Paper List
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A Theoretical Framework for the Formation of Large Animal Groups: Topological Coordination, Subgroup Merging, and Velocity Inheritance
This paper addresses the core problem of how large, coordinated animal groups form in nature, challenging the classical view of gradual aggregation by...
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CONFIDE: Hallucination Assessment for Reliable Biomolecular Structure Prediction and Design
This paper addresses the critical limitation of current protein structure prediction models (like AlphaFold3) where high-confidence scores (pLDDT) can...
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Generative design and validation of therapeutic peptides for glioblastoma based on a potential target ATP5A
This paper addresses the critical bottleneck in therapeutic peptide design: how to efficiently optimize lead peptides with geometric constraints while...
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Pharmacophore-based design by learning on voxel grids
This paper addresses the computational bottleneck and limited novelty in conventional pharmacophore-based virtual screening by introducing a voxel cap...
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Human-Centred Evaluation of Text-to-Image Generation Models for Self-expression of Mental Distress: A Dataset Based on GPT-4o
This paper addresses the critical gap in evaluating how AI-generated images can effectively support cross-cultural mental distress communication, part...
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ANNE Apnea Paper
This paper addresses the core challenge of achieving accurate, event-level sleep apnea detection and characterization using a non-intrusive, multimoda...
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DeeDeeExperiment: Building an infrastructure for integrating and managing omics data analysis results in R/Bioconductor
This paper addresses the critical bottleneck of managing and organizing the growing volume of differential expression and functional enrichment analys...
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Cross-Species Antimicrobial Resistance Prediction from Genomic Foundation Models
This paper addresses the core challenge of predicting antimicrobial resistance across phylogenetically distinct bacterial species, where traditional m...
A Standardized Framework for Evaluating Gene Expression Generative Models
University of Cambridge | Wellcome Sanger Institute | Sapienza University of Rome | ISTI-CNR
30秒速读
IN SHORT: This paper addresses the critical lack of standardized evaluation protocols for single-cell gene expression generative models, where inconsistent metric implementations and computation spaces make cross-study comparisons impossible.
核心创新
- Methodology Introduces GGE, the first unified Python framework with explicit computation space parameterization (raw, PCA, DEG-restricted) for standardized evaluation of generative models.
- Methodology Proposes perturbation-effect correlation metric that measures direction and magnitude of perturbation responses rather than raw expression correlation, focusing evaluation on biologically relevant signals.
- Methodology Demonstrates that Wasserstein distance values vary by nearly an order of magnitude (17.2 to 104.3) depending solely on computation space, quantifying the standardization problem.
主要结论
- Metric values vary substantially with implementation choices: W₂ distance ranges from 17.2 (PCA-25) to 104.3 (raw space) on identical data, highlighting critical need for standardization.
- DEG selection strategy affects correlation metrics: top-20 DEG selection yields Pearson correlation of 0.614±0.066 vs strict threshold selection (lfc>1, p<0.01) yielding 0.506±0.217 on Norman dataset.
- Perturbation-effect correlation in DEG space provides biologically meaningful evaluation, focusing on genes that actually respond to perturbations rather than steady-state background expression.
摘要: The rapid development of generative models for single-cell gene expression data has created an urgent need for standardised evaluation frameworks. Current evaluation practices suffer from inconsistent metric implementations, incomparable hyperparameter choices, and a lack of biologically-grounded metrics. We present Generated Genetic Expression Evaluator (GGE), an open-source Python framework that addresses these challenges by providing a comprehensive suite of distributional metrics with explicit computation space options and biologically-motivated evaluation through differentially expressed gene (DEG)-focused analysis and perturbation-effect correlation, enabling standardized reporting and reproducible benchmarking. Through extensive analysis of the single-cell generative modeling literature, we identify that no standardized evaluation protocol exists. Methods report incomparable metrics computed in different spaces with different hyperparameters. We demonstrate that metric values vary substantially depending on implementation choices, highlighting the critical need for standardization. GGE enables fair comparison across generative approaches and accelerates progress in perturbation response prediction, cellular identity modeling, and counterfactual inference.