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成纤维细胞生长因子对静止3T3细胞早期转运变化的调节作用。

The regulation by fibroblast growth factor of early transport changes in quiescent 3T3 cells.

作者信息

Quinlan D C, Hochstadt J

出版信息

J Cell Physiol. 1977 Nov;93(2):237-46. doi: 10.1002/jcp.1040930209.

Abstract

This study involves the use of fibroblast growth factor (FGF) as a substitute for exogenous serum to examine the early transport changes which occur when quiescent 3T3 cells re-initiate active growth. FGF, in nanogram amounts, together with insulin and dexamethasone, can induce mitogenesis and mitosis in 3T3 cells GO-arrested by holding in growth medium containing 0.8% calf serum. In terms of quiescent cell transport activity enhancement, FGF is 300,000-fold more effective than fresh serum, on a protein basis. In addition, very short exposure of serum-depleted cells to FGF indicates that a distinct temporal or time sequence exists in the transport system activation process. For example, uptake of alpha-aminoisobutyric acid (AIB) and uridine are stimulated very rapidly, whereas hypoxanthine uptake does not respond until much later. Closer analysis shows that AIB uptake is maximally enhanced within zero to two minutes after FGF addition to cells. Finally, the stimulatory effect of FGF on transport system activities is specific in terms of the proliferative state of the cells to which it is added, and in terms of the uptake systems which respond to it.

摘要

本研究涉及使用成纤维细胞生长因子(FGF)替代外源性血清,以检测静止的3T3细胞重新开始活跃生长时发生的早期转运变化。纳克量的FGF与胰岛素和地塞米松一起,可诱导被置于含0.8%小牛血清的生长培养基中而停滞在G0期的3T3细胞发生有丝分裂和细胞分裂。就增强静止细胞的转运活性而言,以蛋白质为基础,FGF比新鲜血清有效300,000倍。此外,血清耗尽的细胞与FGF的短暂接触表明,转运系统激活过程中存在明显的时间顺序。例如,α-氨基异丁酸(AIB)和尿苷的摄取很快受到刺激,而次黄嘌呤摄取直到很久以后才会有反应。进一步分析表明,在向细胞添加FGF后的零至两分钟内,AIB摄取得到最大增强。最后,FGF对转运系统活性的刺激作用在其添加到的细胞的增殖状态以及对其作出反应的摄取系统方面具有特异性。

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