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霍乱毒素对多种小鼠造血祖细胞增殖的选择性抑制作用。

Selective inhibition of the proliferation of various murine hemopoietic progenitor cells by cholera toxin.

作者信息

Lanotte M, Gombaud-Saintonge G, Tertian G

出版信息

Exp Hematol. 1986 Sep;14(8):724-31.

PMID:3091385
Abstract

We have studied in detail the effects of cholera toxin (CT), its pentameric B-chain subunit (toxoid) and the A-promoter chain on the differentiation of hemopoietic progenitor cells. Murine marrow cells were treated either with CT or its subunits. After stimulation with either the multilineage growth factor (multi-CSF; also called interleukin 3 or HCGF) or other hemopoietic regulators (colony-stimulating factors, or CSF), the clones grown in semisolid collagen cultures were scored in situ. Pluripotent stem cells (CFU-S) and multilineage (mixed CFU) or lineage-restricted progenitors (CFU-c) were estimated. We found that CT sensitivity is gradually gained by cells through the stepwise differentiation processes (i.e., CFU-S less than multilineage CFC less than committed CFC less than maturing cells). CT also has a selective, dose-dependent inhibitory effect (1 microM to 1 pM) on hemopoietic lineages (basophil-mast cells less than megakaryocytes less than neutrophils less than monomacrophages). These phenomena were obvious when the clonal growth was supported by multi-CSF but, interestingly, were not observed when lineage-restricted CSF were used. They furnished additional evidence that multi-CSF activates cells in a specific manner. This growth factor involved in progenitor cell self-renewal control may contribute to maintaining, on maturing cells, characteristics that are normally the attributes of progenitors.

摘要

我们已经详细研究了霍乱毒素(CT)、其五聚体B链亚基(类毒素)和A启动子链对造血祖细胞分化的影响。用CT或其亚基处理小鼠骨髓细胞。在用多谱系生长因子(多集落刺激因子;也称为白细胞介素3或人绒毛膜促性腺激素)或其他造血调节因子(集落刺激因子,或CSF)刺激后,对在半固体胶原培养物中生长的克隆进行原位计数。评估多能干细胞(CFU-S)、多谱系(混合CFU)或谱系限制祖细胞(CFU-c)。我们发现细胞在逐步分化过程中逐渐获得对CT的敏感性(即CFU-S<多谱系集落形成细胞<定向集落形成细胞<成熟细胞)。CT对造血谱系也有选择性的、剂量依赖性的抑制作用(1微摩尔至1皮摩尔)(嗜碱性粒细胞-肥大细胞<巨核细胞<中性粒细胞<单核巨噬细胞)。当克隆生长由多集落刺激因子支持时,这些现象很明显,但有趣的是,当使用谱系限制的CSF时未观察到这些现象。它们提供了额外的证据,证明多集落刺激因子以特定方式激活细胞。这种参与祖细胞自我更新控制的生长因子可能有助于在成熟细胞上维持通常是祖细胞特征的特性。

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