Your search keyword '"whole-cell modeling"' showing total 26 results

1. Soft X‐ray tomograms provide a structural basis for whole‐cell modeling

Author

Loconte, Valentina, Chen, Jian‐Hua, Vanslembrouck, Bieke, Ekman, Axel A, McDermott, Gerry, Le Gros, Mark A, and Larabell, Carolyn A

Subjects

Biochemistry and Cell Biology, Biological Sciences, Bioengineering, Biomedical Imaging, Generic health relevance, X-Rays, Imaging, Three-Dimensional, Tomography, X-Ray, Organelles, cell structure, soft X-ray tomography, subcellular organization, whole-cell modeling, Physiology, Medical Physiology, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical physiology

Abstract

Developing in silico models that accurately reflect a whole, functional cell is an ongoing challenge in biology. Current efforts bring together mathematical models, probabilistic models, visual representations, and data to create a multi-scale description of cellular processes. A realistic whole-cell model requires imaging data since it provides spatial constraints and other critical cellular characteristics that are still impossible to obtain by calculation alone. This review introduces Soft X-ray Tomography (SXT) as a powerful imaging technique to visualize and quantify the mesoscopic (~25 nm spatial scale) organelle landscape in whole cells. SXT generates three-dimensional reconstructions of cellular ultrastructure and provides a measured structural framework for whole-cell modeling. Combining SXT with data from disparate technologies at varying spatial resolutions provides further biochemical details and constraints for modeling cellular mechanisms. We conclude, based on the results discussed here, that SXT provides a foundational dataset for a broad spectrum of whole-cell modeling experiments.

Published

2023

2. Bayesian metamodeling of complex biological systems across varying representations

Author

Raveh, Barak, Sun, Liping, White, Kate L, Sanyal, Tanmoy, Tempkin, Jeremy, Zheng, Dongqing, Bharath, Kala, Singla, Jitin, Wang, Chenxi, Zhao, Jihui, Li, Angdi, Graham, Nicholas A, Kesselman, Carl, Stevens, Raymond C, and Sali, Andrej

Subjects

Diabetes, Bayes Theorem, Computer Simulation, Humans, Linear Models, Models, Biological, integrative modeling, whole-cell modeling, pancreatic beta-cell, multiscale modeling, Bayesian metamodeling, pancreatic β-cell

Abstract

Comprehensive modeling of a whole cell requires an integration of vast amounts of information on various aspects of the cell and its parts. To divide and conquer this task, we introduce Bayesian metamodeling, a general approach to modeling complex systems by integrating a collection of heterogeneous input models. Each input model can in principle be based on any type of data and can describe a different aspect of the modeled system using any mathematical representation, scale, and level of granularity. These input models are 1) converted to a standardized statistical representation relying on probabilistic graphical models, 2) coupled by modeling their mutual relations with the physical world, and 3) finally harmonized with respect to each other. To illustrate Bayesian metamodeling, we provide a proof-of-principle metamodel of glucose-stimulated insulin secretion by human pancreatic β-cells. The input models include a coarse-grained spatiotemporal simulation of insulin vesicle trafficking, docking, and exocytosis; a molecular network model of glucose-stimulated insulin secretion signaling; a network model of insulin metabolism; a structural model of glucagon-like peptide-1 receptor activation; a linear model of a pancreatic cell population; and ordinary differential equations for systemic postprandial insulin response. Metamodeling benefits from decentralized computing, while often producing a more accurate, precise, and complete model that contextualizes input models as well as resolves conflicting information. We anticipate Bayesian metamodeling will facilitate collaborative science by providing a framework for sharing expertise, resources, data, and models, as exemplified by the Pancreatic β-Cell Consortium.

Published

2021

3. Multi-scale models of whole cells: progress and challenges

Author

Konstantia Georgouli, Jae-Seung Yeom, Robert C. Blake, and Ali Navid

Subjects

whole-cell modeling, systems biology, multi-scale models, data integration, high performance computing, Biology (General), QH301-705.5

Abstract

Whole-cell modeling is “the ultimate goal” of computational systems biology and “a grand challenge for 21st century” (Tomita, Trends in Biotechnology, 2001, 19(6), 205–10). These complex, highly detailed models account for the activity of every molecule in a cell and serve as comprehensive knowledgebases for the modeled system. Their scope and utility far surpass those of other systems models. In fact, whole-cell models (WCMs) are an amalgam of several types of “system” models. The models are simulated using a hybrid modeling method where the appropriate mathematical methods for each biological process are used to simulate their behavior. Given the complexity of the models, the process of developing and curating these models is labor-intensive and to date only a handful of these models have been developed. While whole-cell models provide valuable and novel biological insights, and to date have identified some novel biological phenomena, their most important contribution has been to highlight the discrepancy between available data and observations that are used for the parametrization and validation of complex biological models. Another realization has been that current whole-cell modeling simulators are slow and to run models that mimic more complex (e.g., multi-cellular) biosystems, those need to be executed in an accelerated fashion on high-performance computing platforms. In this manuscript, we review the progress of whole-cell modeling to date and discuss some of the ways that they can be improved.

