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  • Development positions malignant cellular states but does notexplain their diversification
    by Poyatos, J. F.
    Epithelial cancers are often described as aberrant reactivations of embryonic or tissue-forming programs, but whether malignant cellular-state diversification is actually constrained by developmental trajectories remains unclear. Here, we present a quantitative framework to test this idea in pancreatic ductal adenocarcinoma (PDAC). Using representation learning on large-scale single-cell data, we build a reference space that captures the main axes of normal foregut and pancreatic epithelial variation. Malignant cells can be mapped into this space, showing that developmental biology helps interpret their […]
  • Extracellular vesicles from Manila clam (Ruditapes philippinarum): tailored isolation from hemolymph and insights into water-derived vesicles
    by Moccia, V., Dalla Rovere, g., Minh, T. T., Zendrini, A., Kleinjan, M., Roelofs, M., Berto, P., Zeev-Ben-Mordehai, T., Zaal, E. A., Bergese, P., Radeghieri, A., Milan, M., Wauben, M. H. M., Zappulli, V.
    Extracellular vesicles (EVs) are evolutionarily conserved mediators of intercellular communication released by cells into biological fluids and the extracellular environment. Despite their growing relevance in biomedical and veterinary research, knowledge on EVs in marine bivalves remains limited. The aim of this study was to optimize tailored protocols for EV isolation from the hemolymph of the Manila clam (Ruditapes philippinarum) based on density gradient ultracentrifugation (dgUC) or size exclusion chromatography (SEC). EV-enriched fractions were identified through nanoparticle tracking analysis, protein quantification, […]
  • iSsus3744: A Genome-Scale Model-Guided Strategy for Rational Media Design for Cultivated Pork
    by Gomez Romero, S. I., Vigliotti, M., Ramirez Lopez, V., Nguyen, K., Marchitto, V., Boyle, N. R.
    Cultivated meat production is currently limited by high production costs and an incomplete understanding of cellular metabolism in agriculturally relevant species. Genome-scale metabolic models (GEMs) have successfully guided media optimization in biopharmaceutical systems but have not been widely applied to cultivated meat. In this study, we present iSsus3744, the first genome-scale metabolic reconstruction for Sus scrofa and demonstrate its application for rational media design in cultivated pork production. iSsus3744 was reconstructed using HumanGEM and Recon3D as template models and further […]
  • Growth-resolved genome-scale metabolic modeling of Priestia megaterium SR7 validated by chemostat and 13-C flux analysis
    by Chang, K. Y. W., Song, Y., Hing, N. Y. K., Vethathirri, R. S., Wang, Y., Thompson, J. R.
    Priestia megaterium SR7 is a promising candidate chassis for bioprocess engineering, but its development is limited by the availability of condition-grounded, mechanistic models that can translate experimental measurements into predictive design hypotheses. Here, we present PMSR7, a genome-scale metabolic model for SR7, and evaluate it under a growth-resolved chemostat framework spanning a dilution-rate series. Stable steady states were established across the growth regime, with the highest dilution rate (D = 1.1538 per hr) excluded from growth interpretation due to biomass […]
  • Intestinal Dysbiosis in Necrotic Enteritis: Dissecting the Roles of Eimeria and Clostridium perfringens
    by Liu, J., Guo, J., Whitmore, M. A., Tobin, I., Kim, D. M., Zhang, G.
    Necrotic enteritis (NE), caused by Clostridium perfringens, is major enteric disease in poultry with substantial economic impact. NE is frequently triggered by co-infection with Eimeria spp., yet the relative contributions of Eimeria and C. perfringens to NE-induced dysbiosis and disease progression remain poorly defined. To address this, Cobb broiler chickens were challenged with Eimeria maxima, C. perfringens, or both, and ileal and cecal microbiota were analyzed using 16S rRNA gene sequencing and shotgun metagenomics. Temporal dynamics of intestinal microbiota shifts […]
  • EndoTwin-W: glycodelin-A and CA-125 as non-invasive biomarkers of endometrial receptivity derived from a multiscale computational digital twin
    by Goyal, R.
    Endometrial receptivity assessment currently requires invasive tissue biopsy, yet recent randomized trials have questioned the clinical utility of biopsy-based approaches. Here we present EndoTwin-W, a four-layer mechanistic computational model that simulates human endometrial remodeling from hormone inputs through receptor binding, pathway scoring, and continuous-time Markov chain cell-state transitions across 17 cell states. Transition rates were optimized against scRNA-seq and microarray data, then validated by 5-fold cross-validation on an independent bulk RNA-seq cohort (n=236 biopsies), achieving significant correlations for 16 of […]
  • Analyzing the dynamics in defense/counter-defense games among hosts and pathogens
    by Dwivedi, S., Ona, L., Schuster, S.
