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Abstract

Acute respiratory distress syndrome (ARDS) is a devastating condition of acute inflammatory lung injury and causes high morbidity and mortality. Therefore, investigations on the effective biomarkers will be significant for the understanding of ARDS. In our research, the gene expression profiles of 27 samples from ARDS patients (n = 18) and healthy controls (n = 9) were analyzed and eight gene co-expression modules were identified by constructing weighted gene co-expression network. The correlation analysis of modules with phenotypes showed that genes in the yellow and black modules, which were significantly enriched in the ARDS-related pathways, such as TNF signaling pathway, Toll-like receptor signaling pathway, and NF-kappa B signaling pathway, were associated with the phenotype “time postinfection.” Genes DDX58 and CXCL10, which were highly expressed after infection and significantly enriched in ARDS-related pathways, presented high score in protein–protein interaction analysis, indicating that they may be associated with ARDS and providing novel biomarkers for its diagnosis, treatment, and surveillance.

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References

ARDS Definition Task Force, Ranieri, V.M., Rubenfeld, G.D., Thompson, B.T., Ferguson, N.D., Caldwell, E.., et al. (2012). Acute respiratory distress syndrome: the berlin definition. JAMA 307, 2526.

Baum

, Sachidanandam

, and GarcíaSastre

(2011). Preference of RIG-I for short viral RNA molecules in infected cells revealed by next-generation sequencing. Proc Natl Acad Sci U S A, 107, 16303–16308.

Biondo

, Lentini

, Beninati

, and Teti

(2019). The dual role of innate immunity during influenza. Biomed J, 42, 8–18.

Chi

, Zhu

, Wen

, Cui

, Ge

, Jiao

, et al. (2013). Cytokine and chemokine levels in patients infected with the novel avian influenza a (h7n9) virus in china. J Infect Dis, 208, 1962–1967.

Combes

, Pesenti

, and Ranieri

V.M.

(2017). Fifty years of research in ARDS. Is extracorporeal circulation the future of acute respiratory distress syndrome management? Am J Resp Crit Care Med 195, 1161.

Confalonieri

, Salton

, and Fabiano

(2017). Acute respiratory distress syndrome. Eur Respir Rev 26, 160116.

Cutts

, Talboys

, Paspula

, Prempeh

E.M.

, Fanous

, and Ail

(2017). Adult respiratory distress syndrome. Ann R Coll Surg Engl, 99, 12–16.

De Jong

M.D.

, Simmons

C.P.

, Thanh

T.T.

, Hien

V.M.

, Smith

G.J.D.

, Chau

T.N.B.

, et al. (2006). Fatal outcome of human influenza a (h5n1) is associated with high viral load and hypercytokinemia. Nat Med, 12, 1203–1207.

Efe

, Major

J.M.

, and Gilbert

M.L.I.

(2018). National incidence rates for acute respiratory distress syndrome (ARDS) and ARDS cause-specific factors in the United States (2006–2014). J Crit Care, 47, 192–197.

10.

Hornung

, Ellegast

, Kim

, Brzozka

, Jung

, Kato

, et al. (2006). 5\′′-triphosphate RNA is the ligand for RIG-I. Science, 314, 994–997.

11.

Ichikawa

, Kuba

, Morita

, Chida

, Tezuka

, and Hara

(2013). Cxcl10-cxcr3 enhances the development of neutrophil-mediated fulminant lung injury of viral and nonviral origin. Am J Respir Crit Care Med, 187, 65–77.

12.

Jesús

, Sulemanji

, and Kacmarek

R.M.

(2013). The acute respiratory distress syndrome: incidence and mortality, has it changed?. Curr Opin Crit Care, 20, 3–9.

13.

Kandasamy

, Suryawanshi

, Tundup

, Perez

J.T.

, and Manicassamy

(2016). Rig-i signaling is critical for efficient polyfunctional t cell responses during influenza virus infection. PLoS Pathogens 12, e1005754.

14.

Kato

, Takeuchi

, Sato

, Yoneyama

, Yamamoto

, Matsui

, et al. (2006). Differential roles of mda5 and RIG-I helicases in the recognition of RNA viruses. Nature (London), 441, 101–105.

