Evaluating length heteroplasmy in the human mitochondrial DNA control region

被引:23
作者
Forster, Lucy [2 ]
Forster, Peter [1 ,2 ,3 ]
Gurney, Susan M. R. [4 ]
Spencer, Matthew [5 ]
Huang, Christopher [6 ]
Roehl, Arne [2 ,3 ]
Brinkmann, Bernd [7 ]
机构
[1] Univ Cambridge Churchhill Coll, Cambridge Soc Applicat Res, Cambridge CB3 0DS, England
[2] Univ Munster, Inst Legal Med, D-48149 Munster, Germany
[3] Genet Ancestor Ltd, Cambridge CB1 0AN, England
[4] Univ Cambridge, Inst Continuing Educ, Cambridge CB23 8AQ, England
[5] Univ Liverpool, Sch Environm Sci, Liverpool L69 7ZB, Merseyside, England
[6] Univ Cambridge, Physiol Lab, Cambridge CB2 3EG, England
[7] Inst Forens Genet, D-48161 Munster, Germany
来源
INTERNATIONAL JOURNAL OF LEGAL MEDICINE | 2010年 / 124卷 / 02期
关键词
C-stretch; D-loop; Displacement loop; Indel; Radioactivity; Mutagenesis; Kerala; Thorium; Monazite; MTDNA CONTROL REGION; IDENTIFICATION; SEQUENCE; REMAINS; SAMPLES; ORIGIN;
D O I
10.1007/s00414-009-0385-0
中图分类号
DF [法律]; D9 [法律]; R [医药、卫生];
学科分类号
0301 ; 10 ;
摘要
We present allelic data for three known and one new C-tract in the human mitochondrial DNA (mtDNA) control region, and we measure intergenerational mutation rates at such C-tracts. In detail, in a sample of 1,172 mtDNA sequences, we demonstrate the existence of an instability threshold of eight consecutive cytosines, at and above which the phenomenon of length heteroplasmy arises. To determine mutation rates, we draw on mtDNA sequences in up to four generations of 248 pedigrees for families living in high or low-radiation environmental conditions. The high-radiation sample gives the most conservative (fastest) mutation rate likely to be encountered in any forensic context. We find that the C-tract mutation rate is up to 6% per generation, and we observe an excess of cytosine gains over losses. Case studies and guidelines for evaluating mtDNA heteroplasmy are provided.
引用
收藏
页码:133 / 142
页数:10
相关论文
共 20 条
  • [1] SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME
    ANDERSON, S
    BANKIER, AT
    BARRELL, BG
    DEBRUIJN, MHL
    COULSON, AR
    DROUIN, J
    EPERON, IC
    NIERLICH, DP
    ROE, BA
    SANGER, F
    SCHREIER, PH
    SMITH, AJH
    STADEN, R
    YOUNG, IG
    [J]. NATURE, 1981, 290 (5806) : 457 - 465
  • [2] Consistent treatment of length variants in the human mtDNA control region: a reappraisal
    Bandelt, H. -J.
    Parson, W.
    [J]. INTERNATIONAL JOURNAL OF LEGAL MEDICINE, 2008, 122 (01) : 11 - 21
  • [3] BENDALL KE, 1995, AM J HUM GENET, V57, P248
  • [4] PRIMING OF HUMAN MITOCHONDRIAL-DNA REPLICATION OCCURS AT THE LIGHT-STRAND PROMOTER
    CHANG, DD
    CLAYTON, DA
    [J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (02) : 351 - 355
  • [5] Mitochondrial DNA CA dinucleotide repeats in Koreans: the presence of length heteroplasmy
    Chung, UH
    Lee, HY
    Yoo, JE
    Park, MJ
    Shin, KJ
    [J]. INTERNATIONAL JOURNAL OF LEGAL MEDICINE, 2005, 119 (01) : 50 - 53
  • [6] Discovery of a major D-loop replication origin reveals two modes of human mtDNA synthesis
    Fish, J
    Raule, N
    Attardi, G
    [J]. SCIENCE, 2004, 306 (5704) : 2098 - 2101
  • [7] Natural radioactivity and human mitochondrial DNA mutations
    Forster, L
    Forster, P
    Lutz-Bonengel, S
    Willkomm, H
    Brinkmann, B
    [J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2002, 99 (21) : 13950 - 13954
  • [8] FORSTER L, 2004, THESIS U MUNSTER
  • [9] Forster P., 2008, SIMULATIONS GENETICS
  • [10] IDENTIFICATION OF THE REMAINS OF THE ROMANOV FAMILY BY DNA ANALYSIS
    GILL, P
    IVANOV, PL
    KIMPTON, C
    PIERCY, R
    BENSON, N
    TULLY, G
    EVETT, I
    HAGELBERG, E
    SULLIVAN, K
    [J]. NATURE GENETICS, 1994, 6 (02) : 130 - 135
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