    In the dynamic interplay between hosts and pathogens, hosts may produce a defense compound that acts as a toxin to deter pathogen attack. Conversely, pathogens may evolve to produce a counter-defense enzyme, neutralizing the host's toxin. This evolutionary arms race incurs costs for both parties, prompting adaptations and strategic shifts. We conceptualize this interaction as an asymmetric game, with hosts and pathogens as players, and their potential responses – defense, counter-defense, or inaction – as their strategic options. In this […]
  • Ultrasensitive response in bacterial replication initiation
    by Sassi, A. S., Pigolotti, S.
    Bacteria are able to coordinate cell growth and genome replication in different growth conditions.The DNA-binding protein DnaA is responsible for determining initiation of replication,thereby playing a central role in this coordination. Theoretical and experimental studies have shown that stability of the cell cycle requires an ultrasensitive response, i.e., a sharp dependence of the initiation firing rate on the cell volume. However, the source of such ultrasensitivity remains elusive. In this work, we elucidate how the structure and binding affinities of […]
  • Modeling of Glucosinolate Biosynthesis During Biotic Stress as a Function of mRNA
    by Earle, J., Neefjes, A. C. M., Ploeger, X. S. D., van Laar, M., Van Wees, S. C. M., Schuurink, R. C., van Dijk, A. D. J., Bleeker, P., Hoefsloot, H.
    Glucosinolates are an important group of specialized metabolites in the Brassicaceae family, playing a role as defensive compounds against biotic attackers. In response to biotic stress, plants upregulate glucosinolate biosynthesis in part by increasing the abundance of enzymes in the glucosinolate biosynthetic pathway. As an increase in enzyme abundance is often preceded by an increase in the corresponding mRNA levels, the dynamic changes in mRNA levels should capture the information required to infer how metabolite levels change over time. In […]
  • Explainable machine learning reveals an RBP regulatory logic of exon skipping
    by Raghav, Y., Paul, A., Anderson, R., Karthyk, S., Iturralde, A., Vyas, J., Dy, J., Jones, B. C., Castaldi, P. J., Platig, J.
    RNA binding proteins (RBPs) regulate the life cycle of an mRNA, often through RBP-RNA interactions. This life cycle includes splicing, whereby the intronic sequence of a pre-mRNA is removed and the exons are joined together. However, the patterns of RBP binding that lead to different splicing outcomes are still incompletely understood. Here, we build machine learning models from RBP-RNA binding and knockdown RNA-seq data for over 168 RBPs in two cell lines (HepG2 and K562) to better understand the binding […]
  • Multi-state Continuous-Time Markov Chain Modeling for Chronic Kidney Disease Progression
    by Li, Q., Chu, W., Shahriyari, L.
    This paper presents a unified six-state Continuous-Time Markov Chain (CTMC) framework for Chronic Kidney Disease (CKD) progression, with CKD stages 1-5 modeled as transient states and death as an absorbing state. Under a non-homogeneous CTMC formulation, we derive integral representations for transition probabilities, state distributions, sojourn times, and survival-related quantities. We then study the homogeneous case as a tractable baseline and provide explicit formulas for key quantities. Although the methodology is rooted in standard multi-state theory, these expressions are often […]
  • Reconstructing heterogeneous metabolic trajectories of E. coli diauxie via a dynamical Maximum Entropy Principle
    by Ferrero, A., Kratzl, F. P., Kelley, L., Korolev, K., Masoero, D., Segre, D., Dukovski, I., de Martino, D.
    The glucose-acetate diauxic shift in E. coli is classically described as an abrupt, population-wide switch from glucose to acetate consumption. Recent experiments challenge this view, revealing a robust intermediate regime of co-consumption whose single-cell basis remains unresolved: does it reflect coexisting specialized subpopulations, or genuine mixed metabolic states within individual cells? We first develop a two-state consumer-resource model in which cells optimally grow on either glucose or acetate, and show that observed co-consumption trajectories cannot be decomposed into convex combinations […]
  • Endocytosis suppresses stochastic collapse in fibroblast-macrophage circuits under shared resource competition
    by Inoue, K.-i., Ishii, Y., Hariyama, M.
    Interdependent multicellular circuits must maintain stable coexistence despite competition for shared environmental resources. Fibroblast-macrophage circuits represent a conserved signaling architecture in which fibroblasts produce colony-stimulating factor 1 (CSF) to support macrophages, whereas macrophages produce platelet-derived growth factor (PDGF) to support fibroblasts. Previous analytical models proposed receptor-mediated endocytosis as a stabilizing negative-feedback mechanism, but these formulations assumed spatial homogeneity and independently assigned carrying capacities. Here, we constructed a spatial agent-based fibroblast-macrophage circuit model using PhysiCell to investigate how PDGF and CSF […]
  • Learning dynamical systems with biochemically informed neural ordinary differential equations
    by Fonseca, L. L., Laubenbacher, R., Boettcher, L.
    Ordinary differential equation models of biochemical reactions are often formulated as stoichiometric systems in which the dynamics arise from a collection of interacting processes. A central challenge is that the functional form of each process is rarely known a priori and may be difficult to infer from data. We propose biochemically informed neural ordinary differential equations (BINODEs), a neural-ODE framework that retains the stoichiometric structure of mechanistic models while representing individual processes by neural networks. In BINODEs, the outputs of […]
  • Spatiotemporal remodeling of cytoskeletal and junction networks during somatic cell reprogramming
    by Samson, R., Kitaygorodsky, J., Tersigni, M., Tursun, T., Hu, Q., Hardy, W. R., Trcka, D., Rost, H., Wrana, J. L., Samavarchi-Tehrani, P., Gingras, A.-C.
