Comparison of lymphoblast mitochondria from normal subjects and patients with Barth syndrome using electron microscopic tomography

Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic...

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Published in	Laboratory investigation Vol. 87; no. 1; pp. 40 - 48
Main Authors	Acehan, Devrim, Xu, Yang, Stokes, David L, Schlame, Michael
Format	Journal Article
Language	English
Published	New York Elsevier Inc 01.01.2007 Nature Publishing Group US Nature Publishing Nature Publishing Group
Subjects	Acyltransferases Biological and medical sciences Biotechnology cardiomyopathy Cardiomyopathy, Dilated - genetics Cardiomyopathy, Dilated - pathology Cell Line, Transformed - ultrastructure Child Child, Preschool electron microscopic tomography Fundamental and applied biological sciences. Psychology Genetic Diseases, X-Linked - pathology Genetic Diseases, X-Linked - ultrastructure Humans Image Processing, Computer-Assisted Imaging, Three-Dimensional Infant Investigative techniques, diagnostic techniques (general aspects) Laboratory Medicine Lymphocyte Activation Lymphocytes - ultrastructure Male Medical sciences Medicine Medicine & Public Health Microscopy, Electron Mitochondria - pathology Mitochondria - ultrastructure mitochondrial disease Mitochondrial Diseases - genetics mitochondrial ultrastructure Pathology Proteins - genetics research-article skeletal myopathy Syndrome Tomography, Optical Transcription Factors - genetics mitochondrial ultrastructure cardiomyopathy skeletal myopathy mitochondrial disease electron microscopic tomography Biotechnology Cardiomyopathy Cardiovascular disease Hemopathy Lymphoblast Enzymopathy Myocardial disease Mitochondrial disorder Osteoarticular system Barth syndrome Mitochondria Ultrastructure Heart disease Clinical biology Tomography Skeleton Human Metabolic diseases Electron microscopy Normal Genetic disease Striated muscle disease Bone Comparative study Myopathy
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ISSN	0023-6837 1530-0307
DOI	10.1038/labinvest.3700480

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Abstract	Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 and 150 nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well-aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30–150 nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space.
AbstractList	Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 nm and 150 nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased, mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30-150 nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space. Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 and 150 nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well-aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30-150 nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space.Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 and 150 nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well-aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30-150 nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space. Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 and 150 nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well-aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30–150 nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space. Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine whether this defect leads to alterations in the internal three-dimensional organization of mitochondrial membranes, we applied electron microscopic tomography to lymphoblast mitochondria from BTHS patients and controls. Tomograms were formed from 50 and 150nm sections of chemically fixed lymphoblasts and the data were used to manually segment volumes of relevant structural details. Normal lymphoblast mitochondria contained well-aligned, lamellar cristae with slot-like junctions to the inner boundary membrane. In BTHS, mitochondrial size was more variable and the total mitochondrial volume per cell increased mainly due to clusters of fragmented mitochondria inside nuclear invaginations. However, mitochondria showed reduced cristae density, less cristae alignment, and inhomogeneous cristae distribution. Three-dimensional reconstruction of BTHS mitochondria revealed zones of adhesion of the opposing inner membranes, causing obliteration of the intracrista space. We found small isolated patches of adhesion as well as extended adhesion zones, resulting in sheets of collapsed cristae packaged in multiple concentric layers. We also found large tubular structures (diameter 30-150nm) that appeared to be derivatives of the adhesion zones. The data suggest that mitochondrial abnormalities of BTHS involve adhesions of inner mitochondrial membranes with subsequent collapse of the intracristae space.Laboratory Investigation (2007) 87, 40-48. doi:10.1038/labinvest.3700480; published online 16 October 2006
Author	Xu, Yang Stokes, David L Acehan, Devrim Schlame, Michael
AuthorAffiliation	1 Skirball Institute and Department of Cell Biology, New York University School of Medicine, New York, NY, USA 2 Department of Anesthesiology, New York University School of Medicine, New York, NY, USA 3 New York Structural Biology Center, New York, NY, USA
AuthorAffiliation_xml	– name: 3 New York Structural Biology Center, New York, NY, USA – name: 1 Skirball Institute and Department of Cell Biology, New York University School of Medicine, New York, NY, USA – name: 2 Department of Anesthesiology, New York University School of Medicine, New York, NY, USA
Author_xml	– sequence: 1 givenname: Devrim surname: Acehan fullname: Acehan, Devrim organization: Skirball Institute and Department of Cell Biology, New York University School of Medicine, New York, NY, USA – sequence: 2 givenname: Yang surname: Xu fullname: Xu, Yang organization: Department of Anesthesiology, New York University School of Medicine, New York, NY, USA – sequence: 3 givenname: David L surname: Stokes fullname: Stokes, David L organization: Skirball Institute and Department of Cell Biology, New York University School of Medicine, New York, NY, USA – sequence: 4 givenname: Michael surname: Schlame fullname: Schlame, Michael email: michael.schlame@med.nyu.edu organization: Skirball Institute and Department of Cell Biology, New York University School of Medicine, New York, NY, USA
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Keywords	mitochondrial ultrastructure cardiomyopathy skeletal myopathy mitochondrial disease electron microscopic tomography Biotechnology Cardiomyopathy Cardiovascular disease Hemopathy Lymphoblast Enzymopathy Myocardial disease Mitochondrial disorder Osteoarticular system Barth syndrome Mitochondria Ultrastructure Heart disease Clinical biology Tomography Skeleton Human Metabolic diseases Electron microscopy Normal Genetic disease Striated muscle disease Bone Comparative study Myopathy
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Snippet	Barth syndrome (BTHS) is a mitochondrial disorder that is caused by mutations in the tafazzin gene, which affects phospholipid composition. To determine...
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SubjectTerms	Acyltransferases Biological and medical sciences Biotechnology cardiomyopathy Cardiomyopathy, Dilated - genetics Cardiomyopathy, Dilated - pathology Cell Line, Transformed - ultrastructure Child Child, Preschool electron microscopic tomography Fundamental and applied biological sciences. Psychology Genetic Diseases, X-Linked - pathology Genetic Diseases, X-Linked - ultrastructure Humans Image Processing, Computer-Assisted Imaging, Three-Dimensional Infant Investigative techniques, diagnostic techniques (general aspects) Laboratory Medicine Lymphocyte Activation Lymphocytes - ultrastructure Male Medical sciences Medicine Medicine & Public Health Microscopy, Electron Mitochondria - pathology Mitochondria - ultrastructure mitochondrial disease Mitochondrial Diseases - genetics mitochondrial ultrastructure Pathology Proteins - genetics research-article skeletal myopathy Syndrome Tomography, Optical Transcription Factors - genetics
Title	Comparison of lymphoblast mitochondria from normal subjects and patients with Barth syndrome using electron microscopic tomography
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