Serum microRNA signatures as "liquid biopsies" for interrogating hepatotoxic mechanisms and liver pathogenesis in human

Julian Krauskopf; Theo M. de Kok; Shelli J. Schomaker; Mark Gosink; Deborah A. Burt; Patricia Chandler; Roscoe L. Warner; Kent J. Johnson; Florian Caiment; Jos C. Kleinjans; Jiri Aubrecht

doi:10.1371/journal.pone.0177928

Serum microRNA signatures as "liquid biopsies" for interrogating hepatotoxic mechanisms and liver pathogenesis in human

Julian Krauskopf^*, Theo M. de Kok, Shelli J. Schomaker, Mark Gosink, Deborah A. Burt, Patricia Chandler, Roscoe L. Warner, Kent J. Johnson, Florian Caiment, Jos C. Kleinjans, Jiri Aubrecht

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

MicroRNAs (miRNAs) released into the peripheral circulation upon cellular injury have shown a promise as a new class of tissue-specific biomarkers. We were first to demonstrate that next-generation sequencing analysis of serum from human subjects with acetaminophen-induced liver injury revealed a specific signature of circulating miRNAs. We consequently hypothesized that different types of hepatic liver impairments might feature distinct signatures of circulating miRNAs and that this approach might be useful as minimally invasive diagnostic "liquid biopsies" enabling the interrogation of underlying molecular mechanisms of injury in distant tissues. Therefore we examined serum circulating miRNAs in a total of 72 serum samples from a group of 53 subjects that included patients with accidental acetaminophen overdose, hepatitis B infection, liver cirrhosis and type 2 diabetes as well as gender-and age-matched healthy subjects with no evidence of liver disease. The miRNA signatures were identified using next-generation sequencing that provided analysis for the whole miRNome, including miRNA isoforms. Compared to the healthy subjects, a total of 179 miRNAs showed altered serum levels across the diseased subjects. Although many subjects have elevated alanine aminotransferase suggesting liver impairments, we identified distinct miRNA signatures for different impairments with minimum overlap. Furthermore, the bioinformatics analysis of miRNA signatures revealed relevant molecular pathways associated with the mechanisms of toxicity and or pathogenesis of disease. Interestingly, the high proportion of miRNA isoforms present in the respective signatures indicated a new level of complexity in cellular response to stress or disease. Our study demonstrates for the first time that signatures of circulating miRNAs show specificity for liver injury phenotypes and, once validated, might become useful for diagnosis of organ pathologies as "liquid biopsies".

Original language	English
Article number	0177928
Number of pages	17
Journal	PLOS ONE
Volume	12
Issue number	5
DOIs	https://doi.org/10.1371/journal.pone.0177928
Publication status	Published - 17 May 2017

Keywords

HEPATITIS-B-VIRUS
CIRCULATING MICRORNAS
ACETAMINOPHEN HEPATOTOXICITY
POTENTIAL BIOMARKERS
INJURY
EXPRESSION
REVEALS
MIRNAS
IDENTIFICATION
SEQUENCE

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Krauskopf, J., de Kok, T. M., Schomaker, S. J., Gosink, M., Burt, D. A., Chandler, P., Warner, R. L., Johnson, K. J., Caiment, F., Kleinjans, J. C., & Aubrecht, J. (2017). Serum microRNA signatures as "liquid biopsies" for interrogating hepatotoxic mechanisms and liver pathogenesis in human. PLOS ONE, 12(5), Article 0177928. https://doi.org/10.1371/journal.pone.0177928

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abstract = "MicroRNAs (miRNAs) released into the peripheral circulation upon cellular injury have shown a promise as a new class of tissue-specific biomarkers. We were first to demonstrate that next-generation sequencing analysis of serum from human subjects with acetaminophen-induced liver injury revealed a specific signature of circulating miRNAs. We consequently hypothesized that different types of hepatic liver impairments might feature distinct signatures of circulating miRNAs and that this approach might be useful as minimally invasive diagnostic {"}liquid biopsies{"} enabling the interrogation of underlying molecular mechanisms of injury in distant tissues. Therefore we examined serum circulating miRNAs in a total of 72 serum samples from a group of 53 subjects that included patients with accidental acetaminophen overdose, hepatitis B infection, liver cirrhosis and type 2 diabetes as well as gender-and age-matched healthy subjects with no evidence of liver disease. The miRNA signatures were identified using next-generation sequencing that provided analysis for the whole miRNome, including miRNA isoforms. Compared to the healthy subjects, a total of 179 miRNAs showed altered serum levels across the diseased subjects. Although many subjects have elevated alanine aminotransferase suggesting liver impairments, we identified distinct miRNA signatures for different impairments with minimum overlap. Furthermore, the bioinformatics analysis of miRNA signatures revealed relevant molecular pathways associated with the mechanisms of toxicity and or pathogenesis of disease. Interestingly, the high proportion of miRNA isoforms present in the respective signatures indicated a new level of complexity in cellular response to stress or disease. Our study demonstrates for the first time that signatures of circulating miRNAs show specificity for liver injury phenotypes and, once validated, might become useful for diagnosis of organ pathologies as {"}liquid biopsies{"}.",

