IN PROGRESS G6PD Gene Curation

Gene-disease assertions not curated here (add link or write note): anemia, nonspherocytic hemolytic, due to G6PD deficiency

Disease	G6PD deficiency
Inheritance	X-linked
Prevalence Possible sources Orphanet Medline Plus Genetics	Most common enzyme deficiency. 1 in 10 African American males in the US Source: https://medlineplus.gov/genetics/condition/glucose-6-phosphate-dehydrogenase-deficiency
Rapid or full curation?	Rapid Full
ClinGen / GenCC / BabySeq / HGMD / OMIM	Definitive
Clinical Validity Scoring Notes and points	Mutations in G6PD have long been known as the cause of X linked G6PD deficiency. In most cases, G6PD deficiency, the most common enzymopathy, is better described as a genetic trait rather than a disease, with an estimated over 500 million affected individuals worldwide. These individuals, individuals without a chronic affected state, only present with acute hemolytic anemia upon exposure to an exogenous oxidative stressor, such as fava beans. In contrast, there exists a subset of very rare mutations that severely disrupt the enzyme function sufficient to cause chronic nonspherocytic hemolytic anemia, which likewise can cause acute hemolytic anemia after exposure to exogenous oxidative stressors. Patients with chronic nonspherocytic hemolytic anemia (CNSHA), also referred to as class 1 variants, may require blood transfusions and often present with severe neonatal jaundice. Importantly, a decision to split chronic nonspherocytic anemia due to G6PD deficiency (class 1) from G6PD deficiency without chronic nonspherocytic hemolytic anemia was made by the general IEM GCEP and G6PD VCEP on 4/14/2023. This decision was based upon the specific phenotypic differences observed in patients with CNSHA from other G6PD patients. Additionally, the decision was made off observable differences in the underlying enzymatic function, whereby individuals with CNSHA typically have 1% to undetectable (but existing) enzymatic function that causes an insufficiency in NADPH causing hemolysis even in the presence of endogenous stressors. This curation will only classify the gene-disease relationship between G6PD and G6PD deficiency without CNSHA. The underlying disease mechanism is loss of enzymatic function. In this curation, 8 variants were scored from 7 publications (PMIDs: 8081374, 22906047, 10782016, 17653668, 30279493, 16607506, 36145477), to reach a maximum score of genetic evidence, though over 100 variants have been associated with G6PD without CNSHA (PMID:32702756). All variants are missense variants. Complete loss of function is embryonic lethal. Evidence supporting this gene-disease relationship includes case-level data and experimental data. Experimentally, this gene-disease relationship is supported by the biochemical function of G6PD, which is a rate limiting step in the pentose phosphate pathway. When G6PD enzymatic activity is significantly diminished, insufficient NADPH is produced. NADPH is crucial to reducing oxidative stressors by mediating several cellular oxidative defense lines. In the absence of NADPH, red blood cells are particularly sensitive to oxidative stressors, resulting in phenotypes such acute hemolytic anemia upon exposure to an exogenous oxidative stressor such as fava beans (PMID:32702756). Further evidence comes from a knock out HeLa cell model, where transfection of G6PD WT rescues phenotypes observed in the KO cells such as, loss of G6PD enzymatic activity, increased sensitization to oxidative stressors including hydrogen peroxide, and decreased NADPH (PMID:36243112). Finally, the gene-disease relationship is supported by a G6PD deficient mouse model. Severely deficient mice are embryonic lethal, while mice with diminished G6PD deficiency recapitulated phenotypes such as significantly decreased NADPH levels, significantly decreased G6PD enzymatic activity, increased oxidative stress, and decreases in glutathione (PMIDs:19805580). In summary G6PD is definitively associated with X linked G6PD deficiency without CNSHA. This has been repeatedly demonstrated in both the research and clinical diagnostic settings, and has been upheld over time. This classification was approved by the ClinGen General Inborn Errors of Metabolism on the meeting date 6/23/2023 (SOP Version 9). Gene Clinical Validity Standard Operating Procedures (SOP) - SOP9
Clinical Validity Points Total	Source:
Clinical Validity Classification Classifications (pts) Definitive (12pts) Strong (12pts) Moderate (7-11pts) Limited (0.1-6pts) No genetic evidence Refuted Disputed	Source:
Molecular Mechanism Mechanisms Loss of function Gain of function Dominant negative Unknown Other	Loss of function
Penetrance options Complete (100%) High (≥80%) Moderate (<80% and >20%) Low (≤20%) (list source/PMID)	Source:
Age of Onset options Congenital Pediatric Adolescent Adulthood Late adulthood (list source/PMID)
Severity Options Embryonic lethal - presence of a pathogenic variant or variants is not compatible with life. The penetrance must be complete. Severe - presence of a pathogenic variant or variant(s) results in significantly reduced fitness. The penetrance must be complete or high. Moderate - significant morbidity or mortality due to clinical features, but fitness may not be reduced, or penetrance is reduced. Mild - Presence of a variant or variant(s) is not associated with reduced fitness, no significant morbidity or mortality, and/or penetrance is low. None - presence of a variant results in no phenotype. An example is recessive disorders in which no phenotype is reported in carriers.
Clinical Features	Sources:
HPO Terms https://hpo.jax.org/app/
Gene SOPs & Notes	There are several haplotypes in G6PD: A- Haplotype: Consists of two variants NM_001042351.2:c.376A>G p.Asn126Asp and c.202G>A p.Val68Met (aka NM_000402.4:c.466A>G p.Asn156Asp and c.292G>A p.Val98Met) The two variants have different MAF in gnomAD. c.376A>G p.Asn126Asp is the variant that is shared across several haplotypes (A-, Betica, ) We may want to classify this variant as a VUS since if we ever saw it in isolation we should not report it as pathogenic. Variants have been observed to https://gnomad.broadinstitute.org/variant-cooccurrence?dataset=gnomad_r2_1&variant=X-153764217-C-T&variant=X-153763492-T-C https://www.pharmgkb.org/vip/PA166169539
Curation Summary Examples - The @GENE@ is associated with @inheritance pattern@ @condition@, which is characterized by @clinical features@ (PMIDs). - Variable expression or severity: The severity and expressivity of the disorder is highly variable, even within families. - If multiple conditions associated with the gene: It has also been associated with @inheritance pattern@ @condition@, which is characterized by @clinical features@ (PMIDs). - Limited evidence gene: The PCNA gene has been reported in individuals with early onset autosomal recessive ataxia (PMID: 33426167, 24911150), however, evidence supporting this gene-dIsease relationship is limited
Case ID, Curator name, Date, Jira ticket link

IN PROGRESS G6PD Gene Curation

G6PD deficiency

Gene SOPs & Notes