Accurate proteome-wide missense variant effect prediction with AlphaMissense

Author:

Cheng Jun1ORCID,Novati Guido1,Pan Joshua1,Bycroft Clare1ORCID,Žemgulytė Akvilė1,Applebaum Taylor1ORCID,Pritzel Alexander1,Wong Lai Hong1,Zielinski Michal1ORCID,Sargeant Tobias1ORCID,Schneider Rosalia G.1ORCID,Senior Andrew W.1ORCID,Jumper John1ORCID,Hassabis Demis1ORCID,Kohli Pushmeet1ORCID,Avsec Žiga1ORCID

Affiliation:

1. Google DeepMind, London, UK.

Abstract

The vast majority of missense variants observed in the human genome are of unknown clinical significance. We present AlphaMissense, an adaptation of AlphaFold fine-tuned on human and primate variant population frequency databases to predict missense variant pathogenicity. By combining structural context and evolutionary conservation, our model achieves state-of-the-art results across a wide range of genetic and experimental benchmarks, all without explicitly training on such data. The average pathogenicity score of genes is also predictive for their cell essentiality, capable of identifying short essential genes that existing statistical approaches are underpowered to detect. As a resource to the community, we provide a database of predictions for all possible human single amino acid substitutions and classify 89% of missense variants as either likely benign or likely pathogenic.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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