Systematic Analysis of Blood Cell Transcriptome in End-Stage Chronic Respiratory Diseases

Background End-stage chronic respiratory diseases (CRD) have systemic consequences, such as weight loss and susceptibility to infection. However the mechanisms of such dysfunctions are as yet poorly explained. We hypothesized that the genes putatively involved in these mechanisms would emerge from a systematic analysis of blood mRNA profiles from pre-transplant patients with cystic fibrosis (CF), pulmonary hypertension (PAH), and chronic obstructive pulmonary disease (COPD). Methods Whole blood was first collected from 13 patients with PAH, 23 patients with CF, and 28 Healthy Controls (HC). Microarray results were validated by quantitative PCR on a second and independent group (7PAH, 9CF, and 11HC). Twelve pre-transplant COPD patients were added to validate the common signature shared by patients with CRD for all causes. To further clarify a role for hypoxia in the candidate gene dysregulation, peripheral blood mononuclear cells from HC were analysed for their mRNA profile under hypoxia. Results Unsupervised hierarchical clustering allowed the identification of 3 gene signatures related to CRD. One was common to CF and PAH, another specific to CF, and the final one was specific to PAH. With the common signature, we validated T-Cell Factor 7 (TCF-7) and Interleukin 7 Receptor (IL-7R), two genes related to T lymphocyte activation, as being under-expressed. We showed a strong impact of the hypoxia on modulation of TCF-7 and IL-7R expression in PBMCs from HC under hypoxia or PBMCs from CRD. In addition, we identified and validated genes upregulated in PAH or CF, including Lectin Galactoside-binding Soluble 3 and Toll Like Receptor 4, respectively. Conclusions Systematic analysis of blood cell transcriptome in CRD patients identified common and specific signatures relevant to the systemic pathologies. TCF-7 and IL-7R were downregulated whatever the cause of CRD and this could play a role in the higher susceptibility to infection of these patients.

Mots clés

Chronic obstructive pulmonary disease Microarrays Gene expression Cystic fibrosis Metabolic processes Blood Gene ontologies Toll-like receptors

Domaines

Sciences du Vivant [q-bio] Médecine humaine et pathologie

Fichier principal

journal.pone.0109291.PDF (2.99 Mo)

Origine : Fichiers éditeurs autorisés sur une archive ouverte

Sarah Hamant : Connectez-vous pour contacter le contributeur

https://hal.univ-grenoble-alpes.fr/hal-01969399

Soumis le : mercredi 22 mai 2019-09:22:48

Dernière modification le : vendredi 19 avril 2024-16:18:56

Dates et versions

hal-01969399 , version 1 (22-05-2019)

Licence

Paternité

Identifiants

HAL Id : hal-01969399 , version 1
DOI : 10.1371/journal.pone.0109291
PRODINRA : 287219
PUBMED : 25329529
WOS : 000343942100020

Citer

Julie Chesne, Richard Danger, Karine Botturi, Martine Reynaud-Gaubert, Sacha Mussot, et al.. Systematic Analysis of Blood Cell Transcriptome in End-Stage Chronic Respiratory Diseases. PLoS ONE, 2014, 9 (10), pp.e109291. ⟨10.1371/journal.pone.0109291⟩. ⟨hal-01969399⟩

Exporter

BibTeX XML-TEI Dublin Core DC Terms EndNote DataCite

Collections

IRD UNIV-PARIS7 UNIV-NANTES EPHE UGA CNRS UNIV-AMU UNIV-FCOMTE UNIV-BM UNIV-LYON1 INRA FEMTO-ST FNCLCC CURIE UNIV-BM-THESE TIMC-IMAG-PRETA UVSQ PSL THORAX-UMR CRTI LBFA UDL INRAE ANR GS-HEALTH-DRUG-SCIENCES NANTES-UNIVERSITE CR2TI HPPIT UFR-MEDECINE-NANTES

1299 Consultations

125 Téléchargements