Recognition and management of fatty acid oxidation defects: A series of 107 patients

Saudubray, Jean‐Marie; Martin, Delphine; Lonlay, Pascale de; Touati, Guy; Poggi-Travert, F.; Bonnet, Damien; Jouvet, Philippe; Boutron, M C; Slama, Abdelhamid; Vianey‐Saban, Christine; Bonnefont, Jean‐Paul; Rabier, Daniel; Kamoun, P.; Brivet, M.

doi:10.1023/a:1005556207210

Cited by 294 publications

(78 citation statements)

References 47 publications

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“…This difference made comparison unequal. For example, mortality in the previously reported studies was 51.2% [2], and 65.1% [3,4] and was reduced to 11.5% in the TH trial. (Table 3)…”

Section: Discussionmentioning

confidence: 95%

“…Previous reports of mortality included many more patients with the neonatal-onset form of CPT II deficiency and CACT patients and did not describe the causes of death. [2–4] The TH trial included only 1 patient with neonatal CPT II and two patients with CACT deficiency. This difference made comparison unequal.…”

Section: Discussionmentioning

confidence: 99%

“…The adjusted mortality rates were only slightly reduced from 51.2% to 45% [2] and from 65.1 % to 60 % [3,4] compared to 8% for the 49 patients in the TH trial. The mortality rate with the TH trial was significantly reduced by either analysis.…”

Section: Discussionmentioning

confidence: 99%

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Anaplerotic treatment of long-chain fat oxidation disorders with triheptanoin: Review of 15years Experience

Roe

Brunengraber

2015

Molecular Genetics and Metabolism

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Background The treatment of long-chain mitochondrial β-oxidation disorders (LC-FOD) with a low fat-high carbohydrate diet, a diet rich in medium-even-chain triglycerides (MCT), or a combination of both has been associated with high morbidity and mortality for decades. The pathological tableau appears to be caused by energy deficiency resulting from reduced availability of citric acid cycle (CAC) intermediates required for optimal oxidation of acetyl-CoA. This hypothesis was investigated by diet therapy with carnitine and anaplerotic triheptanoin (TH). Methods Fifty-two documented LC-FOD patients were studied in this investigation (age range: birth to 51 years). Safety monitoring included serial quantitative measurements of routine blood chemistries, blood levels of carnitine and acylcarnitines, and urinary organic acids. Results The average frequency of serious clinical complications were reduced from ~ 60 % with conventional diet therapy to 10 % with TH and carnitine treatment and mortality decreased from ~ 65 % with conventional diet therapy to 3.8 %. Carnitine supplementation was uncomplicated. Conclusion The energy deficiency in LC-FOD patients was corrected safely and more effectively with the triheptanoin diet and carnitine supplement than with conventional diet therapy. Safe intervention in neonates and infants will permit earlier intervention following pre-natal diagnosis or diagnosis by expanded newborn screening.

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“…This difference made comparison unequal. For example, mortality in the previously reported studies was 51.2% [2], and 65.1% [3,4] and was reduced to 11.5% in the TH trial. (Table 3)…”

Section: Discussionmentioning

confidence: 95%

Section: Discussionmentioning

confidence: 99%

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Anaplerotic treatment of long-chain fat oxidation disorders with triheptanoin: Review of 15years Experience

Roe

Brunengraber

2015

Molecular Genetics and Metabolism

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“…Several inborn nuclear DNA (nDNA) defects impair the mitochondrial function (β-oxidation of fatty acids, respiration, tricarboxylic acid cycle, etc.) causing hepatic steatosis and energy deficiency during fasting episodes [2]. Inborn nDNA or mitochondrial DNA (mtDNA) mutations can decrease mitochondrial energy production and cause mitochondrial cytopathies [3], while acquired somatic mtDNA mutations and mtDNA damage play an important role in the ageing process [4] as well as in alcohol- and drug-induced liver toxicity [5,6,7,8,9,10,11,12].…”

Section: Introductionmentioning

confidence: 99%

MnSOD Overexpression Prevents Liver Mitochondrial DNA Depletion after an Alcohol Binge but Worsens This Effect after Prolonged Alcohol Consumption in Mice

