Abstract

Repeat elements, such as transposable elements (TE), are highly repetitive DNA sequences that compose around 50% of the genome. TEs such as Alu, SVA, HERV, and L1 elements can cause disease through disrupting genes, causing frameshift mutations or altering splicing patters. These are elements challenging to characterize using short-read genome sequencing, due to its read length and TEs repetitive nature. Long-read genome sequencing (lrGS) enables bridging of TEs, allowing increased resolution across repetitive DNA sequences. lrGS therefore present an opportunity for improved TE detection and analysis not only from a research perspective but also for future clinical detection. When choosing an lrGS TE caller, parameters such as runtime, CPU hours, sensitivity, precision, and compatibility with inclusion into pipelines are crucial for efficient detection. We therefore developed sTELLeR, (s) Transposable ELement in Long (e) Read, for accurate, fast, and effective TE detection. Particularly, sTELLeR exhibit higher precision and sensitivity for calling of Alu elements than similar tools. The caller is 5-48× as fast and uses <2% of the CPU hours compared to competitive callers. The caller is haplotype aware and output results in a variant call format (VCF) file, enabling compatibility with other variant callers and downstream analysis. sTELLeR is a python-based tool and is available at https://github.com/kristinebilgrav/sTELLeR. Altogether, we show that sTELLeR is a fast, sensitive, and precise caller for detection of TE elements, and can easily be implemented into variant calling workflows.

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