Predicting eye and hair colour in a Norwegian population using Verogen's ForenSeq™ DNA signature prep kit

Nina Mjølsnes Salvo; Kirstin Janssen; Maria Kristine Kirsebom; Olivia Strunge Meyer; Thomas Berg; Gunn-Hege Olsen

doi:10.1016/j.fsigen.2021.102620

Predicting eye and hair colour in a Norwegian population using Verogen's ForenSeq™ DNA signature prep kit

Forensic Sci Int Genet. 2022 Jan:56:102620. doi: 10.1016/j.fsigen.2021.102620. Epub 2021 Oct 24.

Authors

Nina Mjølsnes Salvo¹, Kirstin Janssen², Maria Kristine Kirsebom², Olivia Strunge Meyer³, Thomas Berg², Gunn-Hege Olsen²

Affiliations

¹ Centre for Forensic Genetics, Department of Medical Biology, Faculty of Health Sciences, UiT - The Arctic University of Norway, Norway. Electronic address: nina.mjolsnes@uit.no.
² Centre for Forensic Genetics, Department of Medical Biology, Faculty of Health Sciences, UiT - The Arctic University of Norway, Norway.
³ Section of Forensic Genetics, Department of Forensic Medicine, Faculty of Health and Medical Sciences, University of Copenhagen, Denmark.

PMID: 34735941
DOI: 10.1016/j.fsigen.2021.102620

Abstract

Prediction of eye and hair colour from DNA can be an important investigative tool in forensic cases if conventional DNA profiling fails to match DNA from any known suspects or cannot obtain a hit in a DNA database. The HIrisPlex model for simultaneous eye and hair colour predictions was developed for forensic usage. To genotype a DNA sample, massively parallel sequencing (MPS) has brought new possibilities to the analysis of forensic DNA samples. As part of an in-house validation, this study presents the genotyping and predictive performance of the HIrisPlex SNPs in a Norwegian study population, using Verogen's ForenSeq™ DNA Signature Prep Kit on the MiSeq FGx system and the HIrisPlex webtool. DNA-profiles were successfully typed with DNA input down to 125 pg. In samples with DNA input < 125 pg, false homozygotes were observed with as many as 92 reads. Prediction accuracies in terms of AUC were high for red (0.97) and black (0.93) hair colours, as well as blue (0.85) and brown (0.94) eye colours. The AUCs for blond (0.72) and brown (0.70) hair colour were considerably lower. None of the individuals was predicted to have intermediate eye colour. Therefore, the error rates of the overall eye colour predictions were 37% with no predictive probability threshold (pmax) and 26% with a probability threshold of 0.7. We also observed that more than half of the incorrect predictions were for individuals carrying the rs12913832 GG genotype. For hair colour, 65% of the individuals were correctly predicted when using the highest probability category approach. The main error was observed for individuals with brown hair colour that were predicted to have blond hair. Utilising the prediction guide approach increased the correct predictions to 75%. Assessment of phenotype-genotype associations of eye colours using a quantitative eye colour score (PIE-score), revealed that rs12913832 AA individuals of Norwegian descent had statistically significantly higher PIE-score (less brown eye colour) than individuals of non-northern European descent. To our knowledge, this has not been reported in other studies. Our study suggests that careful assessment of the target population prior to the implementation of forensic DNA phenotyping to case work is beneficial.

Keywords: Forensic DNA phenotyping; Genetic prediction; Genotyping performance; HIrisPlex; Human pigmentation; Massively parallel sequencing.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

DNA / genetics
DNA Fingerprinting
Eye Color* / genetics
Genotype
Hair Color* / genetics
Humans
Norway
Polymorphism, Single Nucleotide

Substances

DNA