single-molecule late-pcr analysis of human mitochondrial genomic sequence variations单分子late-pcr人类线粒体基因组序列变化的分析.pdfVIP
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single-molecule late-pcr analysis of human mitochondrial genomic sequence variations单分子late-pcr人类线粒体基因组序列变化的分析
Single-Molecule LATE-PCR Analysis of Human
Mitochondrial Genomic Sequence Variations
Adam Osborne, Arthur H. Reis, Jr., Loren Bach, Lawrence J. Wangh*
Department of Biology, Brandeis University, Waltham, Massachusetts, United States of America
Abstract
It is thought that changes in mitochondrial DNA are associated with many degenerative diseases, including Alzheimer’s and
diabetes. Much of the evidence, however, depends on correlating disease states with changing levels of heteroplasmy
within populations of mitochondrial genomes, rather than individual mitochondrial genomes. Thus these measurements are
likely to either overestimate the extent of heteroplasmy due to technical artifacts, or underestimate the actual level of
heteroplasmy because only the most abundant changes are observable. In contrast, Single Molecule (SM) LATE-PCR analysis
achieves efficient amplification of single-stranded amplicons from single target molecules. The product molecules, in turn,
can be accurately sequenced using a convenient Dilute-‘N’-Go protocol, as shown here. Using these novel technologies we
have rigorously analyzed levels of mitochondrial genome heteroplasmy found in single hair shafts of healthy adult
individuals. Two of the single molecule sequences (7% of the samples) were found to contain mutations. Most of the
mtDNA sequence changes, however, were due to the presence of laboratory contaminants. Amplification and sequencing
errors did not result in mis-identification of mutations. We conclude that SM-LATE-PCR in combination with Dilute-‘N’-Go
Sequencing are convenient technologies for detecting infrequent mutations in mitochondrial genomes, provided great care
is taken to control and document contamination. We plan to use these technologies in the future to look for age, drug, and
disease relat
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