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利用单克隆抗体Mx35对卵巢癌中NaPi2b蛋白表达进行计算机分析和免疫组织化学特征分析。

In silico analysis and immunohistochemical characterization of NaPi2b protein expression in ovarian carcinoma with monoclonal antibody Mx35.

作者信息

Soares Ibere Cauduro, Simões Kleber, de Souza Jorge Estefano Santana, Okamoto Oswaldo Keith, Wakamatsu Alda, Tuma Maria Carolina, Ritter Gerd, Alves Venancio Avancini Ferreira

机构信息

LIM14 – Department of Pathology, Faculdade de Medicina da Universidade de São Paulo, Brazil.

出版信息

Appl Immunohistochem Mol Morphol. 2012 Mar;20(2):165-72. doi: 10.1097/pai.0b013e318228e232.

Abstract

INTRODUCTION

Ovarian adenocarcinoma is frequently detected at the late stage, when therapy efficacy is limited and death occurs in up to 50% of the cases. A potential novel treatment for this disease is a monoclonal antibody that recognizes phosphate transporter sodium-dependent phosphate transporter protein 2b (NaPi2b).

MATERIALS AND METHODS

To better understand the expression of this protein in different histologic types of ovarian carcinomas, we immunostained 50 tumor samples with anti-NaPi2b monoclonal antibody MX35 and, in parallel, we assessed the expression of the gene encoding NaPi2b (SCL34A2) by in silico analysis of microarray data.

RESULTS

Both approaches detected higher expression of NaPi2b (SCL34A2) in ovarian carcinoma than in normal tissue. Moreover, a comprehensive analysis indicates that SCL34A2 is the only gene of the several phosphate transporters genes whose expression differentiates normal from carcinoma samples, suggesting it might exert a major role in ovarian carcinomas. Immunohistochemical and mRNA expression data have also shown that 2 histologic subtypes of ovarian carcinoma express particularly high levels of NaPi2b: serous and clear cell adenocarcinomas. Serous adenocarcinomas are the most frequent, contrasting with clear cell carcinomas, rare, and with worse prognosis.

CONCLUSION

This identification of subgroups of patients expressing NaPi2b may be important in selecting cohorts who most likely should be included in future clinical trials, as a recently generated humanized version of MX35 has been developed.

摘要

引言

卵巢腺癌常在晚期被发现,此时治疗效果有限,高达50%的病例会死亡。针对这种疾病的一种潜在新疗法是一种识别磷酸转运体钠依赖性磷酸转运蛋白2b(NaPi2b)的单克隆抗体。

材料与方法

为了更好地了解该蛋白在不同组织学类型卵巢癌中的表达情况,我们用抗NaPi2b单克隆抗体MX35对50个肿瘤样本进行了免疫染色,同时,我们通过对微阵列数据的计算机分析评估了编码NaPi2b的基因(SCL34A2)的表达。

结果

两种方法均检测到卵巢癌中NaPi2b(SCL34A2)的表达高于正常组织。此外,综合分析表明,SCL34A2是几种磷酸转运体基因中唯一其表达能区分正常样本与癌样本的基因,这表明它可能在卵巢癌中发挥主要作用。免疫组织化学和mRNA表达数据还显示,卵巢癌的两种组织学亚型表达特别高水平的NaPi2b:浆液性和透明细胞腺癌。浆液性腺癌最为常见,与透明细胞癌形成对比,后者罕见且预后较差。

结论

由于最近已开发出MX35的人源化版本,识别表达NaPi2b的患者亚组对于选择最有可能纳入未来临床试验的队列可能很重要。

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