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循环、肝细胞特异性信使 RNA 和 microRNA 作为慢性乙型和丙型肝炎生物标志物的比较。

Comparison of circulating, hepatocyte specific messenger RNA and microRNA as biomarkers for chronic hepatitis B and C.

机构信息

Shanghai Public Health Clinical Center, Key Laboratory of Medical Molecular Virology at Shanghai Medical College, Fudan University, Shanghai, China.

Department of Viral Hepatitis, Shanghai Public Health Clinical Center, Fudan University, Shanghai, China.

出版信息

PLoS One. 2014 Mar 18;9(3):e92112. doi: 10.1371/journal.pone.0092112. eCollection 2014.

Abstract

Circulating microRNAs have been widely recognized as a novel category of biomarker in a variety of physiological and pathological conditions. Other reports revealed that fragments of organ specific messenger RNAs are also detectable in serum/plasma and can be utilized as sensitive indicators of liver pathology and cancer. In order to assess the sensitivity and reliability of these two class of RNAs as marker of hepatitis B or C induced chronic liver disease, we collected plasma samples from 156 chronic hepatitis B or C patients (HBV active n = 112, HBV carrier n = 19, hepatitis C n = 25) and 22 healthy donors and quantified their circulating mRNA for albumin, HP (haptoglobin), CYP2E1 (cytochrome P450, family 2, subfamily E) and ApoA2 (Apolipoprotein A2) in conjunction with microRNA-122, a well established marker for acute and chronic liver injury. We found that plasma microRNA-122 level is significantly elevated in patients with active HBV but not in HBV carriers. Furthermore, microRNA-122 is not elevated in HCV patients even though their median serum alanine aminotransferase (sALT) was three fold of the healthy donors. Nevertheless, circulating mRNAs, especially albumin mRNA, showed much more sensitivity in distinguishing active hepatitis B, hepatitis B carrier or HCV patients from healthy control. Correlation and multiple linear regression analysis suggested that circulating mRNAs and miRNAs are much more related to HBsAg titre than to sALT. Immunoprecipitation of HBsAg in HBV patients' plasma resulted in enrichment of albumin and HP mRNA suggesting that fragments of liver specific transcripts can be encapsidated into HBsAg particles. Taken together, our results suggest that hepatocyte specific transcripts in plasma like albumin mRNA showed greater sensitivity and specificity in differentiating HBV or HCV induced chronic liver disease than microRNA-122. Circulating mRNA fragments merit more attention in the quest of next generation biomarkers for various maladies.

摘要

循环 microRNAs 已被广泛认为是多种生理和病理条件下的新型生物标志物。其他报告显示,器官特异性信使 RNA 的片段也可在血清/血浆中检测到,并可作为肝病理和癌症的敏感指标。为了评估这两类 RNA 作为乙型肝炎或丙型肝炎引起的慢性肝病标志物的敏感性和可靠性,我们收集了 156 例慢性乙型肝炎或丙型肝炎患者(乙型肝炎活跃 n = 112,乙型肝炎携带者 n = 19,丙型肝炎 n = 25)和 22 名健康供体的血浆样本,并定量检测了它们的循环 mRNA 白蛋白、HP(触珠蛋白)、CYP2E1(细胞色素 P450,家族 2,亚家族 E)和 ApoA2(载脂蛋白 A2),以及 microRNA-122,这是一种急性和慢性肝损伤的成熟标志物。我们发现,乙型肝炎活跃患者的血浆 microRNA-122 水平显著升高,但乙型肝炎携带者的水平没有升高。此外,丙型肝炎患者的 microRNA-122 水平即使比健康供体高 3 倍也没有升高。然而,循环 mRNAs,特别是白蛋白 mRNA,在区分乙型肝炎活跃、乙型肝炎携带者或丙型肝炎患者与健康对照方面具有更高的敏感性。相关性和多元线性回归分析表明,循环 mRNAs 和 miRNAs 与 HBsAg 滴度的相关性远大于与 sALT 的相关性。HBV 患者血浆中 HBsAg 的免疫沉淀导致白蛋白和 HP mRNA 的富集,表明肝特异性转录物的片段可以被包裹到 HBsAg 颗粒中。综上所述,我们的结果表明,血浆中的肝细胞特异性转录物,如白蛋白 mRNA,在区分乙型肝炎或丙型肝炎引起的慢性肝病方面比 microRNA-122 具有更高的敏感性和特异性。循环 mRNA 片段在寻找各种疾病的下一代生物标志物方面值得更多关注。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f74/3958472/bf8aeb8b8a55/pone.0092112.g001.jpg

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