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TargetCall: eliminating the wasted computation in basecalling via pre-basecalling filtering.

Authors :
Cavlak, Meryem Banu
Singh, Gagandeep
Alser, Mohammed
Firtina, Can
Lindegger, Joël
Sadrosadati, Mohammad
Mansouri Ghiasi, Nika
Alkan, Can
Mutlu, Onur
Source :
Frontiers in Genetics; 2024, p1-13, 13p
Publication Year :
2024

Abstract

Basecalling is an essential step in nanopore sequencing analysis where the raw signals of nanopore sequencers are converted into nucleotide sequences, that is, reads. State-of-the-art basecallers use complex deep learning models to achieve high basecalling accuracy. This makes basecalling computationally inefficient and memory-hungry, bottlenecking the entire genome analysis pipeline. However, for many applications, most reads do not match the reference genome of interest (i.e., target reference) and thus are discarded in later steps in the genomics pipeline, wasting the basecalling computation. To overcome this issue, we propose TargetCall, the first pre-basecalling filter to eliminate the wasted computation in basecalling. TargetCall's key idea is to discard reads that will not match the target reference (i.e., off-target reads) prior to basecalling. TargetCall consists of two main components: (1) LightCall, a lightweight neural network basecaller that produces noisy reads, and (2) Similarity Check, which labels each of these noisy reads as on-target or off-target by matching them to the target reference. Our thorough experimental evaluations show that TargetCall 1) improves the end-to-end basecalling runtime performance of the state-of-the-art basecaller by 3.31 × while maintaining high (98.88 %) recall in keeping on-target reads, 2) maintains high accuracy in downstream analysis, and 3) achieves better runtime performance, throughput, recall, precision, and generality than prior works. TargetCall is available at https://github.com/CMU-SAFARI/TargetCall. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
16648021
Database :
Complementary Index
Journal :
Frontiers in Genetics
Publication Type :
Academic Journal
Accession number :
180779185
Full Text :
https://doi.org/10.3389/fgene.2024.1429306