人胆汁中含有富含 microRNA 的细胞外囊泡,可用于胆管癌的诊断。

Human bile contains microRNA-laden extracellular vesicles that can be used for cholangiocarcinoma diagnosis.

机构信息

Division of Gastrenterology and Hepatology, Department of Medicine, Johns Hopkins Hospital, Baltimore, Maryland; USA.

出版信息

Hepatology. 2014 Sep;60(3):896-907. doi: 10.1002/hep.27050. Epub 2014 Jul 25.

Abstract

UNLABELLED

Cholangiocarcinoma (CCA) presents significant diagnostic challenges, resulting in late patient diagnosis and poor survival rates. Primary sclerosing cholangitis (PSC) patients pose a particularly difficult clinical dilemma because they harbor chronic biliary strictures that are difficult to distinguish from CCA. MicroRNAs (miRs) have recently emerged as a valuable class of diagnostic markers; however, thus far, neither extracellular vesicles (EVs) nor miRs within EVs have been investigated in human bile. We aimed to comprehensively characterize human biliary EVs, including their miR content. We have established the presence of extracellular vesicles in human bile. In addition, we have demonstrated that human biliary EVs contain abundant miR species, which are stable and therefore amenable to the development of disease marker panels. Furthermore, we have characterized the protein content, size, numbers, and size distribution of human biliary EVs. Utilizing multivariate organization of combinatorial alterations (MOCA), we defined a novel biliary vesicle miR-based panel for CCA diagnosis that demonstrated a sensitivity of 67% and specificity of 96%. Importantly, our control group contained 13 PSC patients, 16 with biliary obstruction of varying etiologies (including benign biliary stricture, papillary stenosis, choledocholithiasis, extrinsic compression from pancreatic cysts, and cholangitis), and 3 with bile leak syndromes. Clinically, these types of patients present with a biliary obstructive clinical picture that could be confused with CCA.

CONCLUSION

These findings establish the importance of using extracellular vesicles, rather than whole bile, for developing miR-based disease markers in bile. Finally, we report on the development of a novel bile-based CCA diagnostic panel that is stable, reproducible, and has potential clinical utility.

摘要

未注明

胆管癌 (CCA) 存在重大诊断挑战,导致患者诊断较晚,生存率低。原发性硬化性胆管炎 (PSC) 患者构成了特别困难的临床难题,因为他们存在慢性胆道狭窄,难以与 CCA 区分。MicroRNAs (miRs) 最近成为一种有价值的诊断标志物类别;然而,到目前为止,尚未在人类胆汁中研究过细胞外囊泡 (EVs) 或 EV 中的 miR。我们旨在全面描述人类胆汁外泌体,包括其 miR 含量。我们已经证实了人类胆汁中外泌体的存在。此外,我们已经证明人类胆汁外泌体含有丰富的 miR 种类,这些 miR 种类稳定,因此适合开发疾病标志物组合。此外,我们还对人类胆汁外泌体的蛋白含量、大小、数量和大小分布进行了描述。利用组合改变的多元组织 (MOCA),我们定义了一个新的基于胆管囊泡 miR 的 CCA 诊断面板,该面板的敏感性为 67%,特异性为 96%。重要的是,我们的对照组包含 13 名 PSC 患者、16 名具有不同病因的胆道梗阻患者(包括良性胆道狭窄、乳头狭窄、胆总管结石、胰腺囊肿的外在压迫和胆管炎)和 3 名胆汁漏综合征患者。临床上,这些类型的患者表现出胆道阻塞的临床表现,可能与 CCA 混淆。

结论

这些发现确立了使用细胞外囊泡而不是整个胆汁来开发胆汁中基于 miR 的疾病标志物的重要性。最后,我们报告了一种新型基于胆汁的 CCA 诊断面板的开发,该面板稳定、可重复,具有潜在的临床应用价值。

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