A deep-learning based multi-omics bulk sequencing data integration suite with a focus on (pre-)clinical endpoint prediction.
Project description
flexynesis
Flexynesis: a flexible deep learning toolkit for interpretable multi-omics integration and clinical outcome prediction.
Flexynesis is a deep learning suite for multi-omics data integration, designed for (pre-)clinical endpoint prediction. It supports diverse neural architectures — from fully connected networks and supervised variational autoencoders to graph convolutional and multi-triplet models — with flexible options for omics layer fusion, automated feature selection, and hyperparameter optimization.
Built with interpretability in mind, Flexynesis incorporates integrated gradients (via Captum) for marker discovery, helping researchers move beyond black-box models.
The framework is continuously benchmarked on public datasets, particularly in oncology, and has been applied to tasks such as drug response prediction in patients and preclinical models (cell lines, PDXs), cancer subtype classification, and clinically relevant outcomes in regression, classification, survival, and cross-modality settings.
Citing our work
In order to refer to our work, please cite our manuscript currently available at BioRxiv.
Getting started with Flexynesis
Command-line tutorial
Jupyter notebooks for interactive usage
- Modeling Breast Cancer Subtypes
- Survival Markers of Lower Grade Gliomas
- Unsupervised Analysis of Bone Marrow Cells
Benchmarks
For the latest benchmark results see: https://bimsbstatic.mdc-berlin.de/akalin/buyar/flexynesis-benchmark-datasets/dashboard.html
The code for the benchmarking pipeline is at: https://github.com/BIMSBbioinfo/flexynesis-benchmarks
Documentation
Documentation generated using mkdocs
pip install mkdocstrings[python]
mkdocs build --clean
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