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领域生物信息学生物信息学
方法族Process / pipelineProcess / pipeline
起源年份2001–20052009–2010 (modern high-throughput era)
提出者Ian Holmes & William J. Bruno; Benjamin Redelings & Marc SuchardLi et al. (SAMtools/bcftools, 2009); McKenna et al. (GATK, 2010)
类型Probabilistic computational methodComputational genomics pipeline
开创性文献Redelings, B. D., & Suchard, M. A. (2005). Joint Bayesian estimation of alignment and phylogeny. Systematic Biology, 54(3), 401–418. link ↗McKenna, A., Hanna, M., Banks, E., Sivachenko, A., Cibulskis, K., Kernytsky, A., ... & DePristo, M. A. (2010). The Genome Analysis Toolkit: A MapReduce framework for analyzing next-generation DNA sequencing data. Genome Research, 20(9), 1297–1303. DOI ↗
别名Bayesian MSA, probabilistic sequence alignment, statistical alignment, BAli-Phy alignmentSNP calling, genotyping from sequencing, mutation detection, variant detection
相关56
摘要Bayesian sequence alignment treats the alignment of biological sequences (DNA, RNA, or protein) as a probabilistic inference problem rather than a deterministic optimization. Instead of returning a single best alignment, it samples from a posterior distribution over all plausible alignments given a substitution model and gap penalty priors, thereby quantifying alignment uncertainty. It is particularly valuable when downstream analyses such as phylogenetic inference or functional annotation are sensitive to alignment error.Variant calling is the computational process of identifying positions in a sequenced genome that differ from a reference sequence — including single nucleotide polymorphisms (SNPs), small insertions and deletions (indels), and structural variants. It transforms aligned sequencing reads into an interpretable catalogue of genetic differences, forming the foundation for population genetics, disease-gene discovery, and clinical genomics applications.
ScholarGate数据集
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  1. v1
  2. 2 来源
  3. PUBLISHED

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ScholarGate方法对比: Bayesian Sequence Alignment · Variant Calling. 于 2026-06-15 检索自 https://scholargate.app/zh/compare