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Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa

South Africa faces grave challenges with high crime rates and associated unidentified bodies each year. DNA profiling using capillary electrophoresis (CE) is typically utilised for human identification purposes but is limiting when applied to degraded post-mortem samples. The ForenSeqTM DNA Signatur...

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Main Author: Martin, Donna-Lee
Other Authors: Heathfield, Laura
Format: Thesis
Language:English
English
Published: Department of Pathology 2025
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access_status_str Open Access
author Martin, Donna-Lee
author2 Heathfield, Laura
author_browse Heathfield, Laura
Martin, Donna-Lee
author_facet Heathfield, Laura
Martin, Donna-Lee
author_sort Martin, Donna-Lee
collection Thesis
description South Africa faces grave challenges with high crime rates and associated unidentified bodies each year. DNA profiling using capillary electrophoresis (CE) is typically utilised for human identification purposes but is limiting when applied to degraded post-mortem samples. The ForenSeqTM DNA Signature Prep kit was the first massively parallel sequencing (MPS) workflow validated on the MiSeq FGxTM system, addressing several challenges identified in CE-based methods. With forensic laboratories in developing regions showing proclivity towards a seemingly impossible adoption of MPS, sequence-based studies in Africa are sorely needed to leverage emerging advancements for forensic human identification. This study proposed a four-phased approach for laboratories to facilitate the implementation of MPS for forensic human identification, and included: optimisation, population data generation, internal validation and demonstration of applicability. An optimisation study was carried out to ensure high first-time success rates of analysing reference samples (crude buccal swab lysates) with the ForenSeqTM DNA Signature Prep kit. This entailed systematic adjustments to a direct PCR approach and the development of a lysate purification method. This optimised approach was subsequently used to conduct a population study comprising 463 consenting South African volunteers, wherein the first sequence-based allele frequency data pertaining to autosomal short tandem repeat (A-STR) markers were generated for South African populations. Rich variation was observed, where 80 novel allele sequences were recorded. An increase of 86% was observed in length- to sequence-based allele counts across several A-STR markers, with additional variation recorded in flanking regions. Furthermore, a concordance rate exceeding 99% was achieved. The novel findings and abundance of variation observed in the South African population surpasses that which has been previously characterised on a global scale, warranting further research into characterising sequence data for other forensically relevant markers. The final facet of this study involved the internal validation of the optimised MPS workflow, from sample preparation to sequencing. The workflow was deemed fit for purpose and reported the first performance parameters for post-mortem crude buccal swab lysates. The validated workflow was then applied to a forensic cold case to generate investigative leads from a severely decomposed body, demonstrating the comprehensive capability of the workflow. The synthesis of results obtained in this study have led to key recommendations for under-resourced laboratories to maximise resources for large-scale studies.
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institution University of Cape Town (South Africa)
language English
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last_indexed 2026-06-10T12:34:38.153Z
license_str Not specified — see source repository
provenance_str_mv Harvested via OAI-PMH from UCTD — University of Cape Town Open Access Repository
publishDate 2025
publishDateRange 2025
publishDateSort 2025
publisher Department of Pathology
publisherStr Department of Pathology
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source_str UCTD — University of Cape Town Open Access Repository
spelling oai:open.uct.ac.za:11427/41765 Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa Martin, Donna-Lee Heathfield, Laura DNA South Africa South Africa faces grave challenges with high crime rates and associated unidentified bodies each year. DNA profiling using capillary electrophoresis (CE) is typically utilised for human identification purposes but is limiting when applied to degraded post-mortem samples. The ForenSeqTM DNA Signature Prep kit was the first massively parallel sequencing (MPS) workflow validated on the MiSeq FGxTM system, addressing several challenges identified in CE-based methods. With forensic laboratories in developing regions showing proclivity towards a seemingly impossible adoption of MPS, sequence-based studies in Africa are sorely needed to leverage emerging advancements for forensic human identification. This study proposed a four-phased approach for laboratories to facilitate the implementation of MPS for forensic human identification, and included: optimisation, population data generation, internal validation and demonstration of applicability. An optimisation study was carried out to ensure high first-time success rates of analysing reference samples (crude buccal swab lysates) with the ForenSeqTM DNA Signature Prep kit. This entailed systematic adjustments to a direct PCR approach and the development of a lysate purification method. This optimised approach was subsequently used to conduct a population study comprising 463 consenting South African volunteers, wherein the first sequence-based allele frequency data pertaining to autosomal short tandem repeat (A-STR) markers were generated for South African populations. Rich variation was observed, where 80 novel allele sequences were recorded. An increase of 86% was observed in length- to sequence-based allele counts across several A-STR markers, with additional variation recorded in flanking regions. Furthermore, a concordance rate exceeding 99% was achieved. The novel findings and abundance of variation observed in the South African population surpasses that which has been previously characterised on a global scale, warranting further research into characterising sequence data for other forensically relevant markers. The final facet of this study involved the internal validation of the optimised MPS workflow, from sample preparation to sequencing. The workflow was deemed fit for purpose and reported the first performance parameters for post-mortem crude buccal swab lysates. The validated workflow was then applied to a forensic cold case to generate investigative leads from a severely decomposed body, demonstrating the comprehensive capability of the workflow. The synthesis of results obtained in this study have led to key recommendations for under-resourced laboratories to maximise resources for large-scale studies. 2025-09-11T10:14:50Z 2025-09-11T10:14:50Z 2025 2025-09-11T09:33:16Z Thesis / Dissertation Doctoral PhD http://hdl.handle.net/11427/41765 en eng application/pdf Department of Pathology Faculty of Health Sciences University of Cape Town
spellingShingle DNA
South Africa
Martin, Donna-Lee
Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
thesis_degree_str Doctoral
title Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
title_full Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
title_fullStr Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
title_full_unstemmed Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
title_short Investigation into implementing a massively parallel sequencing workflow for forensic human identification in South Africa
title_sort investigation into implementing a massively parallel sequencing workflow for forensic human identification in south africa
topic DNA
South Africa
url http://hdl.handle.net/11427/41765
work_keys_str_mv AT martindonnalee investigationintoimplementingamassivelyparallelsequencingworkflowforforensichumanidentificationinsouthafrica