10.26091/ESRNZ.7963997.v1 Tamyra Moretti Tamyra Moretti Rebecca Just Rebecca Just Susannah C. Kehl Susannah C. Kehl Leah E. Willis Leah E. Willis John S. Buckleton John S. Buckleton Jo-Anne Bright Jo-Anne Bright Duncan Taylor Duncan Taylor Anthony J. Onorato Anthony J. Onorato Internal validation of STRmix (TM) for the interpretation of single source and mixed DNA profiles Institute of Environmental Science and Research 2019 STRs DNA Mixtures Probabilistic Genotyping Likelihood Ratios STRmix Forensic Biology 2019-04-10 04:02:26 Online resource https://research.esr.cri.nz/articles/online_resource/Internal_validation_of_STRmix_TM_for_the_interpretation_of_single_source_and_mixed_DNA_profiles/7963997 The interpretation of DNA evidence can entail analysis of challenging STR typing results. Genotypes inferred from low quality or quantity specimens, or mixed DNA samples originating from multiple contributors, can result in weak or inconclusive match probabilities when a binary interpretation method and necessary thresholds (such as a stochastic threshold) are employed. Probabilistic genotyping approaches, such as fully continuous methods that incorporate empirically determined biological parameter models, enable usage of more of the profile information and reduce subjectivity in interpretation. As a result, software-based probabilistic analyses tend to produce more consistent and more informative results regarding potential contributors to DNA evidence. Studies to assess and internally validate the probabilistic genotyping software STRmix (TM) for casework usage at the Federal Bureau of Investigation Laboratory were conducted using lab-specific parameters and more than 300 single-source and mixed contributor profiles. Simulated forensic specimens, including constructed mixtures that included DNA from two to five donors across a broad range of template amounts and contributor proportions, were used to examine the sensitivity and specificity of the system via more than 60,000 tests comparing hundreds of known contributors and non-contributors to the specimens. Conditioned analyses, concurrent interpretation of amplification replicates, and application of an incorrect contributor number were also performed to further investigate software performance and probe the limitations of the system. In addition, the results from manual and probabilistic interpretation of both prepared and evidentiary mixtures were compared. The findings support that STRmix (TM) is sufficiently robust for implementation in forensic laboratories, offering numerous advantages over historical methods of DNA profile analysis and greater statistical power for the estimation of evidentiary weight, and can be used reliably in human identification testing. With few exceptions, likelihood ratio results reflected intuitively correct estimates of the weight of the genotype possibilities and known contributor genotypes. This comprehensive evaluation provides a model in accordance with SWGDAM recommendations for internal validation of a probabilistic genotyping system for DNA evidence interpretation.