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在长期和短期缺乏雌激素的情况下培养的MCF-7人乳腺癌细胞的增殖、激素反应性及雌激素受体含量

Proliferation, hormonal responsiveness, and estrogen receptor content of MCF-7 human breast cancer cells grown in the short-term and long-term absence of estrogens.

作者信息

Katzenellenbogen B S, Kendra K L, Norman M J, Berthois Y

出版信息

Cancer Res. 1987 Aug 15;47(16):4355-60.

PMID:3607768
Abstract

We have examined the effect of short-term and long-term growth in the absence of estrogens on the proliferation rate and estrogen and antiestrogen responsiveness of MCF-7 human breast cancer cells. The removal of phenol red, the pH indicator in tissue culture medium that is weakly estrogenic (Y. Berthois et al., Proc. Natl. Acad. Sci. USA, 83:2496-2500, 1986), immediately slows the cell proliferation rate, and MCF-7 cells grown in phenol red-free medium with charcoal dextran-treated serum for periods up to 1 mo maintain this reduced rate of cell proliferation. In these short-term phenol red-withdrawn cells, estradiol stimulates proliferation markedly and reproducibly, and antiestrogens inhibit estrogen-stimulated proliferation. Antiestrogens by themselves appear as partial agonists/antagonists; at low concentrations they stimulate proliferation weakly, but they show no stimulation at the high concentrations where they fully inhibit estrogen-stimulated proliferation. In contrast to the short-term phenol red-withdrawn cells, cells maintained for several months (5 to 6 mo) in the apparently complete absence of estrogens (no phenol red, with charcoal dextran-treated calf serum) show a markedly increased basal rate of cell proliferation; estradiol is unable to increase this rate of proliferation further, but antiestrogens are able to decrease proliferation. This change in growth pattern is associated with a 3-fold increase in cellular estrogen receptor levels. Despite their differing basal growth rates, cells grown in either the short-term (less than 1 mo) or long-term (greater than 6 mo) absence of estrogens both have progesterone receptor levels that are very low and, in both cases, estradiol increases progesterone receptor levels markedly. Thus, under long-term estrogen-free conditions, there is a dissociation between the stimulation of cell proliferation and of specific protein synthesis (progesterone receptor) by estrogen. The increase in the cell proliferation rate observed in cells grown in the long-term absence of estrogen may reflect altered regulation of growth factor production or altered sensitivity to growth factors in the medium or produced by the cells themselves. Hence, these breast cancer cells adapt significantly to long-term growth in estrogen-free conditions, an observation that may be relevant to understanding the growth of hormone-responsive human breast cancers in vivo.

摘要

我们研究了在缺乏雌激素的情况下短期和长期生长对MCF-7人乳腺癌细胞增殖率以及雌激素和抗雌激素反应性的影响。去除组织培养基中的酚红(一种具有弱雌激素活性的pH指示剂,Y. Berthois等人,《美国国家科学院院刊》,83:2496 - 2500,1986年),会立即减缓细胞增殖速率,并且在不含酚红的培养基中,用经活性炭葡聚糖处理的血清培养长达1个月的MCF-7细胞,其细胞增殖速率维持在降低水平。在这些短期去除酚红的细胞中,雌二醇能显著且可重复地刺激增殖,抗雌激素能抑制雌激素刺激的增殖。抗雌激素本身表现为部分激动剂/拮抗剂;在低浓度时它们能微弱地刺激增殖,但在能完全抑制雌激素刺激增殖的高浓度时则无刺激作用。与短期去除酚红的细胞不同,在明显完全缺乏雌激素(无酚红,用经活性炭葡聚糖处理的小牛血清)的条件下维持数月(5至6个月)的细胞,其基础细胞增殖速率显著增加;雌二醇无法进一步提高这种增殖速率,但抗雌激素能够降低增殖。这种生长模式的变化与细胞雌激素受体水平增加3倍相关。尽管它们的基础生长速率不同,但在短期(少于1个月)或长期(多于6个月)缺乏雌激素条件下生长的细胞,其孕激素受体水平都非常低,并且在这两种情况下,雌二醇都能显著提高孕激素受体水平。因此,在长期无雌激素条件下,雌激素对细胞增殖和特定蛋白质合成(孕激素受体)的刺激作用出现了分离。在长期缺乏雌激素条件下生长的细胞中观察到的细胞增殖速率增加,可能反映了生长因子产生的调节改变,或者对培养基中或细胞自身产生的生长因子的敏感性改变。因此,这些乳腺癌细胞能显著适应无雌激素条件下的长期生长,这一观察结果可能与理解激素反应性人类乳腺癌在体内的生长有关。

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