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Accurately predicting cellular responses to perturbations is essential for understanding cell behavior in both healthy and diseased states. While perturbation data is ideal for building such predictive models, its availability is considerably lower than baseline (non-perturbed) cellular data. To address this limitation, several foundation cell models have been developed using large-scale single-cell gene expression data. These models are fine-tuned after pre-training for specific tasks, such as predicting post-perturbation gene expression profiles, and are considered state-of-the-art for these problems. However, proper benchmarking of these models remains an unsolved challenge.
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