL1 +和KIR3DS1 + NK细胞亚群的表型和功能分析表明，Bw4分子具有不同的调节作用，并在刺激的NK细胞上诱导了KIR3DS1的表达。
3. T-helper function of parent leads to F1 chimeras. Presence of a separate T-cell subgroup able to stimulate allogeneic B cells but not syngeneic B cells. [J] . J Sprent, H von Boehmer The Journal of Experomental Medicine . 1979,第2期

机译：父母的T辅助功能导致F1嵌合体。存在能够刺激同种B细胞但不能刺激同型B细胞的单独T细胞亚群。
4. MESENCHYMAL PROGENITOR CELLS DIFFERENTIALLY RESPOND TO MECHANICAL STIMULATION: MORPHOLOGY, PROLIFERATION, GENE AND PROTEIN EXPRESSION [C] . Timothy M. Maul, Douglas W. Chew, Alejandro Nieponice, ASME Bioengineering Conference . 2007

机译：间充质祖细胞差异响应机械刺激：形态，增殖，基因和蛋白质表达
5. Identification of a major subset of murine NK cells: Generation of a monoclonal antibody detecting the LGL-1 antigen and functional properties of LGL-1(+) and LGL-1(-) NK cells. [D] . Mason, Llewellyn Hoffman. 1992

机译：鉴定鼠类NK细胞的主要子集：产生检测LGL-1抗原和LGL-1（+）和LGL-1（-）NK细胞功能特性的单克隆抗体。
6. Intestinal immunity to Trichinella spiralis is a property of OX8- OX22- T-helper cells that are generated in the intestine. [O] . M Korenaga, C H Wang, R G Bell, 1989

机译：对旋毛虫的肠免疫是在肠中产生的OX8-OX22-T-辅助细胞的特性。
7. Antiidiotypic immunity in interstitial nephritis. II. Rats developing anti-tubular basement membrane disease fail to make an antiidiotypic regulatory response: the modulatory role of an RT7.1+, OX8- suppressor T cell mechanism [O] . 1984

机译：间质性肾炎的抗独特型免疫。二。发生抗肾小管基底膜疾病的大鼠无法做出抗独特型调节反应：RT7.1 +，OX8-抑制性T细胞机制的调节作用
8. Immunological Protection against Mucosal Pathogens by Direct Stimulation of Antibody Forming Cells in the Gut Associated Lymphoid Tissues [R] . Clements, J. D., Garry, R. F. 1986

机译：通过直接刺激肠道相关淋巴组织中的抗体形成细胞对粘膜病原体的免疫保护

T-helper subset function in the gut of rats: differential stimulation of eosinophils mucosal mast cells and antibody-forming cells by OX8- OX22- and OX8- OX22+ cells.

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