Angiotensin II Controls Occludin Function and Is Required for Blood Brain Barrier Maintenance: Relevance to Multiple Sclerosis

doi:10.1523/JNEUROSCI.2088-07.2007

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The Journal of Neuroscience, August 22, 2007, 27(34):9032-9042; doi:10.1523/JNEUROSCI.2088-07.2007

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Multiple Sclerosis

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Neurobiology of Disease
Angiotensin II Controls Occludin Function and Is Required for Blood–Brain Barrier Maintenance: Relevance to Multiple Sclerosis
Karolina Wosik,¹^* Romain Cayrol,¹^* Aurore Dodelet-Devillers,¹ France Berthelet,² Monique Bernard,¹ Robert Moumdjian,³ Alain Bouthillier,³ Timothy L. Reudelhuber,⁵ and Alexandre Prat¹^,4^,6
¹Neuroimmunology Research Laboratory, Center for Study of Brain Diseases, ²Department of Neuropathology, ³Department of Neurosurgery, ⁴Department of Neurology, ⁵Laboratory of Molecular Biochemistry of Hypertension, Clinical Research Institute of Montreal, and ⁶Multiple Sclerosis Clinic, Department of Neurology, Centre Hospitalier de l'Université de Montréal-Notre Dame Hospital, University of Montreal, Montréal, Quebec, Canada H2L 4M1
Correspondence should be addressed to Dr. Alexandre Prat, Multiple Sclerosis Clinic and Neuroimmunology Research Laboratory, Centre Hospitalier de l'Université de Montréal-Notre Dame Hospital, 1560 Sherbrooke Street East, Montréal, Quebec, Canada H2L 4M1. Email: a.prat{at}umontreal.ca

The blood–brain barrier (BBB) restricts molecular andcellular trafficking between the blood and the CNS. Althoughastrocytes are known to control BBB permeability, the moleculardeterminants of this effect remain unknown. We show that angiotensinogen(AGT) produced and secreted by astrocytes is cleaved into angiotensinII (AngII) and acts on type 1 angiotensin receptors (AT₁) expressedby BBB endothelial cells (ECs). Activation of AT₁ restrictsthe passage of molecular tracers across human BBB-derived ECsthrough threonine-phosphorylation of the tight junction proteinoccludin and its mobilization to lipid raft membrane microdomains.We also show that AGT knock-out animals have disorganized occludinstrands at the level of the BBB and a diffuse accumulation ofthe endogenous serum protein plasminogen in the CNS, comparedwith wild-type animals. Finally, we demonstrate a reductionin the number of AGT-immunopositive perivascular astrocytesin multiple sclerosis (MS) lesions, which correlates with areduced expression of occludin similarly seen in the CNS ofAGT knock-out animals. Such a reduction in astrocyte-expressedAGT and AngII is dependent, in vitro, on the proinflammatorycytokines tumor necrosis factor- ${alpha}$ and interferon- ${gamma}$ . Our studydefines a novel physiological role for AngII in the CNS andsuggests that inflammation-induced downregulation of AngII productionby astrocytes is involved in BBB dysfunction in MS lesions.

Key words: astrocytes; tight junctions; renin-angiotensin system; CNS; neuroinflammation; lipid rafts; human; mouse; lymphocytes; immune privilege

Received Feb. 27, 2007; revised June 1, 2007; accepted July 5, 2007.

Correspondence should be addressed to Dr. Alexandre Prat, Multiple Sclerosis Clinic and Neuroimmunology Research Laboratory, Centre Hospitalier de l'Université de Montréal-Notre Dame Hospital, 1560 Sherbrooke Street East, Montréal, Quebec, Canada H2L 4M1. Email: a.prat{at}umontreal.ca

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