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前列腺肿瘤会下调周围良性前列腺上皮中的微精蛋白-β(MSMB),这种反应与肿瘤侵袭性相关。

Prostate tumors downregulate microseminoprotein-beta (MSMB) in the surrounding benign prostate epithelium and this response is associated with tumor aggressiveness.

作者信息

Bergström Sofia Halin, Järemo Helena, Nilsson Maria, Adamo Hanibal Hani, Bergh Anders

机构信息

Department of Medical Biosciences, Pathology, Umeå University, Umeå, Sweden.

出版信息

Prostate. 2018 Mar;78(4):257-265. doi: 10.1002/pros.23466. Epub 2017 Dec 18.

Abstract

BACKGROUND

Microseminoprotein-beta (MSMB) is a major secretory product from prostate epithelial cells. MSMB synthesis is decreased in prostate tumors in relation to tumor grade. MSMB levels are also reduced in the circulation and MSMB is therefore used as a serum biomarker for prostate cancer. We hypothesized that cancers induce a reduction in MSMB synthesis also in the benign parts of the prostate, and that the magnitude of this response is related to tumor aggressiveness. Reduced levels of MSMB in the circulation could therefore be a consequence of reduced MSMB expression not only in tumor tissue but also in the benign prostate tissue.

METHODS

MSMB expression was analyzed in prostatectomy specimens from 36 patients using immunohistochemistry and qRT-PCR. MSMB expression in the benign prostate tissue was analyzed in relation to Gleason score, tumor stage, and distance to the tumor. Furthermore, Dunning rat prostate tumors with different aggressiveness were implanted into the prostate of Copenhagen rats to study if this affected the MSMB expression in the tumor-adjacent benign rat prostate tissue.

RESULTS

In prostatectomy specimens, MSMB expression was reduced in prostate tumors but also in the tumor-adjacent benign parts of the prostate. The reduction in tumor MSMB was related to tumor grade and stage, and the reduction in the benign parts of the prostate to tumor grade, stage, and distance to the tumor. Implantation of Dunning cancer cells into the rat prostate resulted in reduced MSMB protein levels in the tumor-adjacent benign prostate tissue. Rapidly growing and metastatic MatLyLu tumors had a more pronounced effect than slow-growing non-metastatic G tumors.

CONCLUSION

Our data suggest that aggressive prostate tumors suppress MSMB synthesis in the benign prostate and that this could explain why serum levels of MSMB are decreased in prostate cancer patients. This study suggests that markers for aggressive cancer can be found among factors altered in parallel in prostate tumors and in the adjacent benign tissue.

摘要

背景

微小精液蛋白-β(MSMB)是前列腺上皮细胞的主要分泌产物。与肿瘤分级相关,前列腺肿瘤中MSMB的合成减少。循环中MSMB水平也降低,因此MSMB被用作前列腺癌的血清生物标志物。我们推测癌症也会导致前列腺良性部分的MSMB合成减少,且这种反应的程度与肿瘤侵袭性有关。因此,循环中MSMB水平降低可能不仅是肿瘤组织中MSMB表达降低的结果,也是良性前列腺组织中MSMB表达降低的结果。

方法

使用免疫组织化学和qRT-PCR分析36例患者前列腺切除标本中的MSMB表达。分析良性前列腺组织中MSMB表达与 Gleason评分、肿瘤分期及与肿瘤距离的关系。此外,将具有不同侵袭性的邓宁大鼠前列腺肿瘤植入哥本哈根大鼠的前列腺中,以研究这是否会影响肿瘤邻近的良性大鼠前列腺组织中的MSMB表达。

结果

在前列腺切除标本中,前列腺肿瘤及肿瘤邻近的前列腺良性部分中MSMB表达均降低。肿瘤中MSMB降低与肿瘤分级和分期相关,前列腺良性部分中MSMB降低与肿瘤分级、分期及与肿瘤距离相关。将邓宁癌细胞植入大鼠前列腺导致肿瘤邻近的良性前列腺组织中MSMB蛋白水平降低。快速生长和转移的MatLyLu肿瘤比生长缓慢的非转移性G肿瘤影响更明显。

结论

我们的数据表明侵袭性前列腺肿瘤会抑制良性前列腺中的MSMB合成,这可以解释为什么前列腺癌患者血清中MSMB水平会降低。这项研究表明,在前列腺肿瘤和邻近良性组织中平行改变的因素中可以找到侵袭性癌症的标志物。

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