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C-MET 在大多数阴茎鳞癌中表达,并与多倍体-7 相关,但与 MET 癌基因扩增、相关组织病理学参数或癌症特异性生存无关。

C-MET is expressed in the majority of penile squamous cell carcinomas and correlates with polysomy-7 but is not associated with MET oncogene amplification, pertinent histopathologic parameters, or with cancer-specific survival.

机构信息

Department of Pathology, Johanniter Hospital Stendal, Germany.

出版信息

Pathol Res Pract. 2013 Apr;209(4):215-20. doi: 10.1016/j.prp.2013.02.002. Epub 2013 Mar 13.

DOI:10.1016/j.prp.2013.02.002
PMID:23490239
Abstract

We assessed c-MET expression and oncogene amplification in a cohort enrolling 92 surgically treated penile squamous cell carcinomas (PSCCs). A tissue microarray was constructed for c-MET immunohistochemistry (IHC) and chromogenic silver in situ hybridization (SISH). Two independent pathologists evaluated IHC by employing the breast cancer scoring rules, and scored the presence of MET oncogene amplification and/or polysomy-7. Eighty study cases (87%) showed c-MET expression. No study case had MET oncogene amplification, but 42 patients (45.7%) had polysomy-7. Polysomy-7 showed a significant positive correlation with c-MET expression (ρ=0.323, p=0.002). Neither c-MET expression nor polysomy-7 was associated with histopathologic parameters or with cancer-specific survival (median post-surgical follow-up 32 months). Our data suggest that the majority of PSCCs exhibit c-MET expression which is not associated with oncogene amplification, but might be attributable to polysomy-7. Further studies should investigate the expression and activation of downstream molecules functionally involved in c-MET pathway signaling, and clarify the so far unresolved role of c-MET inhibitors as potential targeted therapies in PSCCs with metastatic dissemination.

摘要

我们评估了 92 例接受手术治疗的阴茎鳞状细胞癌 (PSCC) 患者的 c-MET 表达和癌基因扩增情况。构建了组织微阵列,用于 c-MET 免疫组织化学 (IHC) 和显色银原位杂交 (SISH)。两位独立的病理学家采用乳腺癌评分规则评估 IHC,并对 MET 癌基因扩增和/或 7 号染色体三体的存在进行评分。80 例研究病例(87%)显示 c-MET 表达。没有研究病例存在 MET 癌基因扩增,但 42 例患者(45.7%)存在 7 号染色体三体。7 号染色体三体与 c-MET 表达呈显著正相关(ρ=0.323,p=0.002)。c-MET 表达和 7 号染色体三体均与组织病理学参数或癌症特异性生存无关(术后随访中位数为 32 个月)。我们的数据表明,大多数 PSCC 表现出 c-MET 表达,与癌基因扩增无关,但可能归因于 7 号染色体三体。进一步的研究应调查下游分子的表达和激活,这些分子在 c-MET 通路信号中具有功能作用,并阐明 c-MET 抑制剂作为转移性扩散的 PSCC 潜在靶向治疗的作用仍未解决。

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