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造血干细胞:脾集落形成细胞通常在积极增殖。

Haemopoietic stem cells: spleen colony-forming cells are normally actively proliferating.

作者信息

Necas E, Znojil V, Sefc L

机构信息

Department of Pathophysiology, 1st Faculty of Medicine, Charles University, Prague, Czechoslovakia.

出版信息

Cell Tissue Kinet. 1990 Nov;23(6):637-49. doi: 10.1111/j.1365-2184.1990.tb01351.x.

Abstract

The haemopoietic stem cells forming spleen colonies (CFU-S) had on average 30 to 40% of cells engaged in the DNA synthesis in normal mice continuously over 4 years. A majority of experiments aimed at the suppression of the CFU-S proliferation, which included suppression of the T-lymphocytes by means of cyclosporin A or by adult thymectomy, administration of antibacterial and antifungal agents and maintainance of mice in a sterile environment, suppression of antibody-producing cells by a successive administration of the bacterial lipopolysaccharide and cyclophosphamide and attempts to increase the total number of CFU-S in the body through massive transfusions of bone marrow cells or by grafting plugs of the bone marrow under the kidney capsulae, have not been sufficiently effective. A transient suppression of CFU-S proliferation occurred during recovery of the haemopoietic tissue from damage caused by cyclophosphamide. The results support the view that changes in CFU-S numbers and in the proportion of them in DNA synthesis may be positively correlated when CFU-S numbers fluctuate physiologically about their normal values. The failure to manipulate the CFU-S proliferation rate easily suggests that proliferation of these cells may not be under a strong 'switch on - switch off' control.

摘要

在正常小鼠中,形成脾集落的造血干细胞(CFU-S)平均有30%至40%的细胞在4年的时间里持续参与DNA合成。大多数旨在抑制CFU-S增殖的实验,包括通过环孢素A或成年胸腺切除来抑制T淋巴细胞、给予抗菌和抗真菌药物并将小鼠饲养在无菌环境中、通过连续给予细菌脂多糖和环磷酰胺来抑制抗体产生细胞,以及试图通过大量输注骨髓细胞或在肾包膜下移植骨髓小块来增加体内CFU-S的总数,但这些方法都不够有效。在造血组织从环磷酰胺造成的损伤中恢复期间,CFU-S的增殖出现了短暂抑制。这些结果支持了这样一种观点,即当CFU-S数量围绕其正常值发生生理性波动时,CFU-S数量的变化及其在DNA合成中的比例变化可能呈正相关。难以轻易控制CFU-S增殖率这一情况表明,这些细胞的增殖可能不受强大的“开启 - 关闭”控制。

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