E-WE thrombin, a protein C activator, reduces disease severity and spinal cord inflammation in relapsing-remitting murine experimental autoimmune encephalomyelitis

Norah G Verbout; Weiping Su; Peter Pham; Kelley Jordan; Tia Cl Kohs; Erik I Tucker; Owen Jt McCarty; Larry S Sherman

doi:10.21203/rs.3.rs-2802415/v1

E-WE thrombin, a protein C activator, reduces disease severity and spinal cord inflammation in relapsing-remitting murine experimental autoimmune encephalomyelitis

Res Sq [Preprint]. 2023 Apr 17:rs.3.rs-2802415. doi: 10.21203/rs.3.rs-2802415/v1.

Authors

Norah G Verbout¹, Weiping Su², Peter Pham², Kelley Jordan³, Tia Cl Kohs³, Erik I Tucker¹, Owen Jt McCarty³, Larry S Sherman²

Affiliations

¹ Aronora (United States).
² Oregon National Primate Research Center, Oregon Health & Science University.
³ Oregon Health & Science University.

Abstract

Objective: Relapses in patients with relapsing-remitting multiple sclerosis (RRMS) are typically treated with high-dose corticosteroids including methylprednisolone. However, high-dose corticosteroids are associated with significant adverse effects, can increase the risk for other morbidities, and often do not impact disease course. Multiple mechanisms are proposed to contribute to acute relapses in RRMS patients, including neuroinflammation, fibrin formation and compromised blood vessel barrier function. The protein C activator, E-WE thrombin is a recombinant therapeutic in clinical development for its antithrombotic and cytoprotective properties, including protection of endothelial cell barrier function. In mice, treatment with E-WE thrombin reduced neuroinflammation and extracellular fibrin formation in myelin oligodendrocyte glycoprotein (MOG)-induced experimental autoimmune encephalomyelitis (EAE). We therefore tested the hypothesis that E-WE thrombin could reduce disease severity in a relapsing-remitting model of EAE.

Methods: Female SJL mice were inoculated with proteolipid protein (PLP) peptide and treated with E-WE thrombin (25 μg/kg; iv) or vehicle at onset of detectable disease. In other experiments, E-WE thrombin was compared to methylprednisolone (100 mg/kg; iv) or the combination of both.

Results: Compared to vehicle, administration of E-WE thrombin significantly improved disease severity of the initial attack and relapse and delayed onset of relapse as effectively as methylprednisolone. Both methylprednisolone and E-WE thrombin reduced demyelination and immune cell recruitment, and the combination of both treatments had an additive effect.

Conclusion: The data presented herein demonstrate that E-WE thrombin is protective in mice with relapsing-remitting EAE, a widely used model of MS. Our data indicate that E-WE thrombin is as effective as high-dose methylprednisolone in improving disease score and may exert additional benefit when administered in combination. Taken together, these data suggest that E-WE thrombin may be an effective alternative to high-dose methylprednisolone for managing acute MS attacks.

Keywords: Animal model; Demyelination; Inflammation; Multiple sclerosis; Relapsing/remitting; Steroids; Thrombin.

Publication types

Preprint

Grants and funding

This work was supported by a grant from the National Multiple Sclerosis Society (RG-1702-27047; LS, WS, NV, OM) and National Institutes of Health grants HL117589 (NV, ET), HL101972 (OM) and P51 OD011092 for support of the Oregon National Primate Research Center (LS).