Comprehensive cDNA study and quantitative analysis of mutant HADHA and HADHB transcripts in a French cohort of 52 patients with mitochondrial trifunctional protein deficiency.
暂无分享,去创建一个
A. Munnich | D. Rabier | J. Saudubray | P. de Lonlay | A. Cano | F. Labarthe | T. D. de Villemeur | N. Guffon | D. Dobbelaere | M. Brivet | O. Rigal | F. Feillet | C. Acquaviva | A. Boutron | T. B. Villemeur | D. Lamireau | H. D. de Baulny | P. Lonlay | C. Vianey-Saban | H. D. Baulny
[1] Martina Mueller,et al. Outcome in six patients with mitochondrial trifunctional protein disorders identified by newborn screening. , 2010, Molecular genetics and metabolism.
[2] T. Fukao,et al. Clinical and molecular aspects of Japanese patients with mitochondrial trifunctional protein deficiency. , 2009, Molecular genetics and metabolism.
[3] H. Waterham,et al. Mitochondrial trifunctional protein deficiency with recurrent rhabdomyolysis. , 2009, Pediatric neurology.
[4] T. Fukao,et al. Study of deep intronic sequence exonization in a Japanese neonate with a mitochondrial trifunctional protein deficiency. , 2008, Molecular genetics and metabolism.
[5] C. Vianey‐Saban,et al. Partial hypoparathyroidism associated with mitochondrial trifunctional protein deficiency , 2006, European Journal of Pediatrics.
[6] Ronald J A Wanders,et al. Isolated mitochondrial long-chain ketoacyl-CoA thiolase deficiency resulting from mutations in the HADHB gene. , 2006, Clinical chemistry.
[7] F. Muntoni,et al. Biochemical, clinical and molecular findings in LCHAD and general mitochondrial trifunctional protein deficiency , 2005, Journal of Inherited Metabolic Disease.
[8] S. Liebhaber,et al. Nonsense Mutations in Close Proximity to the Initiation Codon Fail to Trigger Full Nonsense-mediated mRNA Decay* , 2004, Journal of Biological Chemistry.
[9] M. Bennett,et al. General Mitochondrial Trifunctional Protein (TFP) Deficiency as a Result of Either α- or β-Subunit Mutations Exhibits Similar Phenotypes Because Mutations in Either Subunit Alter TFP Complex Expression and Subunit Turnover , 2004, Pediatric Research.
[10] M. Bennett,et al. Molecular and phenotypic heterogeneity in mitochondrial trifunctional protein deficiency due to β‐subunit mutations , 2003 .
[11] R. Wanders,et al. Complete deficiency of mitochondrial trifunctional protein due to a novel mutation within the β-subunit of the mitochondrial trifunctional protein gene leads to failure of long-chain fatty acid β-oxidation with fatal outcome , 2003, European Journal of Pediatrics.
[12] J. Haines,et al. Uniparental disomy of chromosome 2 resulting in lethal trifunctional protein deficiency due to homozygous α‐subunit mutations , 2002, Human mutation.
[13] J. Ibdah,et al. Fetal genotypes and pregnancy outcomes in 35 families with mitochondrial trifunctional protein mutations. , 2002, American journal of obstetrics and gynecology.
[14] H. Dietz,et al. A strategy for disease gene identification through nonsense-mediated mRNA decay inhibition , 2001, Nature Biotechnology.
[15] M. Bennett,et al. Placental floor infarction complicating the pregnancy of a fetus with long-chain 3-hydroxyacyl-CoA dehydrogenase (LCHAD) deficiency. , 2001, Molecular genetics and metabolism.
[16] V. Solovyev,et al. Analysis of canonical and non-canonical splice sites in mammalian genomes. , 2000, Nucleic acids research.
[17] E. Mayatepek,et al. Diagnosis of Mitochondrial Trifunctional Protein Deficiency in a Blood Spot from the Newborn Screening Card by Tandem Mass Spectrometry and DNA Analysis , 1999, Pediatric Research.
[18] J. Ibdah,et al. A Fetal Fatty-Acid Oxidation Disorder as a Cause of Liver Disease in Pregnant Women , 1999 .
[19] T. Hashimoto,et al. Genes for the Human Mitochondrial Trifunctional Protein α- and β-Subunits Are Divergently Transcribed from a Common Promoter Region* , 1999, The Journal of Biological Chemistry.
