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抑癌基因WWOX与相关基因p73、Bax在结直肠癌中的表达及意义 被引量:6

Expression of WWOX,p73 and Bax in colorectal carcinoma and its significance
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摘要 目的探讨含有WW结构域的氧化还原酶基因(WW domain containing oxidoreductase,WWOX)的表达与结直肠癌生物学行为及p73、Bax表达的相关性。方法应用免疫组化Envision二步法检测58例结直肠癌中WWOX、p73及Bax的表达,并以20例结直肠黏膜炎症为对照。结果①WWOX、Bax在结直肠癌组织中的阳性率分别为25.86%、58.62%,显著低于结直肠黏膜炎症的65%、85%(P<0.01,P<0.05);二者在结直肠癌中的表达与患者的预后相关(P<0.01,P<0.05),且WWOX的表达在癌组织与浸润深度相关(P<0.05);②p73在癌组织中的阳性率显著高于炎症组(63.79%vs 30%,P<0.01),在结直肠癌中的表达与淋巴结转移及浸润深度有关(P<0.05);③WWOX与p73的表达无关(χ2=0.072,P>0.05),而与Bax的表达有关(χ2=6.561,P<0.05)。结论 WWOX、p73及Bax参与调控结直肠癌的发生、发展,且WWOX与Bax协同作用,在结直肠癌的预后中扮演了重要角色。 Objective To study the correlation between the expression of WW domain containing oxidoreductase (WWOX) and the biological behavior of colorectal cancer, and the correlation between WWOX and the expressions of P73 and Bax in eolorectal carcinoma. Methods The expressions of WWOX, p73 and Bax were detected by immunohistoehemistry ( using Envision twotep method) in 58 cases of colorectal carcinoma. Twenty cases of colorectal mucosal inflammation were chosen as controls. Results The positive rates of WWOX and Bax in colorectal carcinoma were 25 colorectal mucosal inflammations (65% and 85% ,P 〈 0 86% and 58.62% respectively,which were significantly lower than those in 01 and P 〈 0.05 ). The expressions of WWOX and Bax were correlated with the prognosis of patients (P 〈 0. 01 ,P 〈 0.05 ). The expression of WWOX was correlated with the infiltration of cancer tissues (P 〈 0.05). Difference was significant between colorectal carcinoma patients and colorectal mucosal inflammation patients in the positive rate of P73 (63.79% vs 30%, P 〈 0.01 ). The expression of P73 in colorectal carcinoma tissues was correlated with the metastasis and invasion of lymph nodes (P 〈 0.05 ). The expression of WWOX was not correlated with that of P73 ( x^2 = 0. 072, P 〉 0. 05 ) and was correlated with that of BAX (x^2 = 6.561, P 〈 0. 05 ). Conclusion s WWOX, P73 and Bax are correlated with the occurrence and development of colorectal carcinoma. The synergism of WWOX and Bax plays a key role in the prognosis of colorectal carcinoma.
作者 陈志英 何常 李佽 刘莉 刘都礼
机构地区 成都大学附属医院病理科 贵阳医学院病理学教研室
出处 《实用医院临床杂志》 2012年第1期57-59,共3页 Practical Journal of Clinical Medicine
关键词 WWOX P73 BAX 结直肠癌 免疫组化 基因 WWOX P73 Bax Colorectal carcinoma Immunohistochemistry Gene
分类号 R735.35 [医药卫生—肿瘤] R394.21 [医药卫生—医学遗传学]
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参考文献12

