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α-甲基酰基辅酶A消旋酶:一种新的前列腺癌分子标志物。

Alpha-methylacyl-CoA racemase: a new molecular marker for prostate cancer.

作者信息

Luo Jun, Zha Shan, Gage Wesley R, Dunn Thomas A, Hicks Jessica L, Bennett Christina J, Ewing Charles M, Platz Elizabeth A, Ferdinandusse Sacha, Wanders Ronald J, Trent Jeffrey M, Isaacs William B, De Marzo Angelo M

机构信息

Department of Pathology, Brady Urological Institute, Johns Hopkins University, School of Medicine, Baltimore, MD 21287, USA.

出版信息

Cancer Res. 2002 Apr 15;62(8):2220-6.

Abstract

Identification of genes that are dysregulated in association with prostate carcinogenesis can provide disease markers and clues relevant to disease etiology. Of particular interest as candidate markers of disease are those genes that are frequently overexpressed. In this study, we describe a gene, alpha-methylacyl-CoA racemase (AMACR), whose expression is consistently up-regulated in prostate cancer. Analysis of mRNA levels of AMACR revealed an average up-regulation of approximately 9 fold in clinical prostate cancer specimens compared with normal. Western blot and immunohistochemical analysis confirms the up-regulation at the protein level and localizes the enzyme predominantly to the peroxisomal compartment of prostate cancer cells. A detailed immunohistochemical analysis of samples from 168 primary prostate cancer cases using both standard slides and tissue microarrays demonstrates that both prostate carcinomas and the presumed precursor lesion (high-grade prostatic intraepithelial neoplasia) consistently scored significantly higher than matched normal prostate epithelium; 88% of the carcinomas had a staining score higher than the highest score observed for any sample of normal prostate epithelium. Both untreated metastases (n = 32 patients) and hormone refractory prostate cancers (n = 14 patients) were generally strongly positive for AMACR. To extend the utility of this marker for prostate cancer diagnosis, we combined staining for cytoplasmic AMACR with staining for the nuclear protein, p63, a basal cell marker in the prostate that is absent in prostate cancer. In a simple assay that can be useful for the diagnosis of prostate cancer on both biopsy and surgical specimens, combined staining for p63 and AMACR resulted in a staining pattern that greatly facilitated the identification of malignant prostate cells. The enzyme encoded by the AMACR gene plays a critical role in peroxisomal beta oxidation of branched chain fatty acid molecules. These observations could have important epidemiological and preventive implications for prostate cancer, as the main sources of branched chain fatty acids are dairy products and beef, the consumption of which has been associated with an increased risk for prostate cancer in multiple studies. On the basis of its consistency and magnitude of cancer cell-specific expression, we propose AMACR as an important new marker of prostate cancer and that its use in combination with p63 staining will form the basis for an improved staining method for the identification of prostate carcinomas. Furthermore, the absence of AMACR staining in the vast majority of normal tissues coupled with its enzymatic activity makes AMACR the ideal candidate for development of molecular probes for the noninvasive identification of prostate cancer by imaging modalities.

摘要

鉴定与前列腺癌发生相关的失调基因可以提供疾病标志物以及与疾病病因相关的线索。作为疾病候选标志物,特别值得关注的是那些经常过度表达的基因。在本研究中,我们描述了一种基因,α-甲基酰基辅酶A消旋酶(AMACR),其在前列腺癌中表达持续上调。对AMACR的mRNA水平分析显示,与正常组织相比,临床前列腺癌标本中的平均上调约9倍。蛋白质印迹和免疫组织化学分析证实了该酶在蛋白质水平的上调,并将其主要定位在前列腺癌细胞的过氧化物酶体区室。使用标准载玻片和组织微阵列对168例原发性前列腺癌病例的样本进行详细的免疫组织化学分析表明,前列腺癌和推测的前体病变(高级别前列腺上皮内瘤变)的评分始终显著高于匹配的正常前列腺上皮;88%的癌组织染色评分高于正常前列腺上皮任何样本中观察到的最高评分。未经治疗的转移瘤(n = 32例患者)和激素难治性前列腺癌(n = 14例患者)的AMACR通常呈强阳性。为了扩展该标志物在前列腺癌诊断中的应用,我们将细胞质AMACR染色与核蛋白p63染色相结合,p63是前列腺中的一种基底细胞标志物,在前列腺癌中不存在。在一种可用于活检和手术标本中前列腺癌诊断的简单检测方法中,p63和AMACR的联合染色产生了一种染色模式,极大地促进了恶性前列腺细胞的识别。AMACR基因编码的酶在支链脂肪酸分子的过氧化物酶体β氧化中起关键作用。这些观察结果可能对前列腺癌具有重要的流行病学和预防意义,因为支链脂肪酸的主要来源是乳制品和牛肉,多项研究表明食用这些食物会增加患前列腺癌的风险。基于其在癌细胞特异性表达的一致性和程度,我们提出AMACR作为前列腺癌的一种重要新标志物,并且其与p63染色联合使用将为改进前列腺癌鉴定的染色方法奠定基础。此外,绝大多数正常组织中不存在AMACR染色及其酶活性使得AMACR成为通过成像方式无创鉴定前列腺癌的分子探针开发的理想候选物。

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