A Phase Ib open label, randomized, safety study of SANGUINATE™ in patients with sickle cell anemia

Treatment of sickle cell anemia is a challenging task and despite the well understood genetic and biochemical pathway of sickle hemoglobin, current therapy continues to be limited to the symptomatic treatment of pain, supplemental oxygen, antibiotics, red blood cell transfusions and hydroxyurea. SAN...

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Bibliographic Details
Published in:Revista brasileira de hematologia e hemoterapia 2017-01, Vol.39 (1), p.20-27
Main Authors: Misra, Hemant, Bainbridge, James, Berryman, John, Abuchowski, Abraham, Galvez, Kenneth Mauricio, Uribe, Luis Fernando, Hernandez, Angel Luis, Sosa, Nestor Rodolfo
Format: Article
Language:English
Subjects:
Clinical trial
HEMATOLOGY
MEDICINE, RESEARCH & EXPERIMENTAL
Original
Safety
SANGUINATE
Sickle cell disease
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Summary:Treatment of sickle cell anemia is a challenging task and despite the well understood genetic and biochemical pathway of sickle hemoglobin, current therapy continues to be limited to the symptomatic treatment of pain, supplemental oxygen, antibiotics, red blood cell transfusions and hydroxyurea. SANGUINATE is a carbon monoxide releasing molecule and oxygen transfer agent under clinical development for the treatment of sickle cell anemia and comorbidities. An open-label randomized Phase Ib study was performed in adult sickle cell anemia patients. Two dose levels of SANGUINATE were compared to hydroxyurea in 24 homozygotes for Hb SS. Twelve subjects received either a low dose (160mg/kg) of SANGUINATE or 15mg/kg hydroxyurea. Another 12 subjects received either a high dose (320mg/kg) of SANGUINATE or 15mg/kg hydroxyurea. The primary endpoint was the safety of SANGUINATE versus hydroxyurea in sickle cell anemia patients. Secondary endpoints included determination of the plasma pharmacokinetics and assessment of hematologic measurements. Musculoskeletal related adverse events were the most common. Transient troponin I levels increased in three patients, one of whom had an increase in tricuspid regurgitant velocity; however, no clinical signs were noted. Following an assessment of vital signs, tricuspid regurgitant velocity, electrocardiogram, serum biochemistry, hematology, urinalysis, and analysis of reported adverse events, SANGUINATE was found to be safe in stable sickle cell anemia patients. The clinical trial met its primary objective of demonstrating an acceptable safety profile for SANGUINATE in patients with sickle cell anemia. This trial established the safety of SANGUINATE at both dose levels and permitted its advance to Phase II trials.
ISSN:1516-8484
1806-0870
1806-0870
DOI:10.1016/j.bjhh.2016.08.004