  • 1Bednarek AK, Laflin KJ, Daniel RL, et al. WWOX, a novel WW domain-contain protein mapping to human chromosome 16q23.3-24.1, a region frequently affected in breast cancer[J]. Cancer Res,2000, 60(8) :2140-2145.
  • 2周玉龙,徐永健,张珍祥.抑癌基因WWOX在肺腺癌细胞株A549中表达的研究[J].中国癌症杂志,2005,15(3):234-237. 被引量:10
  • 3Kuroki T, Yendamuri S, Trapasso F, et al. The Tumor Suppressor Gene WWOX at FRA16D Is Involved in Pancreatic Carcinogenesis [J]. Clin Cancer Res,2004,10(7) :2459-2465.
  • 4Iliopoulos D, Guler G, Han SY, et al. Fragile gene as biomarkers : epigenetic control of WWOX and FHIT in lung, breast and bladder cancer [ J ]. Oncogene, 2005,24 : 1625-1633.
  • 5Paige AJ,Taylor KJ,Taylor C,et al. WWOX:a candidate tumor suppressor gene involved in multiple tumor types [ J ]. Proc Natl Acad Sci USA ,2001,98 (20) : 11417-11422.
  • 6Kuroki T, Trapasso F, Shiraishi T, et al. Genetic alterations of the tumor suppressor geneWWOXin esophageal squamous cell carcinoma [J]. Cancer Res, 2002,62 ( 8 ) : 2258-2260.
  • 7Jost CA, Maric MC, Kaelin WG. p73 is a human p53 related protein that can induce apotosis[ J]. Nature ,1997,389 : 191-194.
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  • 9Sarbia M, Bittinger F, Grabellus F, et al. Expression of Bax, a pro-apoptotic member of the Bcl-2 family, in esophageal squamous cell carcinoma[ J]. Int J Cancer, 1997,73 (4) :508-513.
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二级参考文献10

  • 1李雯,徐永健,张珍祥.慢性阻塞性肺疾病患者气道上皮细胞阿米洛利敏感钠通道mRNA表达水平的研究[J].中华结核和呼吸杂志,2004,27(8):533-536. 被引量:6
  • 2Bednarek AK, Daniel RL, Laflin KJ, et al. WWOX, the FRA16D gene, behaves as a suppressor of tumor growth[J].Cancer Res,2001,61(22):8068-8073.
  • 3Stein CK, Glover TW, Palmer JL,,et al. Direct correlation between FRA3B expression and cigarette smoking[J].Genes,Chromosomes and Cancer,2002,34(3):333-340.
  • 4Dhillon VS, Hmsain SK, Ray GN, et al. Expression of aphidicolin-Induced fragile sites and their relationship between genetic susceptibility in breast cancer, ovarian cancer, and non-small cell lung cancer patients[J].Teratogenesis; Carcinogens and Mutagensis,2003,23(S1):35-45.
  • 5Kuroki T, Yendamuri S, Trapasso F, et al. The tumor suppressor gene WWOX at FRA16D is involved in pancratic carcimogenesis[J].Clinnical Cancer Research,2004,10(7):2459-2465.
  • 6Ludes-Meyers,JH, Bednarek AK, Popescu,NC, et al. WWOX, the common chromosomal fragile site, FRA16D, cancer gene[J].Cytogenetic and Genome Res,2003,100(4):101-110.
  • 7Bednarek AK, Laflin KJ, Daniel RL, et al. WWOX, a novel WW Domain-containing protein mapping to human chromosome 16q23.3-24.1, a region frequently affected in breast cancer[J].Cancer Res,2000,60(8):2140-2145.
  • 8Paris PL, Witte JS, Kupelian PA, et al. Identification and fine mapping of a region showing a high frequency of allelic imbalance on chromosome 16q23.2 that corresponds to a prostate cancer susceptibility focus[J].Cancer Res, 2000,60(13): 3645-3649.
  • 9Paige AJW, Taylor KJ, Taylor C, et al. WWOX: a candidate tumor suppressor gene involved in multiple tumor types[J].Genetics,2001,98(20):11417-11422.
  • 10Kuroki T, Trapasso F, Shiraishi T, et al. Genetic alterations of the tumor suppressor gene WWOX in esophageal squamous cell carcinoma[J].Cancer Research,2002,62(8):2258-2260.

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实用医院临床杂志
2012年 第1期

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