|本期目录/Table of Contents|

[1]冒晓蓓,刘小北,褚晓源,等.叉头框蛋白M1、环氧合酶2在结肠癌组织中的表达及相关性分析[J].医学研究与战创伤救治(原医学研究生学报),2014,16(03):225-228.[doi:10.3969/j.issn.1672-271X.2014.03.001]
 MAO Xiao-bei,LIU Xiao-bei,CHU Xiao-yuan,et al.Expression and correlation of FoxM1 and COX-2 in colorectal cancer[J].JOURNAL OF MEDICALRESEARCH —COMBAT TRAUMA CARE,2014,16(03):225-228.[doi:10.3969/j.issn.1672-271X.2014.03.001]
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叉头框蛋白M1、环氧合酶2在结肠癌组织中的表达及相关性分析()
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《医学研究与战创伤救治》(原医学研究生学报)[ISSN:1672-271X/CN:32-1713/R]

卷:
第16卷
期数:
2014年03期
页码:
225-228
栏目:
出版日期:
2014-05-20

文章信息/Info

Title:
Expression and correlation of FoxM1 and COX-2 in colorectal cancer
作者:
冒晓蓓刘小北褚晓源郁红菊
210002 江苏南京,第二军医大学南京临床医学院(南京军区南京总医院)肿瘤内科
Author(s):
MAO Xiao-beiLIU Xiao-beiCHU Xiao-yuanYU Hong-ju.
Department of Internal Medicine-Oncology,Nanjing Clinical Medical College of Second Military Medical University,Nanjing General Hospital of Nanjing Military Region,Nanjing,Jiangsu 210002,China
关键词:
结肠癌叉头框蛋白M1环氧合酶2免疫组织化学
Keywords:
colorectal cancer FoxM1 COX-2 immunohistochemistry
分类号:
R735.35
DOI:
10.3969/j.issn.1672-271X.2014.03.001
文献标志码:
A
摘要:
目的 探讨叉头框蛋白M1(fork head box M1,FoxM1)和环氧合酶2(cyclooxygenase2,COX-2)在结肠癌(colorectal carcinoma,CRC)中的表达及两者的相关性。方法 采用免 疫组织化学法检测FoxM1和COX-2在95例CRC组织和40例正常结肠组织中的表达,分析FoxM1和COX-2与结肠癌临床病理参数间的关系及两者表达的相关性。结果 FoxM1和COX-2在CRC组 织中表达阳性率分别为 85.3%(81/95)和 87.4%(83/95),显著高于正常结肠组织的 7.5%(3/40)和 12.5%(5/40)(P<0.05)。FoxM1和COX-2的高表达与较多的淋巴结转移及较晚的临 床分期密切相关(P<0.05),且两者在CRC中的表达强度呈正相关(r=0.638,P<0.05)。结论 FoxM1和COX-2的表达与CRC临床分期和淋巴结转移密切相关,提示其可能与CRC患者较差 的预后相关。
Abstract:
Objective To investigate the expression of fork head box M1(FoxM1) and cyclooxygenase-2 (COX-2) in colorectal cancer (CRC) and analyze the correlation between them.Methods Expressions of FoxM1and COX-2 were examined in 95 CRC tissues and 40 normal colon tissues by immunohistochemistry.Then the relationships among expression of FoxM1and COX-2 and clinicopathological parameters of CRC analyzed.Results Both the positivity rates of FoxM1 and COX-2 in CRC tissues were significantly higher than in normal colon tissues [FoxM1:85.3%(81/95 )vs 7.5%(3/40);COX-2:87.4%(83/95) vs 12.5%(5/40);P<0.05].Enhanced expressions of FoxM1 and COX-2 were still significantly correlated with the lymph node metastasis and advanced clinical stages in CRC (P<0.05).Meanwhile,a positive correlation was observed between FoxM1 and COX-2 experssions (r=0.638,P<0.05).Conclusion Over-expressions of FoxM1 and COX-2 are significantly correlated with the lymph node metastasis and advanced clinical stage of CRC in the development and advancement of CRC.

参考文献/References:

[1]Siegel R,Naishadham D,Jemal A.Cancer statistics,2012[J].CA Cancer J Clin,2012,62(1):10-29.
[2]Chen HM,Weng YR,Jiang B,et al.Epidemiological study of colorectal adenoma and cancer in symptomatic patients in China between 1990 and 2009[J].J Diges Dis,2011,12(5):371-378.
[3]Wonsey DR,Follettie MT.Loss of the forkhead transcription factor FoxM1 causes centrosome amplification and mitotic catastrophe[J].Cancer Res,2005,65 (12):5181-5189.
[4]Khan Z,Khan N,Tiwari RP,et al.Biology of Cox-2:an application in cancer therapeutics[J].Curr Drug Targets,2011,12(7):1082-1093.
[5]Chu XY,Zhu ZM,Chen LB,et al.FOXM1expression correlates with tumor invasion and a poor prognosis ofcolorectal cancer[J].Acta Histochem,2012,114(8):755-762.
[6]Pirkebner D,Fuetsch M,Wittmann W,et al.Reduction of intracellular pH inhibits constitutive expression of cyclooxygenase-2 in human colon cancer cells[J].J Cell Physiol,2004,198(2):295-301.
[7]Laoukili J,Kooistra MR,Bras A,et al.FoxM1 is required for execution of the mitotic programme and chromosome stability[J].Nat Cell Biol,2005,7(2):126-36.
[8]Laoukili J,Stahl M,Medema RH.FoxM1:at the crossroads of ageing and cancer[J].Biochim Biophys Acta,2007,1775(1):92–102.
[9]Koo CY,Muir KW,Lam EW.FOXM1:from cancer initiation to progression and treatment[J].Biochim Biophys Acta,2012,1819(1):28-37.
[10]Uddin S,Hussain AR,Ahmed M,et al.Overexpression of FoxM1 offers a promising therapeutic target in diffuse large B-cell lymphoma[J].Haematologica,2012,97 (7):1092-1100.
[11]Cao Y1,Prescott SM.Many actions of cyclooxygenase-2 in cellular dynamics and in cancer[J].J Cell Physiol,2002,190(3):279-286.
[12]Khan Z,Khan N,Tiwari RP,et al.Biology of Cox-2:an application in cancer therapeutics[J].Curr Drug Targets,2011,12(7):1082-1093.
[13]Lin PC,Lin YJ,Lee CT,et al.Cyclooxygenase-2 expression in the tumor environment is associated with poor prognosis in colorectal cancer patients[J].Oncol Lett,2013,6(3):733-739.
[14]Balli D,Ren X,Chou FS,et al.Foxm1 transcription factor is required for macrophage migration during lung inflammation and tumor formation [J].Oncogene,2012,31(34):3875-3888.
[15]Wang IC,Meliton L,Tretiakova M,et al.Transgenic expression of the forkhead box M1 transcription factor induces formation of lung tumors [J].Oncogene,2008,27(30):4137-4149.
[16]Xu K,Shu HK.Transcription factor interactions mediate EGF-dependent COX-2 expression[J].Mol Cancer Res,2013,11(8):875-886.

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备注/Memo

备注/Memo:
国家自然科学基金(81272394)
更新日期/Last Update: 2014-05-20