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Pro-inflammatory Monocyte Phenotype During Acute Progression of Cerebral Small Vessel Disease.

Frontiers in cardiovascular medicine

Authors: Marlies P Noz, Annemieke Ter Telgte, Kim Wiegertjes, Anil M Tuladhar, Charlotte Kaffa, Simone Kersten, Siroon Bekkering, Charlotte D C C van der Heijden, Alexander Hoischen, Leo A B Joosten, Mihai G Netea, Marco Duering, Frank-Erik de Leeuw, Niels P Riksen

The etiology of cerebral small vessel disease (SVD) remains elusive, though evidence is accumulating that inflammation contributes to its pathophysiology. We recently showed retrospectively that pro-inflammatory monocytes are associated with the long-term progression of white matter hyperintensities (WMHs). In this prospective high-frequency imaging study, we hypothesize that the incidence of SVD progression coincides with a pro-inflammatory monocyte phenotype. Individuals with SVD underwent monthly magnetic resonance imaging (MRI) for 10 consecutive months to detect SVD progression, defined as acute diffusion-weighted imaging-positive (DWI+) lesions, incident microbleeds, incident lacunes, and WMH progression. Circulating inflammatory markers were measured, cytokine production capacity of monocytes was assessed after stimulation, and RNA sequencing was performed on isolated monocytes in a subset of participants. 13 out of 35 individuals developed SVD progression (70 ± 6 years, 54% men) based on incident lesions ( = 7) and/or upper quartile WMH progression ( = 9). Circulating E-selectin concentration ( < 0.05) and the cytokine production capacity of interleukin (IL)-1β and IL-6 ( < 0.01) were higher in individuals with SVD progression. Moreover, RNA sequencing revealed a pro-inflammatory monocyte signature including genes involved in myelination, blood-brain barrier, and endothelial-leukocyte interaction. Circulating monocytes of individuals with progressive SVD have an inflammatory phenotype, characterized by an increased cytokine production capacity and a pro-inflammatory transcriptional signature.

Copyright © 2021 Noz, Telgte, Wiegertjes, Tuladhar, Kaffa, Kersten, Bekkering, van der Heijden, Hoischen, Joosten, Netea, Duering, de Leeuw and Riksen.

PMID: 34055930

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