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对致病性鼠伤寒沙门氏菌有反应的原发性B细胞的克隆分析。

Clonal analysis of primary B cells responsive to the pathogenic bacterium Salmonella typhimurium.

作者信息

Duran L W, Metcalf E S

出版信息

J Exp Med. 1987 Feb 1;165(2):340-58. doi: 10.1084/jem.165.2.340.

Abstract

In the present study, a modification of the splenic focus system is used to analyze the S. typhimurium strain TML (TML)-specific B cell repertoire. The results show that the frequency of primary TML-specific splenic B cells in CBA/Ca mice is approximately 1 per 10(5) B cells and less than 30% of these B cells are specific for LPS. In contrast, the frequency of memory TML-specific cells is approximately 1 per 5-8 X 10(3) splenic B cells and greater than 95% of these B cells are specific for LPS. These results suggest that the frequency of primary TML-specific B cells is extremely low and that it expands 15-20-fold after antigen exposure. It is interesting that less than 30% of the primary B cells are specific for the LPS molecule since it is considered to be the major antigenic determinant on Salmonella organisms. Furthermore, the majority of the LPS-specific anti-TML antibody-producing clones are directed against the LPS O antigen region. Conversely, more than half to two-thirds of the memory LPS-specific anti-TML B cell clones are directed against the KDO or lipid A region of the LPS molecule. These results indicate that the preferential expansion of LPS-specific B cell clones observed after immunization resides primarily in the B cell subsets responsive to the KDO/lipid A moieties on the LPS molecule. Finally, unlike B cell responses to chemically defined antigens, TML stimulates very little IgG1 antibody. IgG2 and IgA isotypes appear to play a predominant role in anti-TML antibody responses, although all H chain classes are produced to some extent. Collectively, these findings are consistent with the responses reported for two other natural antigens, HA and PC. Hence, the pattern of stimulation by infectious agents, such as S. typhimurium, appears to be distinct from that of synthetic antigens. Thus, the studies presented herein have begun to provide insights into those subsets of B cells responsive to S. typhimurium and other infectious disease organisms.

摘要

在本研究中,对脾集落系统进行了改良,以分析鼠伤寒沙门氏菌菌株TML(TML)特异性B细胞库。结果显示,CBA/Ca小鼠中初级TML特异性脾B细胞的频率约为每10⁵个B细胞中有1个,且这些B细胞中不到30%对LPS特异。相比之下,记忆性TML特异性细胞的频率约为每5 - 8×10³个脾B细胞中有1个,且这些B细胞中超过95%对LPS特异。这些结果表明,初级TML特异性B细胞的频率极低,且在抗原暴露后会扩增15 - 20倍。有趣的是,不到30%的初级B细胞对LPS分子特异,因为LPS被认为是沙门氏菌属生物体上的主要抗原决定簇。此外,大多数产生LPS特异性抗TML抗体的克隆针对LPS O抗原区域。相反,超过一半至三分之二的记忆性LPS特异性抗TML B细胞克隆针对LPS分子的KDO或脂质A区域。这些结果表明,免疫后观察到的LPS特异性B细胞克隆的优先扩增主要存在于对LPS分子上KDO/脂质A部分有反应的B细胞亚群中。最后,与B细胞对化学定义抗原的反应不同,TML刺激产生的IgG1抗体极少。IgG2和IgA同种型似乎在抗TML抗体反应中起主要作用,尽管所有重链类别在一定程度上都有产生。总体而言,这些发现与针对另外两种天然抗原HA和PC报道的反应一致。因此,鼠伤寒沙门氏菌等感染因子的刺激模式似乎与合成抗原不同。因此,本文所呈现的研究已开始为那些对鼠伤寒沙门氏菌和其他传染病生物体有反应的B细胞亚群提供见解。

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