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纯胰液中分泌型凋亡相关蛋白2(SARP2)的异常甲基化在胰腺肿瘤诊断中的作用

Aberrant methylation of secreted apoptosis-related protein 2 (SARP2) in pure pancreatic juice in diagnosis of pancreatic neoplasms.

作者信息

Watanabe Hiroyuki, Okada Gensaku, Ohtsubo Koushiro, Yao Fan, Jiang Pei-Hong, Mouri Hisatsugu, Wakabayashi Tokio, Sawabu Norio

机构信息

Department of Internal Medicine and Medical Oncology, Cancer Research Institute, Kanazawa University, Kanazawa, Japan.

出版信息

Pancreas. 2006 May;32(4):382-9. doi: 10.1097/01.mpa.0000221617.89376.38.

Abstract

OBJECTIVE

Secreted apoptosis-related protein (SARP) families are considered to counteract the oncogenic Wnt signaling pathway, and inactivation of this gene may aid cancer development and progression. Recently, the aberrant methylation of SARP2 was detected frequently in pancreatic carcinoma (PCa) tissue, but not in normal pancreatic tissue. We evaluated the hypermethylation of SARP2 in pure pancreatic juices (PPJ) aspirated endoscopically from patients with PCa, intraductal papillary mucinous neoplasm of the pancreas (IPMN), chronic pancreatitis (CP), and a control group who were consequently free of pancreatic diseases according to the differential diagnosis of PCa.

METHODS

We investigated the aberrant methylation of SARP2 in 9 human PCa cell lines and in the PPJ samples from 33 patients with PCa, 20 with IPMN, 19 with CP, and 10 control patients. DNAs extracted from not only sediment, but also the supernatant of the PPJ and PCa cell lines were treated with sodium bisulfite and analyzed by methylation-specific polymerase chain reaction (PCR) (MSP). Moreover, real-time MSP was also performed for the melting curve analysis and the quantitative analysis of SARP2 in the PPJ.

RESULTS

The incidence of the aberrant methylation of SARP2 using MSP was 8/9 (89%) in PCa cell lines, 26/33 (79%) in the PPJ with PCa, and 17/20 (85%) with IPMN. However, it was only 1/19 (5%) in the PPJ with CP, and 0/10 (0%) in the PPJ of the control patients, respectively. The incidences of aberrant methylation of SARP2 in the PPJ with PCa and IPMN were significantly higher than that in the PPJ with CP (P < 0.001, P < 0.001). Melting curve analysis by real-time MSP revealed that the incidences of aberrant methylation of SARP2 in PPJ was 28/33 (85%) with PCa, 9/11 (82%) with the malignant group of IPMN, 5/9 (56%) with the benign group of IPMN and 5/19 (26%) with CP. In this analysis, there were significant differences between PCa and CP (P < 0.001), and between the malignant group of IPMN and CP (P < 0.005). In the quantitative analysis by real-time MSP with a suitable cut-off value, the incidences of aberrant methylation of SARP2 in the PPJ with PCa, the malignant group of IPMN, the benign group of IPMN, and CP were 19/33 (58%), 6/11 (55%), 3/9 (33%), and 2/19 (11%), respectively. The incidence of the aberrant methylation of SARP2 in the PPJ was significantly different between PCa and CP and between the malignant group of IPMN and CP (P < 0.005 and P < 0.05, respectively).

CONCLUSIONS

Hypermethylation of SARP2 in the PPJ may be a highly sensitive and useful marker for the detection of pancreatic neoplasms, including PCa and the malignant group of IPMN.

摘要

目的

分泌型凋亡相关蛋白(SARP)家族被认为可对抗致癌性Wnt信号通路,该基因的失活可能有助于癌症的发生和发展。最近,在胰腺癌(PCa)组织中经常检测到SARP2的异常甲基化,但在正常胰腺组织中未检测到。我们评估了通过内镜从PCa、胰腺导管内乳头状黏液性肿瘤(IPMN)、慢性胰腺炎(CP)患者以及根据PCa鉴别诊断结果无胰腺疾病的对照组患者中获取的纯胰液(PPJ)中SARP2的高甲基化情况。

方法

我们研究了9种人PCa细胞系以及33例PCa患者、20例IPMN患者、19例CP患者和10例对照患者的PPJ样本中SARP2的异常甲基化情况。从PPJ和PCa细胞系的沉淀物以及上清液中提取的DNA用亚硫酸氢钠处理,并通过甲基化特异性聚合酶链反应(PCR)(MSP)进行分析。此外,还对PPJ中的SARP2进行了实时MSP的熔解曲线分析和定量分析。

结果

使用MSP检测到SARP2异常甲基化的发生率在PCa细胞系中为8/9(89%),在PCa患者的PPJ中为26/33(79%),在IPMN患者中为17/20(85%)。然而,在CP患者的PPJ中仅为1/19(5%),在对照患者的PPJ中为0/10(0%)。PCa和IPMN患者的PPJ中SARP2异常甲基化的发生率显著高于CP患者的PPJ(P < 0.001,P < 0.001)。实时MSP的熔解曲线分析显示,PCa患者的PPJ中SARP2异常甲基化的发生率为28/33(85%),IPMN恶性组为9/11(82%),IPMN良性组为5/9(56%),CP患者为5/19(26%)。在该分析中,PCa与CP之间(P < 0.001)以及IPMN恶性组与CP之间(P < 0.005)存在显著差异。在使用合适临界值的实时MSP定量分析中,PCa患者的PPJ、IPMN恶性组、IPMN良性组和CP患者中SARP2异常甲基化的发生率分别为19/33(58%)、6/11(55%)、3/9(33%)和2/19(11%)。PPJ中SARP2异常甲基化的发生率在PCa与CP之间以及IPMN恶性组与CP之间存在显著差异(分别为P < 0.005和P < 0.05)。

结论

PPJ中SARP2的高甲基化可能是检测包括PCa和IPMN恶性组在内的胰腺肿瘤的一种高度敏感且有用的标志物。

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