Establishing reference samples for detection of somatic mutations and germline variants with NGS technologies

Fang, Li Tai; Zhu, Bin; Zhao, Yongjiu; Chen, W.; Yang, Zujun; Kerrigan, Liz; Langenbach, Kurt J.; Mars, Maryellen de; Lu, Charles; Idler, Kenneth B.; Jacob, Howard J.; Yu, Yangli; Ren, Liang; Zheng, Yuanting; Jaeger, Erich B.; Schroth, Gary P.; Abaan, Ogan D.; Lack, Justin; Shen, T-W; Talsania, Keyur; Chen, Z.; Stanbouly, Seta; Shetty, Jyoti; Tran, Bao; Meerzaman, Daoud; Nguyen, Cu; Petitjean, Virginie; Sultan, Marc; Cam, Margaret C.; Hung, Tiffany; Peters, Eric; Kalamegham, Rasika; Sahraeian, Sayed Mohammad Ebrahim; Mohiyuddin, Marghoob; Guo, Yunfei; Yao, Lijing; Song, Lei; Lam, Hugo Y. K.; Drábek, Jir̆ı́; Maestro, Roberta; Gasparotto, Daniela; Kõks, Sulev; Reimann, Ene; Scherer, Andreas; Nordlund, Jessica; Liljedahl, Ulrika; Jensen, Roderick V.; Pirooznia, Mehdi; Li, Zhimin; Xiao, Chunlin; Sherry, Stephen T.; Kusko, Rebecca; Moos, Malcolm; Donaldson, Eric F.; Težak, Živana; Li, J.; Duerken-Hughes, Penelope; Hong, Huixiao; Shi, Leming; Wang, C.; Xiao, Wenming

doi:10.1101/625624

Cited by 9 publications

(18 citation statements)

References 27 publications

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“…For full-spectrum analysis of the somatic mutation detection problem, we used the first comprehensive whole-genome characterized reference tumor-normal paired breast cancer cell lines (HCC1395 and HCC1395BL), developed by the Somatic Mutation Working Group of the SEQC-II consortium 12,13 . We leveraged high-confidence somatic mutations (39,536 SNVs and 2,020 INDELs) derived by the consortium as our ground truth set ( Suppl.…”

Section: Resultsmentioning

confidence: 99%

“…We used several different training models in our analysis. First, we used the already available model published recently 11 which was trained using in silico spike-ins from the DREAM Challenge Stage 3 dataset 13 . Despite the large discrepancy between the sample types, sequencing platforms, coverages, spike-in mutation frequencies, and heterogeneity of the samples used to train the DREAM3 model, this model outperformed other conventional techniques across the real cancer datasets of diverse characteristics by more than ∼4% by the mean F1-score averaged across different samples for both SNVs and INDELs ( Figure 1a ).…”

Section: Resultsmentioning

confidence: 99%

“…We used the SEQC-II reference matched samples, a human triple-negative breast cancer cell line (HCC1395) and a matched B lymphocyte derived normal cell line (HCC1395BL) in our analysis. Detailed sample information can be found in the SEQC-II reference samples manuscripts 12,13 . The SEQC-II somatic mutation working group has established a gold standard truth set of somatic mutations for these samples 13 ( Suppl.…”

Section: Methodsmentioning

confidence: 99%

“…Detailed sample information can be found in the SEQC-II reference samples manuscripts 12,13 . The SEQC-II somatic mutation working group has established a gold standard truth set of somatic mutations for these samples 13 ( Suppl. Figure 1 ).…”

Section: Methodsmentioning

confidence: 99%

“…Recently, the Somatic Mutation Working Group in the FDA-led Sequencing Quality Control Phase II (SEQC-II) consortium developed reference matched tumor-normal samples: a human triple-negative breast cancer cell line (HCC1395) and a matched B lymphocyte derived normal cell line (HCC1395BL) 12,13 . Using orthogonal sequencing technologies, multiple sequencing replicates, and multiple bioinformatics analysis pipelines, the SEQC-II consortium has developed a well-defined “Gold Set” of somatic Single Nucleotide Variants (SNVs) and insertion/deletions (INDELs) for HCC1395.…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Robust Cancer Mutation Detection with Deep Learning Models Derived from Tumor-Normal Sequencing Data

