Abstract
BACKGROUND: Calling structural variants (SVs), i.e., genomic alterations of ≥50bp, from whole genome short-read data remains challenging, as existing callers are known to lack accuracy and robustness. Therefore, meta-caller approaches combining the results of multiple standalone tools in a consensus set of reported SV calls, are widely used. Here, SV-MeCa (Structural Variant Meta-Caller) is presented, the first SV meta-caller incorporating variant-specific quality metrics from individual VCF outputs, rather than relying solely on number and combination of tools supporting consensus SV calls. In addition, SV-MeCa offers a suitable score to rank obtained consensus SV calls according to evidence of representing true positive calls, i.e., real-world variants. RESULTS: SV-MeCa applies seven standalone SV callers and merges resulting deletion and insertion calls into a union VCF file using SURVIVOR. For each entry in the SURVIVOR-generated consensus, caller-specific quality measures are extracted from corresponding standalone VCF files, and serve as input for an either deletion- or insertion-specific XGBoost decision tree classifier, which was previously trained on the HG002 SV benchmark data provided by the Genome in a Bottle consortium. The SV-MeCa XGBoost models assign a probability to (consensus) SV calls to represent true positive calls, which can be used for ranking the final output according to evidence. Performance of SV-MeCa and four previously published meta-caller approaches were evaluated based on autosomal SV calls in samples curated by the Human Genome Structural Variation Consortium, Phase 2. With regard to F[Formula: see text] scores, which were 0.58 on average for deletions and 0.42 on average for insertions, SV-MeCa outperformed the other meta-callers. With regard to precision, only ConsensuSV achieved higher values (0.97 versus 0.64 on average for deletions, 0.75 versus 0.53 on average for insertions), and with regard to recall, SV-MeCa was outperformed exclusively by Meta-SV for deletions (0.55 versus 0.53). CONCLUSIONS: SV-MeCa, publicly available at https://github.com/ccfboc-bioinformatics/SV-MeCa , outperforms existing SV meta-caller approaches by taking variant-specific quality measures into account. Moreover, due to the XGBoost prediction probabilities serving as scores, the output of SV-MeCa can be continuously adjusted to user needs in terms of sensitivity and precision.