Technology ID
TAB-3741
Ribose Derivatives as A3 Adenosine Receptor Modulator for Various Therapeutic Uses
E-Numbers
E-089-2017-0
Lead Inventor
Jacobson, Kenneth (NIDDK)
Co-Inventors
Tosh, Dilip (NIDDK)
Applications
Therapeutics
Therapeutic Areas
Ophthalmology
Oncology
Neurology
Infectious Disease
Endocrinology
Dental
Cardiology
Lead IC
NIDDK
ICs
NIDDK
This technology includes a class of A3AR-selective agonists to be used therapeutically to treat a variety of conditions, including chronic pain, cancer, and inflammatory diseases. This class of compounds produced full agonists of the human A3AR of nanomolar affinity that were consistently highly selective (>1000-fold vs. A1AR and A2AAR). The selectivity at mouse A3 receptors is smaller, but the compounds are still effective in vivo in reducing or preventing development of neuropathic pain. The advantages over previous, structurally similar compounds are a smaller molecular weight, and therefore greater oral bioavailability. We have carried out phenotypic screening – thus we have identified unexpected in vivo activity of specific C2 substituents in a chronic neuropathic pain model.
Commercial Applications
The discovery could be primarily utilized therapeutically, with the main focus in the present set of compounds being chronic neuropathic pain. Other A3 agonists (our prototypical A3 agonists) are in advanced clinical trials for treatment of autoimmune inflammatory diseases and cancer, and the present compounds might be superior in animal tests in those diseases.
Competitive Advantages
This class of compounds produced full agonists of the human A3AR of nanomolar affinity that were consistently highly selective (>1000-fold vs. A1AR and A2AAR), and have a small molecular weight, and therefore greater oral bioavailability.
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