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初始再循环B细胞在脾脏和骨髓中同时成熟。

Naive recirculating B cells mature simultaneously in the spleen and bone marrow.

作者信息

Cariappa Annaiah, Chase Catharine, Liu Haoyuan, Russell Paul, Pillai Shiv

机构信息

Massachusetts General Hospital and Harvard Medical School, Boston, MA 02129, USA.

出版信息

Blood. 2007 Mar 15;109(6):2339-45. doi: 10.1182/blood-2006-05-021089. Epub 2006 Nov 21.

Abstract

We have recently demonstrated that IgD(hi) B cells can occupy an extravascular perisinusoidal niche in the bone marrow in addition to the well-established follicular niche in conventional secondary lymphoid organs. The spleen has long been considered to be the site at which newly formed B lymphocytes mature into IgD(hi) naive recirculating B cells, but the existence of mutant mice that have selectively lost mature B cells in the bone marrow prompted an examination of B-cell maturation at this latter site. Following a single pulse of BrdU in intact mice, sequential labeling of more mature B-cell populations in the bone marrow suggested ongoing maturation at this site. Further evidence for B-cell maturation in the bone marrow was obtained from analyses of transitional B cells in splenectomized lymphotoxin alpha-deficient mice that lack all secondary lymphoid organs. In these mice, antibody-secreting cells recognizing multivalent antigens were also observed in the bone marrow following an intravenous microbial challenge. These data suggest that newly formed B cells mature into IgD(hi) B cells simultaneously in the spleen and the bone marrow and establish in a stringent manner that humoral immune responses can be initiated in situ in the bone marrow.

摘要

我们最近证明,除了传统二级淋巴器官中已确立的滤泡微环境外,IgD(hi) B细胞还可占据骨髓血管外的窦周微环境。长期以来,脾脏一直被认为是新形成的B淋巴细胞成熟为IgD(hi) 初始循环B细胞的场所,但存在选择性地在骨髓中失去成熟B细胞的突变小鼠促使人们对后一部位的B细胞成熟情况进行研究。在完整小鼠中单次注射BrdU后,对骨髓中更成熟B细胞群体的连续标记表明该部位存在持续的成熟过程。对缺乏所有二级淋巴器官的脾切除淋巴毒素α缺陷小鼠的过渡性B细胞进行分析,进一步获得了骨髓中B细胞成熟的证据。在这些小鼠中,静脉注射微生物刺激后,在骨髓中也观察到了识别多价抗原的抗体分泌细胞。这些数据表明,新形成的B细胞在脾脏和骨髓中同时成熟为IgD(hi) B细胞,并严格确定体液免疫反应可在骨髓中就地启动。

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