MDM2基因与前列腺癌相关性的初步研究
摘要
期为前列腺癌分子标志物的判定奠定基础。方法:使用SPSS23.0软件对数据进行分析,采用χ2
检验、t检验和非参
数检验等方法对患者相关因素进行组间比较。结果:1.MDM2的表达基于不同因素表达结果各有不同:在正常人与
高加索患者间的表达差异极显著,有统计学意义(P=0.00776<0.01);在正常人与TP53突变患者间的表达差异有
统计学意义(P=0.0351<0.05);在正常人与格里森得分6的患者及格里森得分6与9的患者间的表达均有统计学意
义(P=0.0152<0.05,P=0.0475<0.05),在格里森得分6与7的患者之间,差异极显著有统计学意义(P=0.00646
<0.01)。2.经Log-Rank检验比较,MDM2的表达水平基于格里森评分是患者预后的不良因素,P=0.00033<0.01,
差异极显著且有统计学意义。3.经Log-Rank检验,MDM2相关基因NOTCH、LEDM3、FRS2和NDUF87的表达水
平不是前列腺癌患者预后的不良因素。结论:前列腺癌的发病率和死亡率与人群所处地域和种族相关;临床诊断应
重视TP53突变及格里森得分指标,尽早检测。1
关键词
全文:
PDF参考
[1] Siegel RL, Miller KD,Jemal A. Cancer statistics,
2019[J]. CACancer J Clin, 2019, 69(1):7-34.
[2] Chen W, Zheng R, Baade PD, et al. Cancer statistics
in China, 2015[J]. CACancer J Clin, 2016, 66(2): 115-132.
[3] 刘定益,楚晨龙,周燕峰等 .215 例前列腺癌治疗
分析 [J]. 中国现代医学杂志,2017,27(8):128-132.
[4] Liu DY, Chu CL, Zhou YF, et al. Analysis of
215cases of prostate cancer treatment[J]. Chin J Modern Med,
2017,27(8):128-132.
[5] Jainagul I,Elnura T,Nazira A,et al. The
association of polymorphic markers Arg399Gln of XRCC1
gene,Arg72Pro of TP53 gene and T309G of MDM2 gene with
breast cancer in Kyrgyz females[J]. BMC Cancer, 2017, 17(1) :
758.
[6] Ding H, Dai Y, Ning ZY, et al. Murine double minute
2 SNP T309G polymorphism and urinary tract cancer[J].
Medcine, 2016, 95(12):2941.
[7] Tian XD, Wang B, Guo JT, et al. The MDM2 T309G
polymorphism and risk of lung cancer: An updated meta
analysis of 10, 186 cases and 14, 155 controls[J]. Panminerva
Medical, 2016, 58(4): 341-348.
[8] Chen JY, Yang H, Wen J, et al. Association
between positive murine double minute 2 expression and
clinicopathological characteristics of esophageal squamous cell
carcinoma: A Meta-analysis[J]. Diseases of the Esophagus,
2016, 29(7): 856-863.
[9] Xue ZW, Zhu XL, Teng YC. Relationship between
murine double minute 2(MDM2) T309G polymorphism and
endometrial cancer risk: A Meta- ananlysis[J]. Medical Sci
Monitor, 2016(22): 3186-3190.
[10] Wang C, Cai L, Liu J, et al. MicroRNA-30a-5p
inhibits the growth of renal cell carcinoma by modulating
GRP78 expression[J]. Cell Physiol Biochem, 2017, 43(6):
2405-2419.
[11] Xu S, Kong D, Chen Q, et al. Oncogenic long
noncoding RNA landscape in breast cancer[J]. Mol Cancer,
2017, 16(1):129.
[12] Giulietti M, Occhipinti G, Principato G, et al.
Weighted gene co-expression network analysis reveals
key genes involved in pancreatic ductal adenocarcinoma
development[J]. Cell Oncol, 2016, 39(4): 379-388.
[13] 顾方六 . 现代前列腺病学 [M]. 北京:人民军医出
版社,2002:276.
[14] 鲍镇美 . 晚期前列腺癌的治疗新动向 [J]. 中华泌
尿外科杂志,2002,23(2):69-71.
[15] 韩苏军,张思维,陈万青等 . 中国前列腺癌发病
现状和流行趋势分析 [J]. 临床肿瘤学杂志,2013,18(4):
330-334.
DOI: http://dx.doi.org/10.12361/2705-0459-04-07-93334
Refbacks
- 当前没有refback。
数据库合作单位
