Anti-inflammatory genes in PBMCs post-spontaneous intracerebral hemorrhage

Author:

Nguyen Doan1,Tran Vi1,Shirazian Alireza1,Velasco-Gonzalez Cruz2,Iwuchukwu Ifeanyi1345

Affiliation:

1. Institute for Translational Research, Ochsner Medical Center, Ochsner Health , 1514 Jefferson Highway , New Orleans , LA 70121 , United States of America

2. Center for Outcomes and Health Services Research, Ochsner Health , 1514 Jefferson Highway , New Orleans , LA 70121 , United States of America

3. Neurocritical Care and Neurology, University of Queensland, Ochsner Clinical School, Ochsner Medical Center , Ochsner Health, 1514 Jefferson Highway , New Orleans , LA 70121 , United States of America

4. Neuroscience Center of Excellence, Louisiana State University Health New Orleans, School of Medicine , 2020 Gravier Street, 8th Floor , New Orleans , LA 70112 , United States of America

5. Department of Neurosurgery, Louisiana State University Health New Orleans, School of Medicine , 2020 Gravier Street, 7th Floor , New Orleans , LA 70112 , United States of America

Abstract

Abstract Background Neuroinflammation is important in the pathophysiology of spontaneous intracerebral hemorrhage (ICH) and peripheral inflammatory cells play a role in the clinical evolution and outcome. Methodology Blood samples from ICH patients (n = 20) were collected at admission for 5 consecutive days for peripheral blood mononuclear cells (PBMCs). Frozen PBMCs were used for real-time PCR using Taqman probes (NFKB1, SOD1, PPARG, IL10, NFE2L2, and REL) and normalized to GAPDH. Data on hospital length of stay and modified Rankin score (MRS) were collected with 90-day MRS ≤ 3 as favorable outcome. Statistical analysis of clinical characteristics to temporal gene expression from early to delayed timepoints was compared for MRS groups (favorable vs unfavorable) and hematoma volume. Principle findings and results IL10, SOD1, and REL expression were significantly higher at delayed timepoints in PBMCs of ICH patients with favorable outcome. PPARG and REL increased between timepoints in patients with favorable outcome. NFKB1 expression was not sustained, but significantly decreased from higher levels at early onset in patients with unfavorable outcome. IL10 expression showed a negative correlation in patients with high hematoma volume (>30 mL). Conclusions and significance Anti-inflammatory, pro-survival regulators were highly expressed at delayed time points in ICH patients with a favorable outcome, and IL10 expression showed a negative correlation to high hematoma volume.

Publisher

Walter de Gruyter GmbH

Subject

General Neuroscience

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