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Securin is overexpressed in breast cancer

机译:Securin在乳腺癌中过表达

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Securin regulates sister chromatid separation during mitosis, induces bFGF-mediated angiogenesis, and securin overexpression causes in vitro transformation and in vivo tumor formation in nude mice. As estrogen administration to oophorectomized rats increased pituitary securin expression, we used immunohistochemistry to examine securin and estrogen receptor alpha (ER-) expression in 90 breast tumors and 18 normal breast tissues. Breast tumor securin and ER- expression were quantitated by image analysis and expressed as fold difference relative to securin expression in normal breast tissue. Low cytoplasmic securin expression was seen in the normal breast epithelium, whereas abundant cytoplasmic and nuclear securin expression was demonstrated in all 90 breast tumors. Highest securin expression was seen in brain metastatic breast tumors (4.3-fold, PPPPsecurin mRNA expression compared to normal breast mucosa (2.5-fold, P=0.03), with highest securin evident in invasive (3.5-fold) vs noninvasive tumors (1.9-fold, P=0.03). In addition, some tumors that exhibited high securin expression also expressed high ER- levels (P<0.0001). These results demonstrate that the estrogen-induced transforming gene, securin is abundantly expressed in breast carcinoma, and is associated with the presence of metastatic spread, and lymph node invasion. We propose immunohistochemical tumor securin expression as a potential invasive marker, and novel therapeutic target in breast cancer.
机译:Securin在有丝分裂过程中调节姐妹染色单体的分离,诱导bFGF介导的血管生成,而securin的过表达导致裸鼠体内转化和体内肿瘤形成。由于向经去卵巢切除的大鼠施用雌激素会增加垂体分泌的securin表达,我们使用免疫组织化学检查了90个乳腺肿瘤和18个正常乳腺组织中的securin和雌激素受体α(ER-)表达。通过图像分析定量乳腺肿瘤securin和ER-表达,并表示为相对于正常乳腺组织中securin表达的倍数差异。在正常的乳腺上皮细胞中观察到低的细胞质securin表达,而在所有90个乳腺肿瘤中均显示出丰富的细胞质和核securin表达。在脑转移性乳腺肿瘤中观察到最高的Securin表达(4.3倍,PPPPsecurin mRNA表达与正常乳腺粘膜相比(2.5倍,P = 0.03),在侵袭性肿瘤(3.5倍)与非侵袭性肿瘤中,1.9sec的表达最高)(1.9-倍,P = 0.03)。此外,一些表现出高水平securin的肿瘤也表达高ER-水平(P <0.0001),这些结果表明雌激素诱导的转化基因securin在乳腺癌中大量表达,并且与转移性扩散的存在和淋巴结的侵袭有关,我们提出免疫组化肿瘤securin表达作为一种潜在的侵袭性标志物,也是乳腺癌的新型治疗靶点。

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