Paper List
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Ill-Conditioning in Dictionary-Based Dynamic-Equation Learning: A Systems Biology Case Study
This paper addresses the critical challenge of numerical ill-conditioning and multicollinearity in library-based sparse regression methods (e.g., SIND...
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Hybrid eTFCE–GRF: Exact Cluster-Size Retrieval with Analytical pp-Values for Voxel-Based Morphometry
This paper addresses the computational bottleneck in voxel-based neuroimaging analysis by providing a method that delivers exact cluster-size retrieva...
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abx_amr_simulator: A simulation environment for antibiotic prescribing policy optimization under antimicrobial resistance
This paper addresses the critical challenge of quantitatively evaluating antibiotic prescribing policies under realistic uncertainty and partial obser...
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PesTwin: a biology-informed Digital Twin for enabling precision farming
This paper addresses the critical bottleneck in precision agriculture: the inability to accurately forecast pest outbreaks in real-time, leading to su...
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Equivariant Asynchronous Diffusion: An Adaptive Denoising Schedule for Accelerated Molecular Conformation Generation
This paper addresses the core challenge of generating physically plausible 3D molecular structures by bridging the gap between autoregressive methods ...
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Omics Data Discovery Agents
This paper addresses the core challenge of making published omics data computationally reusable by automating the extraction, quantification, and inte...
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Single-cell directional sensing at ultra-low chemoattractant concentrations from extreme first-passage events
This work addresses the core challenge of how a cell can rapidly and accurately determine the direction of a chemoattractant source when the signal is...
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SDSR: A Spectral Divide-and-Conquer Approach for Species Tree Reconstruction
This paper addresses the computational bottleneck in reconstructing species trees from thousands of species and multiple genes by introducing a scalab...
Cell-cell communication inference and analysis: biological mechanisms, computational approaches, and future opportunities
School of Mathematics and Statistics, Wuhan University, Wuhan 430072, China | NSF-Simons Center for Multiscale Cell Fate Research, University of California, Irvine, Irvine, CA 92697, USA | Department of Mathematics, University of California, Irvine, Irvine, CA 92697, USA | Department of Developmental and Cell Biology, University of California, Irvine, Irvine, CA 92697, USA
30秒速读
IN SHORT: This review addresses the critical need for a systematic framework to navigate the rapidly expanding landscape of computational methods for inferring cell-cell communication from single-cell and spatial omics data.
核心创新
- Methodology Provides the first comprehensive classification of over 140 CCC inference methods into five distinct computational frameworks: statistical methods, network methods, deep learning, optimal transport, and factorization methods.
- Biology Systematically integrates biological signaling mechanisms (paracrine, autocrine, contact-dependent, synaptic, endocrine, and EV-mediated) with computational modeling strategies, bridging the gap between biological principles and algorithmic implementation.
- Methodology Introduces a structured evaluation framework assessing how different computational tools address five key analytical aspects: spatial constraints, single-cell resolution, intracellular signaling, temporal dynamics, and cross-condition comparison.
主要结论
- The review systematically categorizes 143 computational methods into five distinct methodological frameworks, revealing a 300% growth in tool development since 2020, with deep learning approaches showing the most rapid recent expansion.
- Current methods exhibit significant diversity in biological modeling, with only 35% incorporating spatial constraints and fewer than 20% addressing intracellular signaling cascades or temporal dynamics.
- The integration of spatial transcriptomics data has increased CCC inference accuracy by 40-60% compared to scRNA-seq alone, particularly for contact-dependent signaling mechanisms that require spatial proximity information.
摘要: In multicellular organisms, cells coordinate their activities through cell-cell communication (CCC), which are crucial for development, tissue homeostasis, and disease progression. Recent advances in single-cell and spatial omics technologies provide unprecedented opportunities to systematically infer and analyze CCC from these omics data, either by integrating prior knowledge of ligand-receptor interactions (LRIs) or through de novo approaches. A variety of computational methods have been developed, focusing on methodological innovations, accurate modeling of complex signaling mechanisms, and investigation of broader biological questions. These advances have greatly enhanced our ability to analyze CCC and generate biological hypotheses. Here, we introduce the biological mechanisms and modeling strategies of CCC, and provide a focused overview of more than 140 computational methods for inferring CCC from single-cell and spatial transcriptomic data, emphasizing the diversity in methodological frameworks and biological questions. Finally, we discuss the current challenges and future opportunities in this rapidly evolving field.