A case of severe glutathione synthetase deficiency with novel GSS mutations

Xia, Hongping; Ye, J; Wang, L; Zhu, Jiang; He, Zhiping

doi:10.1590/1414-431x20176853

Cited by 14 publications

(14 citation statements)

References 18 publications

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“…Multiple factors such as acetaminophen use, malnutrition, and hypothyroidism could have led to alterations in the enzymatic processes of the gamma-glutamyl pathway leading this patient to develop a 5-oxoprolinemia elevated anion gap metabolic acidosis. However, the incidence of 5-oxoprolinemia is frequently described in the literature in pediatric populations rather than adults [ 1 ]. An autosomal recessive form of glutathione synthetase deficiency that predisposes pediatric populations to develop elevated anion gap metabolic acidoses with 5-oxoprolinemia typically begins in the neonatal period and has devastating outcomes [ 1 ].…”

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

“…5-oxoprolinemia, also known as pyroglutamic acidosis, is caused by a lack of glutathione produced by the gamma-glutamyl cycle [ 1 , 2 ]. The predilection to this process is related to transient polymorphisms of multiple enzymes in the cycle occurring throughout the patient's life as well as toxic metabolic insult in the adult population [ 1 - 3 ]. The presenting symptoms usually include altered mental status and hyperventilation in the setting of elevated anion gap metabolic acidosis, but patients may also be neurologically intact if presenting early [ 1 - 2 ].…”

Section: Introductionmentioning

confidence: 99%

“…The predilection to this process is related to transient polymorphisms of multiple enzymes in the cycle occurring throughout the patient's life as well as toxic metabolic insult in the adult population [ 1 - 3 ]. The presenting symptoms usually include altered mental status and hyperventilation in the setting of elevated anion gap metabolic acidosis, but patients may also be neurologically intact if presenting early [ 1 - 2 ]. Risk factors for 5-oxoprolinemia include malnourishment, ingestion of certain medications such as acetaminophen, flucloxacillin, netilmicin, vigabatrin, and risk factors like diabetes, liver disease, and pregnancy [ 1 - 2 ].…”

Section: Introductionmentioning

confidence: 99%

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5-Oxoprolinemia in a Patient With Severe Hypothyroidism and Chronic Acetaminophen Use

Uczkowski¹,

Gundavarapu²

2023

Cureus

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5-oxoprolinemia is caused by a defect in the gamma-glutamyl pathway which can present with severe anion gap metabolic acidosis not caused by ketoacidosis, lactic acidosis, methanol/ethylene glycol ingestion, renal failure, ethanol, iron/isoniazid or salicylate ingestion. This case will describe a 59-year-old female presenting with elevated anion gap metabolic acidosis with no discernible classical cause, chronic acetaminophen use, malnourishment, and severe hypothyroidism with 5-oxoprolinemia after extensive investigation of other causes. Treatment involved correcting the acidosis with bicarbonate, IV fluid administration, oral levothyroxine and avoiding further acetaminophen use. The patient’s acidosis resolved soon after and she was counseled on the avoidance of acetaminophen in the future. This case highlights the importance of pharmacologic vigilance with everyday over-the-counter medicines such as acetaminophen and metabolic states such as hypothyroidism which can lead to tumultuous cases of metabolic acidosis. This is the first case in which we know that 5-oxoprolinemia has presented with concomitant severe hypothyroidism. Due to this patient’s course, it may have been the preceding factor for the development of her oxoprolinemia alongside her acetaminophen consumption.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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5-Oxoprolinemia in a Patient With Severe Hypothyroidism and Chronic Acetaminophen Use

Uczkowski¹,

Gundavarapu²

2023

Cureus

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“…Glutathione synthase (GSS) gene is the source of glutathione synthase enzyme, which is an essential enzyme in the biosynthesis of glutathione that acts as a cofactor for antioxidant enzymes (see figure .4). [23]…”

Section: Overviewmentioning

confidence: 99%

Polymorphisms of Genes Related to Phase-II Metabolism and the Resistance of Clopidogrel

Alkattan¹,

Alkhalifah²,

Alsalameen³

et al. 2021

Preprint

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Clopidogrel is one of the thienopyridine antiplatelet drugs commonly used as a prophylactic medication to prevent coagulation in vessels and cardiovascular events. The molecule of clopidogrel is metabolized in the liver via phase-I and phase-II metabolism pathways. The sulfenic acid clopidogrel metabolite undergoes phase-II metabolism through conjugation with glutathione by the glutathione-s-transferase (GST) to form a glutathione conjugate of clopidogrel (inactive metabolite). A glutaredoxin enzyme removes the glutathione conjugated with clopidogrel to form cis-thiol-clopidogrel. This review focused on the polymorphisms of genes related to phase-II metabolism during the clopidogrel bioactivation process. Overall, no well-controlled studies were done about the relationship between the clopidogrel bioactivation process and genes related to phase-II metabolism’s enzymes. Nevertheless, some polymorphisms of G6PD, GCLC, GCLM, GSS, GST, GSR, HK, and GLRX genes could be responsible for clopidogrel resistance due to low glutathione conjugate or glutaredoxin plasma levels. Studies needed to be concerned with the relationship between clopidogrel resistance and phase-II metabolism issues in the near future.

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