Mansouri

Tarhuni

Larosche

et al. 2010

Dig Dis

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Both acute and chronic alcohol consumption increase reactive oxygen species (ROS) formation and lipid peroxidation, whose products damage hepatic mitochondrial DNA (mtDNA). To test whether manganese superoxide dismutase (MnSOD) overexpression modulates acute and chronic alcohol-induced mtDNA lesions, transgenic MnSOD-overexpressing (TgMnSOD⁺⁺⁺) mice and wild-type (WT) mice were treated by alcohol, either chronically (7 weeks in drinking water) or acutely (single intragastric dose of 5 g/kg). Acute alcohol administration increased mitochondrial ROS formation, decreased mitochondrial glutathione, depleted and damaged mtDNA, durably increased inducible nitric oxide synthase (NOS) expression, plasma nitrites/nitrates and the nitration of tyrosine residues in complex V proteins and decreased complex V activity in WT mice. These effects were prevented in TgMnSOD⁺⁺⁺ mice. In acutely alcoholized WT mice, mtDNA depletion was prevented by tempol, a superoxide scavenger, L-NAME and 1400W, two NOS inhibitors, or uric acid, a peroxynitrite scavenger. In contrast, chronic alcohol consumption decreased cytosolic glutathione and increased hepatic iron, lipid peroxidation products and respiratory complex I protein carbonyls only in ethanol-treated TgMnSOD⁺⁺⁺ mice but not in WT mice. In chronic ethanol-fed TgMnSOD⁺⁺⁺ mice, but not WT mice, mtDNA was damaged and depleted, and the iron chelator, deferoxamine (DFO), prevented this effect. In conclusion, MnSOD overexpression prevents mtDNA depletion after an acute alcohol binge but aggravates this effect after prolonged alcohol consumption, which selectively triggers iron accumulation in TgMnSOD⁺⁺⁺ mice but not in WT mice. In the model of acute alcohol binge, the protective effects of MnSOD, tempol, NOS inhibitors and uric acid suggested a role of the superoxide anion reacting with NO to form mtDNA-damaging peroxynitrite. In the model of prolonged ethanol consumption, the protective effects of DFO suggested the role of iron reacting with hydrogen peroxide to form mtDNA-damaging hydroxyl radical.

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“…Many LCHAD deficient patients develop retinal problems, peripheral neuropathy and recurrent episodes of aching muscle pain despite avoidance of hypoglycemic episodes. Patients who are diagnosed with the cardiac phenotype are permanently exposed to the risk of unexpected death, despite therapy [90].…”

Section: Current Management Of Mtp Defectsmentioning

confidence: 99%

Mitochondrial Trifunctional Protein Defects: Molecular Basis and Novel Therapeutic Approaches

Angdisen

Moore

Cline

et al. 2005

curr drug targets immune endocr metabol disord

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Mitochondrial trifunctional protein (MTP) is a complex protein that catalyzes the last three steps of long chain fatty acid oxidation. MTP defects have emerged recently as important inborn errors of metabolism because of their clinical implications. These disorders are recessively inherited and display a spectrum of clinical phenotypes in affected children including hepatic dysfunction, cardiomyopathy, neuro-myopathy, and may cause sudden unexpected infant death if undiagnosed and untreated. Interestingly, mothers who carry fetuses with MTP defects develop life-threatening complications during pregnancy. Recently, we delineated disease-causing mutations in MTP and reported the molecular basis for the pediatric and fetal-maternal genotype-phenotype correlations.Current management of patients with MTP defects include long-term dietary therapy of fasting avoidance, low fat diet with the restriction of long chain fatty acid intake and substitution with medium chain fatty acids. The long-term outcome of patients treated by dietary modifications remains unknown. Thus, treatment that aims at correcting the metabolic defect remains the therapy of choice for this disorder. Currently, we are exploring the potential use of protein transfection domains (PTD) for treatment of these disorders. We have shown that the transactivator of transcription (TAT) peptide from the human immunodeficiency virus can deliver proteins to mitochondria. We have further developed methods to localize these proteins to mitochondria by including a mitochondrial targeting in the fusion protein construct. Finally, we have shown that the fusion protein can cross the placenta and was detectable in the fetus and newborn pups. The practical therapeutic implications of this novel approach will be discussed.

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Recognition and management of fatty acid oxidation defects: A series of 107 patients

Cited by 294 publications

References 47 publications

Anaplerotic treatment of long-chain fat oxidation disorders with triheptanoin: Review of 15years Experience

Anaplerotic treatment of long-chain fat oxidation disorders with triheptanoin: Review of 15years Experience

MnSOD Overexpression Prevents Liver Mitochondrial DNA Depletion after an Alcohol Binge but Worsens This Effect after Prolonged Alcohol Consumption in Mice

Mitochondrial Trifunctional Protein Defects: Molecular Basis and Novel Therapeutic Approaches

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