Materials Map

Discover the materials research landscape. Find experts, partners, networks.

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The Materials Map is an open tool for improving networking and interdisciplinary exchange within materials research. It enables cross-database search for cooperation and network partners and discovering of the research landscape.

The dashboard provides detailed information about the selected scientist, e.g. publications. The dashboard can be filtered and shows the relationship to co-authors in different diagrams. In addition, a link is provided to find contact information.

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Materials Map under construction

The Materials Map is still under development. In its current state, it is only based on one single data source and, thus, incomplete and contains duplicates. We are working on incorporating new open data sources like ORCID to improve the quality and the timeliness of our data. We will update Materials Map as soon as possible and kindly ask for your patience.

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in Cooperation with on an Cooperation-Score of 37%

Topics

Publications (1/1 displayed)

  • 2003Accumulation of Mitochondrial DNA Mutations in Human Immunodeficiency Virus-Infected Patients Treated with Nucleoside-Analogue Reverse-Transcriptase Inhibitors81citations

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Chart of shared publication
Hammond, E.
1 / 1 shared
Martin, A. M.
1 / 1 shared
Pace, C.
1 / 2 shared
Mallal, S.
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Christiansen, Frank
1 / 1 shared
Taylor, L.
1 / 1 shared
Boer, M. Den
1 / 1 shared
Martinez, Olga
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2003

Co-Authors (by relevance)

  • Hammond, E.
  • Martin, A. M.
  • Pace, C.
  • Mallal, S.
  • Christiansen, Frank
  • Taylor, L.
  • Boer, M. Den
  • Martinez, Olga
OrganizationsLocationPeople

article

Accumulation of Mitochondrial DNA Mutations in Human Immunodeficiency Virus-Infected Patients Treated with Nucleoside-Analogue Reverse-Transcriptase Inhibitors

  • Hammond, E.
  • Martin, A. M.
  • Pace, C.
  • Nolan, D.
  • Mallal, S.
  • Christiansen, Frank
  • Taylor, L.
  • Boer, M. Den
  • Martinez, Olga
Abstract

Nucleoside reverse-transcriptase inhibitor (NRTI) therapy for human immunodeficiency virus (HIV) infection has been associated with mitochondrial DNA (mtDNA) polymerase-γ inhibition and subsequent mtDNA depletion. Effects on mtDNA mutation, although suggested by critical involvement of polymerase-γ in DNA-repair reactions, are unknown. In the present study, we assessed the nature and frequency of mitochondrial genome sequence differences in peripheral-blood samples taken prior to NRTI therapy and after 6–77 mo of treatment in 16 NRTI-treated patients. Samples from 10 HIV-infected, treatment-naive control individuals were taken at similar time intervals. Single-stranded conformation polymorphism (SSCP) and DNA-sequencing analysis techniques were used to detect mitochondrial genome sequence variants between paired longitudinal samples, and heteroplasmic populations were quantified after cloning and repeat SSCP/sequencing. Of 16 individuals treated with NRTIs, 5 exhibited altered SSCP profiles associated with the development of novel heteroplasmic DNA sequence changes, whereas no SSCP pattern change within these regions was observed in the control individuals. Heteroplasmic sequence changes were distributed across four regions of the genome: the noncoding region to 12S ribosomal RNA, reduced-nicotinamide-adenine-dinucleotide dehydrogenase 1, and cytochrome oxidase subunits I and III. Of the total of 26 patients who were examined in the present study, 4 of 5 patients with detectable mtDNA sequence changes since commencement of therapy developed evidence of peripheral fat wasting (lipoatrophy) between sample intervals (P=.031). One patient, without detectable sequence changes on NRTI therapy, also developed lipoatrophy. Levels of mtDNA copies/cell in blood samples were determined by quantitative PCR for 11 of the 16 NRTI-exposed patients; 7 of these 11 patients showed reduced levels of mtDNA in blood after therapy, including all 3 patients tested with evidence of mtDNA sequence changes on therapy. These data indicate that NRTI therapy provides conditions permissive for the development of peripheral-blood mtDNA mutations in vivo.

Topics