Evaluation of a Novel Quantitative Test for Glucose-6-Phosphate Dehydrogenase Deficiency: Bringing Quantitative Testing for Glucose-6-Phosphate Dehydrogenase Deficiency Closer to the Patient

Sampa Pal,Maria Kahn,Sevan Hrutkay,Germana Bancone,Gornpan Gornsawun,Pooja Bansil,Cindy S Chu,Gonzalo J Domingo,François Nosten,Pimsupah Penpitchaporn

doi:10.4269/ajtmh.18-0612

Abstract

.Glucose-6-phosphate dehydrogenase (G6PD) deficiency, a common genetic blood condition, can result in kernicterus at birth, and later in life as severe hemolysis on exposure to certain infections, foods, and drugs. The unavailability of point-of-care tests for G6PD deficiency is a barrier to routine curative treatment of Plasmodium vivax malaria with 8-aminoquinolines, such as primaquine. Two quantitative reference tests (Trinity Biotech, Bray, Ireland and Pointe Scientific, Canton, MI; Cat No. G7583) and the point-of-care STANDARD™ G6PD test (SD Biosensor, Suwon, South Korea) were evaluated. The STANDARD G6PD test was evaluated at multiple temperatures, in anticoagulated venous and capillary samples, including 79 G6PD-deficient and 66 intermediate samples and across two laboratories, one in the United States and one in Thailand. The STANDARD test performed equivalently to a reference assay for its ability to diagnose G6PD deficiency (< 30% normal) with a sensitivity of 100% (0.95 confidence interval [CI]: 95.7–100) and specificity of 97% (0.95 CI: 94.5–98.5), and could reliably identify females with less than 70% normal G6PD activity with a sensitivity of 95.5% (0.95 CI: 89.7–98.5) and specificity of 97% (0.95 CI: 94.5–98.6). The STANDARD G6PD product represents an opportunity to diagnose G6PD deficiency equally for males and females in basic clinical laboratories in high- and low-resource settings. This quantitative point-of-care diagnostic test for G6PD deficiency can provide equal access to safe radical cure of P. vivax cases in high- and low-resource settings, for males and females and may support malaria elimination, in countries where P. vivax is endemic.

Highlights

Glucose-6-phosphate dehydrogenase (G6PD) is an essential enzyme that protects red blood cells from oxidative damage caused by certain drugs, diseases, and foods.[1,2] The X-linked human G6PD gene is highly polymorphic with many mutations resulting in reduced enzyme activity in red blood cells or G6PD deficiency
The STANDARD test performed equivalently to a reference assay for its ability to diagnose G6PD deficiency (< 30% normal) with a sensitivity of 100% (0.95 confidence interval [CI]: 95.7–100) and specificity of 97% (0.95 CI: 94.5–98.5), and could reliably identify females with less than 70% normal G6PD activity with a sensitivity of 95.5% (0.95 CI: 89.7–98.5) and specificity of 97% (0.95 CI: 94.5–98.6)
Area under the curve (AUC) of the receiving operating characteristic (ROC) curve was calculated at different activity thresholds to analyze clinical performance of the STANDARD G6PD test.[22]

Summary

Introduction

Glucose-6-phosphate dehydrogenase (G6PD) is an essential enzyme that protects red blood cells from oxidative damage caused by certain drugs, diseases, and foods.[1,2] The X-linked human G6PD gene is highly polymorphic with many mutations resulting in reduced enzyme activity in red blood cells or G6PD deficiency. Glucose-6-phosphate dehydrogenase deficiency presents clinically in the neonate as jaundice resulting from hyperbilirubinemia; this may lead to kernicterus, a form of brain damage.[3,4] Several medications including rasburicase- and 8-aminoquinoline–based antimalarial drugs, such as primaquine, are known to cause clinically significant hemolysis in G6PD-deficient individuals. Tafenoquine has been approved by the FDA with a different dosage for

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