Do you want to publish a course? Click here

Do Large Scale Molecular Language Representations Capture Important Structural Information?

502   0   0.0 ( 0 )
 Added by Youssef Mroueh
 Publication date 2021
and research's language is English




Ask ChatGPT about the research

Predicting chemical properties from the structure of a molecule is of great importance in many applications including drug discovery and material design. Machine learning based molecular property prediction holds the promise of enabling accurate predictions at much less complexity, when compared to, for example Density Functional Theory (DFT) calculations. Features extracted from molecular graphs, using graph neural nets in a supervised manner, have emerged as strong baselines for such tasks. However, the vast chemical space together with the limited availability of labels makes supervised learning challenging, calling for learning a general-purpose molecular representation. Recently, pre-trained transformer-based language models (PTLMs) on large unlabeled corpus have produced state-of-the-art results in many downstream natural language processing tasks. Inspired by this development, here we present molecular embeddings obtained by training an efficient transformer encoder model, referred to as MoLFormer. This model was employed with a linear attention mechanism and highly paralleized training on 1D SMILES sequences of 1.1 billion unlabeled molecules from the PubChem and ZINC datasets. Experiments show that the learned molecular representation performs competitively, when compared to existing graph-based and fingerprint-based supervised learning baselines, on the challenging tasks of predicting properties of QM8 and QM9 molecules. Further task-specific fine-tuning of the MoLFormerr representation improves performance on several of those property prediction benchmarks. These results provide encouraging evidence that large-scale molecular language models can capture sufficient structural information to be able to accurately predict quantum chemical properties and beyond.



rate research

Read More

Protein is linked to almost every life process. Therefore, analyzing the biological structure and property of protein sequences is critical to the exploration of life, as well as disease detection and drug discovery. Traditional protein analysis methods tend to be labor-intensive and time-consuming. The emergence of deep learning models makes modeling data patterns in large quantities of data possible. Interdisciplinary researchers have begun to leverage deep learning methods to model large biological datasets, e.g. using long short-term memory and convolutional neural network for protein sequence classification. After millions of years of evolution, evolutionary information is encoded in protein sequences. Inspired by the similarity between natural language and protein sequences, we use large-scale language models to model evolutionary-scale protein sequences, encoding protein biology information in representation. Significant improvements are observed in both token-level and sequence-level tasks, demonstrating that our large-scale model can accurately capture evolution information from pretraining on evolutionary-scale individual sequences. Our code and model are available at https://github.com/THUDM/ProteinLM.
How to produce expressive molecular representations is a fundamental challenge in AI-driven drug discovery. Graph neural network (GNN) has emerged as a powerful technique for modeling molecular data. However, previous supervised approaches usually suffer from the scarcity of labeled data and have poor generalization capability. Here, we proposed a novel Molecular Pre-training Graph-based deep learning framework, named MPG, that leans molecular representations from large-scale unlabeled molecules. In MPG, we proposed a powerful MolGNet model and an effective self-supervised strategy for pre-training the model at both the node and graph-level. After pre-training on 11 million unlabeled molecules, we revealed that MolGNet can capture valuable chemistry insights to produce interpretable representation. The pre-trained MolGNet can be fine-tuned with just one additional output layer to create state-of-the-art models for a wide range of drug discovery tasks, including molecular properties prediction, drug-drug interaction, and drug-target interaction, involving 13 benchmark datasets. Our work demonstrates that MPG is promising to become a novel approach in the drug discovery pipeline.
Model parallelism has become a necessity for training modern large-scale deep language models. In this work, we identify a new and orthogonal dimension from existing model parallel approaches: it is possible to perform pipeline parallelism within a single training sequence for Transformer-based language models thanks to its autoregressive property. This enables a more fine-grained pipeline compared with previous work. With this key idea, we design TeraPipe, a high-performance token-level pipeline parallel algorithm for synchronous model-parallel training of Transformer-based language models. We develop a novel dynamic programming-based algorithm to calculate the optimal pipelining execution scheme given a specific model and cluster configuration. We show that TeraPipe can speed up the training by 5.0x for the largest GPT-3 model with 175 billion parameters on an AWS cluster with 48 p3.16xlarge instances compared with state-of-the-art model-parallel methods.
Pretrained Language Models (LMs) have been shown to possess significant linguistic, common sense, and factual knowledge. One form of knowledge that has not been studied yet in this context is information about the scalar magnitudes of objects. We show that pretrained language models capture a significant amount of this information but are short of the capability required for general common-sense reasoning. We identify contextual information in pre-training and numeracy as two key factors affecting their performance and show that a simple method of canonicalizing numbers can have a significant effect on the results.
In this work, we study the large-scale pretraining of BERT-Large with differentially private SGD (DP-SGD). We show that combined with a careful implementation, scaling up the batch size to millions (i.e., mega-batches) improves the utility of the DP-SGD step for BERT; we also enhance its efficiency by using an increasing batch size schedule. Our implementation builds on the recent work of [SVK20], who demonstrated that the overhead of a DP-SGD step is minimized with effective use of JAX [BFH+18, FJL18] primitives in conjunction with the XLA compiler [XLA17]. Our implementation achieves a masked language model accuracy of 60.5% at a batch size of 2M, for $epsilon = 5.36$. To put this number in perspective, non-private BERT models achieve an accuracy of $sim$70%.

suggested questions

comments
Fetching comments Fetching comments
Sign in to be able to follow your search criteria
mircosoft-partner

هل ترغب بارسال اشعارات عن اخر التحديثات في شمرا-اكاديميا