Genotypes and phenotypes of G6PD deficiency among Indonesian females across diagnostic thresholds of G6PD activity guiding safe primaquine therapy of latent malaria

Satyagraha, Ari Winasti; Sadhewa, Arkasha; Panggalo, Lydia Visita; Subekti, Decy; Elyazar, Iqbal; Soebianto, Saraswati; Mahpud, Nunung; Harahap, Alida; Baird, J. Kevin

doi:10.1371/journal.pntd.0009610

Cited by 7 publications

(6 citation statements)

References 45 publications

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“…The results from this study identified (i) confirmed hemizygous males with G6PD activity as low as 68% and (ii) confirmed homozygous females with G6PD activity below 80%. These observations are supported by a recent large US based study correlating percent activity against reference range [ 39 ] and a study with females in Indonesia [ 40 ]. Establishing a performance threshold for intermediates at 80% G6PD activity will result in (i) a significant lowering of the positive predictive power of the test for G6PD intermediate cases due to the lower AUC and (ii) a significantly higher proportion of females with homozygous G6PD normal alleles included in the intermediate group, if they have equivalent activity distributions to hemizygous normal males.…”

Section: Discussionsupporting

confidence: 63%

Reference and point-of-care testing for G6PD deficiency: Blood disorder interference, contrived specimens, and fingerstick equivalence and precision

et al. 2021

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Certain clinical indications and treatments such as the use of rasburicase in cancer therapy and 8-aminoquinolines for Plasmodium vivax malaria treatment would benefit from a point-of-care test for glucose-6-phosphate dehydrogenase (G6PD) deficiency. Three studies were conducted to evaluate the performance of one such test: the STANDARD™ G6PD Test (SD BIOSENSOR, South Korea). First, biological interference on the test performance was evaluated in specimens with common blood disorders, including high white blood cell (WBC) counts. Second, the test precision on fingerstick specimens was evaluated against five individuals of each, deficient, intermediate, and normal G6PD activity status. Third, clinical performance of the test was evaluated at three point-of-care settings in the United States. The test performed equivalently to the reference assay in specimens with common blood disorders. High WBC count blood samples resulted in overestimation of G6PD activity in both the reference assay and the STANDARD G6PD Test. The STANDARD G6PD Test showed good precision on multiple fingerstick specimens from the same individual. The same G6PD threshold values (U/g Hb) were applied for a semiquantitative interpretation for fingerstick- and venous-derived results. The sensitivity/specificity values (95% confidence intervals) for the test for G6PD deficiency were 100 (92.3–100.0)/97 (95.2–98.2) and 100 (95.7–100.0)/97.4 (95.7–98.5) for venous and capillary specimens, respectively. The same values for females with intermediate (> 30% to ≤ 70%) G6PD activity were 94.1 (71.3–99.9)/88.2 (83.9–91.7) and 82.4 (56.6–96.2)/87.6(83.3–91.2) for venous and capillary specimens, respectively. The STANDARD G6PD Test enables point-of-care testing for G6PD deficiency.

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Section: Discussionsupporting

confidence: 63%

Reference and point-of-care testing for G6PD deficiency: Blood disorder interference, contrived specimens, and fingerstick equivalence and precision

et al. 2021

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“…Glucose-6-phosphate dehydrogenase deficiency is one of the most common human enzyme deficiencies, affecting approximately 500 million people worldwide or 6.3% of the estimated 7.9 billion persons alive ( Cappellini and Fiorelli, 2008 ; Frank, 2005 ; Louicharoen et al., 2009 ; Luzzatto et al., 2020 ; Nkhoma et al., 2009 ; Satyagraha et al., 2021 ; WHO, 2019 ). G6PD deficiency, an X-linked recessive condition, makes RBCs more vulnerable to oxidative stress ( Cappellini and Fiorelli, 2008 ; Frank, 2005 ; Louicharoen et al., 2009 ; Satyagraha et al., 2021 ; WHO, 2019 ). G6PD is the rate-limiting enzyme of the pentose phosphate pathway, which produces NADPH that, in turn, maintains glutathione in a reduced state, thereby protecting cells from reactive oxygen species ( Ravikumar and Greenfield, 2020 ).…”

Section: Common Human Enzyme Deficienciesmentioning

confidence: 99%

ABO blood group antigens and differential glycan expression: Perspective on the evolution of common human enzyme deficiencies

Jajosky

Zheng

et al. 2023

iScience

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“…Most hemi- and homozygous individuals have G6PD activities below 30% (G6PD deficient) or above 70% to 80% of normal activity (G6PD normal) [ 36 ]. Conversely heterozygous females have enzyme activities ranging from close to 0% to almost normal activities, with activities of the majority of heterozygous females clustering around the 50% mark [ 37 ].…”

Section: G6pd Deficiencymentioning

confidence: 99%

A Review of the Current Status of G6PD Deficiency Testing to Guide Radical Cure Treatment for Vivax Malaria

et al. 2023

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Plasmodium vivax malaria continues to cause a significant burden of disease in the Asia-Pacific, the Horn of Africa, and the Americas. In addition to schizontocidal treatment, the 8-aminoquinoline drugs are crucial for the complete removal of the parasite from the human host (radical cure). While well tolerated in most recipients, 8-aminoquinolines can cause severe haemolysis in glucose-6-phosphate dehydrogenase (G6PD) deficient patients. G6PD deficiency is one of the most common enzymopathies worldwide; therefore, the WHO recommends routine testing to guide 8-aminoquinoline based treatment for vivax malaria whenever possible. In practice, this is not yet implemented in most malaria endemic countries. This review provides an update of the characteristics of the most used G6PD diagnostics. We describe the current state of policy and implementation of routine point-of-care G6PD testing in malaria endemic countries and highlight key knowledge gaps that hinder broader implementation. Identified challenges include optimal training of health facility staff on point-of-care diagnostics, quality control of novel G6PD diagnostics, and culturally appropriate information and communication with affected communities around G6PD deficiency and implications for treatment.

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Genotypes and phenotypes of G6PD deficiency among Indonesian females across diagnostic thresholds of G6PD activity guiding safe primaquine therapy of latent malaria

Cited by 7 publications

References 45 publications

Reference and point-of-care testing for G6PD deficiency: Blood disorder interference, contrived specimens, and fingerstick equivalence and precision

Reference and point-of-care testing for G6PD deficiency: Blood disorder interference, contrived specimens, and fingerstick equivalence and precision

ABO blood group antigens and differential glycan expression: Perspective on the evolution of common human enzyme deficiencies

A Review of the Current Status of G6PD Deficiency Testing to Guide Radical Cure Treatment for Vivax Malaria

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