2013
DOI: 10.4269/ajtmh.12-0682
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An In vivo Drug Screening Model Using Glucose-6-Phosphate Dehydrogenase Deficient Mice to Predict the Hemolytic Toxicity of 8-Aminoquinolines

Abstract: Abstract. Anti-malarial 8-aminoquinolines drugs cause acute hemolytic anemia in individuals with glucose-6-phosphate dehydrogenase deficiency (G6PDD). Efforts to develop non-hemolytic 8-aminoquinolines have been severely limited caused by the lack of a predictive in vivo animal model of hemolytic potential that would allow screening of candidate compounds. This report describes a G6PDD mouse model with a phenotype closely resembling the G6PDD phenotype found in the African A-type G6PDD human. These G6PDD mice,… Show more

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Cited by 9 publications
(8 citation statements)
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“…Large inter- and intra-individual variation was also observed in reticulocyte counts without consistent differences between PQ-treated and non-treated individuals or between G6PDd and G6PD-normal individuals. Reticulocytosis is potentially an important marker for acute hemolysis and reticulocyte counts were elevated following various doses of PQ in an in vivo drug screening model using G6PDd mice [ 46 ]. We aimed to obtain further insights in hemolysis after PQ by measuring LDH, released from hemolysed red blood cells, and haptoglobin, which binds to hemoglobin released during intravascular or extravascular hemolysis.…”
Section: Discussionmentioning
confidence: 99%
“…Large inter- and intra-individual variation was also observed in reticulocyte counts without consistent differences between PQ-treated and non-treated individuals or between G6PDd and G6PD-normal individuals. Reticulocytosis is potentially an important marker for acute hemolysis and reticulocyte counts were elevated following various doses of PQ in an in vivo drug screening model using G6PDd mice [ 46 ]. We aimed to obtain further insights in hemolysis after PQ by measuring LDH, released from hemolysed red blood cells, and haptoglobin, which binds to hemoglobin released during intravascular or extravascular hemolysis.…”
Section: Discussionmentioning
confidence: 99%
“…The mouse has a splicing mutation in the G6PD gene (Sanders et al , 1997 ), and it has been used extensively to investigate the possible role of G6PD with respect to cardiovascular disorders (Matsui et al , 2006 ). It appeared that this mutant mouse did not develop drug-induced AHA [(personal communication from the late Ulrich Bienzle of the Institute of Tropical Medicine, Berlin)]; however, very recently Zhang et al ( 2013 ) have achieved AHA in these mice by administering PQ, although at much higher doses (per body weight) than are used therapeutically in humans. Thus, it appears that an outright knock-out of G6PD is too drastic, whereas in the available mutant mice G6PD deficiency is rather mild.…”
Section: Management and Prevention Of G6pd-related Ahamentioning
confidence: 99%
“…Some studies suggest that HCQ can be safely administered in the setting of G6PD deficiency [ 2 , 3 ]. In a retrospective chart review of 275 rheumatology patients taking HCQ chronically, 11 African American patients with G6PD deficiency were evaluated through 700 months of therapy, without evident complications [ 2 ].…”
Section: Introductionmentioning
confidence: 99%
“…In a retrospective chart review of 275 rheumatology patients taking HCQ chronically, 11 African American patients with G6PD deficiency were evaluated through 700 months of therapy, without evident complications [ 2 ]. Additionally, chloroquine did not induce hemolysis in a heterozygote knock-out murine model of G6PD deficiency with 14% residual enzyme activity [ 3 ]; however, the model’s specific hypomorphic mutation is not present in humans.…”
Section: Introductionmentioning
confidence: 99%