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首页> 外文期刊>American Journal of Cancer Research >Pancreatic cancer screening in different risk individuals with family history of pancreatic cancer-a prospective cohort study in Taiwan
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Pancreatic cancer screening in different risk individuals with family history of pancreatic cancer-a prospective cohort study in Taiwan

机译:在具有胰腺癌家族史的不同风险人群中进行胰腺癌筛查的一项前瞻性队列研究

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摘要

Pancreatic cancer (PC) is usually diagnosed at advanced stage. Our aim was to investigate the risk of malignant and premalignant pancreatic lesions in individuals with family history of PC. Individuals at risk of PC were enrolled prospectively in a screening program in Taiwan. All risk individuals received genetic testing of cationic trypsinogen (PRSS1) gene and the serine protease inhibitor Kazal type 1 (SPINK1) gene. They were stratified into three risk groups (high, moderate, and low) based on the family history and genetic testing. Magnetic resonance imaging (MRI) with magnetic resonance cholangiopancreatogram (MRCP) were performed in all screened individuals. A total of three hundred and three risk individuals in 165 families were enrolled with the mean age of 51.1 years, 38.3% of whom were male. A total of 24 of 303 (7.9%) screened individuals had the PRSS1 mutation, and 7/234 (0.3%) had the SPINK1 mutation. Nineteen (6.3%) risk individuals had pancreatic pathology including seven with pancreatic cancer, and four with pancreatic mucinous neoplasms. The earliest age of onset of PC in affected members was an independent factor associated with risk of developing PC in all risk groups. DM was associated with much-increased risk of developing PC in low and moderate risk groups (OR45.8. 95% CI. 13.82-151.64, P=0.001). Combined family history of non-PC malignancy in the family in the low-risk individual was associated with abnormal findings on MRI (OR8.4, 95% CI 3.29-21.88, P < 0.0001). There was no any complication of screening. In summary, pancreatic cancer screening may benefit in risk individuals with family history of pancreatic cancer in our population. The diagnostic yield is similar to prior studies. MRCP as initial screening modality is safe and effective. Future study will be needed to tailor PC screening strategy in different risk populations.
机译:胰腺癌(PC)通常被诊断为晚期。我们的目的是调查有PC家族史的个体发生恶性和恶性胰腺损害的风险。前瞻性地将有PC风险的个人纳入台湾的筛查计划。所有危险个体均接受了阳离子胰蛋白酶原(PRSS1)基因和丝氨酸蛋白酶抑制剂Kazal 1型(SPINK1)基因的基因测试。根据家族病史和基因检测,他们分为三个风险组(高,中和低)。在所有筛查的个体中进行磁共振成像(MRI)和磁共振胰胆管造影(MRCP)。纳入165个家庭的303个风险个体,平均年龄为51.1岁,其中38.3%是男性。 303个筛查个体中有24个(7.9%)具有PRSS1突变,而7/234(0.3%)具有SPINK1突变。 19名(6.3%)高危人群患有胰腺病理,包括7名胰腺癌和4名胰腺黏液性肿瘤。在所有风险组中,受影响成员中PC发病的最早年龄是与PC发生风险相关的独立因素。 DM与中低风险组患PC的风险大大增加有关(OR45.8。95%CI。13.82-151.64,P = 0.001)。低危个体家庭中非PC恶性肿瘤的合并家族史与MRI异常相关(OR8.4,95%CI 3.29-21.88,P <0.0001)。筛查没有任何并发​​症。总之,在我们的人群中,胰腺癌筛查可能对具有胰腺癌家族史的高危人群有益。诊断结果与先前的研究相似。 MRCP作为初始筛查方式是安全有效的。未来的研究将需要针对不同风险人群量身定制PC筛查策略。

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