Performance of the Early Access AmpliSeq™ Mitochondrial Panel with degraded DNA samples using the Ion Torrent™ platform

Wai, Ka Tak; Barash, Mark; Gunn, Peter

doi:10.1002/elps.201700371

Cited by 13 publications

(15 citation statements)

References 54 publications

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“…On the other hand, the application of new genetic markers to the genotyping of highly degraded samples has made great progress. Single nucleotide polymorphisms (SNPs) are being studied and applied for identifying degraded DNA due to the low mutation rate and short amplicon [8] and lots of interesting work have been reported [9][10][11][12][13]. Rachel et al [14] focus on investigating highly degraded forensic samples, provided a 27 identity-testing SNPs panel with amplicon lengths smaller than 50bp.…”

Section: Introductionmentioning

confidence: 99%

An 18 Multi‐InDels panel for analysis of highly degraded forensic biological samples

Lin

Jiang

et al. 2021

Electrophoresis

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DNA genotyping from trace and highly degraded biological samples is one of the most significant challenges of forensic DNA identification. There is a lack of simple and effective methods for genotyping highly degraded samples. In this study, a multiple loci insertion/deletion polymorphisms (Multi-InDels) panel was designed for detecting 18 autosomal Multi-InDels through capillary electrophoresis (CE) with amplicon sizes no longer than 125 bp. Studies of sensitivity, degradation, and species specificity were performed and a population study was carried out using 192 samples from Han populations in Hunan province in the south of China. The combined random match probability (CMP) of these 18 Multi-InDels was 3.23 × 10 -12 and the cumulative probability of exclusion (CPE) was 0.9989, suggesting this panel could be used independently for human identification and could provide efficient supporting information for parentage testing. Complete profiles were obtained from as low as 62.5 pg of total input DNA after increasing the number of PCR cycles. Moreover, all alleles were detected from artificially highly degraded DNA after 80 min of boiling water bath treatment. This 18 Multi-InDels panel is simple, fast, and effective for the forensic analysis of highly degraded DNA.

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Section: Introductionmentioning

confidence: 99%

An 18 Multi‐InDels panel for analysis of highly degraded forensic biological samples

Lin

Jiang

et al. 2021

Electrophoresis

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“…Recently, a novel approach to mtDNA NGS through whole genome sequencing (WGS) has been developed with the Applied Biosystems™ Precision ID mtDNA Whole Genome Panel (Thermo Fisher Scientific, USA) [ 25 ]. This library preparation kit, with 162 amplicons that target the whole mtDNA, is mostly used for forensic samples, achieving reliable results in often degraded samples [ 26 , 27 , 28 , 29 ] and with low DNA input (usually 0.1 ng of genomic DNA, but 6.25 pg [ 30 ] and, very recently, 0.6 pg [ 31 ] have been reported). Despite its most common use in forensic sciences, it has also been used in a range of other applications, from worldwide lineage studies [ 32 ], to rare mtDNA differences in monozygotic twins [ 33 ].…”

Section: Introductionmentioning

confidence: 99%

From Forensics to Clinical Research: Expanding the Variant Calling Pipeline for the Precision ID mtDNA Whole Genome Panel

Cortes-Figueiredo

Carvalho

Fonseca

et al. 2021

IJMS

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Despite a multitude of methods for the sample preparation, sequencing, and data analysis of mitochondrial DNA (mtDNA), the demand for innovation remains, particularly in comparison with nuclear DNA (nDNA) research. The Applied Biosystems™ Precision ID mtDNA Whole Genome Panel (Thermo Fisher Scientific, USA) is an innovative library preparation kit suitable for degraded samples and low DNA input. However, its bioinformatic processing occurs in the enterprise Ion Torrent Suite™ Software (TSS), yielding BAM files aligned to an unorthodox version of the revised Cambridge Reference Sequence (rCRS), with a heteroplasmy threshold level of 10%. Here, we present an alternative customizable pipeline, the PrecisionCallerPipeline (PCP), for processing samples with the correct rCRS output after Ion Torrent sequencing with the Precision ID library kit. Using 18 samples (3 original samples and 15 mixtures) derived from the 1000 Genomes Project, we achieved overall improved performance metrics in comparison with the proprietary TSS, with optimal performance at a 2.5% heteroplasmy threshold. We further validated our findings with 50 samples from an ongoing independent cohort of stroke patients, with PCP finding 98.31% of TSS’s variants (TSS found 57.92% of PCP’s variants), with a significant correlation between the variant levels of variants found with both pipelines.

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“…Hyper-variable regions I and II (HV-I and HV-II, respectively) encompass most of the individual variation among samples, even those belonging to the same haplotype, and as such are considered the most informative region of the mtDNA genome [4]. However, its complete sequence comprises over 16k base pairs, and ˜75% of total reported polymorphic variants are observed in nucleotide positions located in the coding region, usually not included in forensic mtDNA examination based on limitations inherent to SS applications [5,6].…”

Section: Introductionmentioning

confidence: 99%

“…It was designed to generate small-sized amplicons and successfully allow processing of highly degraded, low-input and other challenging forensic samples. Validation studies show that robust, sensitive, efficient and reliable typing of forensic samples can be accomplished with different versions of this product, allowing its use in forensic individual identification or parentage testing [5,[15][16][17].…”

Section: Introductionmentioning

confidence: 99%

“…Adoption of proposed analytical alternatives in current forensic casework also demands protocol validation with real evidence obtained from crime scenes. Several studies [5,[15][16][17]26] have already evaluated present commercial solution (as well as posterior versions of the same product) efficiency in mock or real forensic cases with remarkable success. Some particular issues intrinsically linked to the very nature of biological evidence in criminal DNA analysis have also been addressed by several research groups regarding mtDNA evaluation, as mixture occurrence or samples presenting highly degraded DNA or DNA template low-copy numbers [5,[15][16][17]26].…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Full mtDNA genome sequencing of Brazilian admixed populations: A forensic-focused evaluation of a MPS application as an alternative to Sanger sequencing methods

Avila

Graebin

Chemale

et al. 2019

Forensic Science International: Genetics

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Performance of the Early Access AmpliSeq™ Mitochondrial Panel with degraded DNA samples using the Ion Torrent™ platform

Cited by 13 publications

References 54 publications

An 18 Multi‐InDels panel for analysis of highly degraded forensic biological samples

An 18 Multi‐InDels panel for analysis of highly degraded forensic biological samples

From Forensics to Clinical Research: Expanding the Variant Calling Pipeline for the Precision ID mtDNA Whole Genome Panel

Full mtDNA genome sequencing of Brazilian admixed populations: A forensic-focused evaluation of a MPS application as an alternative to Sanger sequencing methods

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