Hao Z, Rajewsky K
Department of Immunology, Institute for Genetics, University of Cologne, D-50931 Cologne, Germany.
J Exp Med. 2001 Oct 15;194(8):1151-64. doi: 10.1084/jem.194.8.1151.
To study homeostasis of peripheral B lymphocytes in the absence of B cell influx from the bone marrow, we generated a mouse mutant in which the recombination-activating gene (RAG)-2 can be inducibly deleted. When RAG-2 was deleted at the age of 8-10 wk, splenic naive follicular B cells were gradually lost over a year of observation, with a half-life of approximately 4.5 mo. By contrast, the pool of marginal zone B cells in the spleen and of B-1 cells in the peritoneal cavity were kept at normal level. In lymph nodes, approximately 90% of the B cells were lost within 4 mo, and B cell numbers remained constant thereafter. Mice in which RAG-2 was deleted at birth maintained a small population of activated B cells with an increased proportion of marginal zone B cells. Additionally, an increase of the pool of IgM secreting cells and B-1a cells was observed.
为了研究在没有骨髓来源的B细胞流入情况下外周B淋巴细胞的稳态,我们构建了一种小鼠突变体,其中重组激活基因(RAG)-2可以被诱导删除。当在8-10周龄时删除RAG-2,在一年的观察期内,脾脏幼稚滤泡B细胞逐渐减少,半衰期约为4.5个月。相比之下,脾脏边缘区B细胞池和腹腔B-1细胞池保持在正常水平。在淋巴结中,约90%的B细胞在4个月内丢失,此后B细胞数量保持恒定。出生时删除RAG-2的小鼠维持着一小群活化B细胞,边缘区B细胞比例增加。此外,还观察到分泌IgM的细胞和B-1a细胞池增加。
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