Biochemical and molecular predictors for prognosis in nonketotic hyperglycinemia

Swanson, Michael A.; Coughlin, Curtis R.; Scharer, Gunter; Szerlong, Heather; Bjoraker, Kendra; Spector, Elaine; Creadon‐Swindell, Geralyn; Mahieu, Vincent; Matthijs, Gert; Hennermann, Julia B.; Applegarth, Derek A.; Toone, Jennifer R.; Tong, Suhong; Williams, Kristina; Hove, Johan L.K. Van

doi:10.1002/ana.24485

Cited by 83 publications

(161 citation statements)

References 38 publications

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“…Our results strongly agree with a previous study that the total loss of GCS P‐protein activity causes a classic severe NKH phenotype, whereas milder phenotypes correspond to variants maintaining reduced but present activities, with the mildest phenotype observed in patients with both alleles with mutations that confer residual activity such as P23 in this study (Swanson et al., ). Data from Western blot and protein structure analysis suggest that for an important number of mutants in our series, the loss‐of‐function character could correlate with a decreased stability, thus identifying in many patients classic NKH as a conformational disease.…”

Section: Discussionsupporting

confidence: 93%

“…Relative to the wild type, GCS P‐protein activities were less than 1% in homogenates from cells expressing p.Thr146Lys, p.Leu173Pro, p.His580Tyr, p.Pro581Arg, pAla624Asp, p.Gly763Asp, p.Gly768Glu, or p.Gly994Arg, and retained measurable activities between 1% and 10% of wild type with the p.Pro267Ala, p.Arg362Cys, p.Arg373Trp, p.Leu548Pro, p.Asp866His, and p.Val905Gly variants. Homogenates from cells transfected with the variants p.Met1Ile, p.Lys376Glu, p.Arg461Trp, p.Arg790Trp, and p.Ile933Thr rendered GCS P‐protein glycine exchange activities ranging from 12% to 50% and were identified as very mild, similar to previously published data (Swanson et al., ). Due to the nature of this functional assay, far from the natural biological environment of patient's cells, it is possible that the effect of certain variants could be missed; this could be the case for p.Met1Ile, which affects the initiation start codon.…”

Section: Resultssupporting

confidence: 88%

“…This compendium of new 19 GLDC missense mutations analyzed in the context of a genotype–phenotype correlation will be helpful for clinicians when evaluating the benefit of specific interventions during the neonatal period. Patients who have at least one mutation that allows for residual enzyme activity, many of them described here, have the potential to develop attenuated NKH, and data from a sibling study indicate that early treatment improves outcome (Bjoraker et al., ; Swanson et al., ). This extended study of expressed mutations helps clinicians identify more patients with residual activity that best benefit from early treatment.…”

Section: Discussionmentioning

confidence: 92%

“…Based on a combination of CSF glycine levels, age at onset, and clinical outcome, we distinguished between attenuated NKH and severe NKH with poor developmental outcome or neonatal fatality in combination with high levels of glycine in CSF and neonatal onset (Swanson et al., ). In this study, 16 out of the 26 patients had severe NKH with an initial onset of hypotonia, apnea, myoclonic jerks, and deceased in the neonatal or early infancy period with a severe outcome.…”

Section: Resultsmentioning

confidence: 99%

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Nonketotic hyperglycinemia: Functional assessment of missense variants inGLDCto understand phenotypes of the disease

et al. 2017

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The rapid analysis of genomic data is providing effective mutational confirmation in patients with clinical and biochemical hallmarks of a specific disease. This is the case for nonketotic hyperglycinemia (NKH), a Mendelian disorder causing seizures in neonates and early-infants, primarily due to mutations in the GLDC gene. However, understanding the impact of missense variants identified in this gene is a major challenge for the application of genomics into clinical practice. Herein, a comprehensive functional and structural analysis of 19 GLDC missense variants identified in a cohort of 26 NKH patients was performed. Mutant cDNA constructs were expressed in COS7 cells followed by enzymatic assays and Western blot analysis of the GCS P-protein to assess the residual activity and mutant protein stability. Structural analysis, based on molecular modeling of the 3D structure of GCS P-protein, was also performed. We identify hypomorphic variants that produce attenuated phenotypes with improved prognosis of the disease. Structural analysis allows us to interpret the effects of mutations on protein stability and catalytic activity, providing molecular evidence for clinical outcome and disease severity. Moreover, we identify an important number of mutants whose loss-of-functionality is associated with instability and, thus, are potential targets for rescue using folding therapeutic approaches.

