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Adoptive transfer of gut mucosal antitoxin memory by isolated B cells 1 year after oral immunization with cholera toxin.

机译：口服霍乱毒素免疫1年后分离的B细胞过早转移了肠粘膜抗毒素记忆。

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A protocol was elaborated for the adoptive transfer of lymphocytes from mice which were orally immunized with cholera toxin (CT) to enable the study of long-term gut mucosal immunological memory at the single-cell level. Mesenteric lymph node (MLN) cells were transferred 1 year after priming immunizations, and recipient animals were challenged perorally on days 1 and 2 with CT before sacrifice on day 6 to 7 following transfer of cells. Strong antitoxin ELISPOT spot-forming cell (SFC) responses were recorded in spleens, MLN, and laminae propriae (LP) of recipient mice. In contrast, no SFC were found in Peyer's patches. The magnitude of the response equaled that of the acute response seen after optimal oral CT immunization and was directly dependent on the number of transferred cells. The memory antitoxin response in MLN and LP required oral challenge with CT as opposed to the spleen SFC response, which could also be triggered by intravenous challenge with antigen. Spleen cells from mice immunized perorally with CT were as effective as MLN cells in transferring immunological memory detectable in the gut immune system. Irrespective of the tissue source of transferring immunological memory detectable in the gut immune system. Irrespective of the tissue source of the memory cells, the isotype distribution of the antitoxin SFC response in recipient mice was similar with predominantly immunoglobulin A (96%) in LP and immunoglobulin G (66%) in MLN and spleen. Transfer of antitoxic memory was completely abrogated by treatment of the cells with J11d monoclonal antibody and complement prior to their injection into recipient mice by was unaffected by treatment with anti-Thy-1.2 antibody and complement, suggesting that long-term gut mucosal memory is carried by B cells. Antitoxin B memory cells might help explain the long-term protection against recurrent disease seen in convalescents from cholera in cholera-endemic areas.

机译：制定了一项协议，用于从口服霍乱毒素（CT）免疫的小鼠中过继转移淋巴细胞，从而能够在单细胞水平上研究长期肠道粘膜免疫记忆。初次免疫后1年，转移了肠系膜淋巴结（MLN）细胞，在转移细胞后的第6至7天，在接受CT攻击的第1天和第2天，用CT对接受动物进行了口周攻击。在受体小鼠的脾脏，MLN和固有层（LP）中记录了强抗毒素ELISPOT点形成细胞（SFC）反应。相反，在Peyer的补丁程序中未发现SFC。最佳口服CT免疫后，反应的强度等于急性反应的强度，并且直接取决于转移细胞的数量。与脾脏SFC反应相反，MLN和LP中的记忆抗毒素反应需要口服CT刺激，这也可以由抗原静脉内激发触发。经肠道经CT免疫的小鼠脾细胞在转移肠道记忆系统可检测的免疫记忆方面与MLN细胞一样有效。不论在肠道免疫系统中可检测到的转移免疫记忆的组织来源如何。无论记忆细胞的组织来源如何，受体小鼠中抗毒素SFC反应的同种型分布与LP中的免疫球蛋白A（96％）和MLN和脾脏中的免疫球蛋白G（66％）相似。在将J11d单克隆抗体和补体注射到受体小鼠体内之前，通过用Thy-1.2抗体和补体治疗不受影响，从而完全消除了抗毒性记忆的转移，这表明可以进行长期肠道粘膜记忆通过B细胞。抗毒素B记忆细胞可能有助于解释对霍乱流行地区霍乱恢复期中复发性疾病的长期保护作用。

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期刊名称 Infection and Immunity
作者
N Lycke; J Holmgren;
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年(卷),期 1989(57),4
年度 1989
页码 1137–1141
总页数 5
原文格式 PDF
正文语种
中图分类免疫学;病毒传染病;
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专利

1. Robust gut associated vaccine-specific antibody-secreting cell responses are detected at the mucosal surface of Bangladeshi subjects after immunization with an oral killed bivalent V. cholerae O1/O139 whole cell cholera vaccine: Comparison with other mucosal and systemic responses. [J] . Shamsuzzaman S, Ahmed T, Mannoor K, Vaccine . 2009,第9期

机译：在口服灭活的二价霍乱弧菌O1 / O139全细胞霍乱疫苗免疫后，在孟加拉国受试者的粘膜表面检测到了与肠道相关的强健的疫苗特异性抗体分泌细胞应答：与其他粘膜和全身应答的比较。
2. In vivo adjuvant-induced mobilization and maturation of gut dendritic cells after oral administration of cholera toxin. [J] . Anjuere F, Luci C, Lebens M, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2004,第8期

机译：口服霍乱毒素后，体内佐剂诱导的肠道树突状细胞动员和成熟。
3. Antitoxic immunity to cholera in dogs immunized orally with cholera toxin. [J] . N F Pierce, W C Cray, P F Engel Infection and immunity . 1980,第2期

机译：口服霍乱毒素免疫的狗对霍乱的抗毒性免疫。
4. MUCOSAL IMMUNE RESPONSES FROM ORAL GENETIC IMMUNIZATION WITH MACROAGGREGATED POLYETHYLENEIMINE-ALBUMIN CONJUGATES [C] . B. M. Kinsey, B. S. Bhogal, L. Song, International symposium on controlled release of bioactive materials;Consumer diversified products conference . 2001

机译：宏观聚合的聚乙烯亚胺-白蛋白结合物对口腔遗传免疫的粘膜免疫反应
5. Oral proliposomal delivery of cromolyn and tiludronate: Formulation and in vitro characterization in Caco-2 cells and isolated rat gut. [D] . Deshmukh, Deepali Damle. 2003

机译：cromolyn和tiludronate的口服脂质体递送：在Caco-2细胞和分离的大鼠肠中的配制和体外表征。
6. Mucosal memory B cells retain the ability to produce IgM antibodies 2 years after oral immunization. [O] . M Vajdy, N Lycke 1995

机译：口服免疫后2年粘膜记忆B细胞保留产生IgM抗体的能力。
7. Adoptive transfer of gut mucosal antitoxin memory by isolated B cells 1 year after oral immunization with cholera toxin [O] . N Lycke, J Holmgren 1989

机译：用霍乱毒素口服免疫后1岁肠粘膜抗毒素记忆肠道粘膜抗毒液记忆
8. Evaluation of Purified Cholera Toxins and Toxoids as Immunizing Agents Against Cholera and Investigations of the Mechanisms by Which Antitoxin Immunity Provides Protection Against Cholera [R] . Pierce, N. F. 1979

机译：评估纯化的霍乱毒素和类毒素作为抗霍乱免疫剂及研究抗毒素免疫为霍乱提供保护的机制

Adoptive transfer of gut mucosal antitoxin memory by isolated B cells 1 year after oral immunization with cholera toxin.

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