卵巢癌患者中3020insC NOD2基因突变
The 3020insC NOD2 gene mutation in patients with ovarian cancer.
作者信息
Magnowski Piotr, Medrek Krzysztof, Magnowska Magdalena, Stawicka Małgorzata, Kedzia Helena, Górski Bohdan, Lubiński Jan, Spaczyński Marek
机构信息
Department of Gynecology, Obstetrics and Gynecological Oncology, Division of Gynecologic Oncology, Poznań University of Medical Sciences, Poland.
出版信息
Ginekol Pol. 2008 Aug;79(8):544-9.
OBJECTIVE
There is an increasing evidence that genetic factors play a role in the etiology of malignant tumors. Mutations of BRCA1 and BRCA2 genes are responsible for an increased risk of ovarian cancer. The role of mutations in NOD2 gene in this type of neoplasm is still under investigation.
THE AIM
The aim of this study was to determine: 1. incidence of NOD 2 3020insC constitutional mutation in a group of consecutive women with ovarian cancer, 2. risk of developing ovarian cancer in patients with NOD2 gene mutation, 3. clinical and pathological features of ovarian cancer in NOD2 gene mutation carriers.
PATIENTS AND METHODS
Clinical and pathological data were collected from 257 non-selected patients with primary epithelial ovarian cancer. The researches identified NOD2 3020insC gene mutation. On the basis of patient source documentation we obtained the data concerning the age of patients at diagnosis, histopathological recognition, FIGO stage and morphological grade G.
RESULTS
19 out of 257 women were identified with germ-line 3020insC mutation of NOD2 gene (7.39%). An increased risk of ovarian cancer in NOD2 mutation carriers was not revealed (OR=1.01; p=0.928; 95% Cl=0.61-1.66). The mean age at diagnosis of patients with NOD2 mutation was 54.8 (SD=9.9), while for non-carriers it was 53.2 (SD=10.2). The difference between these frequencies was statistically irrelevant (p=0.550). Clinical and pathological profile of ovarian cancer was made. We assessed the following features: age at disease onset, histopathology, FIGO stage and morphological grade G. For NOD2 mutation carriers no statistically significant features of ovarian cancer were revealed.
CONCLUSION
- Despite high frequency of constitutional mutations occurrence in NOD2 gene in women with ovarian cancer, genetic testing seem not to be justified in all women diagnosed with this disease. 2. Due to a lack of increased risk of ovarian cancer in NOD2 gene mutation carriers, proceedings for them may not differ from recommendations for general population. 3. It is difficult to determine characteristic clinical and pathological features of ovarian cancer for NOD2 gene mutation carriers.
目的
越来越多的证据表明遗传因素在恶性肿瘤的病因中起作用。BRCA1和BRCA2基因的突变会增加患卵巢癌的风险。NOD2基因突变在这类肿瘤中的作用仍在研究中。
目的
本研究的目的是确定:1. 一组连续的卵巢癌女性中NOD 2 3020insC胚系突变的发生率;2. NOD2基因突变患者患卵巢癌的风险;3. NOD2基因突变携带者卵巢癌的临床和病理特征。
患者与方法
收集了257例未经选择的原发性上皮性卵巢癌患者的临床和病理数据。研究确定了NOD2 3020insC基因突变。根据患者来源文件,我们获得了有关患者诊断时的年龄、组织病理学诊断、国际妇产科联盟(FIGO)分期和形态学分级G的数据。
结果
257名女性中有19名被确定为NOD2基因的胚系3020insC突变(7.39%)。未发现NOD2突变携带者患卵巢癌的风险增加(比值比=1.01;p=0.928;95%可信区间=0.61-1.66)。NOD2突变患者的平均诊断年龄为54.8岁(标准差=9.9),而非携带者为53.2岁(标准差=10.2)。这些频率之间的差异无统计学意义(p=0.550)。对卵巢癌的临床和病理特征进行了分析。我们评估了以下特征:发病年龄、组织病理学、FIGO分期和形态学分级G。对于NOD2突变携带者,未发现卵巢癌有统计学意义的特征。
结论
- 尽管卵巢癌女性中NOD2基因胚系突变的发生率较高,但对所有诊断为该病的女性进行基因检测似乎并不合理。2. 由于NOD2基因突变携带者患卵巢癌的风险没有增加,对他们的治疗程序可能与对普通人群的建议没有差异。3. 很难确定NOD2基因突变携带者卵巢癌的特征性临床和病理特征。
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