Cortical inflammation and brain signs of high-risk atherosclerosis in a non-human primate model

Author:

Di Cataldo Vanessa1,Debatisse Justine12ORCID,Piraquive Joao3,Géloën Alain1,Grandin Clément4,Verset Michaël4ORCID,Taborik Fabrice4,Labaronne Emmanuel1,Loizon Emmanuelle1,Millon Antoine1,Mury Pauline5ORCID,Pialoux Vincent5,Serusclat André6,Lamberton Franck3ORCID,Ibarrola Danielle3,Lavenne Franck3,Le Bars Didier3,Troalen Thomas2,Confais Joachim4,Crola Da Silva Claire1,Mechtouff Laura17,Contamin Hugues4,Fayad Zahi A8,Canet-Soulas Emmanuelle1ORCID

Affiliation:

1. CarMeN Laboratory, Univ Lyon, INSERM U1060, INRAE 1397, Université Claude Bernard Lyon 1, Lyon, France

2. Siemens-Healthcare SAS, Saint-Denis, France

3. CERMEP—Imagerie du Vivant, Lyon, France

4. Cynbiose SAS, Marcy-L'Etoile, France

5. LIBM Laboratory, Univ Lyon, Université Lyon 1, Lyon, France

6. Radiology Department, Louis Pradel Hospital, Hospices Civils de Lyon, Lyon, France

7. Stroke Department, Hospices Civils de Lyon, Lyon, France

8. BioMedical Engineering and Imaging Institute, Icahn School of Medicine at Mount Sinai, New York, NY, USA

Abstract

Abstract Atherosclerosis is a chronic systemic inflammatory disease, inducing cardiovascular and cerebrovascular acute events. A role of neuroinflammation is suspected, but not yet investigated in the gyrencephalic brain and the related activity at blood−brain interfaces is unknown. A non-human primate model of advanced atherosclerosis was first established using longitudinal blood samples, multimodal imaging and gene analysis in aged animals. Non-human primate carotid lesions were compared with human carotid endarterectomy samples. During the whole-body imaging session, imaging of neuroinflammation and choroid plexus function was performed. Advanced plaques were present in multiple sites, premature deaths occurred and downstream lesions (myocardial fibrosis, lacunar stroke) were present in this model. Vascular lesions were similar to in humans: high plaque activity on PET and MRI imaging and systemic inflammation (high plasma C-reactive protein levels: 42 ± 14 µg/ml). We also found the same gene association (metabolic, inflammatory and anti-inflammatory markers) as in patients with similar histological features. Metabolic imaging localized abnormal brain glucose metabolism in the frontal cortex. It corresponded to cortical neuro-inflammation (PET imaging) that correlated with C-reactive protein level. Multimodal imaging also revealed pronounced choroid plexus function impairment in aging atherosclerotic non-human primates. In conclusion, multimodal whole-body inflammation exploration at the vascular level and blood−brain interfaces identified high-risk aging atherosclerosis. These results open the way for systemic and central inflammation targeting in atherosclerosis in the new era of immunotherapy.

Funder

French Ministry of Higher Education & Research

Cifre ANRT and Siemens

CYCLOPS

RHU MARVELOUS

French National Agency of Research

Publisher

Oxford University Press (OUP)

Subject

General Earth and Planetary Sciences,General Environmental Science

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