Abstract

Neuromyelitis optica (NMO) is an autoimmune inflammatory disease of the central nervous system that causes demyelination and neuron loss, mainly affecting optic nerves and spinal cord. While major advances have been made in understanding NMO pathogenesis mechanisms, including the causal role of immunoglobulin G autoantibodies against astrocyte water channel aquaporin-4 (called AQP4-IgG), there remain unknowns in pathogenesis mechanisms of NMO optic neuritis, in part because of lack of suitable animal models, and unmet needs in developing safe and effective therapies for NMO optic neuritis to prevent vision loss. This renewal application builds on discoveries made by our lab on NMO pathogenesis mechanisms, animal models and therapeutics.
In Aim 1, rat models of NMO optic neuritis will be advanced to study pathogenesis mechanisms and test therapeutics. Robust models of NMO optic neuritis will be developed in AQP4-IgG `seropositive' rats, using, as needed, newly generated CD59-/- rats, NMO `superantibodies', and blood-brain barrier permeabilization by high-frequency focused ultrasound. The hypothesis will be tested that passive transfer of AQP4-IgG alone is sufficient to cause NMO optic neuritis. Also, building on advances in NMO T cell biology and our newly generated AQP4-/- rats, the hypothesis will be tested that AQP4-sensitized T cells initiate and amplify NMO optic neuritis in AQP4-IgG seropositive rats.
Aim 2 will test a novel `bystander' mechanism for tissue injury in NMO in which activated soluble complement components produced by AQP4-IgG binding to AQP4 on astrocytes injure nearby oligodendrocytes, providing a potential explanation for the early demyelination in NMO. Utilizing novel models and imaging methods, the hypothesis will be tested that bystander injury is a general pathogenesis mechanism in NMO, not only for complement-dependent oligodendrocyte injury, but also for microvascular injury.
Aim 3 will advance non-immunosuppressive therapies for NMO optic neuritis. Our lab introduced novel NMO therapies targeting AQP4-IgG and its binding to AQP4, the classical complement pathway, granulocytes and remyelination, including an engineered high-affinity anti- AQP4 antibody (`aquaporumab'). We propose to develop `second-generation aquaporumabs' by conjugating an affinity-matured anti-AQP4 antibody with a complement inhibitor such as CD59, thereby targeting a protective molecule exactly where it is needed, effectively boosting the efficacy of aquaporumab and overcoming limitations on affinity and AQP4 binding site saturation. Also, building on recent work, we will prioritize and test drug candidates for remyelination in NMO optic neuritis. The goal is to advance safe and effective non-immunosuppressive drug(s) to preserve vision in NMO optic neuritis.

Public Health Relevance

Neuromyelitis optica (NMO) is an autoimmune inflammatory disease of the central nervous system that causes demyelination and neuron loss, mainly affecting optic nerves and spinal cord. The proposed research will determine the cellular and immune mechanisms responsible for NMO optic neuritis, and advance novel non- immunosuppressive therapies for NMO.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY013574-18
Application #
9928970
Study Section
Diseases and Pathophysiology of the Visual System Study Section (DPVS)
Program Officer
Mckie, George Ann
Project Start
2002-09-01
Project End
2023-04-30
Budget Start
2020-05-01
Budget End
2021-04-30
Support Year
18
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94118

  Publications

Smith, Alex J; Verkman, Alan S (2018) The ""glymphatic"" mechanism for solute clearance in Alzheimer's disease: game changer or unproven speculation? FASEB J 32:543-551
Duan, Tianjiao; Smith, Alex J; Verkman, Alan S (2018) Complement-dependent bystander injury to neurons in AQP4-IgG seropositive neuromyelitis optica. J Neuroinflammation 15:294
Lee, Sujin; Cil, Onur; Diez-Cecilia, Elena et al. (2018) Nanomolar-Potency 1,2,4-Triazoloquinoxaline Inhibitors of the Kidney Urea Transporter UT-A1. J Med Chem 61:3209-3217
Tradtrantip, Lukmanee; Felix, Christian M; Spirig, Rolf et al. (2018) Recombinant IgG1 Fc hexamers block cytotoxicity and pathological changes in experimental in vitro and rat models of neuromyelitis optica. Neuropharmacology 133:345-353
Agbani, Ejaife O; Williams, Christopher M; Li, Yong et al. (2018) Aquaporin-1 regulates platelet procoagulant membrane dynamics and in vivo thrombosis. JCI Insight 3:
Phuan, Puay-Wah; Veit, Guido; Tan, Joseph-Anthony et al. (2018) ?F508-CFTR Modulator Screen Based on Cell Surface Targeting of a Chimeric Nucleotide Binding Domain 1 Reporter. SLAS Discov 23:823-831
Verkman, Alan S; Yao, Xiaoming; Smith, Alex J (2018) The evolving mystery of why skeletal muscle is spared in seropositive neuromyelitis optica. J Cell Mol Med 22:2039-2040
Ludwig, Ralf J; Vanhoorelbeke, Karen; Leypoldt, Frank et al. (2017) Mechanisms of Autoantibody-Induced Pathology. Front Immunol 8:603
Yao, Xiaoming; Verkman, Alan S (2017) Complement regulator CD59 prevents peripheral organ injury in rats made seropositive for neuromyelitis optica immunoglobulin G. Acta Neuropathol Commun 5:57
Son, Jung-Ho; Zhu, Jie S; Phuan, Puay-Wah et al. (2017) High-Potency Phenylquinoxalinone Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) Activators. J Med Chem 60:2401-2410

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