Using Markers to Improve Pancreatic Cancer Screening

使用标记物改善胰腺癌筛查

• 批准号: 8862433
• 负责人: Michael G. Goggins
• 金额: $ 41.67万
• 依托单位: JOHNS HOPKINS UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2013
• 资助国家: 美国
• 起止时间: 2013-07-01 至 2016-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8862433
• 关键词: Age; Biological Assay; Cancer Etiology; Cancer Patient; Carcinoma in Situ; Cessation of life; Clinical; Clinical Trials; Cyst; Cyst Fluid; DNA Sequence Alteration; Data; Detection; Diagnosis; Diagnostic; Disease; Dysplasia; Endoscopy; Enrollment; Evaluation; Excision; Family; Future; Gene Mutation; Goals; Health; Image; In Situ Lesion; Individual; Irrigation; Juice; KRAS2 gene; Lesion; Lesion by Stage; Liquid substance; Malignant Neoplasms; Malignant neoplasm of pancreas; Measurement; Microscopic; Mucinous Neoplasm; Mutation; Neoplasms; Pancreas; Pancreatic Cyst; Pancreatic Diseases; Pancreatic Ductal Adenocarcinoma; Pancreatic Intraepithelial Neoplasia; Pancreatic duct; Papillary; Patients; Population; Premalignant; Prevalence; Recording of previous events; Research; Resected; Risk; Sampling; Specimen; TP53 gene; Testing; Time; Tumor Markers; Ultrasonography; advanced disease; aged; base; chronic pancreatitis; cohort; diagnostic accuracy; disorder control; high risk; improved; molecular marker; mortality; mutant; neoplastic; next generation sequencing; pancreatic juice; pancreatic neoplasm; prospective; screening

DESCRIPTION (provided by applicant): Pancreatic ductal adenocarcinoma is the 4th leading cause of cancer death in the USA and one of the deadliest cancers. Since most patients with pancreatic cancer present with advanced disease, in order to detect curable early-stage lesions, one needs to screen individuals. In our Cancer of the Pancreas Screening (CAPS) clinical trials we have screened ~500 individuals at increased risk of developing pancreatic cancer based on family history or gene mutation status. We find ~5-10% have lesions requiring resection (cancers, cysts-intraductal papillary mucinous neoplasms (IPMNs)), ~10-30% have cysts that require surveillance. The prevalence of lesions increases with age, especially over age 60. In our early CAPS trials, we initiated screening at age 40, later at age 50 and we now suspect screening may be more effective when initiated later (age 55). Although we can identify cysts, we cannot reliably identify very early invasive cancer or microscopic pancreatic intraepithelial neoplasias (PanINs) which are the commonest precursor to pancreatic cancer. Accurate markers are needed to identify these lesions, markers that can be reliably detected in pancreatic fluids and can be used for pancreatic screening. Recently, we found ~99% of low-grade PanINs harbor mutations, mutations that can be detected in pancreatic duct lavages ("pancreatic juice"). We found TP53 mutations in pancreatic juice collected non-invasively during endoscopic ultrasound are detected in patients with pancreatic cancer and patients undergoing pancreatic screening with carcinoma in situ or invasive cancer, not in disease controls or those with low-grade dysplasia. Thus, juice analysis has the potential to provide accurate evidence of cancer or high-grade PanIN. To further evaluate the utility of pancreatic juice analysis we propose: Aim #1: To determine the diagnostic accuracy of mutations detected in pancreatic fluid as indicators of pancreatic neoplasia. We will use nextgen sequencing to search for mutations in patients with pancreatic cancer, chronic pancreatitis, or normal pancreata. Aim #2: To determine the contribution of PanIN mutations to pancreatic fluid mutations among patients undergoing pancreatic resection. We will identify signature mutations of patient's PanIN and search for these mutations in their pre-op pancreatic fluid. Aim #3: To compare the prevalence of mutations in cyst fluid vs. pancreatic fluid among a prospective cohort of patients undergoing pancreatic cyst evaluation. Aim #4: To determine the prevalence of pancreatic lesions and pancreatic fluid mutations among high-risk individuals undergoing pancreatic screening. We will enroll a new older-age high-risk cohort (age >55) and continue surveillance of patients enrolled in prior CAPS trials.

描述（由申请人提供）：胰腺导管腺癌是美国第四大癌症死亡原因，也是最致命的癌症之一。由于大多数胰腺癌患者都处于晚期疾病，为了检测可治愈的早期病变，需要对个体进行筛查。在我们的胰腺癌筛查 (CAPS) 临床试验中，我们根据家族史或基因突变状态筛查了约 500 名罹患胰腺癌风险较高的个体。我们发现约 5-10% 的病变需要切除（癌症、囊肿 - 导管内乳头状粘液性肿瘤 (IPMN)），约 10-30% 的囊肿需要监测。病变的患病率随着年龄的增长而增加，尤其是 60 岁以上。在我们早期的 CAPS 试验中，我们在 40 岁时开始筛查，后来在 50 岁时开始筛查，现在我们怀疑，较晚（55 岁）开始筛查可能会更有效。尽管我们可以识别囊肿，但我们无法可靠地识别非常早期的浸润性癌症或显微镜下胰腺上皮内瘤变 (PanIN)，它们是胰腺癌最常见的前兆。需要准确的标记物来识别这些病变，这些标记物可以在胰腺液中可靠地检测到，并可用于胰腺筛查。最近，我们发现约 99% 的低级 PanIN 含有突变，这些突变可以在胰管灌洗液（“胰液”）中检测到。我们发现，在胰腺癌患者和接受胰腺原位癌或浸润性癌症筛查的患者中，在内窥镜超声过程中非侵入性收集的胰液中检测到了TP53突变，而在疾病对照或患有低度不典型增生的患者中则没有检测到。因此，果汁分析有可能提供癌症或高级 PanIN 的准确证据。为了进一步评估胰液分析的实用性，我们建议： 目标#1：确定胰液中检测到的突变作为胰腺肿瘤指标的诊断准确性。我们将使用下一代测序来寻找胰腺癌、慢性胰腺炎或正常胰腺患者的突变。目标#2：确定 PanIN 突变对接受胰腺切除术的患者胰液突变的影响。我们将识别患者 PanIN 的特征突变，并在其术前胰液中寻找这些突变。目标#3：比较接受胰腺囊肿评估的前瞻性患者队列中囊液与胰液中突变的发生率。目标#4：确定接受胰腺筛查的高危个体中胰腺病变和胰液突变的患病率。我们将招募一个新的老年高危队列（年龄 >55 岁），并继续监测参加先前 CAPS 试验的患者。