[20] M. Hentze,et al. A Perfect Message RNA Surveillance and Nonsense-Mediated Decay , 1999, Cell.
[21] R. Wanders,et al. Mild trifunctional protein deficiency is associated with progressive neuropathy and myopathy and suggests a novel genotype-phenotype correlation. , 1998, The Journal of clinical investigation.
[22] N. Kondo,et al. Genomic and mutational analysis of the mitochondrial trifunctional protein beta-subunit (HADHB) gene in patients with trifunctional protein deficiency. , 1997, Human molecular genetics.
[23] R. Wanders,et al. Molecular basis of long-chain 3-hydroxyacyl-CoA dehydrogenase deficiency: Identification of two new mutations , 1997, Journal of Inherited Metabolic Disease.
[24] H. Heng,et al. The Genes for the α and β Subunits of the Mitochondrial Trifunctional Protein Are Both Located in the Same Region of Human Chromosome 2p23 , 1996 .
[25] J. Isaacs,et al. Maternal Acute Fatty Liver of Pregnancy Associated with Fetal Trifunctional Protein Deficiency: Molecular Characterization of a Novel Maternal Mutant Allele , 1996, Pediatric Research.
[26] R. Wanders,et al. Common missense mutation G1528C in long-chain 3-hydroxyacyl-CoA dehydrogenase deficiency. Characterization and expression of the mutant protein, mutation analysis on genomic DNA and chromosomal localization of the mitochondrial trifunctional protein alpha subunit gene. , 1996, The Journal of clinical investigation.
[27] T. Aoyama,et al. Molecular characterization of mitochondrial trifunctional protein deficiency: formation of the enzyme complex is important for stabilization of both alpha- and beta-subunits. , 1996, American journal of human genetics.
[28] M. Bennett,et al. Two alpha subunit donor splice site mutations cause human trifunctional protein deficiency. , 1995, The Journal of clinical investigation.
[29] A. Legrand,et al. Rapid Diagnosis of Long Chain and Medium Chain Fatty Acid Oxidation Disorders Using Lymphocytes , 1995, Annals of clinical biochemistry.
[30] D. Hale,et al. The molecular basis of pediatric long chain 3-hydroxyacyl-CoA dehydrogenase deficiency associated with maternal acute fatty liver of pregnancy. , 1995, Proceedings of the National Academy of Sciences of the United States of America.
[31] N. Gregersen,et al. One short well conserved region of Alu-sequences is involved in human gene rearrangements and has homology with prokaryotic chi. , 1995, Nucleic acids research.
[32] T. Aoyama,et al. Structural analysis of cDNAs for subunits of human mitochondrial fatty acid beta-oxidation trifunctional protein. , 1994, Biochemical and biophysical research communications.
[33] A. Munnich,et al. Human trifunctional protein deficiency: a new disorder of mitochondrial fatty acid beta-oxidation. , 1992, Biochemical and biophysical research communications.
[34] K. Carpenter,et al. Differential diagnosis of hydroxydicarboxylic aciduria based on release of3H2O from [9,10-3H]myristic and [9,10-3H]palmitic acids by intact cultured fibroblasts , 1992, Journal of Inherited Metabolic Disease.
[35] T Hashimoto,et al. Novel fatty acid beta-oxidation enzymes in rat liver mitochondria. II. Purification and properties of enoyl-coenzyme A (CoA) hydratase/3-hydroxyacyl-CoA dehydrogenase/3-ketoacyl-CoA thiolase trifunctional protein. , 1992, The Journal of biological chemistry.
[36] R. Wanders,et al. Long-chain 3-hydroxyacyl-CoA dehydrogenase deficiency , 1991, Journal of Inherited Metabolic Disease.
[37] Marvin B. Shapiro,et al. RNA splice junctions of different classes of eukaryotes: sequence statistics and functional implications in gene expression. , 1987, Nucleic acids research.
[38] S. Park,et al. Identification of novel mutations of the HADHA and HADHB genes in patients with mitochondrial trifunctional protein deficiency. , 2007, International journal of molecular medicine.
[39] M. Bennett,et al. Molecular and phenotypic heterogeneity in mitochondrial trifunctional protein deficiency due to beta-subunit mutations. , 2003, Human mutation.
[40] H. Heng,et al. The genes for the alpha and beta subunits of the mitochondrial trifunctional protein are both located in the same region of human chromosome 2p23. , 1996, Genomics.