Severe Neonatal Metabolic Decompensation in Methylmalonic Acidemia Caused by CblD Defect

Parini, Rossella; Furlan, Francesca; Brambilla, Arianna; Codazzi, Daniela; Vedovati, Sergio; Corbetta, Carlo; Fedeli, Tiziana; Merinero, Begoña; Pérez, Belén; Ugarte, Magdalena

doi:10.1007/8904_2013_232

Cited by 12 publications

(9 citation statements)

References 13 publications

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“…Cobalamin D deficiency can either result in combined methylmalonic aciduria and homocystinuria, in isolated homocystinuria (variant 1) or in isolated MMA (variant 2). This type of isolated MMA is very rare compared to MCM deficiency and cobalamin A and B deficiency, and results in a cobalamin responsive phenotype similar to mut − and cobalamin A deficiency . MCE deficiency is also very rare and its' natural history is very variable, with asymptomatic patients, patients presenting with acute metabolic decompensations and patients having also a sepiapterin reductase deficiency .…”

Section: Metabolite Accumulation In Pa and Mmamentioning

confidence: 99%

“…This type of isolated MMA is very rare compared to MCM deficiency and cobalamin A and B deficiency, and results in a cobalamin responsive phenotype similar to mut − and cobalamin A deficiency. 11 MCE deficiency is also very rare and its' natural history is very variable, with asymptomatic patients, patients presenting with acute metabolic decompensations and patients having also a sepiapterin reductase deficiency. 12 Despite the differences between the different forms of isolated MMA, many publications assemble research data on MCM, cobalamin A and cobalamin B deficiency, and discuss isolated MMA as one disease entity.…”

Section: Metabolite Accumulation In Pa and Mmamentioning

confidence: 99%

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Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Haijes

Hasselt

Jans

et al. 2019

J of Inher Metab Disea

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Despite realizing increased survival rates for propionic acidemia (PA) and methylmalonic acidemia (MMA) patients, the current therapeutic regimen is inadequate for preventing or treating the devastating complications that still can occur. The elucidation of pathophysiology of these complications allows us to evaluate and rethink treatment strategies. In this review we display and discuss potential therapy targets and we give a systematic overview on current, experimental and unexplored treatment strategies in order to provide insight in what we have to offer PA and MMA patients, now and in the future. Evidence on the effectiveness of treatment strategies is often scarce, since none were tested in randomized clinical trials. This raises concerns, since even the current consensus on best practice treatment for PA and MMA is not without controversy. To attain substantial improvements in overall outcome, gene, mRNA or enzyme replacement therapy is most promising since permanent reduction of toxic metabolites allows for a less strict therapeutic regime. Hereby, both mitochondrial‐associated and therapy induced complications can theoretically be prevented. However, the road from bench to bedside is long, as it is challenging to design a drug that is delivered to the mitochondria of all tissues that require enzymatic activity, including the brain, without inducing any off‐target effects. To improve survival rate and quality of life of PA and MMA patients, there is a need for systematic (re‐)evaluation of accepted and potential treatment strategies, so that we can better determine who will benefit when and how from which treatment strategy.

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Section: Metabolite Accumulation In Pa and Mmamentioning

confidence: 99%

Section: Metabolite Accumulation In Pa and Mmamentioning

confidence: 99%

Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Haijes

Hasselt

Jans

et al. 2019

J of Inher Metab Disea

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“…Mutations predicted to result in a nonfunctional protein resulted in combined homocystinuria and methylmalonic aciduria (Coelho et al 2008). Subsequently identified MMADHC mutations have been consistent with this hypothesis (Miousse et al 2009;Parini et al 2013).…”

Section: Discussionmentioning

confidence: 87%

“…Mutations in the MMADHC (methylmalonic aciduria, cblD type, and homocystinuria) gene on chromosome 2q23.2 have been reported in all identified cblD patients (Coelho et al 2008;Miousse et al 2009;Parini et al 2013;Stucki et al 2011). The MMADHC protein has sequence homology with a bacterial ATP-binding cassette transporter and contains a mitochondrial targeting sequence (Coelho et al 2008).…”

Section: Discussionmentioning

confidence: 99%

“…No additional patients with the cblD disorder were reported until 2004 when Suormala et al (2004) described two patients with cblD-HC and one patient with cblD-MMA using complementation analysis. To date, eighteen cblD patients have been reported; including five patients with the classic form of the disorder, six with cblD-HC, and seven with cblD-MMA (Coelho et al 2008;Miousse et al 2009;Parini et al 2013;Stucki et al 2011). Mutations at the MMADHC gene have been shown to underlie the cblD disorder in all of these patients.…”

Section: Introductionmentioning

confidence: 99%

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Clinical, Biochemical, and Molecular Presentation in a Patient with the cblD-Homocystinuria Inborn Error of Cobalamin Metabolism

et al. 2014

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Pathophysiology of propionic and methylmalonic acidemias. Part 1: Complications

Haijes

Jans

Tas

et al. 2019

J of Inher Metab Disea

127

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Over the last decades, advances in clinical care for patients suffering from propionic acidemia (PA) and isolated methylmalonic acidemia (MMA) have resulted in improved survival. These advances were possible thanks to new pathophysiological insights. However, patients may still suffer from devastating complications which largely determine the unsatisfying overall outcome. To optimize our treatment strategies, better insight in the pathophysiology of complications is needed. Here, we perform a systematic data‐analysis of cohort studies and case‐reports on PA and MMA. For each of the prevalent and rare complications, we summarize the current hypotheses and evidence for the underlying pathophysiology of that complication. A common hypothesis on pathophysiology of many of these complications is that mitochondrial impairment plays a major role. Assuming that complications in which mitochondrial impairment may play a role are overrepresented in monogenic mitochondrial diseases and, conversely, that complications in which mitochondrial impairment does not play a role are underrepresented in mitochondrial disease, we studied the occurrence of the complications in PA and MMA in mitochondrial and other monogenic diseases, using data provided by the Human Phenotype Ontology. Lastly, we combined this with evidence from literature to draw conclusions on the possible role of mitochondrial impairment in each complication. Altogether, this review provides a comprehensive overview on what we, to date, do and do not understand about pathophysiology of complications occurring in PA and MMA and about the role of mitochondrial impairment herein.

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Severe Neonatal Metabolic Decompensation in Methylmalonic Acidemia Caused by CblD Defect

Cited by 12 publications

References 13 publications

Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Clinical, Biochemical, and Molecular Presentation in a Patient with the cblD-Homocystinuria Inborn Error of Cobalamin Metabolism

Pathophysiology of propionic and methylmalonic acidemias. Part 1: Complications

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