CancerOmicsNet is a tool to predict drug (kinase inhibitors ONLY for now) response (growth rate) on a specific cell line given genetic information of the cell line, binding affinity of the drug to the proteins, and the disease association scores of the proteins. It utilizes heterogeneous data to construct a graph for each cell-line-drug combination (instance). The trained model can be used to predict the effect (currently a binary classification) of a drug on a given cell line.
If you find this tool useful, please cite our paper :)
Pu L., Singha M., Ramanujam J., Brylinski M. CancerOmicsNet: a multi-omics network-based approach to anti-cancer drug profiling. Oncotarget. 2022; 13: 695-706
https://www.oncotarget.com/article/28234/text/
This README file is written by Limeng Pu.
- Non-deep-learning (data generation) related dependencies can be installed via
conda env create -f environment.yml. Please change line 12 accordingly. - PyTorch Geometric latest version (https://pytorch-geometric.readthedocs.io/en/latest/notes/installation.html)
The installation of Pytorch and Pytorch Geometric differs from system to system. Thus, for the installation instruction related to those libraries, please refer to the corresponding project site.
The data generation and prediction/training are separated in this repo.
The input data required for the model comes in the form of graphs (eventually converted to matrices), which consists of a list of nodes and a list of edges (edge features are not supported in the currently implementation), which can be downloaded from on the STRING databse (https://string-db.org/). The data generation steps include: graph generation with node feaures, graph reduction, and graph to matrix conversion.
Since the entire data generation process, especially the collection of node features (affinities, disease scores, and gene expressions), is quite cumbersome, thus the following procedure is ONLY for generating testing data (no labels!!). If you wish to generate your own training data (with class labels), you will need to collect all features and GR values for them. Then follow the graph reduction instruction https://github.com/pulimeng/Biology-Network-Reduction/tree/main/PPI.
For the convenient of most users, we provide all the features we collected. The user only need to input the drug-cell-line combinations they wish to generate graphs for. To generate data for desired drug and cell-line, one first need to download and untar the already reduced graph from https://osf.io/dzx7b/. They are named, reduced_node_tables and reduced_edge_tables. Then run
python gr_datagen.py --i example_input --o output_folder--ithe file contains drug-cell-line pair you wish to generate data for, separated by commas. An example file in given asexample_input. Note that available drugs and cell-lines are also provided as drugs.lst and celllines.lst respectively.--othe folder you wish to store the generated data (.h5 files contain the matrices).
Once one finishes generating the desirable data, the prediction module can be carried out by running
python gr_pred.py --m ./trained_model/graphgr_weights.ckpt --c ./trained_mode/configs.json --i your_data_folder --o your_output_file.--mtrained model weight file location.--ctrained model configuration file location.--iinput data folder location.--ooutput file location.
A output will be produced in the form of:
| instance | drug | cellline | score | class |
|---|---|---|---|---|
| pazopanib_1321N1 | pazopanib | 1321N1 | 0.75794625 | 1 |
| motesanib_1321N1 | motesanib | 1321N1 | 0.5741133 | 1 |
| lestaurtinib_1321N1 | lestaurtinib | 1321N1 | 0.7808407 | 1 |
where the score will represent the effectiveness of such drug on the provided cell line.
Before you train your own model, create two folders (raw and processed) under your data folder. Then move the data to ./raw. To train the model using your own data, run
python gr_train.pyIt reads the configurations from the params.json.
pathpath to the training data folder.opathpath to the output folder.embed_dimembedding dimension for the embedding of gene expressions and node types. Not the embedding dimension of GNN.hidden_dimGNN hidden dimension.jk_layerJumpingKnowledge layer parameter, can be 'cat', 'max', or any numbers.process_stepnumber of processing step for Set2Set readout layer.gammagamma for focal loss
All the results will be saved to the output folder, including loss, accuracies and best model weights.
The dataset we used for training and other auxilary files for data generation (reduced_node_tables and reduced_edge_tables) can be downloaded at https://osf.io/enz69/.
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