Sahraeian

Fang

Mohiyuddin

et al. 2019

Preprint

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Accurate detection of somatic mutations is challenging but critical to the understanding of cancer formation, progression, and treatment. We recently proposed NeuSomatic, the first deep convolutional neural network based somatic mutation detection approach and demonstrated performance advantages on in silico data. In this study, we used the first comprehensive and well-characterized somatic reference samples from the SEQC-II consortium to investigate best practices for utilizing deep learning framework in cancer mutation detection. Using the high-confidence somatic mutations established for these reference samples by the consortium, we identified strategies for building robust models on multiple datasets derived from samples representing real scenarios. The proposed strategies achieved high robustness across multiple sequencing technologies such as WGS, WES, AmpliSeq target sequencing for fresh and FFPE DNA input, varying tumor/normal purities, and different coverages (ranging from 10× - 2000×). NeuSomatic significantly outperformed conventional detection approaches in general, as well as in challenging situations such as low coverage, low mutation frequency, DNA damage, and difficult genomic regions.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Robust Cancer Mutation Detection with Deep Learning Models Derived from Tumor-Normal Sequencing Data

Sahraeian

Fang

Mohiyuddin

et al. 2019

Preprint

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Toward best practice in cancer mutation detection with whole-genome and whole-exome sequencing

Xiao¹,

Ren²,

Chen³

et al. 2021

Nat Biotechnol

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Clinical applications of precision oncology require accurate tests that can distinguish true cancer specific mutations from errors introduced at each step of next-generation sequencing (NGS). To date, no bulk sequencing study has addressed the effects of cross-site reproducibility, nor the biological, technical and computational factors that influence variant identification. Here we report a systematic interrogation of somatic mutations in paired tumor-normal cell lines to identify factors affecting detection reproducibility and accuracy at six different centers. Using whole genome sequencing (WGS) and whole-exome sequencing (WES), we evaluated the reproducibility of different sample types with varying input amount and tumor purity, and multiple library construction protocols, followed by processing with nine bioinformatics pipelines. We found that read coverage and callers affected both WGS and WES reproducibility, but WES performance was influenced by insert fragment size, genomic copy content and the global imbalance score (GIV; G > T/C > A). Finally, taking into account library preparation protocol, tumor content, read coverage and bioinformatics processes concomitantly, we recommend actionable practices to improve the reproducibility and accuracy of NGS experiments for cancer mutation detection.

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Calling small variants with universality and Bayesian-frequentist hybridism

Zhao

Wang

et al. 2020

Preprint

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We describe UVC (https://github.com/genetronhealth/uvc), an open-source method for calling small somatic variants. UVC is aware of both unique molecular identifiers (UMIs) and the tumor-matched normal sample. UVC utilizes the following power-law universality that we discovered: allele fraction is inversely proportional to the cubic root of variant-calling error rate. Moreover, UVC utilizes pseudo-neural network (PNN). PNN is similar to deep neural network but does not require any training data. UVC outperformed Mageri and smCounter2, the state-of-the-art UMI-aware variant callers, on the tumor-only datasets used for publishing these two variant callers. Also, UVC outperformed Mutect2 and Strelka2, the state-of-the-art variant callers for tumor-normal pairs, on the Genome-in-a-Bottle somatic truth sets. UVC outperformed Mutect2 and Strelka2 on 21 in silico mixtures simulating 21 combinations of tumor purity and normal purity. Performance is measured by using sensitivity-specificity trade off for all called variants. The improved variant calls generated by UVC from previously published UMI-based sequencing data are able to provide additional biological insight about DNA damage repair. The versatility and robustness of UVC makes it a useful tool for variant calling in clinical settings.

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Establishing reference samples for detection of somatic mutations and germline variants with NGS technologies

Cited by 9 publications

References 27 publications

Robust Cancer Mutation Detection with Deep Learning Models Derived from Tumor-Normal Sequencing Data

Robust Cancer Mutation Detection with Deep Learning Models Derived from Tumor-Normal Sequencing Data

Toward best practice in cancer mutation detection with whole-genome and whole-exome sequencing

Calling small variants with universality and Bayesian-frequentist hybridism

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