15.

Kowalinski

, Lunardi

, Mccarthy

, Louber

, Brunel

, Grigorov

, et al. (2011). Structural basis for the activation of innate immune pattern-recognition receptor RIG-I by viral RNA. Cell, 147, 430–435.

16.

Lang

, Li

, Wang

, Sun

, and Wang

(2017). Cxcl10/ip-10 neutralization can ameliorate lipopolysaccharide-induced acute respiratory distress syndrome in rats. PLoS One 12, e0169100.

17.

Liu

, and Gu

(2011). Retinoic acid inducible gene-i, more than a virus sensor. Protein Cell, 2, 351–357.

18.

Ochiai

(2015). Mechanical ventilation of acute respiratory distress syndrome. J Intensive Care, 3, 1–9.

19.

Onomoto

, Jogi

, Yoo

J.S.

, Narita

, Morimoto

, Takemura

, et al. (2012). Critical role of an antiviral stress granule containing RIG-I and PKR in viral detection and innate immunity. PLoS One, 8, 301–304.

20.

Ramanathan

, Jiang

, Miller

M.T.

, Tang

G.Q.

, Gale

, Patel

S.S.

, et al. (2012). Structural basis of RNA recognition and activation by innate immune receptor RIG-I. Biophys J 102, 601a.

21.

Scolletta

, Colletti

, Di Luigi

, and Crescioli

(2013). Vitamin D receptor agonists target CXCL10: new therapeutic tools for resolution of inflammation. Mediat Inflamm, 2013, 1–11.

22.

Spiropoulou

C.F.

, Ranjan

, Pearce

M.B.

, Sealy

T.K.

, Albariño

C.G.

, Gangappa

, et al. (2015). RIG-I activation inhibits ebolavirus replication. Virology, 392, 11–15.

23.

, Zhai

, Sheu

C.C.

, Gallagher

D.C.

, Gong

M.N.

, Tejera

, et al. (2009). Genetic variants in theangiopoietin-2gene are associated with increased risk of ARDS. Intensive Care Med, 35, 1024–1030.

24.

Tobin

, and Manthous

(2017). What is acute respiratory distress syndrome?. Am J Respir Crit Care Med, 196, P17–P18.

25.

Villar

, Blanco

, Añón

, Santos-Bouza

, Blanch

, Ambrós

, et al. (2011). The alien study: incidence and outcome of acute respiratory distress syndrome in the era of lung protective ventilation. Intensive Care Med, 37, 1932–1941.

26.

Wan

Q.Q.

, Wu

, and Ye

Q.F.

(2017). The expression profiles of circrnas in lung tissues from rats with lipopolysaccharide-induced acute respiratory distress syndrome: a microarray study. Biochem Biophys Res Commun, 493, 684–689.

27.

Wang

, Yan

, He

, Zhong

, Zhan

, and Li

(2016). Candidate genes and pathogenesis investigation for sepsis-related acute respiratory distress syndrome based on gene expression profile. Biol Res 49, 25.

28.

Wonderlich

E.R.

, Swan

Z.D.

, Bissel

S.J.

, Hartman

A.L.

, Carney

J.P.

, O'Malley

KJ.

, et al. (2017). Widespread virus replication in alveoli drives acute respiratory distress syndrome in aerosolized h5n1 influenza infection of macaques. J Immunol, 198, 1616–1626.

29.

Yinghui

, Xiang

, Xingang

, Yuanping

, Man

, and Xiaodan

(2017). Identification of microRNAs in acute respiratory distress syndrome based on microRNA expression profile in rats. Mol Med Rep, 16, 3357–3362.

30.

Yoneyama

, Kikuchi

, Natsukawa

, Shinobu

, Imaizumi

, Miyagishi

, et al. (2004). The RNA helicase RIG-I has an essential function in double-stranded RNA-induced innate antiviral responses. Nat Immunol, 5, 730–737.

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Identification of DDX58 and CXCL10 as Potential Biomarkers in Acute Respiratory Distress Syndrome

Abstract

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