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Section: Discussionsupporting

confidence: 93%

Section: Resultssupporting

confidence: 88%

Section: Discussionmentioning

confidence: 92%

Section: Resultsmentioning

confidence: 99%

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Nonketotic hyperglycinemia: Functional assessment of missense variants inGLDCto understand phenotypes of the disease

et al. 2017

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“…The outcome is poor, some patients dying during the newborn period; survivors usually exhibit severe mental retardation and intractable seizures. Swanson et al 9 published biochemical and molecular predictors for prognosis in nonketotic hyperglycinemia recently. In this study of 124 patients, there were 26 patients (21%) who died in the neonatal or early infantile period.…”

Section: Discussionmentioning

confidence: 99%

Nonketotic hyperglycinemia: novel mutation in the aminomethyl transferase gene. Case report

Gençpınar¹,

Çavuşoğlu

Özbeyler

et al. 2016

Arch Argent Pediat

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Nonketotic hyperglycinemia is a rare autosomal recessively inherited metabolic disorder, caused by a deficiency in the mitochondrial glycine cleavage system. The overall incidence of nonketotic hyperglycinemia is unknown, but is higher in certain populations such as north Finland (1/12,000) and British Colombia (1/63,000). Three genes (GLDC, AMT and GCSH) are known to cause nonketotic hyperglycinemia. Mutations in the AMT gene are responsible for 20% of nonketotic hyperglycinemia cases. We describe a novel stop codon mutation (c.565C>T, p.Q189 * ) in AMT gene in a four-month male infant with nonketotic hyperglycinemia.

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GLYT1 encephalopathy: Further delineation of disease phenotype and discussion of pathophysiological mechanisms

Mademont-Soler

Casellas-Vidal

Trujillo

et al. 2020

American J of Med Genetics Pt A

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GLYT1 encephalopathy is a form of glycine encephalopathy caused by disturbance of glycine transport. The phenotypic spectrum of the disease has not yet been completely described, as only four unrelated families with the disorder have been reported to date. Common features of affected patients include neonatal hypotonia, respiratory failure, encephalopathy, myoclonic jerks, dysmorphic features, and musculoeskeletal anomalies. All reported affected patients harbor biallelic genetic variants in SLC6A9. SNP array together with Sanger sequencing were performed in a newborn with arthrogryposis and severe neurological impairment. The novel genetic variant c.997delC in SLC6A9 was detected in homozygous state in the patient. At protein level, the predicted change is p.(Arg333Alafs*3), which most probably results in a loss of protein function. The variant cosegregated with the disease in the family.A subsequent pregnancy with ultrasound anomalies was also affected. The proband presented the core phenotypic features of GLYT1 encephalopathy, but also a burst suppression pattern on the electroencephalogram, a clinical feature not previously associated with the disorder. Our results suggest that the appearance of this pattern correlates with higher cerebrospinal fluid glycine levels and cerebrospinal fluid/ plasma glycine ratios. A detailed discussion on the possible pathophysiological mechanisms of the disorder is also provided.

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Biochemical and molecular predictors for prognosis in nonketotic hyperglycinemia

Cited by 83 publications

References 38 publications

Nonketotic hyperglycinemia: Functional assessment of missense variants inGLDCto understand phenotypes of the disease

Nonketotic hyperglycinemia: Functional assessment of missense variants inGLDCto understand phenotypes of the disease

Nonketotic hyperglycinemia: novel mutation in the aminomethyl transferase gene. Case report

GLYT1 encephalopathy: Further delineation of disease phenotype and discussion of pathophysiological mechanisms

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