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1
Mechanisms of clonal abortion tolerogenesis. I. Response of immature hapten-specific B lymphocytes.克隆流产耐受发生机制。I. 未成熟的半抗原特异性B淋巴细胞的反应。
J Exp Med. 1978 Nov 1;148(5):1161-70. doi: 10.1084/jem.148.5.1161.
2
Mechanisms of clonal abortion tolerogenesis. II. Clonal behaviour of immature B cells following exposure to anti-mu chain antibody.克隆流产耐受发生机制。II. 未成熟B细胞暴露于抗μ链抗体后的克隆行为。
Immunology. 1979 May;37(1):203-15.
3
Clonal anergy: persistence in tolerant mice of antigen-binding B lymphocytes incapable of responding to antigen or mitogen.克隆无能:耐受小鼠体内存在对抗原或促有丝分裂原无反应的抗原结合B淋巴细胞。
Proc Natl Acad Sci U S A. 1980 Mar;77(3):1602-6. doi: 10.1073/pnas.77.3.1602.
4
Evidence for the clonal abortion theory of B-lymphocyte tolerance.B淋巴细胞耐受性的克隆流产理论的证据。
J Exp Med. 1975 Apr 1;141(4):904-17.
5
Single cell studies on hapten-specific B lymphocytes: differential cloning efficiency of cells of various sizes.对半抗原特异性B淋巴细胞的单细胞研究:不同大小细胞的差异克隆效率。
J Immunol. 1983 Aug;131(2):554-60.
6
Tolerance induction during ontogeny. II. Distinct unresponsive states in immature mice question the generality of clonal abortion.个体发育过程中的耐受性诱导。II. 未成熟小鼠中不同的无反应状态对克隆流产的普遍性提出质疑。
Eur J Immunol. 1983 Nov;13(11):928-35. doi: 10.1002/eji.1830131112.
7
The induction of hapten-specific immunological tolerance and immunity in B lymphocytes. VI. Differential tolerance susceptibility in adult spleen as a function of B-cell maturation level.B淋巴细胞中半抗原特异性免疫耐受与免疫的诱导。VI. 成年脾脏中不同的耐受易感性与B细胞成熟水平的关系。
J Exp Med. 1979 Sep 19;150(3):491-506. doi: 10.1084/jem.150.3.491.
8
A reappraisal of "T-independent" antigens. I. Effect of lymphokines on the response of single adult hapten-specific B lymphocytes.对“非胸腺依赖性”抗原的重新评估。I. 淋巴因子对单个成年半抗原特异性B淋巴细胞反应的影响。
J Immunol. 1984 Apr;132(4):1687-95.
9
Antibody production by single, hapten-specific B lymphocytes: an antigen-driven cloning system free of filler or accessory cells.单个半抗原特异性B淋巴细胞产生抗体:一种无填充细胞或辅助细胞的抗原驱动克隆系统。
Proc Natl Acad Sci U S A. 1981 Dec;78(12):7702-6. doi: 10.1073/pnas.78.12.7702.
10
Clonal anergy: inhibition of antigen-driven proliferation among single B lymphocytes from tolerant animals, and partial breakage of anergy by mitogens.克隆失能:来自耐受动物的单个B淋巴细胞中抗原驱动增殖的抑制,以及有丝分裂原导致的失能部分解除。
Eur J Immunol. 1983 Mar;13(3):214-20. doi: 10.1002/eji.1830130307.

