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小鼠骨髓中的前B细胞:正常小鼠中含细胞质μ链细胞增殖的免疫荧光静止动力学研究。

Pre-B cells in mouse bone marrow: immunofluorescence stathmokinetic studies of the proliferation of cytoplasmic mu-chain-bearing cells in normal mice.

作者信息

Opstelten D, Osmond D G

出版信息

J Immunol. 1983 Dec;131(6):2635-40.

PMID:6417229
Abstract

By using a technique that combines metaphase arrest with immunofluorescence labeling, the proliferation of specifically identified pre-B cells in mouse bone marrow has been analyzed under physiological conditions in vivo. Pre-B cells bearing cytoplasmic mu-chains and no surface mu-chains constituted 12% of marrow nucleated cells, or 27 X 10(5) cells/femur, whereas surface mu-bearing B lymphocytes totaled 33 X 10(5) cells/femur. Pre-B cells measured 7 to 14 micron in diameter, the small number seen in metaphase (1 to 2%) being large cells (greater than 10 microns). After vincristine injection, the metaphase incidence (Imet) of pre-B cells increased with cell size; a broad-dose range of vincristine gave similar Imet values. Mitoses were arrested for 4 hr with no apparent cell death. Linear regression analysis of the increase in Imet of pre-B cells 2 to 4 hr after vincristine revealed a rate of entry into mitosis of 6.3%/hr, relative to all pre-B cells (average compartment turnover time, 16 hr), and 15.3%/hr for the large proliferating pre-B cell subset. This represented a pre-B cell production of 1.3 X 10(5) cells/femoral shaft/hr or 0.5 X 10(8) cells/whole bone marrow organ/day, emphasizing the magnitude of B lymphocyte genesis in normal bone marrow. Combined with reported renewal rates for small pre-B cells and small B lymphocytes, these values form a kinetic model of B lymphocyte development. The results reveal an apparent overproduction of large pre-B cells, consistent with a speculative post-mitotic loss of some immature primary B lymphocytes.

摘要

通过运用一种将中期阻断与免疫荧光标记相结合的技术,已在体内生理条件下分析了小鼠骨髓中特定识别的前B细胞的增殖情况。带有细胞质μ链而无表面μ链的前B细胞占骨髓有核细胞的12%,即每根股骨中有27×10⁵个细胞,而带有表面μ链的B淋巴细胞每根股骨总计有33×10⁵个细胞。前B细胞直径为7至14微米,中期所见的少数细胞(1%至2%)为大细胞(大于10微米)。注射长春新碱后,前B细胞的中期发生率(Imet)随细胞大小增加;长春新碱的宽剂量范围给出相似的Imet值。有丝分裂被阻断4小时,无明显细胞死亡。对长春新碱注射后2至4小时前B细胞Imet增加的线性回归分析显示,相对于所有前B细胞(平均区室周转时间为16小时),进入有丝分裂的速率为6.3%/小时,而大的增殖性前B细胞亚群为15.3%/小时。这代表每根股骨干每小时产生1.3×10⁵个前B细胞,或整个骨髓器官每天产生0.5×10⁸个细胞,强调了正常骨髓中B淋巴细胞生成的规模。结合报道的小前B细胞和小B淋巴细胞的更新率,这些值形成了B淋巴细胞发育的动力学模型。结果显示大前B细胞明显过度产生,这与一些未成熟原代B淋巴细胞有丝分裂后推测性损失一致。

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