Addressing the unmet clinical need for low-volume assays in early diagnosis of pancreatic cancer

Daniel A. Sheik, Kaleb Byers, Mini Thomas, Ummadisetti Chinna Rajesh, Kelli Ifuku, Kimberly Kirkwood, Mohammed Al-Haddad, Charles S. Craik, V. Jo Davisson
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Abstract

The incidental detection of pancreatic cysts, an opportunity for the early detection of pancreatic cancer, is increasing, owing to an aging population and improvements in imaging technology. The classification of pancreatic cystic precursors currently relies on imaging and cyst fluid evaluations, including cytology and protein and genomic analyses. However, there are persistent limitations that obstruct the accuracy and quality of information for clinicians, including the limited volume of the complex, often acellular, and proteinaceous milieu that comprises pancreatic cyst fluid. The constraints of currently available clinical assays lead clinicians to the subjective and inconsistent application of diagnostic tools, which can contribute to unnecessary surgery and missed pancreatic cancers. Herein, we describe the pathway toward pancreatic cyst classification and diagnosis, the volume requirements for several clinically available diagnostic tools, and some analytical and diagnostic limitations for each assay. We then discuss current and future work on novel markers and methods, and how to expand the utility of clinical pancreatic cyst fluid samples. Results of ongoing studies applying SERS as a detection mode suggest that 50 µL of pancreatic cyst fluid is more than sufficient to accurately rule out non-mucinous pancreatic cysts with no malignant potential from further evaluation. This process is expected to leave sufficient fluid to analyze a follow-up, rule-in panel of markers currently in development that can stratify grades of dysplasia in mucinous pancreatic cysts and improve clinical decision-making.
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解决胰腺癌早期诊断中未满足的低容量检测的临床需求
由于人口老龄化和成像技术的进步,胰腺囊肿的偶然发现是早期发现胰腺癌的一个机会,正在增加。胰腺囊性前体的分类目前依赖于影像学和囊肿液评估,包括细胞学、蛋白质和基因组分析。然而,持续存在的限制阻碍了临床医生信息的准确性和质量,包括由胰腺囊肿液组成的复杂的、通常是脱细胞的和蛋白质的环境的有限体积。目前可用的临床分析的限制导致临床医生主观和不一致的诊断工具的应用,这可能导致不必要的手术和漏诊胰腺癌。在此,我们描述了胰腺囊肿分类和诊断的途径,几种临床可用诊断工具的体积要求,以及每种检测的一些分析和诊断局限性。然后,我们讨论了当前和未来在新的标记物和方法方面的工作,以及如何扩大临床胰腺囊肿液样本的效用。正在进行的以SERS为检测模式的研究结果表明,50µL的胰腺囊肿液足以准确地排除无恶性潜能的非粘液性胰腺囊肿。这一过程有望留下足够的液体来分析一个随访的、规则的、目前正在开发的标志物小组,该小组可以对粘液性胰腺囊肿的发育不良等级进行分层,并改善临床决策。
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