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PairK: Pairwise k-mer alignment for quantifying protein motif conservation in disordered regions. | LitMetric

PairK: Pairwise k-mer alignment for quantifying protein motif conservation in disordered regions.

Protein Sci

Department of Biology, MIT, Cambridge, Massachusetts, USA.

Published: January 2025

AI Article Synopsis

Article Abstract

Protein-protein interactions are often mediated by a modular peptide recognition domain binding to a short linear motif (SLiM) in the disordered region of another protein. To understand the features of SLiMs that are important for binding and to identify motif instances that are important for biological function, it is useful to examine the evolutionary conservation of motifs across homologous proteins. However, the intrinsically disordered regions (IDRs) in which SLiMs reside evolve rapidly. Consequently, multiple sequence alignment (MSA) of IDRs often misaligns SLiMs and underestimates their conservation. We present PairK (pairwise k-mer alignment), an MSA-free method to align and quantify the relative local conservation of subsequences within an IDR. Lacking a ground truth for conservation, we tested PairK on the task of distinguishing biologically important motif instances from background motifs, under the assumption that biologically important motifs are more conserved. The method outperforms both standard MSA-based conservation scores and a modern LLM-based conservation score predictor. PairK can quantify conservation over wider phylogenetic distances than MSAs, indicating that some SLiMs are more conserved than MSA-based metrics imply. PairK is available as an open-source python package at https://github.com/jacksonh1/pairk. It is designed to be easily adapted for use with other SLiM tools and for diverse applications.

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Source
http://dx.doi.org/10.1002/pro.70004DOI Listing

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PairK: Pairwise k-mer alignment for quantifying protein motif conservation in disordered regions.

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January 2025

Department of Biology, MIT, Cambridge, Massachusetts, USA.

Protein-protein interactions are often mediated by a modular peptide recognition domain binding to a short linear motif (SLiM) in the disordered region of another protein. To understand the features of SLiMs that are important for binding and to identify motif instances that are important for biological function, it is useful to examine the evolutionary conservation of motifs across homologous proteins. However, the intrinsically disordered regions (IDRs) in which SLiMs reside evolve rapidly.

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PairK: Pairwise k-mer alignment for quantifying protein motif conservation in disordered regions.

bioRxiv

July 2024

MIT Department of Biology, 77 Massachusetts Ave., Cambridge, MA 02139.

Protein-protein interactions are often mediated by a modular peptide recognition domain binding to a short linear motif (SLiM) in the disordered region of another protein. The ability to predict domain-SLiM interactions would allow researchers to map protein interaction networks, predict the effects of perturbations to those networks, and develop biologically meaningful hypotheses. Unfortunately, sequence database searches for SLiMs generally yield mostly biologically irrelevant motif matches or false positives.

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