Your search keyword '"Mitochondriopathy"' showing total 4 results

1. LYRM7 - associated complex III deficiency: A clinical, molecular genetic, MR tomographic, and biochemical study.

Author

Hempel, Maja, Kremer, Laura S., Tsiakas, Konstantinos, Alhaddad, Bader, Haack, Tobias B., Löbel, Ulrike, Feichtinger, René G., Sperl, Wolfgang, Prokisch, Holger, Mayr, Johannes A., and Santer, René

Subjects

*EXOMES, *MOLECULAR genetics, *NUCLEOTIDE sequence, *HOMOZYGOSITY, *BASE pairs, *DELETION mutation

Abstract

LYRM7 is involved in the last steps of mitochondrial complex III assembly where it acts as a chaperone for the Rieske iron‑sulfur (Fe-S) protein in the mitochondrial matrix. Using exome sequencing, we identified homozygosity for a splice site destroying 4 base pair deletion in LYRM7 in a child with recurrent lactic acidotic crises and distinct early-onset leukencephalopathy. Sanger sequencing showed variant segregation in similarly affected family members. Functional analyses revealed a reduced amount of the Rieske Fe-S protein, which was restored after re-expression of LYRM7 . Our data provide further evidence for the importance of LYRM7 for mitochondrial function and emphasize the importance of whole exome sequencing in the diagnosis of rare mitochondrial diseases. [ABSTRACT FROM AUTHOR]

Published

2017

2. Characterization of a Leber's hereditary optic neuropathy (LHON) family harboring two primary LHON mutations m.11778G > A and m.14484T > C of the mitochondrial DNA.

Author

Catarino, Claudia B., Ahting, Uwe, Gusic, Mirjana, Iuso, Arcangela, Repp, Birgit, Peters, Katrin, Biskup, Saskia, von Livonius, Bettina, Prokisch, Holger, and Klopstock, Thomas

Subjects

*LEBER'S hereditary optic atrophy, *MITOCHONDRIAL DNA, *GENETIC mutation, *OXIDATIVE phosphorylation, *MITOCHONDRIAL pathology, *THERAPEUTICS

Abstract

Leber's hereditary optic neuropathy (LHON) is an inherited mitochondrial disease that usually leads to acute or subacute bilateral central vision loss. In 95% of cases, LHON is caused by one of three primary mutations of the mitochondrial DNA (mtDNA), m.11778G > A in the MT- ND4 gene, m.14484T > C in the MT- ND6 gene, or m.3460G > A in the MT- ND1 gene. Here we characterize clinically, genetically, and biochemically a LHON family with multiple patients harboring two of these primary LHON mutations, m.11778G > A homoplasmic and m.14484T > C heteroplasmic. The unusually low male-to-female ratio of affected family members is also seen among the other patients previously reported with two primary LHON mutations m.11778G > A and m.14484T > C. While the index patient had very late onset of symptoms at 75 years and severe visual loss, her two daughters had both onset in childhood (6 and 9 years), with moderate to mild visual loss. A higher degree of heteroplasmy of the m.14484T > C mutation was found to correlate with an earlier age at onset in this family. Ours is the first LHON family harboring two primary LHON mutations where functional studies were performed in several affected family members. A more pronounced bioenergetic defect was found to correlate with an earlier age at onset. The patient with the earliest age at onset had a more significant complex I dysfunction than all controls, including the LHON patient with only the m.11778G > A mutation, suggesting a synergistic effect of the two primary LHON mutations in this patient. [ABSTRACT FROM AUTHOR]

Published

2017

3. Preliminary evidences on mitochondrial injury and impaired oxidative metabolism in breast cancer

Author

Putignani, Lorenza, Raffa, Salvatore, Pescosolido, Roberta, Rizza, Teresa, Del Chierico, Federica, Leone, Laura, Aimati, Laura, Signore, Fabrizio, Carrozzo, Rosalba, Callea, Francesco, Torrisi, Maria Rosaria, and Grammatico, Paola

Subjects

*MITOCHONDRIAL pathology, *BREAST cancer, *OXIDATIVE phosphorylation, *ADENOSINE triphosphate, *DUCTAL carcinoma, *TRANSMISSION electron microscopy, *REACTIVE oxygen species, *CYTOCHROME oxidase

Abstract

Abstract: Mitochondriopathy is emerging as a new cancer theory; however, the relevance of mitochondrial pathobiology in breast cancer has not yet been completely explored. Herein we report on altered expression levels of the oxidative phosphorylation system (OXPHOS) subunits, mitochondrial structural injury and impaired ATP content from a breast-infiltrating ductal carcinoma (IDC). With this purpose, a human mammary carcinoma (HMC-1) cell, referred to a human mammary epithelial cell (HMEC) line, was assayed for: a) OXPHOS levels by quantitative cryo-immunoelectron microscopy (CIEM) labeling; b) morphological characterization by a newly introduced damage grading (scale Mt-g1–3), calculated on the % of intact cristae carrying mitochondria; c) bioenergetic impairment by luminometric determinations of cellular ATP content and cytochemical visualization of COX activity. Drastic OXPHOS reduction was observed in HMC-1 cells for the succinate-dehydrogenase complex II SDH-B protein, while decreasing was reported for the NADH–ubiquinone oxidoreductase complex I NDUFS3 and the ubiquinol cytochrome c reductase complex III UQCRC2 subunits. A significant dropping was detected for the ATP-synthase complex V F1β protein. For the COX complex near-depletion of the mitochondrial-encoded COXI and no apparent variation of the COXIV subunits were observed. Injury grading was categorized assigning three levels of morphological damage in HMC-1 mitochondria: i) severe (4.6%), ii) moderate (23.1%), iii) slight (44.6%), corresponding to 0%, 1–50% and 51–75% of area occupied by intact cristae. ATP generation and COX activity appeared significantly reduced in HMC-1 cells. The structural damage grading here described could provide new insight on IDC mitochondrial impairment and represent hallmark in the breast cancer mitochondriopathy. [Copyright &y& Elsevier]

Published

2012

4. Fatal manifestation of a de novo ND5 mutation: Insights into the pathogenetic mechanisms of mtDNA ND5 gene defects

Author

Zhadanov, Sergey I., Grechanina, Elena Ya., Grechanina, Yulia B., Gusar, Vladislava A., Fedoseeva, Natalya P., Lebon, Sophie, Münnich, Alfred, and Schurr, Theodore G.

Subjects

*GENETIC mutation, *SYNDROMES, *GENETIC disorders, *PATHOGENIC microorganisms, *GENE expression

Abstract

Abstract: We report the de novo occurrence of a heteroplasmic 12706T→C (12705C) ND5 mutation associated with the clinical expression of fatal Leigh syndrome. Phylogenetic analysis of several cases having the 12706C mutation confirmed that this mutation occurred independently in distinctive mtDNA backgrounds. In each of these cases, the low level of heteroplasmy and the association of the mutation with a deleterious phenotype indicated that the 12706C had a primary role in the expression of LS/MELAS in its carriers. Secondary structure analysis of the ND5 protein further supported the deleterious role of the 12706C mutation, as it was found to affect a functionally significant transmembrane domain that is likely responsible for the proton-translocation function of complex I. [Copyright &y& Elsevier]

Published

2007