Extend the Benchmarking Indel Set by Manual Review Using the Individual Cell Line Sequencing Data from the Sequencing Quality Control 2 (SEQC2) Project

Overview

Journal Sci Rep

Specialty Science

Date 2024 Mar 26

PMID 38528062

Authors

Binsheng Gong

Dan Li

Yifan Zhang

Rebecca Kusko

Samir Lababidi

Zehui Cao

Mingyang Chen

Ning Chen

Qiaochu Chen

Qingwang Chen

Jiacheng Dai

Qiang Gan

Yuechen Gao

Mingkun Guo

Gunjan Hariani

Yujie He

Wanwan Hou

He Jiang

Garima Kushwaha

Jian-Liang Li

Jianying Li

Yulan Li

Liang-Chun Liu

Ruimei Liu

Shiming Liu

Edwin Meriaux

Mengqing Mo

Mathew Moore

Tyler J Moss

Quanne Niu

Ananddeep Patel

Luyao Ren

Nedda F Saremi

Erfei Shang

Jun Shang

Ping Song

Siqi Sun

Brent J Urban

Danke Wang

Shangzi Wang

Zhining Wen

Xiangyi Xiong

Jingcheng Yang

Lihui Yin

Chao Zhang

Ruolan Zhang

Ambica Bhandari

Wanshi Cai

Agda Karina Eterovic

Dalila B Megherbi

Tieliu Shi

Chen Suo

Ying Yu

Yuanting Zheng

Natalia Novoradovskaya

Renee L Sears

Leming Shi

Wendell Jones

Weida Tong

Joshua Xu

Affiliations

Soon will be listed here.

Abstract

Accurate indel calling plays an important role in precision medicine. A benchmarking indel set is essential for thoroughly evaluating the indel calling performance of bioinformatics pipelines. A reference sample with a set of known-positive variants was developed in the FDA-led Sequencing Quality Control Phase 2 (SEQC2) project, but the known indels in the known-positive set were limited. This project sought to provide an enriched set of known indels that would be more translationally relevant by focusing on additional cancer related regions. A thorough manual review process completed by 42 reviewers, two advisors, and a judging panel of three researchers significantly enriched the known indel set by an additional 516 indels. The extended benchmarking indel set has a large range of variant allele frequencies (VAFs), with 87% of them having a VAF below 20% in reference Sample A. The reference Sample A and the indel set can be used for comprehensive benchmarking of indel calling across a wider range of VAF values in the lower range. Indel length was also variable, but the majority were under 10 base pairs (bps). Most of the indels were within coding regions, with the remainder in the gene regulatory regions. Although high confidence can be derived from the robust study design and meticulous human review, this extensive indel set has not undergone orthogonal validation. The extended benchmarking indel set, along with the indels in the previously published known-positive set, was the truth set used to benchmark indel calling pipelines in a community challenge hosted on the precisionFDA platform. This benchmarking indel set and reference samples can be utilized for a comprehensive evaluation of indel calling pipelines. Additionally, the insights and solutions obtained during the manual review process can aid in improving the performance of these pipelines.

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