Discovery of Proteasome Inhibitors to Target PMP22 Gene Expression for the Treatment of Charcot-Marie-Tooth Disease Type 1A

E-Numbers

E-529-2013-0

Lead Inventor

Inglese, James (NCATS)

Co-Inventors

Jang, Sung-Wook (NCATS)

Svaren, John (Charcot-Marie-Tooth Association)

Applications

Therapeutics

Therapeutic Areas

Neurology

Lead IC

NCATS

ICs

NCATS

This technology includes the use of proteasome inhibitors, such as Bortezomib, for the treatment of the most prevalent form of Charcot-Marie-Tooth disease type 1A (CMT1A). Duplication of the peripheral myelin protein 22 (PMP22) gene, normally involved in myelination of the peripheral nervous system, is the causative agent in most forms of CMT1A. A drug discovery program was initiated and found that proteasome inhibitors can be used to target PMP22.

Commercial Applications

This discovery can be used to treat CMT1A with existing products such as proteasome inhibitors, including Bortezomib.

Competitive Advantages

This discovery identified a biological pathway for which drugs have already been developed. The current drugs that target the proteasome are highly toxic and used as anticancer agents.

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Licensing Contact:

Vepa, Suryanarayana
sury.vepa@nih.gov

Patents

US
Provisional (PRV) 61/702,295
Filed on 2012-09-18

Publications

Jang S-W, Lopez-Anido C, et al.

Date Published

2022-08-01

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Discovery of Proteasome Inhibitors to Target PMP22 Gene Expression for the Treatment of Charcot-Marie-Tooth Disease Type 1A

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Publications