子宫颈鳞状细胞癌中SCCA1和SCCA2的表达及意义

目的检测子宫颈鳞状细胞癌组织中SCCA(squamous cell carcinoma antigen)1和SCCA2 mRNA的表达,探讨其在子宫颈鳞状细胞癌临床诊断、疗效评价及预后观察中的作用。方法采用实时PCR的方法定量分析60例子宫颈鳞状细胞癌组织和30例正常子宫颈组织中SCCA1和SCCA2 mRNA的表达,并分析二者与临床病理的关系。结果 SCCA2 mRNA的表达在子宫颈鳞状细胞癌组织中较正常子宫颈组织中高,差异有统计学意义(P<0.001),而SCCA1 mRNA的表达则无统计学差异。SCCA2 mRNA的表达随着临床分期的增高而增高(P<0.001),SCCA2 mRNA的表达在有淋巴结转移组较无淋巴结转移组高(P<0.05),SCCA2 mRNA的表达与病理分级和年龄无关(P>0.05),SCCA1 mRNA的表达与年龄、病理分级、临床分期及淋巴结转移均无明显相关性(P>0.05)。结论 SCCA2 mRNA的表达可能为子宫颈鳞状细胞癌临床分期、淋巴结转移提供更为准确的判断信息。

子宫颈鳞状细胞癌中SCCA1和SCCA2的分子表达及其意义

目的探讨子宫颈鳞状细胞癌组织中SCCAl和SCCA2mRNA的表达在子宫颈鳞状细胞癌临床诊断、疗效评价及预后观察中的作用。方法采用TaqMan探针实时聚合酶链反应（RT—PCR）的方法，分析60例子宫颈鳞状细胞癌患者和30例正常子宫颈组织中SCCA1和SCCA2mRNA的表达。结果SCCA2mRNA在子宫颈鳞状细胞癌组织中较对照正常组织中表达水平高（相对表达量分别为4．405±2．310及9．088±2．195），差异有统计学意义（t=-6．513，P〈0．05）。SCCA1mRNA则差异无统计学意义（t=-0．115，P〉0．05）。SCCA2mRNA的表达随着临床分期的增高而增高（F=8．313，P〈0．05），SCCA2mRNA的表达在有淋巴结转移组较无淋巴结转移组高（t=2．853，P〈0．05），SCCA2mRNA的表达与病理分级及患者年龄无关（P〉0．05），SCCA1mRNA的表达与患者年龄、病理分级、临床分期及淋巴结转移均无明显相关性（P〉0．05）。结论SCCA2mRNA的表达可能为子宫颈鳞状细胞癌临床分期、淋巴结转移的判断提供更为准确的信息。

鳞状细胞癌相关抗原在食管癌患者血清和组织表达意义的临床研究

目的:探讨鳞状细胞癌相关抗原在食管癌患者血清和组织表达意义。方法:选取行食管癌手术的鳞状细胞癌患者42例,对切除标本癌组织和癌旁组织中鳞状细胞癌抗原2(SCCA2)进行免疫组化检测,观察SCCA2表达与食管鳞状细胞癌的部位、分化、浸润、淋巴结转移和临床分期的关系;同时在术前、术后3天和术后一周抽取患者外周血检测鳞状细胞癌抗原(SCCAg)水平,观察血清SCCAg与肿瘤分化、浸润、淋巴结转移和临床分期的关系。结果:癌组织中SCCA2阳性率明显高于癌旁组织,差异具有统计学意义(P<0.01);低分化癌SCCA2表达阳性率明显低于高分化、中分化、高中分化癌,差异具有统计学意义(P=0.026);而SCCA2表达与肿瘤浸润深度、淋巴结转移和临床分期无明显的相关性(P>0.05);食管癌患者术前SCCAg阳性率明显高于术后3d和术后1周,差异具有统计学意义(P<0.01);食管癌患者术前血清SCCAg水平明显高于术后,差异具有统计学意义(P<0.01);食管癌患者术前血清SCCAg水平与肿瘤分化程度无明显的相关性,而与肿瘤浸润深度、淋巴结转移和临床分期密切相关(P<0.05)。结论:癌组织中SCCA2表达与血清中SCCAg的表达呈正相关,因此外周血SCCAg检测对食管鳞癌的早期诊断与临床分期有重要意义。

鳞状细胞癌抗原2与炎症性皮肤病

鳞状细胞癌抗原2(Squamous cell carcinoma antigen 2,SCCA2,SERPINB4)作为鳞状细胞癌抗原之一,一直被作为一些鳞状细胞癌的肿瘤标志物,研究人员发现SCCA2在包括银屑病、特应性皮炎的许多炎症性皮肤病中表达上调,其与银屑病和特应性皮炎的发病密切相关,SCCA2可能主要通过诱发炎症反应而参与发病,但在炎症性皮肤病中的具体作用机制目前还不十分明确。本文就近年来SCCA2在炎症性皮肤病的相关研究作一综述。

Hydrophobicity of reactive site loop of SCCA1 affects its binding to hepatitis B virus

AIM: To investigate the role of SCCA2 and other SCCA1 molecules in the process of hepatitis B virus (HBV) binding to mammalian cells.METHODS: SCCA1 and SCCA2 were isolated from HepG2. Binding protein (BP) genes were obtained through PCR. Recombinant baculoviruses expressing SCCA1, SCCA2, BP, and different mutants were constructed and utilized to infect mammalian cells to investigate the binding ability of infected cells to HBV.RESULTS: A SCCA1 gene (A1) was isolated from HepG2, but it appeared to lack the binding ability of infected cells to HBV. Two mutants, A1-BP and BP-A1, were constructed by interchanging the carboxyl terminal of A1 and BP. Cells expressing A1-BP showed an increased virus bindingcapacity, but not BP-A1. Comparison of A1 sequence with the sequence of BP indicated the presence of only three amino acid changes in the carboxyl terminal, two of them were found in the reactive site loop (RSL) of SCCA1. Primary structure assay revealed that the hydrophobicity of BP and AJ515706 in this domain was strong, but A1 was relatively weak. Changing the aa349 of A1 from low hydrophobic glutamic acid to high hydrophobic valine enhanced HBV binding. In contrast, HBV binding was reduced by changing the aa349 of BP from valine to glutamic acid. CONCLUSION: The reslts suggest that the hydrophobicity of RSL of SCCA1 may play an important role in HBV binding to cells.