Polymorphism in the mitochondrial cytochrome B gene in Koreans

Lee, Soong Deok; Lee, Yoon Seong; Lee, Jung Bin

doi:10.1007/s004140100238

Cited by 33 publications

(35 citation statements)

References 12 publications

(12 reference statements)

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“…The three sequences with this motif that appear in the Korean data of Snäll et al (2002), however, tested positively for the RFLP site +4830 HaeII (recognizing a transition at nt 4833) of haplogroup G. We additionally found the 4833 transition (confirmed by +4831 HhaI) in four mtDNAs from China (Table 2). Because all of these mtDNA sequences that belong to haplogroup G have (near-)matches with sequences sampled in Japan (Horai et al 1996;Imaizumi et al 2002;Koyama et al 2002), Korea (Pfeiffer et al 1998;Lee et al 1997Lee et al , 2002, and China (Tsai et al 2001;Yao et al 2000Yao et al , 2003a, it appears that these sequences also belong to haplogroup G. The vast majority of these HVS-I and HVS-II sequences share the 150 polymorphism. In particular, eleven HVS-I and HVS-II sequences from the Korean sample of Lee et al (1997) carry the partial motif 16223-16325; seven of them have the additional part 16362-150 of the motif, Yao et al (2003a) and the data underlying figure 1 of Mishmar et al (2003), respectively; 2 n.d. = not determined.…”

Section: Distinguishing Asian From Native American Mtdnasmentioning

confidence: 78%

Identification of Native American Founder mtDNAs Through the Analysis of Complete mtDNA Sequences: Some Caveats

Bandelt

Herrnstadt²,

Yao

et al. 2003

Annals of Human Genetics

104

116

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SummaryIn this study, a detailed analysis of both previously published and new data was performed to determine whether complete, or almost complete, mtDNA sequences can resolve the long-debated issue of which Asian mtDNAs were founder sequences for the Native American mtDNA pool. Unfortunately, we now know that coding region data and their analysis are not without problems. To obtain and report reasonably correct sequences does not seem to be a trivial task, and to discriminate between Asian and Native American mtDNA ancestries may be more complex than previously believed. It is essential to take into account the effects of mutational hot spots in both the control and coding regions, so that the number of apparent Native American mtDNA founder sequences is not erroneously inflated. As we report here, a careful analysis of all available data indicates that there is very little evidence that more than five founder mtDNA sequences entered Beringia before the Last Glacial Maximum and left their traces in the current Native American mtDNA pool.

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Section: Distinguishing Asian From Native American Mtdnasmentioning

confidence: 78%

Identification of Native American Founder mtDNAs Through the Analysis of Complete mtDNA Sequences: Some Caveats

Bandelt

Herrnstadt²,

Yao

et al. 2003

Annals of Human Genetics

104

116

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“…For this reason, forensically relevant SNPs in the coding region should be chosen to involve neutral variants. We feel that SNP assays like pyrosequencing that reveal a substantial amount of surrounding sequence variation, or the simple sequencing of coding region genes [17], will not prove wise practical choices for reasons of medical genetic privacy and ethics.…”

Section: Introductionmentioning

confidence: 99%

A multiplex allele-specific primer extension assay for forensically informative SNPs distributed throughout the mitochondrial genome

Vallone

Just

Coble

et al. 2004

International Journal of Legal Medicine

122

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The typing of single nucleotide polymorphisms (SNPs) located throughout the mitochondrial genome (mtGenome) can help resolve individuals with an identical HV1/HV2 mitotype. A set of 11 SNPs selected for distinguishing individuals of the most common Caucasian HV1/HV2 mitotype were incorporated in an allele specific primer extension assay. The assay was optimized for multiplex detection of SNPs at positions 3010, 4793, 10211, 5004, 7028, 7202, 16519, 12858, 4580, 477 and 14470 in the mtGenome. Primers were designed to allow for simultaneous PCR amplification of 11 unique regions in the mtGenome and subsequent primer extension. By enzymatically incorporating fluorescently labeled dideoxynucleotides (ddNTPs) onto the 3' end of the extension primer, detection can be accomplished with a capillary-based electrophoresis (CE) platform common in most forensic laboratories. The electrophoretic mobility for the extension primers was compared in denaturing POP4 and POP6 CE running buffers. Empirical adjustment of extension primer concentrations resulted in even signal intensity for the 11 loci probed. We demonstrate that the assay performs well for heteroplasmy and mixture detection, and for typical mtDNA casework samples with highly degraded DNA.

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“…The Korean mtDNA data presented by Lee et al (2002) bear the imprint of several erroneous combinations of the HVR-I and HVR-II sequences with the cytochrome B sequences. Some of the HVR-I and HVR-II sequences were published earlier (Lee et al 1997) but without citation in Lee et al (2002). Alarmingly, some of those recycled HVR-I and HVR-II sequences do not completely match the corresponding ones of the earlier study.…”

Section: Hvr-i Versus Hvr-iimentioning

confidence: 96%

“…Alarmingly, some of those recycled HVR-I and HVR-II sequences do not completely match the corresponding ones of the earlier study. With the present knowledge of the East Asian mtDNA phylogeny Kong et al 2003aKong et al , 2003b, one can allocate almost twothirds of the cytochrome B mutations recorded by Lee et al (2002) to specific branches of the mtDNA phylogeny. When comparing the HVR-I and HVR-II motifs with the cytochrome B motifs, we find the following mosaic types (where the first part refers to the control region and the second part to cytochrome B gene): sample F531.2 is an F1b×D4a type, sample H81 an A5×D4a type, sample H84 an M7a1×D4a type, sample H98 an A5×M type (Kong et al 2003a;Bandelt 2004), and sample H75 is an M10×Y1 type.…”

Section: Hvr-i Versus Hvr-iimentioning

confidence: 98%

Artificial recombination in forensic mtDNA population databases

Bandelt

Salas²,

Lutz-Bonengel

2004

Int J Legal Med

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Artificial recombination of two or more mitochondrial DNA fragments from different samples would constitute a serious cause of error in forensic DNA typing, and yet one can demonstrate that such events have happened in the preparation of several published mtDNA databases. Focussed database searches, phylogenetic analysis, and network representations can highlight mosaic patterns and thus pinpoint sample mix-up. Therefore, we suggest that this approach should be applied to data prior to publication in order to uncover such errors in time.

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Polymorphism in the mitochondrial cytochrome B gene in Koreans

Cited by 33 publications

References 12 publications

Identification of Native American Founder mtDNAs Through the Analysis of Complete mtDNA Sequences: Some Caveats

Identification of Native American Founder mtDNAs Through the Analysis of Complete mtDNA Sequences: Some Caveats

A multiplex allele-specific primer extension assay for forensically informative SNPs distributed throughout the mitochondrial genome

Artificial recombination in forensic mtDNA population databases

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