    Summary/AbstractReprogramming somatic cells into induced pluripotent stem cells involves a dramatic reorganization of the cytoskeleton and junctions during the critical mesenchymal-to-epithelial transition stage. While protein abundance changes have been profiled, the spatiotemporal dynamics of protein-protein associations involving these structural components remain poorly resolved. Here, we present a time-resolved proximity proteomics resource that maps cytoskeletal and junctional remodeling across 27 baits during the early stages of reprogramming. We identified over 1100 high-confidence interactions, including many not previously reported, capturing the dynamic […]
  • hB-PAC: A non-invasive aging clock for quantifying individual differences in aging
    by Ando, Y., Yada, Y., Kashima, M., Bessho, Y., Hirata, H., Naoki, H., MATSUI, T.
    Aging progresses heterogeneously among individuals, and aging clocks that estimate biological age have been developed to quantify this heterogeneity. However, existing methods depend on invasive tissue sampling or long-term longitudinal data, and a mathematical framework that explicitly quantifies individual differences in aging has not yet been established. Here, we employed a progeroid zebrafish model (klotho mutant; kl-/-) and developed a hierarchical Bayesian framework, termed the hierarchical Bayesian-Multimodal Aging Clock (hB-MAC), which integrates non-invasive snapshot data of behavior and morphology with […]
  • A Cross-tissue Temporal Multi-omics Atlas Reveals the Molecular Architecture of Pressure Injury
    by Jiang, F., Li, L., Zhao, Y., Zhang, T., Li, X., Wei, J., Liu, X., Jia, Y., An, M., Jiao, X.
    Pressure injury induces progressive necrosis of skin and deep muscle, yet how mechanical loading reshapes molecular programs across tissues and time remains poorly defined. To address this gap, we established a rat pressure-injury model and performed longitudinal integrated profiling of skin and deep muscle across four stages, combining transcriptomics, proteomics and untargeted metabolomics with histological assessment. This multi-layered atlas revealed a staged injury program dominated by early transcriptional activation of innate immunity and complement-coagulation crosstalk, accompanied by neutrophil-associated responses and […]
  • Fatty acid metabolic interactome atlas linked to cellular longevity
    by Naaz, A., Gao, M., Zhang, Y., Dorajoo, R., Kennedy, B. K., Alfatah, M.
    Fatty acid biosynthesis is a central metabolic process required for membrane formation, organelle maintenance, and cellular proliferation, yet its broader relationship with stress responses and cellular aging remains incompletely understood. Here, we combined human and yeast interactome analyses with transcriptomic profiling and chronological lifespan assays to investigate the systems-level organization of fatty acid metabolic pathways and their relationship to cellular longevity. Integrated interactome mapping of mammalian fatty acid metabolic regulators, including ACACA, FASN, SCD, ACSL, ELOVL, and SLC27 family proteins, […]
  • A conserved transcriptomic model defines metabolic resilience and vulnerability in obesity
    by Su, Y.-Y., Bundalian, L. T., Chen, Y.-C., Gjermeni, E., Gille, B., Richter, S., Jasaszwili, M., Palma-Vera, S., Hoffmann, A., Ghosh, A., Wolfrum, C., Bluher, M., Peleg, S., Garten, A., Le Duc, D., Lin, C.-C.
    BackgroundObesity arises from a complex interplay of genetic and environmental factors, with alterations of transcriptional networks that integrate metabolic, immune, and regulatory pathways. Conventional measures such as body mass index (BMI) quantify body size but fail to capture the molecular heterogeneity underlying divergent metabolic outcomes. We therefore sought to construct a gene expression-based transcriptomic representation of obesity, using BMI as a practical training anchor, and to use this framework to delineate transcriptional programs associated with metabolically healthy and pathogenic obesity, […]
  • A Simulation of Semi-Infectious Particles and Genome Complementation Reproduces Interferon Response by Respiratory Epithelial Cells in vitro during Influenza A Virus Infection
    by Dal-Castel, P. C., Resnick, J. D., Sluka, J. P., Gallagher, M. E., Helfers, M., Bird, I. M., Ratcliff, J. D., Grady, S. L., Glazier, J. A.
    In the respiratory epithelium, interferon (IFN)-induced antiviral resistance acts as a defense against infection. Influenza A viruses (IAVs) have evolved multiple strategies to counteract these defenses, including expression of the viral protein NS1, which inhibits both IFN production and the IFN-mediated transcription of Interferon Stimulated Genes (ISG) in infected cells. However, experiments show that this inhibition is imperfect, especially at a low multiplicity of infection (MOI). One hypothesis to describe this phenomenon relies on the presence of Semi-infectious Particles (SIPs) […]

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