Published

2023

4. Dynamics of chromosome organization in a minimal bacterial cell

Author

Benjamin R. Gilbert, Zane R. Thornburg, Troy A. Brier, Jan A. Stevens, Fabian Grünewald, John E. Stone, Siewert J. Marrink, and Zaida Luthey-Schulten

Subjects

whole-cell modeling, chromosome replication, chromosome segregation, brownian dynamics, smc proteins, topoisomerase, Biology (General), QH301-705.5

Abstract

Computational models of cells cannot be considered complete unless they include the most fundamental process of life, the replication and inheritance of genetic material. By creating a computational framework to model systems of replicating bacterial chromosomes as polymers at 10 bp resolution with Brownian dynamics, we investigate changes in chromosome organization during replication and extend the applicability of an existing whole-cell model (WCM) for a genetically minimal bacterium, JCVI-syn3A, to the entire cell-cycle. To achieve cell-scale chromosome structures that are realistic, we model the chromosome as a self-avoiding homopolymer with bending and torsional stiffnesses that capture the essential mechanical properties of dsDNA in Syn3A. In addition, the conformations of the circular DNA must avoid overlapping with ribosomes identitied in cryo-electron tomograms. While Syn3A lacks the complex regulatory systems known to orchestrate chromosome segregation in other bacteria, its minimized genome retains essential loop-extruding structural maintenance of chromosomes (SMC) protein complexes (SMC-scpAB) and topoisomerases. Through implementing the effects of these proteins in our simulations of replicating chromosomes, we find that they alone are sufficient for simultaneous chromosome segregation across all generations within nested theta structures. This supports previous studies suggesting loop-extrusion serves as a near-universal mechanism for chromosome organization within bacterial and eukaryotic cells. Furthermore, we analyze ribosome diffusion under the influence of the chromosome and calculate in silico chromosome contact maps that capture inter-daughter interactions. Finally, we present a methodology to map the polymer model of the chromosome to a Martini coarse-grained representation to prepare molecular dynamics models of entire Syn3A cells, which serves as an ultimate means of validation for cell states predicted by the WCM.

Published

2023

5. Integrative modeling of the cell

Author

Zhong Xianni, Zhao Jihui, and Sun Liping

Subjects

whole-cell modeling, integrative modeling, compartment model, cell biology, Biochemistry, QD415-436, Genetics, QH426-470

Abstract

A whole-cell model represents certain aspects of the cell structure and/or function. Due to the high complexity of the cell, an integrative modeling approach is often taken to utilize all available information including experimental data, prior knowledge and prior models. In this review, we summarize an emerging workflow of whole-cell modeling into five steps: (i) gather information; (ii) represent the modeled system into modules; (iii) translate input information into scoring function; (iv) sample the whole-cell model; (v) validate and interpret the model. In particular, we propose the integrative modeling of the cell by combining available (whole-cell) models to maximize the accuracy, precision, and completeness. In addition, we list quantitative predictions of various aspects of cell biology from existing whole-cell models. Moreover, we discuss the remaining challenges and future directions, and highlight the opportunity to establish an integrative spatiotemporal multi-scale whole-cell model based on a community approach.

Published

2022

6. Opportunities and Challenges in Building a Spatiotemporal Multi-scale Model of the Human Pancreatic β Cell

Author

Singla, Jitin, McClary, Kyle M, White, Kate L, Alber, Frank, Sali, Andrej, and Stevens, Raymond C

Subjects

Biochemistry and Cell Biology, Biological Sciences, Pancreatic Cancer, Rare Diseases, Cancer, Diabetes, Digestive Diseases, Computational Biology, Drug Discovery, Humans, Insulin-Secreting Cells, Models, Biological, Proteins, Whole-cell modeling, convergent bioscience, data-driven modeling, diabetes, integrative modeling, modeling of dynamics, multi-scale modeling, pancreatic β–cells, structure modeling, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

The construction of a predictive model of an entire eukaryotic cell that describes its dynamic structure from atomic to cellular scales is a grand challenge at the intersection of biology, chemistry, physics, and computer science. Having such a model will open new dimensions in biological research and accelerate healthcare advancements. Developing the necessary experimental and modeling methods presents abundant opportunities for a community effort to realize this goal. Here, we present a vision for creation of a spatiotemporal multi-scale model of the pancreatic β-cell, a relevant target for understanding and modulating the pathogenesis of diabetes.

