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人类乳腺癌内分泌学的新进展:雌激素硫酸酯酶和硫酸转移酶

New developments in intracrinology of human breast cancer: estrogen sulfatase and sulfotransferase.

作者信息

Sasano Hironobu, Nagasaki Shuji, Miki Yasuhiro, Suzuki Takashi

机构信息

Department of Pathology Tohoku University School of Medicine, Sendai, Japan.

出版信息

Ann N Y Acad Sci. 2009 Feb;1155:76-9. doi: 10.1111/j.1749-6632.2008.03683.x.

DOI:10.1111/j.1749-6632.2008.03683.x
PMID:19250194
Abstract

Steroid sulfatase (STS) hydrolyses biologically inactive estrogen sulfates to active estrogens, while estrogen sulfotransferase (EST) sulfonates estrogens to estrogen sulfates. Information regarding the expression of STS in human breast carcinoma tissues is still very limited compared to that of aromatase or 17beta-hydroxysteroid dehydrogenases (17beta-HSDs). In our study, EST and STS immunoreactivity was detected in carcinoma cells in 50 and 84 out of 113 breast carcinomas (44.2% and 74.3%, respectively), which was also associated with mRNA levels determined by RT/real-time PCR. Using microdissection/RT-PCR analyses, EST mRNA was localized to both carcinoma and intratumoral stromal cells, whereas STS was detected only in carcinoma or parenchymal cells. STS immunoreactivity was positively associated with tumor size. EST immunoreactivity was inversely correlated with tumor size or lymph node status and was significantly associated with a decreased risk of recurrence and improved prognosis. These data suggest that both EST and STS play important roles in the regulation of in situ estrogen production in human breast cancer. In addition, EST is an independent prognostic factor in human breast carcinoma and loss of EST may result in altered estrogen metabolism in hormone-dependent breast cancer cells. An inhibition of intratumoral STS in the patients with estrogen-dependent breast carcinoma is also considered to provide more clinical benefits, especially to the patients in which primary source of an availability of intratumoral estrogen is through STS rather than aromatase.

摘要

类固醇硫酸酯酶(STS)可将无生物活性的雌激素硫酸盐水解为活性雌激素,而雌激素磺基转移酶(EST)则将雌激素磺化为雌激素硫酸盐。与芳香化酶或17β-羟基类固醇脱氢酶(17β-HSDs)相比,关于STS在人乳腺癌组织中表达的信息仍然非常有限。在我们的研究中,在113例乳腺癌中的50例(分别为44.2%)和84例(分别为74.3%)的癌细胞中检测到EST和STS免疫反应性,这也与通过RT/实时PCR测定的mRNA水平相关。使用显微切割/RT-PCR分析,EST mRNA定位于癌组织和瘤内基质细胞,而STS仅在癌细胞或实质细胞中检测到。STS免疫反应性与肿瘤大小呈正相关。EST免疫反应性与肿瘤大小或淋巴结状态呈负相关,并且与复发风险降低和预后改善显著相关。这些数据表明,EST和STS在人乳腺癌原位雌激素产生的调节中都起着重要作用。此外,EST是人类乳腺癌的一个独立预后因素,EST的缺失可能导致激素依赖性乳腺癌细胞中雌激素代谢的改变。对于雌激素依赖性乳腺癌患者,抑制瘤内STS也被认为能带来更多临床益处,特别是对于瘤内雌激素的主要来源是通过STS而非芳香化酶的患者。

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