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前体B细胞受体依赖性B细胞增殖和分化不需要骨髓或胎肝环境。

Precursor B cell receptor-dependent B cell proliferation and differentiation does not require the bone marrow or fetal liver environment.

作者信息

Rolink A G, Winkler T, Melchers F, Andersson J

机构信息

Basel Institute for Immunology, CH-4005 Basel, Switzerland.

出版信息

J Exp Med. 2000 Jan 3;191(1):23-32. doi: 10.1084/jem.191.1.23.

Abstract

The capacity of precursor B (pre-B) I cells from fetal liver and bone marrow to proliferate and differentiate into surface immunoglobulin-positive immature B cells in vitro was analyzed. Both fetal liver- and bone marrow-derived progenitors do so in a pre-B cell receptor (pre-BCR)-dependent manner in tissue culture medium alone, without addition of other cells or cytokines. Approximately 20% of the initial pre-B I cells enter more than one division. Analyses at the single-cell level show that approximately 15% divide two to five times. Coculture of pre-B I cells with stromal cells did not enhance proliferation or differentiation, whereas the presence of interleukin 7, especially in combination with stromal cells, resulted mainly in the expansion of pre-B I cells and prevented their further differentiation. Thus, the environment of fetal liver or bone marrow is not required for the pre-BCR to exert its function, which is to select and expand cells that have undergone an inframe V(H)-D(H)J(H) rearrangement that produces a pre-BCR-compatible muH chain. It appears unlikely that a ligand for the pre-BCR drives this pre-B cell proliferation.

摘要

对来自胎儿肝脏和骨髓的前体B(pre-B)I细胞在体外增殖并分化为表面免疫球蛋白阳性未成熟B细胞的能力进行了分析。单独在组织培养基中,无需添加其他细胞或细胞因子,源自胎儿肝脏和骨髓的祖细胞均以依赖前体B细胞受体(pre-BCR)的方式进行增殖和分化。约20%的初始pre-B I细胞进入不止一轮分裂。单细胞水平分析表明,约15%的细胞分裂两到五次。pre-B I细胞与基质细胞共培养并未增强增殖或分化,而白细胞介素7的存在,尤其是与基质细胞联合存在时,主要导致pre-B I细胞扩增并阻止其进一步分化。因此,pre-BCR发挥其功能(即选择并扩增经历了产生与pre-BCR兼容的μH链的框内V(H)-D(H)J(H)重排的细胞)并不需要胎儿肝脏或骨髓的环境。pre-BCR的配体驱动这种前体B细胞增殖的可能性似乎不大。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/411b/2195801/bf5b1f50c394/JEM991130.f1.jpg

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