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绝经前和绝经后乳腺组织中,星形孢菌素诱导的与自发性鳞状化生

Staurosporine-induced versus spontaneous squamous metaplasia in pre- and postmenopausal breast tissue.

作者信息

Heffelfinger S C, Miller M A, Gear R, Devoe G

机构信息

Department of Pathology and Laboratory Medicine, University of Cincinnati, Ohio 45267-0529, USA.

出版信息

J Cell Physiol. 1998 Aug;176(2):245-54. doi: 10.1002/(SICI)1097-4652(199808)176:2<245::AID-JCP3>3.0.CO;2-O.

Abstract

Breast cancers from pre- vs. postmenopausal women display unique characteristics that may be related to differences in epithelial differentiation between these two populations. In addition to lobular development, lactational changes, and involution, breast epithelium can undergo metaplastic alterations, often in association with carcinoma. Because protein kinase C (PKC) regulates differentiation and proliferation in many cell types, we asked whether modulation of PKC activity could define biochemical differences in breast epithelium from pre- vs. postmenopausal women. Organ cultures of normal human breast were treated with PKC agonists and antagonists. Epithelial differentiation was evaluated based on morphologic criteria and the expression of cell-type specific proteins. Staurosporine, a nonspecific but extremely potent inhibitor of PKC, induced squamous metaplasia in eight of eight cases within 2 weeks of treatment. Other inhibitors of PKC, such as calphostin C and tamoxifen, had no effect on epithelial differentiation. Long-term treatment with phorbol esters also did not induce squamous metaplasia. However, stimulation of cAMP levels by forskolin and isobutyl-methyl-xanthene (IMX) rapidly induced squamous metaplasia, as has been previously reported. Surprisingly, squamous metaplasia occurred in 10 of 12 cultures derived from postmenopausal women in the absence of exogenous agents. Untreated cultures derived from premenopausal women never developed this type of epithelium (0 of 11). Therefore, breast epithelium from pre- and postmenopausal women responded differently to in vitro culture. Forskolin/IMX or staurosporine can reproduce these conditions, acting independent of menopausal status. Because staurosporine's action was unique among PKC inhibitors, staurosporine may induce squamous metaplasia of breast epithelium by a PKC-independent mechanism.

摘要

绝经前和绝经后女性的乳腺癌表现出独特的特征,这可能与这两个人群上皮分化的差异有关。除了小叶发育、泌乳变化和退化外,乳腺上皮还可发生化生改变,且常与癌相关。由于蛋白激酶C(PKC)在许多细胞类型中调节分化和增殖,我们研究了PKC活性的调节是否能界定绝经前和绝经后女性乳腺上皮的生化差异。用人正常乳腺组织进行器官培养,并分别用PKC激动剂和拮抗剂处理。根据形态学标准和细胞类型特异性蛋白的表达来评估上皮分化情况。星形孢菌素是一种非特异性但极其有效的PKC抑制剂,在治疗2周内,8例中有8例诱导发生了鳞状化生。其他PKC抑制剂,如钙泊三醇和他莫昔芬,对上皮分化没有影响。佛波酯长期处理也未诱导鳞状化生。然而,如先前报道的那样,福斯高林和异丁基甲基黄嘌呤(IMX)刺激cAMP水平可迅速诱导鳞状化生。令人惊讶的是,在没有外源性试剂的情况下,12例来自绝经后女性的培养物中有10例发生了鳞状化生。来自绝经前女性的未经处理的培养物从未出现过这种类型的上皮(11例中有0例)。因此,绝经前和绝经后女性的乳腺上皮对体外培养的反应不同。福斯高林/IMX或星形孢菌素可重现这些情况,且其作用与绝经状态无关。由于星形孢菌素的作用在PKC抑制剂中是独特的,星形孢菌素可能通过一种不依赖PKC的机制诱导乳腺上皮的鳞状化生。

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