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OKLAHOMA CITY, Aug. 19, 2013 /PRNewswire/ -- Selexys Pharmaceuticals Corporation, a privately held biopharmaceutical company that is developing therapies to treat inflammatory and thrombotic diseases, today announced that enrollment has been initiated in SUSTAIN, a Phase II, multicenter, randomized, placebo-controlled, double-blind, 12-month study to assess safety and efficacy of the anti-P-selectin monoclonal antibody SelG1 with or without hydroxyurea therapy in sickle cell disease patients with sickle cell-related pain crises.
The SUSTAIN trial will randomize approximately 174 patients to receive high dose SelG1, low dose SelG1or placebo in the presence or absence of hydroxyurea therapy, the current standard of treatment. The study will examine the effectiveness of SelG1 in reducing the rate of sickle cell-related pain crises in each active dose level as compared to placebo. The study will be conducted in approximately 60 centers throughout the U.S. Further information on this trial is available at clinicaltrials.gov (NCT01895361).
“With the limited therapies available to patients with sickle cell disease, this trial with a novel P-selectin inhibitor is particularly exciting. Not only does it have the potential to improve the clinical outcomes in patients, its effects may be additive or synergistic with those of hydroxyurea, the only drug currently approved by the FDA for treatment of complications due to sickle cell disease,” stated Dr. Kenneth Ataga, Lead Investigator and Associate Professor of Medicine in the Division of Hematology/Oncology, University of North Carolina at Chapel Hill.
“Data from preclinical sickle cell disease models suggest that blockade of P-selectin effectively prevents the painful stoppage of circulation in small blood vessels called vasoocclusion and maintains patent blood flow,” stated Dr. Russell Rother, Selexys Executive Vice-President and Chief Operating Officer. “In addition, results from our recently completed Phase I study indicate that SelG1 is well tolerated in healthy human subjects. We now look forward to investigating its safety and efficacy in the sickle cell disease patient population.”
SelG1 prevents certain blood cells from binding to one another and to the blood vessel walls. By stopping these cell-cell interactions, SelG1 may prevent small blood vessels from becoming blocked and reduce the occurrence and severity of pain crises as well as downstream complications such as stroke, heart attack and organ failure in sickle cell patients.
“We are excited to initiate our second clinical study with SelG1 and to test its potential benefit in the sickle cell patient population,” said Dr. Scott Rollins, President and Chief Executive Officer of Selexys. “The SUSTAIN study focuses on the ability of our novel anti-P-selectin antibody to reduce or prevent the occurrence of pain crises and thereby improve the lives of patients with sickle cell, a disease that largely affects African-Americans in the U.S.”
About SelG1
SelG1 is an investigational humanized monoclonal antibody directed against P-selectin, a key member of the adhesion molecule family known as the selectins. In preclinical studies, inhibition of P-selectin has been shown to effectively prevent vasoocclusion by blocking critical cell-cell interactions that drive this process. Therapeutic blockade of P-selectin may therefore reduce or prevent vasoocclusive crises in patients with sickle cell disease. The SelG1 program for sickle cell disease is supported by Small Business Innovation Research (SBIR) fast-track award #5R44HL093893-02 and #2R44HL093893-03 through the National Heart, Lung and Blood Institute.
About Sickle Cell Disease
Sickle cell disease is an inherited, progressive, hematologic disease that affects over 100,000 people in the United States including one out of every 500 African-Americans, with one in 12 African-Americans a carrier of the sickle cell disease gene. Patients with sickle cell disease suffer anemia as well as vasoocclusive complications in which sickled red cells, white blood cells and platelets adhere to small vessels blocking blood flow to downstream organs. This vasoocclusive process results in intense pain and repeated hospitalizations. It also leads to progressive multi-organ dysfunction and premature death. Sickle cell disease is considered an orphan indication with major unmet clinical needs.
About Selexys Pharmaceuticals
Selexys Pharmaceuticals Corporation is a privately held biopharmaceutical company that is focused on development of therapeutics for the treatment of inflammation, thrombosis and metastasis across a broad range of severe diseases. Selexys is also developing an antibody directed against PSGL-1 for the treatment of Crohn’s disease, multiple myeloma, and other inflammatory disorders. In September 2012, Selexys completed a $25 million Series A equity financing, led by MPM Capital and entered into an agreement with Novartis Pharmaceuticals whereby Novartis was granted an exclusive option to acquire Selexys and its lead asset, the anti-P-selectin antibody SelG1, following the successful completion of a Phase 2 clinical study in patients with sickle cell disease. Selexys is headquartered in Oklahoma City, OK. For additional information please visit our website at www.selexys.com.
Company Contact: | Media Contact: |
Selexys Pharmaceuticals | Rx Communications Group |
Scott Rollins, Ph.D. | Eric Goldman |
President and Chief Executive Officer | Vice President Public Relations |
405-319-8195 | 917-322-2563 |
SOURCE Selexys Pharmaceuticals
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