Abstract CRISPR-based genetic perturbation screens paired with single-cell transcriptomic readouts (Perturb-seq) offer a powerful tool for interrogating biological systems. Yet the resulting datasets are heterogeneous—particularly in vivo—and currently used cell-level perturbation labels reflect only CRISPR guide RNA exposure rather than perturbation state; further, many perturbations have a minimal effect on gene expression. For perturbations that do alter the transcriptomic state of cells, intracellular guide RNA abundance exhibits a dose-response association with perturbation efficacy. We combine (i) per-perturbation, expression-only classifiers trained with non-negative negative–unlabeled (nnNU) risk to yield calibrated scores reflecting the perturbation state of single cells and (ii) a monotone guide abundance prior to yield a per-cell pseudo-posterior that supports both assignment of perturbation probability and selection of affected gene features. To obtain a low-dimensional representation that allows for the accurate reconstruction of gene-level marginals for counterfactual decoding, we train an autoencoder with a quantile–hurdle reconstruction loss and feature-weighted emphasis on perturbation-affected genes. The result is a perturbation-aware latent embedding amenable to downstream trajectory modeling (e.g., optimal transport or flow matching) and a principled probability of perturbation for each non-control cell derived jointly from its guide counts and transcriptome.

Authors Florian Hugi, Tanmay Tanna, Randall J. Platt, Gunnar Rätsch

Submitted NeurIPS 2025 AI4D3

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Abstract Spot-based spatial transcriptomics (ST) technologies like 10x Visium quantify genome-wide gene expression and preserve spatial tissue organization. However, their coarse spot-level resolution aggregates signals from multiple cells, preventing accurate single-cell analysis and detailed cellular characterization. Here, we present DeepSpot2Cell, a novel DeepSet neural network that leverages pretrained pathology foundation models and spatial multi-level context to effectively predict virtual single-cell gene expression from histopathological images using spot-level supervision. DeepSpot2Cell substantially improves gene expression correlations on a newly curated benchmark we specifically designed for single-cell ST deconvolution and prediction from H&E images. The benchmark includes 20 lung, 7 breast, and 2 pancreatic cancer samples, across which DeepSpot2Cell outperformed previous super-resolution methods, achieving respective improvements of 46%, 65%, and 38% in cell expression correlation for the top 100 genes. We hope that DeepSpot2Cell and this benchmark will stimulate further advancements in virtual single-cell ST, enabling more precise delineation of cell-type-specific expression patterns and facilitating enhanced downstream analyses. Code availability: https://github.com/ratschlab/DeepSpot

Authors Kalin Nonchev, Glib Manaiev, Viktor H Koelzer, Gunnar Rätsch

Submitted NeurIPS 2025 Imageomics

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Abstract Histopathology refers to the microscopic examination of diseased tissues and routinely guides treatment decisions for cancer and other diseases. Currently, this analysis focuses on morphological features but rarely considers gene expression information, which can add an important molecular dimension. Here, we introduce SpotWhisperer, an AI method that links histopathological images to spatial gene expression profiles and their text annotations, enabling molecularly grounded histopathology analysis through natural language. Our method outperforms pathology vision-language models on a newly curated benchmark dataset, dedicated to spatially resolved H&E annotation. Integrated into a web interface, SpotWhisperer enables interactive exploration of cell types and disease mechanisms using free-text queries with access to inferred spatial gene expression profiles. In summary, SpotWhisperer analyzes cost-effective pathology images with spatial gene expression and natural-language AI, demonstrating a path for routine integration of microscopic molecular information into histopathology.

Authors Moritz Schaefer, Kalin Nonchev, Animesh Awasthi, Jake Burton, Viktor H Koelzer, Gunnar Rätsch, Christoph Bock

Submitted ICML 2025 FM4LS

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Abstract Spatial transcriptomics technology remains resource-intensive and unlikely to be routinely adopted for patient care soon. This hinders the development of novel precision medicine solutions and, more importantly, limits the translation of research findings to patient treatment. Here, we present DeepSpot, a deep-set neural network that leverages recent foundation models in pathology and spatial multi-level tissue context to effectively predict spatial transcriptomics from H&E images. DeepSpot substantially improved gene correlations across multiple datasets from patients with metastatic melanoma, kidney, lung, or colon cancers as compared to previous state-of-the-art. Using DeepSpot, we generated 1 792 TCGA spatial transcriptomics samples (37 million spots) of the melanoma and renal cell cancer cohorts. We anticipate this to be a valuable resource for biological discovery and a benchmark for evaluating spatial transcriptomics models. We hope that DeepSpot and this dataset will stimulate further advancements in computational spatial transcriptomics analysis.

Authors Kalin Nonchev, Sebastian Dawo, Karina Selina, Holger Moch, Sonali Andani, Tumor Profiler Consortium, Viktor Hendrik Koelzer, Gunnar Rätsch

Submitted MedRxiv

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Abstract Notable progress has been made in generalist medical large language models across various healthcare areas. However, large-scale modeling of in-hospital time series data - such as vital signs, lab results, and treatments in critical care - remains underexplored. Existing datasets are relatively small, but combining them can enhance patient diversity and improve model robustness. To effectively utilize these combined datasets for large-scale modeling, it is essential to address the distribution shifts caused by varying treatment policies, necessitating the harmonization of treatment variables across the different datasets. This work aims to establish a foundation for training large-scale multi-variate time series models on critical care data and to provide a benchmark for machine learning models in transfer learning across hospitals to study and address distribution shift challenges. We introduce a harmonized dataset for sequence modeling and transfer learning research, representing the first large-scale collection to include core treatment variables. Future plans involve expanding this dataset to support further advancements in transfer learning and the development of scalable, generalizable models for critical healthcare applications.

Authors Manuel Burger, Fedor Sergeev, Malte Londschien, Daphné Chopard, Hugo Yèche, Eike Gerdes, Polina Leshetkina, Alexander Morgenroth, Zeynep Babür, Jasmina Bogojeska, Martin Faltys, Rita Kuznetsova, Gunnar Rätsch

Submitted Best Paper @ NeurIPS AIM-FM Workshop 2024

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