Evaluating the suitability of current mitochondrial DNA interpretation guidelines for multigenerational whole mitochondrial genome comparisons

, , , , , Wright, Kirsty M., & (2022) Evaluating the suitability of current mitochondrial DNA interpretation guidelines for multigenerational whole mitochondrial genome comparisons. Journal of Forensic Sciences, 67(5), pp. 1766-1775.

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Sanger sequencing of the mitochondrial DNA (mtDNA) control region was previously the only method available for forensic casework involving degraded samples from skeletal remains. The introduction of Next Generation Sequencing (NGS) has transformed genetic data generation and human identification using mtDNA. Whole mitochondrial genome (mtGenome) analysis is now being introduced into forensic laboratories around the world to analyze historical remains. Research into large pedigrees using the mtGenome is critical to evaluate currently available interpretation guidelines for mtDNA analysis, which were developed for comparisons using the control region. This study included mtGenomes from 225 individuals from the last four generations of the Norfolk Island (NI) genetic isolate pedigree consisting of 49 distinct maternal lineages. The data from these individuals were arranged into 2339 maternally related pairs separated by up to 18 meioses. Our results show that 97.3% of maternally related pairs were concordant at all nucleotide positions, resulting in the correct interpretation of “Cannot Exclude”; 2.7% of pairs produced an “Inconclusive” result, and there were no instances of false exclusion. While these results indicate that existing guidelines are suitable for multigenerational whole mtGenome analysis, we recommend caution be taken when classifying heteroplasmic changes as differences for human identification. Our data showed the classification of heteroplasmic changes as differences increases the prevalence of inconclusive identification by 6%, with false exclusions observed in 0.34% of pairs examined. Further studies of multigenerational pedigrees, however, are needed to validate mtGenome interpretation guidelines for historical case work to more fully utilize emerging advancements.

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ID Code: 234472
Item Type: Contribution to Journal (Journal Article)
Refereed: Yes
ORCID iD:
Connell, Jasmine R.orcid.org/0000-0003-4155-5750
Benton, Miles C.orcid.org/0000-0003-3442-965X
Sutherland, Heidi G.orcid.org/0000-0002-8512-1498
Haupt, Larisa M.orcid.org/0000-0002-7735-8110
Griffiths, Lyn R.orcid.org/0000-0002-6774-5475
Additional Information: Funding Information: The Norfolk Island mitochondrial analysis was supported by NHMRC grants 376608, 536518 and 1058806 (LRG). This research was also supported by infrastructure purchased with Australian Government EIF Super Science Funds as part of the Therapeutic Innovation Australia–Queensland Node project (LRG). In addition, Jasmine Connell was the recipient of an Institute of Health and Biomedical Innovation (IHBI) Queensland University of Technology (QUT) postgraduate student scholarship and Miles Benton was supported by a Corbett Postgraduate Research Grant.
Measurements or Duration: 10 pages
Keywords: DNA analysis, DNA Commission of the International Society of Forensic Genetics, heteroplasmy, historical casework, historical military identification, historical military remains, historical remains, human identification, ISFG, mitochondrial DNA interpretation guidelines, mtDNA interpretation guidelines, Scientific Working Group of DNA Analysis Methods, SWGDAM, whole mitochondrial genome, whole mtGenome
DOI: 10.1111/1556-4029.15097
ISSN: 0022-1198
Pure ID: 113754785
Divisions: Current > Research Centres > Centre for Genomics and Personalised Health
Current > QUT Faculties and Divisions > Academic Division
Current > QUT Faculties and Divisions > Faculty of Health
Current > Schools > School of Biomedical Sciences
Funding Information: The Norfolk Island mitochondrial analysis was supported by NHMRC grants 376608, 536518 and 1058806 (LRG). This research was also supported by infrastructure purchased with Australian Government EIF Super Science Funds as part of the Therapeutic Innovation Australia–Queensland Node project (LRG). In addition, Jasmine Connell was the recipient of an Institute of Health and Biomedical Innovation (IHBI) Queensland University of Technology (QUT) postgraduate student scholarship and Miles Benton was supported by a Corbett Postgraduate Research Grant.
Funding:
Copyright Owner: 2022 The Authors
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Deposited On: 09 Aug 2022 01:20
Last Modified: 24 Jul 2024 10:00