Using simulated microhaplotype genotyping data to evaluate the value of machine learning algorithms for inferring DNA mixture contributor numbers

Haoyu Wang; Qiang Zhu; Yuguo Huang; Yueyan Cao; Yuhan Hu; Yifan Wei; Yuting Wang; Tingyun Hou; Tiantian Shan; Xuan Dai; Xiaokang Zhang; Yufang Wang; Ji Zhang

doi:10.1016/j.fsigen.2024.103008

Using simulated microhaplotype genotyping data to evaluate the value of machine learning algorithms for inferring DNA mixture contributor numbers

Forensic Sci Int Genet. 2024 Mar:69:103008. doi: 10.1016/j.fsigen.2024.103008. Epub 2024 Jan 9.

Authors

Haoyu Wang¹, Qiang Zhu¹, Yuguo Huang¹, Yueyan Cao¹, Yuhan Hu¹, Yifan Wei¹, Yuting Wang¹, Tingyun Hou¹, Tiantian Shan¹, Xuan Dai¹, Xiaokang Zhang¹, Yufang Wang², Ji Zhang³

Affiliations

¹ West China School of Basic Medical Sciences & Forensic Medicine, Sichuan University, China.
² West China School of Basic Medical Sciences & Forensic Medicine, Sichuan University, China. Electronic address: wangyufang@scu.edu.cn.
³ West China School of Basic Medical Sciences & Forensic Medicine, Sichuan University, China. Electronic address: zhangj@scu.edu.cn.

PMID: 38244524
DOI: 10.1016/j.fsigen.2024.103008

Abstract

Inferring the number of contributors (NoC) is a crucial step in interpreting DNA mixtures, as it directly affects the accuracy of the likelihood ratio calculation and the assessment of evidence strength. However, obtaining the correct NoC in complex DNA mixtures remains challenging due to the high degree of allele sharing and dropout. This study aimed to analyze the impact of allele sharing and dropout on NoC inference in complex DNA mixtures when using microhaplotypes (MH). The effectiveness and value of highly polymorphic MH for NoC inference in complex DNA mixtures were evaluated through comparing the performance of three NoC inference methods, including maximum allele count (MAC) method, maximum likelihood estimation (MLE) method, and random forest classification (RFC) algorithm. In this study, we selected the top 100 most polymorphic MH from the Southern Han Chinese (CHS) population, and simulated over 40 million complex DNA mixture profiles with the NoC ranging from 2 to 8. These profiles involve unrelated individuals (RM type) and related pairs of individuals, including parent-offspring pairs (PO type), full-sibling pairs (FS type), and second-degree kinship pairs (SE type). Our results indicated that how the number of detected alleles in DNA mixture profiles varied with the markers' polymorphism, kinship's involvement, NoC, and dropout settings. Across different types of DNA mixtures, the MAC and MLE methods performed best in the RM type, followed by SE, FS, and PO types, while RFC models showed the best performance in the PO type, followed by RM, SE, and FS types. The recall of all three methods for NoC inference were decreased as the NoC and dropout levels increased. Furthermore, the MLE method performed better at low NoC, whereas RFC models excelled at high NoC and/or high dropout levels, regardless of the availability of a priori information about related pairs of individuals in DNA mixtures. However, the RFC models which considered the aforementioned priori information and were trained specifically on each type of DNA mixture profiles, outperformed RFC_ALL model that did not consider such information. Finally, we provided recommendations for model building when applying machine learning algorithms to NoC inference.

Keywords: Complex DNA mixtures; Inference of the number of contributors; Machine learning; Microhaplotypes.

Publication types

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

MeSH terms

Algorithms*
DNA / genetics
DNA Fingerprinting* / methods
Genotype
Humans
Machine Learning

Substances

DNA