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1
Memory IgM protects endogenous insulin from autoimmune destruction.记忆性 IgM 可保护内源性胰岛素免受自身免疫破坏。
EMBO J. 2021 Sep 1;40(17):e107621. doi: 10.15252/embj.2020107621. Epub 2021 Aug 9.
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A current perspective on cancer immune therapy: step-by-step approach to constructing the magic bullet.癌症免疫治疗的当前视角:构建神奇子弹的循序渐进方法。
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3
Lipopolysaccharide prevents apoptosis and induces responsiveness to antigen receptor cross-linking in immature B cells.脂多糖可防止未成熟B细胞凋亡,并诱导其对抗原受体交联产生反应。
Immunology. 1996 Nov;89(3):356-62. doi: 10.1046/j.1365-2567.1996.d01-749.x.
4
A disease-related rheumatoid factor autoantibody is not tolerized in a normal mouse: implications for the origins of autoantibodies in autoimmune disease.与疾病相关的类风湿因子自身抗体在正常小鼠中未被耐受:对自身免疫性疾病中自身抗体起源的启示。
J Exp Med. 1996 Oct 1;184(4):1269-78. doi: 10.1084/jem.184.4.1269.
5
Deregulation of idiotype expression. Induction of tolerance in an anti-idiotypic response.独特型表达失调。抗独特型反应中耐受性的诱导。
J Exp Med. 1982 Sep 1;156(3):898-911. doi: 10.1084/jem.156.3.898.
6
Relative sensitivity of fetal and newborn mice to induction of hapten-specific B cell tolerance.胎儿和新生小鼠对半抗原特异性B细胞耐受性诱导的相对敏感性。
J Exp Med. 1980 Nov 1;152(5):1407-12. doi: 10.1084/jem.152.5.1407.
7
Mathematical models of antibody response.抗体反应的数学模型。
Folia Microbiol (Praha). 1980;25(5):430-8. doi: 10.1007/BF02876697.
8
Early B lymphocytes in man.人类早期B淋巴细胞。
Experientia. 1980 Sep 15;36(9):1124-5. doi: 10.1007/BF01966008.
9
Clonal anergy: persistence in tolerant mice of antigen-binding B lymphocytes incapable of responding to antigen or mitogen.克隆无能:耐受小鼠体内存在对抗原或促有丝分裂原无反应的抗原结合B淋巴细胞。
Proc Natl Acad Sci U S A. 1980 Mar;77(3):1602-6. doi: 10.1073/pnas.77.3.1602.
10
A natural model of immunologic tolerance. Tolerance to murine C5 is mediated by T cells, and antigen is required to maintain unresponsiveness.一种免疫耐受的天然模型。对小鼠C5的耐受由T细胞介导,且需要抗原以维持无反应性。
J Exp Med. 1982 Aug 1;156(2):567-84. doi: 10.1084/jem.156.2.567.

本文引用的文献

1
Cellular events in the induction and loss of tolerance to pneumococcal polysaccharides.肺炎球菌多糖诱导和丧失耐受性过程中的细胞事件。
Transplant Rev. 1972;8:50-75. doi: 10.1111/j.1600-065x.1972.tb01564.x.
2
Effector cell blockade. A new mechanism of immune hyporeactivity induced by multivalent antigens.效应细胞阻断。一种由多价抗原诱导的免疫低反应性新机制。
J Exp Med. 1974 Jun 1;139(6):1582-98. doi: 10.1084/jem.139.6.1582.
3
Fate of antigen-binding cells in unresponsive and immune mice.无反应性和免疫小鼠中抗原结合细胞的命运
J Exp Med. 1973 Feb 1;137(2):461-9. doi: 10.1084/jem.137.2.461.
4
B cell tolerance induced by polymeric antigens. IV. Antigen-mediated inhibition of antibody-forming cells.聚合抗原诱导的B细胞耐受性。IV. 抗原介导的抗体形成细胞抑制作用。
Eur J Immunol. 1976 Mar;6(3):200-7. doi: 10.1002/eji.1830060311.
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Receptor-mediated inactivation of early B lymphocytes.受体介导的早期B淋巴细胞失活。
Nature. 1975 Sep 11;257(5522):149-51. doi: 10.1038/257149a0.
6
Differences in susceptibility of mature and immature mouse B lymphocytes to anti-immunoglobulin-induced immunoglobulin suppression in vitro. Possible implications for B-cell tolerance to self.成熟和未成熟小鼠B淋巴细胞在体外对抗免疫球蛋白诱导的免疫球蛋白抑制的敏感性差异。对B细胞自身耐受性的可能影响。
J Exp Med. 1975 Nov 1;142(5):1052-64. doi: 10.1084/jem.142.5.1052.
7
In vitro tolerance induction of bone marrow cells: a marker for B cell maturation.骨髓细胞的体外耐受性诱导:B细胞成熟的一个标志物。
J Immunol. 1977 Jun;118(6):2111-6.
8
Sequential use of hapten-gelatin fractionation and fluorescence-activated cell sorting in the enrichment of hapten-specific B llymphocytes.在富集半抗原特异性B淋巴细胞中依次使用半抗原-明胶分级分离和荧光激活细胞分选技术。
Eur J Immunol. 1978 Mar;8(3):151-7. doi: 10.1002/eji.1830080302.
9
Cellular events in tolerance. VI. Neonatal vs adult B cell tolerance: differences in antigen-binding cell patterns and lipopolysaccharide stimulation.耐受性中的细胞事件。VI. 新生与成年B细胞耐受性:抗原结合细胞模式和脂多糖刺激的差异。
J Immunol. 1977 Dec;119(6):1879-81.
10
Tolerance in differentiating B lymphocytes.分化B淋巴细胞中的耐受性。
Eur J Immunol. 1977 Jan;7(1):6-10. doi: 10.1002/eji.1830070103.

