Technology Offer

Mouse model of progressive multiple sclerosis

Summary of the technology

MS Animal Model
Project ID : 2-2011-158

Details of the Technology Offer

The Technology

Multiple sclerosis (MS) is an autoimmune disease of the central nervous system characterized by damage to the neuronal myelin sheath, which results in different levels of muscle paralysis that can lead to neuronal death. In most MS mouse models, the neurologic damage mostly affects the spinal cord with limited damage to the brain, which cannot be monitored by magnetic resonance imaging (MRI) as used for humans.

We show that immunization of non-obese diabetic (NOD) mice with myelin oligodendrocyte glycoprotein peptide 35–55 leads to the development of relapsing–remitting stages, evident from days 20 to 70, which then develops into a chronic progressive stage. This cycle is similar to MS stages found in humans. Brain MRI gadolinium-enhanced T1-weighted image analysis showed an increased blood–brain barrier permeability in brain gray and white matter specific to the corpus callosum, fimbria, and internal capsule as found in humans. MRI fractional anisotropy analysis showed demyelination and axonal damage in identical regions. Immunohistologic analysis supported the MRI data. No evidence of brain lesions was found in a common model of MS using C57BL/6 mice.

We suggest that an increase in astrocyte toxicity in experimental autoimmune encephalomyelitis-induced NOD mice may be linked to brain lesion development.

We suggest using NOD mice as a suitable model for studying MS using MRI methods toward future diagnostic and drug development.

By characterizing a chronic stage following the formation of brain lesions, the NOD model of MS could contribute to the understanding of pathologic processes in the MS brain and the development of new therapeutic approaches that would address the chronic progressive stage, demyelination processes, and axonal injury in the brain, which can be monitored by MRI as done in humans.

Publication

H. Levy et al. / Experimental Neurology 226 (2010) 148–158.

Project manager

Elisha Natan
Director BD

Project researchers

Dan Frenkel
T.A.U Tel Aviv University, Life Sciences
Neurobiology

Related Keywords

  • Medicine, Human Health
  • Medical Technology / Biomedical Engineering
  • Biology / Biotechnology
  • Cellular and Molecular Biology Technology
  • Microbiology Technology
  • Genome Research
  • Bioinformatics Technology
  • Micro- and Nanotechnology related to Biological sciences
  • Microbiology Market
  • Micro- and Nanotechnology related to Biological sciences
  • Biochemistry / Biophysics Market
  • Stem cells and biobanks
  • Cellular and Molecular Biology Market
  • Bioinformatics Market
  • Diagnostic
  • Therapeutic
  • Other Medical/Health Related
  • Clinical Medicine
  • Life Sciences and Biotechnology
  • Pharmaceutical Indications
  • cns
  • Life Sciences and Biotechnology
  • Research / Development tools
  • cns

About RAMOT at Tel Aviv University Ltd.

RAMOT at Tel Aviv University Ltd.

RAMOT at Tel Aviv University Ltd.

Technology Transfer Office from Israel

Ramot is Tel Aviv University's (TAU) technology transfer company and its liaison to industry, bringing promising scientific discoveries made at the university to industry's attention. The company provides the legal and commercial frameworks for inventions made by TAU faculty, students and researchers, protecting discoveries with patents and working jointly with industry to bring scientific innovations to the market.

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