Sarepta Therapeutics

Sarepta Therapeutics Inc. (NASDAQ: SRPT) is a medical research and drug development company with corporate offices and research facility in Cambridge, Massachusetts, United States. Incorporated in 1980, the company maintains some laboratory capability in Corvallis, Oregon. As of 2008^[update], the company has 170 issued medical patents, and over 150 patents pending.^[1] The company changed its name from AVI BioPharma and stock symbol from AVII in July 2012 to Sarepta Therapeutics and SRPT respectively.^[2]

History

At its founding in 1980, the company was named AntiVirals, Inc.^[3] After occupying several research laboratory spaces in Corvallis, the company opened a production laboratory in Corvallis, Oregon, in February 2002 and was renamed AVI BioPharma Inc. ^[4] The company made headlines in 2003 when it announced work on treatments for severe acute respiratory syndrome (SARS) and the West Nile virus.^[4][5] In July 2009, the company announced they would move their headquarters from Portland, Oregon, north to Bothell, Washington, near Seattle.^[6] At that time the company led by president and CEO Leslie Hudson had 83 employees and quarterly revenues of $3.2 million.^[6] AVI had yet to turn a profit nor developed any commercial products as of July 2009.^[6] The company lost $19.7 million in the second quarter of 2009,^[7] and then won a $11.5 million contract with the U.S. Department of Defense's Defense Threat Reduction Agency in October 2009.^[8] By this time the company had completed its headquarters move to Bothell.^[6][8]

In 2012 the company moved a second time, to Cambridge, Massachusetts, retaining their Corvallis laboratory facility. At the time, CEO Chris Garabedian indicated the move was motivated by the need to recruit expertise in rare diseases.^[9]

Products

Its primary products are Morpholino oligomers (PMOs), synthetic nucleic acid analogs that were conceived of by James Summerton and invented by Summerton with Dwight Weller, and are being developed under the name NeuGene Antisense. Since morpholino oligomers can form sequence-specific double-stranded complexes with RNA they are suitable use in antisense therapy. In this application a morpholino oligomer binds to messenger RNA produced by a known disease-causing gene to prevent it from being translated in to protein.

Morpholinos have been tested for a wide range of applications including prevention of cardiac restenosis after angioplasty, treatment of coronary artery bypass grafts, treatment of polycystic kidney disease, redirection of drug metabolism, Duchenne muscular dystrophy (DMD), and infectious diseases. Their greatest success thus far has been in DMD and as antiviral agents. Clinical trials of eteplirsen, a Morpholino oligo targeting exon 51 of the dystrophin mRNA, are ongoing. Morpholinos have been used in preclinical studies to inhibit replication of a broad range of viruses, including influenza, West Nile Virus, SARS, Hepatitis C, dengue fever, Ebola and Calicivirus, all of which are single stranded RNA viruses. They are in advanced development for prevention and treatment of Ebola and Marburg viruses. In March 2013, the Company announced positive results from a non-human primate study of AVI-7288, the drug candidate for treatment of Marburg virus infection. The results showed that intramuscular administration of AVI-7288 resulted in survival rates up to 100 percent in monkeys exposed to this fatal virus. These results are similar to those in previous studies when the drug was given by intravenous injection.^[10]

In addition to development of Morpholinos as therapeutics, AVI has conducted six human trials for colorectal and pancreatic cancers using their cancer vaccine AVICINE.

References

External links

• AVI BioPharma drops two directors, shareholder group to dissolve - Portland Business Journal