keywords = "HEPATITIS-B-VIRUS, CIRCULATING MICRORNAS, ACETAMINOPHEN HEPATOTOXICITY, POTENTIAL BIOMARKERS, INJURY, EXPRESSION, REVEALS, MIRNAS, IDENTIFICATION, SEQUENCE",

author = "Julian Krauskopf and {de Kok}, {Theo M.} and Schomaker, {Shelli J.} and Mark Gosink and Burt, {Deborah A.} and Patricia Chandler and Warner, {Roscoe L.} and Johnson, {Kent J.} and Florian Caiment and Kleinjans, {Jos C.} and Jiri Aubrecht",

year = "2017",

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doi = "10.1371/journal.pone.0177928",

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AU - Krauskopf, Julian

AU - de Kok, Theo M.

AU - Schomaker, Shelli J.

AU - Gosink, Mark

AU - Burt, Deborah A.

AU - Chandler, Patricia

AU - Warner, Roscoe L.

AU - Johnson, Kent J.

AU - Caiment, Florian

AU - Kleinjans, Jos C.

AU - Aubrecht, Jiri

PY - 2017/5/17

Y1 - 2017/5/17

N2 - MicroRNAs (miRNAs) released into the peripheral circulation upon cellular injury have shown a promise as a new class of tissue-specific biomarkers. We were first to demonstrate that next-generation sequencing analysis of serum from human subjects with acetaminophen-induced liver injury revealed a specific signature of circulating miRNAs. We consequently hypothesized that different types of hepatic liver impairments might feature distinct signatures of circulating miRNAs and that this approach might be useful as minimally invasive diagnostic "liquid biopsies" enabling the interrogation of underlying molecular mechanisms of injury in distant tissues. Therefore we examined serum circulating miRNAs in a total of 72 serum samples from a group of 53 subjects that included patients with accidental acetaminophen overdose, hepatitis B infection, liver cirrhosis and type 2 diabetes as well as gender-and age-matched healthy subjects with no evidence of liver disease. The miRNA signatures were identified using next-generation sequencing that provided analysis for the whole miRNome, including miRNA isoforms. Compared to the healthy subjects, a total of 179 miRNAs showed altered serum levels across the diseased subjects. Although many subjects have elevated alanine aminotransferase suggesting liver impairments, we identified distinct miRNA signatures for different impairments with minimum overlap. Furthermore, the bioinformatics analysis of miRNA signatures revealed relevant molecular pathways associated with the mechanisms of toxicity and or pathogenesis of disease. Interestingly, the high proportion of miRNA isoforms present in the respective signatures indicated a new level of complexity in cellular response to stress or disease. Our study demonstrates for the first time that signatures of circulating miRNAs show specificity for liver injury phenotypes and, once validated, might become useful for diagnosis of organ pathologies as "liquid biopsies".

AB - MicroRNAs (miRNAs) released into the peripheral circulation upon cellular injury have shown a promise as a new class of tissue-specific biomarkers. We were first to demonstrate that next-generation sequencing analysis of serum from human subjects with acetaminophen-induced liver injury revealed a specific signature of circulating miRNAs. We consequently hypothesized that different types of hepatic liver impairments might feature distinct signatures of circulating miRNAs and that this approach might be useful as minimally invasive diagnostic "liquid biopsies" enabling the interrogation of underlying molecular mechanisms of injury in distant tissues. Therefore we examined serum circulating miRNAs in a total of 72 serum samples from a group of 53 subjects that included patients with accidental acetaminophen overdose, hepatitis B infection, liver cirrhosis and type 2 diabetes as well as gender-and age-matched healthy subjects with no evidence of liver disease. The miRNA signatures were identified using next-generation sequencing that provided analysis for the whole miRNome, including miRNA isoforms. Compared to the healthy subjects, a total of 179 miRNAs showed altered serum levels across the diseased subjects. Although many subjects have elevated alanine aminotransferase suggesting liver impairments, we identified distinct miRNA signatures for different impairments with minimum overlap. Furthermore, the bioinformatics analysis of miRNA signatures revealed relevant molecular pathways associated with the mechanisms of toxicity and or pathogenesis of disease. Interestingly, the high proportion of miRNA isoforms present in the respective signatures indicated a new level of complexity in cellular response to stress or disease. Our study demonstrates for the first time that signatures of circulating miRNAs show specificity for liver injury phenotypes and, once validated, might become useful for diagnosis of organ pathologies as "liquid biopsies".

KW - HEPATITIS-B-VIRUS

KW - CIRCULATING MICRORNAS

KW - ACETAMINOPHEN HEPATOTOXICITY

KW - POTENTIAL BIOMARKERS

KW - INJURY

KW - EXPRESSION

KW - REVEALS

KW - MIRNAS

KW - IDENTIFICATION

KW - SEQUENCE

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