Isolated Sulfite Oxidase Deficiency: A Case Report With a Novel Mutation and Review of the Literature

Tan, Wen‐Hann; Eichler, Florian; Hoda, Sadaf; Lee, Melissa S.; Baris, Hagit N.; Hanley, Catherine; Grant, P. Ellen; Krishnamoorthy, Kalpathy S.; Shih, Vivian E.

doi:10.1542/peds.2004-1897

Cited by 131 publications

(99 citation statements)

References 44 publications

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“…Agenesis or hypoplasia of the corpus callosum was described in 5 (type A: 1; type unknown: 4) of 12 cases of MoCoD in Turkey 18 as well as in infants with ISOD 19 and was also seen in both infants in this report. Dysgenesis of the corpus callosum has a heterogeneous etiology and may be associated with metabolic disorders of organic acids, such as propionic acidemia or pyruvate dehydrogenase complex deficiency.…”

Section: Figuresupporting

confidence: 58%

Early Features in Neuroimaging of Two Siblings With Molybdenum Cofactor Deficiency

et al. 2014

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We report the features of neuroimaging within 24 hours after birth in 2 siblings with molybdenum cofactor deficiency. The first sibling was delivered by emergency cesarean section because of fetal distress and showed pedaling and crawling seizures soon after birth. Brain ultrasound revealed subcortical multicystic lesions in the frontal white matter, and brain MRI at 4 hours after birth showed restricted diffusion in the entire cortex, except for the area adjacent to the subcortical cysts. The second sibling was delivered by elective cesarean section. Cystic lesions were seen in the frontal white matter on ultrasound, and brain MRI showed low signal intensity on T1-weighted image and high signal intensity on T2-weighted image in bifrontal white matter within 24 hours after birth, at which time the infant sucked sluggishly. Clonic spasm appeared at 29 hours after birth. The corpus callosum could not be seen clearly on ultrasound or MRI in both infants. Cortical atrophy and white matter cystic lesions spread to the entire hemisphere and resulted in severe brain atrophy within ∼1 month in both infants. Subcortical multicystic lesions on ultrasound and a cortex with nonuniform, widespread, restricted diffusion on diffusion-weighted images are early features of neuroimaging in patients with molybdenum cofactor deficiency type A. Dr Higuchi instructed the doctors in charge of the 2 infants and drafted the initial manuscript; Drs Tamura and Higa were in charge of follow-up of the 2 infants at the outpatient clinic and reviewed and revised the manuscript; Dr Sugimoto was in charge of the first sibling in the NICU after admission soon after birth and reviewed and revised the manuscript; Dr Kioka analyzed the DNA obtained from the 2 patients and their family and reviewed and revised the manuscript; Dr Tsuno was in charge of the second sibling in the NICU after admission soon after birth and reviewed and revised the manuscript; Dr Yoshikawa instructed the doctors in charge of the 2 infants and reviewed and revised the manuscript; and all authors approved the final manuscript as submitted.www.pediatrics.org/cgi

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Section: Figuresupporting

confidence: 58%

Early Features in Neuroimaging of Two Siblings With Molybdenum Cofactor Deficiency

et al. 2014

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“…These severe neurological symptoms result from either point mutations in the SO protein itself (so-called isolated SO deficiency, in which only SO activity is affected), or the inability to properly produce the pyranopterindithiolate cofactor, which results in deficiencies in all Mo-containing enzymes (so-called Mo cofactor deficiency) [10][11][12]. The development of methods to clone and express human SO has revealed several different clinical point mutations that result in isolated SO deficiency [13][14][15][16]. The X-ray structure of the human SO is not yet available, although the structure of the human SO heme domain was reported [17].…”

Section: Introductionmentioning

confidence: 99%

Sulfite-oxidizing enzymes

Kappler

Enemark

2014

J Biol Inorg Chem

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Sulfite oxidizing enzymes are essential mononuclear molybdenum (Mo) proteins involved in sulfur metabolism of animals, plants and bacteria. There are three such enzymes presently known: (1) sulfite oxidase (SO) in animals, (2) SO in plants, and (3) sulfite dehydrogenase (SDH) in bacteria. X-ray crystal structures of enzymes from all three sources (chicken SO, Arabidopsis thaliana SO, and Starkeya novella SDH) show nearly identical square pyramidal coordination around the Mo atom, even though the overall structures of the proteins and the presence of additional cofactors vary. This structural information provides a molecular basis for studying the role of specific amino acids in catalysis. Animal SO catalyzes the final step in the degradation of sulfur-containing amino acids and is critical in detoxifying excess sulfite. Human SO deficiency is a fatal genetic disorder that leads to early death, and impaired SO activity is implicated in sulfite neurotoxicity. Animal SO and bacterial SDH contain both Mo and heme domains, whereas plant SO only has the Mo domain. Intraprotein electron transfer (IET) between the Mo and Fe centers in animal SO and bacterial SDH is a key step in the catalysis, which can be studied by laser flash photolysis in the presence of deazariboflavin. IET studies on animal SO and bacterial SDH clearly demonstrate the similarities and differences between these two types of sulfite oxidizing enzymes. Conformational change is involved in the IET of animal SO, in which electrostatic interactions may play a major role in guiding the docking of the heme domain to the Mo domain prior to electron transfer. In contrast, IET measurements for SDH demonstrate that IET occurs directly through the protein medium, which is distinctly different from that in animal SO. Point mutations in human SO can result in significantly impaired IET or no IET, thus rationalizing their fatal effects. The recent developments in our understanding of sulfite oxidizing enzyme mechanisms that are driven by a combination of molecular biology, rapid kinetics, pulsed electron paramagnetic resonance (EPR), and computational techniques are the subject of this review.

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“…Affected patients exhibit severe neurological abnormalities, such as microcephaly, seizures, and usually die in early childhood (Johnson and Duran 2001). Sulfite oxidase deficiency (SOD) is less frequent but clinically similar to MoCD, which renders sulfite oxidase as the most important Moco enzyme in humans (Tan et al 2005). Sulfite oxidase catalyzes the oxidation of sulfite, which is generated throughout the catabolism of sulfur-containing amino acids, to sulfate (Griffith 1987;Johnson and Duran 2001).…”

Section: Introductionmentioning

confidence: 99%

Molybdenum Cofactor Deficiency: A New HPLC Method for Fast Quantification of S-Sulfocysteine in Urine and Serum

et al. 2011

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Isolated Sulfite Oxidase Deficiency: A Case Report With a Novel Mutation and Review of the Literature

Cited by 131 publications

References 44 publications

Early Features in Neuroimaging of Two Siblings With Molybdenum Cofactor Deficiency

Early Features in Neuroimaging of Two Siblings With Molybdenum Cofactor Deficiency

Sulfite-oxidizing enzymes

Molybdenum Cofactor Deficiency: A New HPLC Method for Fast Quantification of S-Sulfocysteine in Urine and Serum

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