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纤溶酶原激活剂的激素调节:一种预测人类乳腺肿瘤反应性的方法。

Hormonal modulation of plasminogen activator: an approach to prediction of human breast tumor responsiveness.

作者信息

Mira-y-Lopez R, Ossowski L

出版信息

Cancer Res. 1987 Jul 1;47(13):3558-64.

PMID:3107811
Abstract

We have determined that the primary reason for the frequently encountered poor survival of human scirrhous breast carcinomas in short-term (4 days) organ culture is mechanical injury to the tumor tissue during explant preparation. It was possible to minimize this injury by preparing 0.5-mm-thick slices using very sharp blades. This resulted in much improved preservation of tissue structure and function, as assessed by histology, DNA content, and enzyme synthesis and secretion. With the exception of insulin, which was always present in the culture medium, exogenous hormones, including estrogen, or serum did not further improve explant preservation. In rodent mammary tumors, growth in vivo and production of the serine protease plasminogen activator (PA) in organ culture are coordinately regulated by hormones, suggesting that PA may be a valuable indicator of tumor hormone responsiveness. We have now tested the effect of estrogen and other hormones on PA secretion in organ cultures of primary human breast carcinomas. We found that: modulation of PA by 17-beta-estradiol (10-8) M) occurred only in carcinomas which were positive for both estrogen and progesterone receptors; of 21 such tumors, 11 (52%) were responsive. Plasminogen activator was not modulated by estradiol in any of the 22 tumors which were negative for one or both receptors; hydrocortisone (10(-7) M) effectively inhibited, and 3,5,3'-L-triiodothyronine (10(-8) M) and adenylate cyclase activators effectively stimulated PA in most breast tumors, regardless of their estrogen and progesterone receptor status. Prolactin (5 micrograms/ml) had no effect when tested alone; urokinase-type PA was found to be the principal PA produced by human breast tumors. Changes in its rate of synthesis and secretion and not in the content of PA inhibitors appeared to be the prevailing mechanism of enzyme regulation by hormones. In summary, short-term organ culture coupled with the use of PA as an index of response appears to be a promising approach to the study of hormone sensitivity of primary human breast carcinomas.

摘要

我们已经确定,在短期(4天)器官培养中,人硬癌性乳腺癌存活率常常很低,其主要原因是在组织块制备过程中肿瘤组织受到机械损伤。使用非常锋利的刀片制备0.5毫米厚的切片,可以将这种损伤降至最低。通过组织学、DNA含量以及酶的合成和分泌评估发现,这使得组织结构和功能的保存有了很大改善。除了培养基中始终存在的胰岛素外,包括雌激素在内的外源性激素或血清并不能进一步改善组织块的保存。在啮齿动物乳腺肿瘤中,体内生长和器官培养中丝氨酸蛋白酶纤溶酶原激活物(PA)的产生受激素协同调节,这表明PA可能是肿瘤激素反应性的一个有价值的指标。我们现在已经测试了雌激素和其他激素对原发性人乳腺癌器官培养中PA分泌的影响。我们发现:17-β-雌二醇(10^(-8) M)对PA的调节仅发生在雌激素和孕激素受体均为阳性的癌中;在21个这样的肿瘤中,11个(52%)有反应。在22个一种或两种受体为阴性的肿瘤中,雌二醇对PA均无调节作用;氢化可的松(10^(-7) M)有效抑制,而3,5,3'-L-三碘甲状腺原氨酸(10^(-8) M)和腺苷酸环化酶激活剂在大多数乳腺肿瘤中均有效刺激PA,无论其雌激素和孕激素受体状态如何。单独测试时,催乳素(5微克/毫升)没有作用;发现尿激酶型PA是人乳腺肿瘤产生的主要PA。激素对酶的调节主要机制似乎是其合成和分泌速率的变化,而非PA抑制剂含量的变化。总之,短期器官培养加上使用PA作为反应指标,似乎是研究原发性人乳腺癌激素敏感性的一种有前景的方法。

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