BMLGMLOct 28, 2019

AMP0: Species-Specific Prediction of Anti-microbial Peptides using Zero and Few Shot Learning

arXiv:1911.06106v113 citations
Originality Incremental advance
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This work addresses the need for targeted antimicrobial peptide discovery to combat drug-resistant microbes, offering a computational tool for rapid screening, though it is incremental as it builds on existing machine learning methods for a specific domain.

The authors tackled the problem of predicting antimicrobial peptides (AMPs) effective against specific microbial species, which existing predictors cannot do, by developing AMP0, a zero-shot and few-shot learning model that uses peptide sequences and target species genomic data to achieve targeted predictions, showing effectiveness in computational cross-validation especially with limited training examples.

The evolution of drug-resistant microbial species is one of the major challenges to global health. The development of new antimicrobial treatments such as antimicrobial peptides needs to be accelerated to combat this threat. However, the discovery of novel antimicrobial peptides is hampered by low-throughput biochemical assays. Computational techniques can be used for rapid screening of promising antimicrobial peptide candidates prior to testing in the wet lab. The vast majority of existing antimicrobial peptide predictors are non-targeted in nature, i.e., they can predict whether a given peptide sequence is antimicrobial, but they are unable to predict whether the sequence can target a particular microbial species. In this work, we have developed a targeted antimicrobial peptide activity predictor that can predict whether a peptide is effective against a given microbial species or not. This has been made possible through zero-shot and few-shot machine learning. The proposed predictor called AMP0 takes in the peptide amino acid sequence and any N/C-termini modifications together with the genomic sequence of a target microbial species to generate targeted predictions. It is important to note that the proposed method can generate predictions for species that are not part of its training set. The accuracy of predictions for novel test species can be further improved by providing a few example peptides for that species. Our computational cross-validation results show that the pro-posed scheme is particularly effective for targeted antimicrobial prediction in comparison to existing approaches and can be used for screening potential antimicrobial peptides in a targeted manner especially for cases in which the number of training examples is small. The webserver of the method is available at http://ampzero.pythonanywhere.com.

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