首页> 外文期刊>Genes, Chromosomes and Cancer >Next generation sequencing of the cellular and liquid fraction of pancreatic cyst fluid supports discrimination of IPMN from pseudocysts and reveals cases with multiple mutated driver clones: First findings from the prospective ZYSTEUS biomarker study
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Next generation sequencing of the cellular and liquid fraction of pancreatic cyst fluid supports discrimination of IPMN from pseudocysts and reveals cases with multiple mutated driver clones: First findings from the prospective ZYSTEUS biomarker study

机译:胰腺囊肿流体的细胞和液体分数的下一代测序支持来自假囊肿的IPMN的判断,并揭示了多个突变的驾驶员克隆的病例:从前瞻性Zysteus生物标志物研究中的第一次发现

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摘要

Approximately half of all pancreatic cysts are neoplastic, mainly comprising intraductal papillary mucinous neoplasms (IPMN), which can progress to invasive carcinoma. Current Fukuoka guidelines have limited sensitivity and specificity in predicting progression of asymptomatic pancreatic cysts. We present first results of the prospective ZYSTEUS biomarker study investigating (i) whether detection of driver mutations in IPMN by liquid biopsy is technically feasible, (ii) which compartment of IPMN is most suitable for analysis, and (iii) implications for clinical diagnostics. Twenty-two patients with clinical inclusion criteria were enrolled in ZYSTEUS. Fifteen cases underwent endoscopic ultrasound (EUS)-guided fine-needle aspiration and cytological diagnostics. Cellular and liquid fraction of the cysts of each case were separated and subjected to deep targeted next generation sequencing (NGS). Clinical parameters, imaging findings (EUS and MRI), and follow-up data were collected continuously. All IPMN cases (n = 12) showed at least one mutation in either KRAS (n = 11) or GNAS (n = 4). Three cases showed both KRAS and GNAS mutations. Six cases harbored multiple KRAS/GNAS mutations. In the three cases with pseudocysts, no KRAS or GNAS mutations were detected. DNA yields were higher and showed higher mutation diversity in the cellular fraction. In conclusion, mutation detection in pancreatic cyst fluid is technically feasible with more robust results in the cellular than in the liquid fraction. Current results suggest that, together with imaging, targeted sequencing supports discrimination of IPMN from pseudocysts. The prospective design of ZYSTEUS will provide insight into diagnostic value of NGS in preoperative risk stratification. Our data provide evidence for an oligoclonal nature of IPMN.
机译:大约一半的胰腺囊肿是肿瘤族,主要包括内科乳头状乳糖瘤(IPMN),其可以进入侵入性癌。目前的福冈指南在预测无症状胰腺囊肿的进展方面具有有限的敏感性和特异性。我们展示了前瞻性Zysteus生物标志物研究的第一个结果研究(i)液体活检的IPMN中的驾驶员突变是否在技术上是可行的,(ii)该IPMN的哪​​个隔间最适合分析,(III)对临床诊断的影响。二十两名临床含有标准的患者注册了Zysteus。十五件病例接受内窥镜超声(EUS) - 导胶精细针吸气和细胞学诊断。分离各种情况下囊肿的细胞和液体分数,并进行深针对靶向的下一代测序(NGS)。临床参数,成像结果(EUS和MRI)以及连续收集的后续数据。所有IPMN病例(n = 12)显示KRAS(n = 11)或GNA(n = 4)中的至少一个突变。三种病例显示KRAS和GNAS突变。患有多个KRAS / GNAS突变的六种病例。在三种患者中,未检测到kras或gnas突变。 DNA产率较高,并且在细胞级分中显示出更高的突变多样性。总之,胰囊肿流体中的突变检测在技术上是可行的,在细胞中比液体分数更稳定的结果。目前的结果表明,与成像一起,目标测序支持来自伪细胞的IPMN的判断。 Zysteus的前瞻性设计将在术前风险分层中提供NGS诊断价值的洞察力。我们的数据为IPMN的寡头龙神经性质提供了证据。

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