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基质细胞对淋巴细胞和髓细胞分化的调节。

Stromal cell regulation of lymphoid and myeloid differentiation.

作者信息

Quesenberry P J, McNiece I K, Robinson B E, Woodward T A, Baber G B, McGrath H E, Isakson P C

机构信息

University of Virginia, School of Medicine, Charlottesville 22908.

出版信息

Blood Cells. 1987;13(1-2):137-46.

PMID:3311214
Abstract

In vitro microenvironmental influences seem to be critical for both B lymphocyte and myeloid differentiation. Studies on murine Dexter cultures and Whitlock-Witte lymphocyte cultures suggest the presence of two critical stromal regulatory cells: an alkaline-phosphatase-positive epithelioid cell and a macrophage. Further data suggest that these cells are capable of producing colony stimulating factor-1, granulocyte-macrophage CSF, a myeloid synergizing activity, and probably separate B cell growth factors. Isolation of a cell line from Dexter stroma was accomplished and this line produced CSF-1, GM-CSF, a pre-B cell and myeloid synergizing activity, and an activity acting on differentiated B cells. We speculate that the Dexter and Whitlock-Witte in vitro culture systems are regulated by factors produced by the two adherent cell types. A lineage nonspecific factor capable of inducing cells into the B lineage or synergizing with interleukin-3, GM-CSF, and CSF-1 is produced, which presumably acts on early stem cells. In addition, the cell line produces GM-CSF, CSF-1, and a factor acting on differentiated B cells. We speculate that in these culture systems, these "terminal differentiating hormones" regulate the final pathway of differentiation, whereas the pre-B-synergizing activity supports early stem cells that can then respond to the other differentiating hormones.

摘要

体外微环境影响对于B淋巴细胞和髓系分化似乎都至关重要。对小鼠德克斯特培养物和惠特洛克-维特淋巴细胞培养物的研究表明存在两种关键的基质调节细胞:一种碱性磷酸酶阳性的上皮样细胞和一种巨噬细胞。进一步的数据表明这些细胞能够产生集落刺激因子-1、粒细胞-巨噬细胞集落刺激因子、一种髓系协同活性因子,以及可能的单独的B细胞生长因子。从德克斯特基质中分离出了一种细胞系,该细胞系产生集落刺激因子-1、粒细胞-巨噬细胞集落刺激因子、一种前B细胞和髓系协同活性因子,以及一种作用于分化B细胞的活性因子。我们推测德克斯特和惠特洛克-维特体外培养系统受这两种贴壁细胞类型产生的因子调节。产生了一种能够诱导细胞进入B谱系或与白细胞介素-3、粒细胞-巨噬细胞集落刺激因子和集落刺激因子-1协同作用的谱系非特异性因子,推测其作用于早期干细胞。此外,该细胞系产生粒细胞-巨噬细胞集落刺激因子、集落刺激因子-1,以及一种作用于分化B细胞的因子。我们推测在这些培养系统中,这些“终末分化激素”调节分化的最终途径,而前B协同活性支持早期干细胞,这些干细胞随后能够对其他分化激素作出反应。

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