Yuan-Ke Zhou scite author profile

Noncoding RNAs (ncRNAs) play crucial roles in many biological processes. Experimental methods for identifying ncRNA–protein interactions (NPIs) are always costly and time-consuming. Many computational approaches have been developed as alternative ways. In this work, we collected five benchmarking datasets for predicting NPIs. Based on these datasets, we evaluated and compared the prediction performances of existing machine-learning based methods. Graph neural network (GNN) is a recently developed deep learning algorithm for link predictions on complex networks, which has never been applied in predicting NPIs. We constructed a GNN-based method, which is called Noncoding RNA–Protein Interaction prediction using Graph Neural Networks (NPI-GNN), to predict NPIs. The NPI-GNN method achieved comparable performance with state-of-the-art methods in a 5-fold cross-validation. In addition, it is capable of predicting novel interactions based on network information and sequence information. We also found that insufficient sequence information does not affect the NPI-GNN prediction performance much, which makes NPI-GNN more robust than other methods. As far as we can tell, NPI-GNN is the first end-to-end GNN predictor for predicting NPIs. All benchmarking datasets in this work and all source codes of the NPI-GNN method have been deposited with documents in a GitHub repo (https://github.com/AshuiRUA/NPI-GNN).

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Predicting lncRNA–Protein Interactions With miRNAs as Mediators in a Heterogeneous Network Model

Zhou

Shen

et al. 2020

Front. Genet.

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Long non-coding RNAs (lncRNAs) play important roles in various biological processes, where lncRNA-protein interactions are usually involved. Therefore, identifying lncRNAprotein interactions is of great significance to understand the molecular functions of lncRNAs. Since the experiments to identify lncRNA-protein interactions are always costly and time consuming, computational methods are developed as alternative approaches. However, existing lncRNA-protein interaction predictors usually require prior knowledge of lncRNA-protein interactions with experimental evidences. Their performances are limited due to the number of known lncRNA-protein interactions. In this paper, we explored a novel way to predict lncRNA-protein interactions without direct prior knowledge. MiRNAs were picked up as mediators to estimate potential interactions between lncRNAs and proteins. By validating our results based on known lncRNA-protein interactions, our method achieved an AUROC (Area Under Receiver Operating Curve) of 0.821, which is comparable to the state-of-the-art methods. Moreover, our method achieved an improved AUROC of 0.852 by further expanding the training dataset. We believe that our method can be a useful supplement to the existing methods, as it provides an alternative way to estimate lncRNA-protein interactions in a heterogeneous network without direct prior knowledge. All data and codes of this work can be downloaded from GitHub (https://github.com/zyk2118216069/LncRNA-protein-interactions-prediction).

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LPI-SKF: Predicting lncRNA-Protein Interactions Using Similarity Kernel Fusions

Zhou

Shen

et al. 2020

Front. Genet.

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Long non-coding RNAs (lncRNAs) play an important role in serval biological activities, including transcription, splicing, translation, and some other cellular regulation processes. lncRNAs perform their biological functions by interacting with various proteins. The studies on lncRNA-protein interactions are of great value to the understanding of lncRNA functional mechanisms. In this paper, we proposed a novel model to predict potential lncRNA-protein interactions using the SKF (similarity kernel fusion) and LapRLS (Laplacian regularized least squares) algorithms. We named this method the LPI-SKF. Various similarities of both lncRNAs and proteins were integrated into the LPI-SKF. LPI-SKF can be applied in predicting potential interactions involving novel proteins or lncRNAs. We obtained an AUROC (area under receiver operating curve) of 0.909 in a 5-fold cross-validation, which outperforms other state-of-the-art methods. A total of 19 out of the top 20 ranked interaction predictions were verified by existing data, which implied that the LPI-SKF had great potential in discovering unknown lncRNA-protein interactions accurately. All data and codes of this work can be downloaded from a GitHub repository (https://github.com/zyk2118216069/LPI-SKF).

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Predicting LncRNA Subcellular Localization Using Unbalanced Pseudo-k Nucleotide Compositions

Yang

Zhou

Zhang

et al. 2020

CBIO

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Background: Long non-coding RNAs (lncRNAs) are transcripts with a length more than 200 nucleotides, functioning in the regulation of gene expression. More and more evidence has shown that the biological functions of lncRNAs are intimately related to their subcellular localizations. Therefore, it is very important to confirm the lncRNA subcellular localization. Method: In this paper, we proposed a novel method to predict the subcellular localization of lncRNAs. To more comprehensively utilize lncRNA sequence information, we exploited both k-mer nucleotide composition and sequence order correlated factors of lncRNA to formulate lncRNA sequences. Meanwhile, a feature selection technique which was based on the analysis of variance (ANOVA) was applied to obtain the optimal feature subset. Finally, we used the support vector machine (SVM) to perform the prediction. Results: The AUC value of the proposed method can reach 0.9695, which indicated the proposed predictor is an efficient and reliable tool for determining lncRNA subcellular localization. Furthermore, the predictor can reach the maximum overall accuracy of 90.37% in leave-one-out cross validation, which clearly outperforms the existing state-of- the-art method. Conclusion: It is demonstrated that the proposed predictor is feasible and powerful for the prediction of lncRNA subcellular. To facilitate subsequent genetic sequence research, we shared the source code at https://github.com/NicoleYXF/lncRNA.

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KNIndex: a comprehensive database of physicochemical properties fork-tuple nucleotides

Zhang

Wang

et al. 2020

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With the development of high-throughput sequencing technology, the genomic sequences increased exponentially over the last decade. In order to decode these new genomic data, machine learning methods were introduced for genome annotation and analysis. Due to the requirement of most machines learning methods, the biological sequences must be represented as fixed-length digital vectors. In this representation procedure, the physicochemical properties of k-tuple nucleotides are important information. However, the values of the physicochemical properties of k-tuple nucleotides are scattered in different resources. To facilitate the studies on genomic sequences, we developed the first comprehensive database, namely KNIndex (https://knindex.pufengdu.org), for depositing and visualizing physicochemical properties of k-tuple nucleotides. Currently, the KNIndex database contains 182 properties including one for mononucleotide (DNA), 169 for dinucleotide (147 for DNA and 22 for RNA) and 12 for trinucleotide (DNA). KNIndex database also provides a user-friendly web-based interface for the users to browse, query, visualize and download the physicochemical properties of k-tuple nucleotides. With the built-in conversion and visualization functions, users are allowed to display DNA/RNA sequences as curves of multiple physicochemical properties. We wish that the KNIndex will facilitate the related studies in computational biology.

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Yuan-Ke Zhou

NPI-GNN: Predicting ncRNA–protein interactions with deep graph neural networks

Predicting lncRNA–Protein Interactions With miRNAs as Mediators in a Heterogeneous Network Model

LPI-SKF: Predicting lncRNA-Protein Interactions Using Similarity Kernel Fusions

Predicting LncRNA Subcellular Localization Using Unbalanced Pseudo-k Nucleotide Compositions

KNIndex: a comprehensive database of physicochemical properties fork-tuple nucleotides

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