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利用基质细胞克隆ST2单层培养系统对小鼠胚胎中的B细胞个体发生进行研究:B细胞祖细胞首先在胚体中发育,而非在卵黄囊中发育。

B cell ontogeny in murine embryo studied by a culture system with the monolayer of a stromal cell clone, ST2: B cell progenitor develops first in the embryonal body rather than in the yolk sac.

作者信息

Ogawa M, Nishikawa S, Ikuta K, Yamamura F, Naito M, Takahashi K, Nishikawa S

机构信息

Institute for Medical Immunology, Kumamoto University Medical School, Japan.

出版信息

EMBO J. 1988 May;7(5):1337-43. doi: 10.1002/j.1460-2075.1988.tb02949.x.

Abstract

A stromal cell clone, ST2, which can support both myelopoiesis and B lymphopoiesis of adult bone marrow was used as an in vitro microenvironment for investigating the ontogeny of the B cell progenitor in murine embryos. The B cell progenitor clonable on an ST2 layer first become detectable in the embryonal body rather than in the yolk sac around day 9.5 of gestation. As soon as it develops in the embryo, it enters the blood circulation and becomes detectable both in the developing fetal liver and the yolk sac of the 10 day embryo. On the other hand, mast cell and polymorphonuclear cell progenitors, which are also generated on the ST2 layer, develop first in the yolk sac and migrate to the fetal liver around day 10-11 of gestation. At the late stage of embryonal development, day 15-16 of gestation, the B cell progenitor enters the femur as vascularization of the femur starts. These results suggest that the localization of the committed stem cells for various hemopoietic cell lineages differs in the early embryo, although the localization of the pluripotent stem cells is yet to be determined.

摘要

一种能够支持成年骨髓髓系造血和B淋巴细胞生成的基质细胞克隆ST2,被用作体外微环境,用于研究小鼠胚胎中B细胞祖细胞的个体发生。可在ST2层上克隆的B细胞祖细胞在妊娠约9.5天时首先在胚体中而非卵黄囊中被检测到。一旦它在胚胎中发育,就会进入血液循环,并在发育中的胎儿肝脏和10天胚胎的卵黄囊中被检测到。另一方面,同样在ST2层上产生的肥大细胞和多形核细胞祖细胞首先在卵黄囊中发育,并在妊娠约10 - 11天时迁移到胎儿肝脏。在胚胎发育后期,妊娠15 - 16天时,随着股骨开始血管化,B细胞祖细胞进入股骨。这些结果表明,尽管多能干细胞的定位尚未确定,但各种造血细胞谱系的定向干细胞在早期胚胎中的定位是不同的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de29/458381/29617ea73363/emboj00142-0093-a.jpg

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