克隆流产耐受发生机制。I. 未成熟的半抗原特异性B淋巴细胞的反应。

Mechanisms of clonal abortion tolerogenesis. I. Response of immature hapten-specific B lymphocytes.

作者信息

Nossal G J, Pike B L

出版信息

J Exp Med. 1978 Nov 1;148(5):1161-70. doi: 10.1084/jem.148.5.1161.

DOI:10.1084/jem.148.5.1161
PMID:82602
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2185042/
Abstract

B lymphocytes with receptors specific for the hapten fluorescein (FLU) were prepared from the spleens of mice of various ages. For most experiments, a one-step fractionation procedure based on the adherence of FLU-specific cells to FLU-gelatin was used. For some experiments, a subset of higher FLU-binding capacity was prepared from the FLU-gelatin binding population through the use of the fluorescence-activated cell sorter (FACS). FLU-specific B cells were placed into microculture with either FLU(3.6)-human gamma globulin (FLU(3.6)HGG) or FLU(12)HGG usually for 24 h at 37 degrees C. The tolerogen was then removed and 0.1 mug/ml of a T-independent antigen, FLU-polymerized flagellin, was substituted. 3 days later, cells were harvested from the microcultures and assayed for FLU-specific plaque-forming cells to determine any reduction in clonable hapten-specific B cells which the tolerogenesis treatment might have induced. The results showed that with FLU(3.6)HGG, hapten-specific newborn B cells could be tolerized at 1,000-fold lower tolerogen concentrations than adult splenic B cells of equal antigen-binding capacity. The high-avidity subset was even more susceptible to tolerance induction. Tolerance could be induced within 8 but not within 2 h, and at lower tolerogen concentrations, longer periods of tolerogenesis were required for a given effect. Using a 24-h tolerogenesis phase, 50 percent reduction in clone frequency among newborn FLU-gelatin fractionated cells was achieved at 0.08 mug/ml of FLU(3.6)HGG. Tolerance induction in immature B cells was inhibited by the concomitant presence of a polyclonal B-cell activator, Escherichia coli lipopolysaccharide (LPS) but tolerance once induced, was stable to challenge with LPS. Tolerogenesis was hapten specific. The proportion of tolerizable cells in spleens decreased with increasing age, reaching 50 percent at around 9 days. FLUI(12)HGG proved a more powerful tolerogen than FLU(3.6)HGG. It had an effect on adult cells, 50 percent reduction in clone frequency being noted at around 1 mug/ml. However, and in contrast to results claimed for other T- independent systems, there still was a major difference between immature and mature B cells, the immature cells displaying much greater sensitivity to tolerogenesis.

摘要

从不同年龄小鼠的脾脏中制备出对半抗原荧光素(FLU)具有特异性受体的B淋巴细胞。在大多数实验中,采用基于FLU特异性细胞与FLU-明胶结合的一步分离程序。在一些实验中,通过使用荧光激活细胞分选仪(FACS),从FLU-明胶结合群体中制备出具有更高FLU结合能力的亚群。将FLU特异性B细胞与FLU(3.6)-人γ球蛋白(FLU(3.6)HGG)或FLU(12)HGG一起置于微量培养中,通常在37℃下培养24小时。然后去除耐受原,并用0.1μg/ml的非T细胞依赖性抗原FLU-聚合鞭毛蛋白替代。3天后,从微量培养物中收获细胞,并检测FLU特异性空斑形成细胞,以确定耐受原处理可能诱导的可克隆半抗原特异性B细胞的任何减少。结果表明,对于FLU(3.6)HGG,与具有同等抗原结合能力的成年脾B细胞相比,半抗原特异性新生B细胞在耐受原浓度低1000倍时即可被耐受。高亲和力亚群对耐受诱导更为敏感。耐受可在8小时内而非2小时内诱导产生,并且在较低的耐受原浓度下,对于给定的效应需要更长的耐受发生期。使用24小时的耐受发生期,在0.08μg/ml的FLU(3.6)HGG作用下,新生FLU-明胶分离细胞中的克隆频率降低了50%。多克隆B细胞激活剂大肠杆菌脂多糖(LPS)的同时存在可抑制未成熟B细胞中的耐受诱导,但一旦诱导产生耐受,则对LPS的攻击具有抗性。耐受发生具有半抗原特异性。脾脏中可耐受细胞的比例随年龄增长而降低,在约9天时降至50%。事实证明,FLU(12)HGG比FLU(3.6)HGG是一种更强有力的耐受原。它对成年细胞有作用,在约1μg/ml时可使克隆频率降低50%。然而,与其他非T细胞依赖性系统所宣称的结果相反,未成熟和成熟B细胞之间仍然存在重大差异,未成熟细胞对耐受发生表现出更高的敏感性。