Protein structure prediction aims to determine the three-dimensional shape of a protein from its amino acid sequence 1. This problem is of fundamental importance to biology as the structure of a protein largely determines its function 2 but can be hard to determine experimentally. In recent years, considerable progress has been made by leveraging genetic information: analysing the co-variation of homologous sequences can allow one to infer which amino acid residues are in contact, which in turn can aid structure prediction 3. In this work, we show that we can train a neural network to accurately predict the distances between pairs of residues in a protein which convey more about structure than contact predictions. With this information we construct a potential of mean force 4 that can accurately describe the shape of a protein. We find that the resulting potential can be optimised by a simple gradient descent algorithm, to realise structures without the need for complex sampling procedures. The resulting system, named AlphaFold, has been shown to achieve high accuracy, even for sequences with relatively few homologous sequences. In the most recent Critical Assessment of Protein Structure Prediction 5 (CASP13), a blind assessment of the state of the field of protein structure prediction, AlphaFold created high-accuracy structures (with TM-scores † of 0.7 or higher) for 24 out of 43 free modelling domains whereas the next best method, using sampling and contact information, achieved such accuracy for only 14 out of 43 domains. AlphaFold represents a significant advance in protein structure prediction. We expect the increased accuracy of structure predictions for proteins to enable insights in understanding the function and malfunction of these proteins, especially in cases where no homologous proteins have been experimentally determined 7. Proteins are at the core of most biological processes. Since the function of a protein is dependent on its structure, understanding protein structure has been a grand challenge in biology for decades. While several experimental structure determination techniques have been developed † Template Modelling score 6 , between 0 and 1, measures the degree of match of the overall (backbone) shape of a proposed structure to a native structure.
While the vast majority of well-structured single protein chains can now be predicted to high accuracy due to the recent AlphaFold [1] model, the prediction of multi-chain protein complexes remains a challenge in many cases. In this work, we demonstrate that an AlphaFold model trained specifically for multimeric inputs of known stoichiometry, which we call AlphaFold-Multimer, significantly increases accuracy of predicted multimeric interfaces over input-adapted single-chain AlphaFold while maintaining high intra-chain accuracy. On a benchmark dataset of 17 heterodimer proteins without templates (introduced in [2]) we achieve at least medium accuracy (DockQ [3]≥0.49) on 14 targets and high accuracy (DockQ≥0.8) on 6 targets, compared to 9 targets of at least medium accuracy and 4 of high accuracy for the previous state of the art system (an AlphaFold-based system from [2]). We also predict structures for a large dataset of 4,433 recent protein complexes, from which we score all non-redundant interfaces with low template identity. For heteromeric interfaces we successfully predict the interface (DockQ≥0.23) in 67% of cases, and produce high accuracy predictions (DockQ≥0.8) in 23% of cases, an improvement of +25 and +11 percentage points over the flexible linker modification of AlphaFold [4] respectively. For homomeric interfaces we successfully predict the interface in 69% of cases, and produce high accuracy predictions in 34% of cases, an improvement of +5 percentage points in both instances.
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The goal of this work is to recognise phrases and sentences being spoken by a talking face, with or without the audio. Unlike previous works that have focussed on recognising a limited number of words or phrases, we tackle lip reading as an open-world problem -unconstrained natural language sentences, and in the wild videos.Our key contributions are: (1) a 'Watch, Listen, Attend and Spell' (WLAS) network that learns to transcribe videos of mouth motion to characters; (2) a curriculum learning strategy to accelerate training and to reduce overfitting; (3) a 'Lip Reading Sentences' (LRS) dataset for visual speech recognition, consisting of over 100,000 natural sentences from British television.The WLAS model trained on the LRS dataset surpasses the performance of all previous work on standard lip reading benchmark datasets, often by a significant margin. This lip reading performance beats a professional lip reader on videos from BBC television, and we also demonstrate that visual information helps to improve speech recognition performance even when the audio is available.
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