Detailed evaluation of cancer sequencing pipelines in different microenvironments and heterogeneity levels

Batuhan Kisakol, Şahin Sarihan, Mehmet Arif Ergün, Mehmet Baysan*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

1 Citation (Scopus)

Abstract

The importance of next generation sequencing (NGS) rises in cancer research as accessing this key technology becomes easier for researchers. The sequence data created by NGS technologies must be processed by various bioinformatics algorithms within a pipeline in order to convert raw data to meaningful information. Mapping and variant calling are the two main steps of these analysis pipelines, and many algorithms are available for these steps. Therefore, detailed benchmarking of these algorithms in different scenarios is crucial for the efficient utilization of sequencing technologies. In this study, we compared the performance of twelve pipelines (three mapping and four variant discovery algorithms) with recommended settings to capture single nucleotide variants. We observed significant discrepancy in variant calls among tested pipelines for different heterogeneity levels in real and simulated samples with overall high specificity and low sensitivity. Additional to the individual evaluation of pipelines, we also constructed and tested the performance of pipeline combinations. In these analyses, we observed that certain pipelines complement each other much better than others and display superior performance than individual pipelines. This suggests that adhering to a single pipeline is not optimal for cancer sequencing analysis and sample heterogeneity should be considered in algorithm optimization.

Original languageEnglish
Pages (from-to)114-126
Number of pages13
JournalTurkish Journal of Biology
Volume45
Issue number2
DOIs
Publication statusPublished - 2021

Bibliographical note

Publisher Copyright:
© TÜBİTAK.

Keywords

  • Cancer
  • Clinical bioinformatics
  • Mapping algorithms
  • Next generation sequencing
  • Variant discovery algorithms

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