Schöniger-Hekele Maximilian, Hänel Sabine, Wrba Fritz, Müller Christian
Universitätsklinik für Innere Medizin IV, Klinische Abteilung Gastroenterologie und Hepatologie, University of Vienna, A-1090 Vienna, Austria.
Liver Int. 2005 Feb;25(1):62-9. doi: 10.1111/j.1478-3231.2004.0997.x.
Many genes participate in the regulation of cell proliferation and growth of tumor cells. Altered expression and loss of function of some of these gene products have been found in malignant tumors and correlated with progression and poor prognosis.
Our aim was to correlate the expression of various molecular histologic markers with tumor characteristics and survival time of patients with hepatocellular carcinoma (HCC).
Tumor tissues of 81 patients with HCC were investigated immunohistochemically for the expression of cellular proliferation markers Mib1 (Ki67) and c-erbB-2 (HER2/neu), cellcycle markers (p53, mdm2 and p21), CD81 (TAPA1), a marker shown to be associated with metastasis, and human leukocyte antigen (HLA)-DR expression, involved in immunological antigen presentation.
p21 was expressed in a higher percentage (83.3 vs. 50%, P=0.014) in undifferentiated histological tumor grades (Edmondson Steiner G3 vs. G1/G2). HCC in patients with enlarged lymph nodes expressed HLA-DR in a higher percentage (28.6%) than tumors without lymph node enlargement (5.7%, P=0.006). Patients with distant metastases were less likely to express CD 81 (11.1%) on tumor cells than patients without distant metastases (38.3%, P=0.0335). No other correlation with clinical or tumor characteristics or molecular histologic markers investigated was found. P53 accumulating patients showed a worse survival than patients with tumors p53 non-accumulating (median 4.1 months vs. median 9.3 months, P=0.01798). Neither the expression nor the non-expression of proliferation, cell cycle, immunologic or cell adhesion markers was associated with differences in survival. However, patients with a low expression of cell cycle marker mdm2 survived significantly longer (median 9.4 months) as compared with patients with high expression (median 3.9 months).
Our results suggest that p53 nuclear accumulation and mdm2 high expression are associated with poor survival in patients withHCC. Furthermore, patients with enlarged lymph nodes had HLA-DR-positive tumors more frequently and patients with distant metastases had tumors with CD81 expression less often.
许多基因参与肿瘤细胞的增殖和生长调控。在恶性肿瘤中已发现其中一些基因产物的表达改变和功能丧失,且与肿瘤进展和预后不良相关。
我们的目的是将各种分子组织学标志物的表达与肝细胞癌(HCC)患者的肿瘤特征和生存时间相关联。
对81例HCC患者的肿瘤组织进行免疫组织化学研究,以检测细胞增殖标志物Mib1(Ki67)和c-erbB-2(HER2/neu)、细胞周期标志物(p53、mdm2和p21)、CD81(TAPA1,一种显示与转移相关的标志物)以及参与免疫抗原呈递的人类白细胞抗原(HLA)-DR的表达。
在未分化组织学肿瘤分级(Edmondson Steiner G3与G1/G2)中,p21的表达百分比更高(83.3%对50%,P = 0.014)。有肿大淋巴结的患者的HCC中HLA-DR的表达百分比(28.6%)高于无淋巴结肿大的肿瘤(5.7%,P = 0.006)。有远处转移的患者肿瘤细胞表达CD81的可能性(11.1%)低于无远处转移的患者(38.3%,P = 0.0335)。未发现与所研究的临床或肿瘤特征或分子组织学标志物有其他相关性。p53累积的患者比p53不累积的患者生存情况更差(中位生存期4.1个月对9.3个月,P = 0.01798)。增殖、细胞周期、免疫或细胞黏附标志物的表达或不表达均与生存差异无关。然而,细胞周期标志物mdm2低表达的患者比高表达的患者生存时间显著更长(中位生存期9.4个月对3.9个月)。
我们的结果表明,p53核累积和mdm2高表达与HCC患者的不良生存相关。此外,有肿大淋巴结的患者HLA-DR阳性肿瘤更常见,有远处转移的患者肿瘤CD81表达较少见。
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