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造血细胞生长因子通过其对葡萄糖转运的作用介导细胞存活。

Haemopoietic cell growth factor mediates cell survival via its action on glucose transport.

作者信息

Whetton A D, Bazill G W, Dexter T M

出版信息

EMBO J. 1984 Feb;3(2):409-13. doi: 10.1002/j.1460-2075.1984.tb01821.x.

Abstract

A number of haematopoietic precursor cell lines have been established which exhibit an absolute dependence on haematopoietic cell growth factor (HCGF) which is secreted by WEHI-3 myelomonocytic leukaemia cells. In the presence of HCGF, ATP levels are maintained in these factor-dependent cells (FDC-P cells); in the absence of HCGF, intracellular ATP levels undergo a steady depletion. The cell death that follows this ATP depletion can be prevented by supplying exogenous ATP suggesting that HCGF maintains these cells via its effects on energy metabolism. We have investigated the effect of HCGF on FDC-P cells further and found that: (i) HCGF markedly and rapidly increases lactate production; (ii) high extracellular glucose or glycolytic intermediate concentrations can maintain FDC-P cell viability to some extent whilst stimulating lactate production; (iii) the uptake of 2-deoxyglucose by FDC-P2 cells is stimulated by HCGF in a dose-dependent fashion. This uptake is inhibited by cytochalasin B; (iv) HCGF does not stimulate L-glucose uptake by FDC-P cells. These results suggest that HCGF acts to maintain FDC-P cells via its action on glucose transport. The significance of these results to haemopoiesis and leukaemogenesis is discussed.

摘要

已经建立了许多造血前体细胞系,这些细胞系表现出对由WEHI-3骨髓单核细胞白血病细胞分泌的造血细胞生长因子(HCGF)的绝对依赖性。在存在HCGF的情况下,这些因子依赖性细胞(FDC-P细胞)中的ATP水平得以维持;在不存在HCGF的情况下,细胞内ATP水平会持续消耗。通过提供外源性ATP可以防止这种ATP消耗后的细胞死亡,这表明HCGF通过其对能量代谢的影响来维持这些细胞。我们进一步研究了HCGF对FDC-P细胞的作用,发现:(i)HCGF显著且迅速地增加乳酸生成;(ii)高细胞外葡萄糖或糖酵解中间产物浓度在刺激乳酸生成的同时可以在一定程度上维持FDC-P细胞的活力;(iii)HCGF以剂量依赖性方式刺激FDC-P2细胞对2-脱氧葡萄糖的摄取。这种摄取受到细胞松弛素B的抑制;(iv)HCGF不刺激FDC-P细胞对L-葡萄糖的摄取。这些结果表明,HCGF通过其对葡萄糖转运的作用来维持FDC-P细胞。讨论了这些结果对造血和白血病发生的意义。

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