Published

2018

7. Learning causal networks using inducible transcription factors and transcriptome‐wide time series

Author

Sean R Hackett, Edward A Baltz, Marc Coram, Bernd J Wranik, Griffin Kim, Adam Baker, Minjie Fan, David G Hendrickson, Marc Berndl, and R Scott McIsaac

Subjects

causal inference, gene expression, transcription factors, whole‐cell modeling, dynamical systems, Biology (General), QH301-705.5, Medicine (General), R5-920

Abstract

Abstract We present IDEA (the Induction Dynamics gene Expression Atlas), a dataset constructed by independently inducing hundreds of transcription factors (TFs) and measuring timecourses of the resulting gene expression responses in budding yeast. Each experiment captures a regulatory cascade connecting a single induced regulator to the genes it causally regulates. We discuss the regulatory cascade of a single TF, Aft1, in detail; however, IDEA contains > 200 TF induction experiments with 20 million individual observations and 100,000 signal‐containing dynamic responses. As an application of IDEA, we integrate all timecourses into a whole‐cell transcriptional model, which is used to predict and validate multiple new and underappreciated transcriptional regulators. We also find that the magnitudes of coefficients in this model are predictive of genetic interaction profile similarities. In addition to being a resource for exploring regulatory connectivity between TFs and their target genes, our modeling approach shows that combining rapid perturbations of individual genes with genome‐scale time‐series measurements is an effective strategy for elucidating gene regulatory networks.

Published

2020

8. Whole-Cell Modeling and Simulation: A Brief Survey.

Author

Bhat, Nayana G. and Balaji, S.

Subjects

*BIOENGINEERING, *BIOLOGICAL systems, *SIMULATION methods & models, *LIFE sciences, *ENGINEERING systems, *SYNTHETIC biology

Abstract

Gaining knowledge and engineering of biological systems require comprehensive models of cellular physiology with 100% predictability. The whole-cell models direct experiments in molecular biological science and empower simulation and computer-aided design in synthetic biology. Whole-cell modeling and simulation help in personalized medical treatment building a biological system through cell interactions. In addition, the whole-cell model can address specific issues such as transcription, regulation, pathways for protein expression and many more. Constructing comprehensive whole-cell models with enough detail and validating them is a massive work. Though considering available parameters and pathways, modeling and simulation of a cell are partially successful, still, there exist a lot of more challenges that need to be tackled. Notwithstanding the immense challenges, whole-cell models are quickly getting to be viable. This paper briefly reviews the cutting edge of existing methods and techniques with their present status and the reason for improvements required in various stages of whole-cell modeling such as (1) collection of data, (2) designing tools and model building, (3) acceleration of simulation speed and (4) visualizing and analyzing. [ABSTRACT FROM AUTHOR]

Published

2020

9. Learning causal networks using inducible transcription factors and transcriptome‐wide time series.

Author

Hackett, Sean R, Baltz, Edward A, Coram, Marc, Wranik, Bernd J, Kim, Griffin, Baker, Adam, Fan, Minjie, Hendrickson, David G, Berndl, Marc, and McIsaac, R Scott

Subjects

*TRANSCRIPTION factors, *TIME series analysis, *REGULATOR genes, *GENE expression, *DYNAMICAL systems, *CIS-regulatory elements (Genetics), *FUNGAL gene expression

Abstract

We present IDEA (the Induction Dynamics gene Expression Atlas), a dataset constructed by independently inducing hundreds of transcription factors (TFs) and measuring timecourses of the resulting gene expression responses in budding yeast. Each experiment captures a regulatory cascade connecting a single induced regulator to the genes it causally regulates. We discuss the regulatory cascade of a single TF, Aft1, in detail; however, IDEA contains > 200 TF induction experiments with 20 million individual observations and 100,000 signal‐containing dynamic responses. As an application of IDEA, we integrate all timecourses into a whole‐cell transcriptional model, which is used to predict and validate multiple new and underappreciated transcriptional regulators. We also find that the magnitudes of coefficients in this model are predictive of genetic interaction profile similarities. In addition to being a resource for exploring regulatory connectivity between TFs and their target genes, our modeling approach shows that combining rapid perturbations of individual genes with genome‐scale time‐series measurements is an effective strategy for elucidating gene regulatory networks. Synopsis: A transcriptional induction system is used to conditionally express hundreds of transcription factors in yeast. The resulting time‐course transcriptomics data are used to train parametric models and predict regulatory connections between genes. Chechik & Koller model is used to obtain kinetic parameters for > 100,000 regulatory connections between transcription factors and their target genes.Regulator‐target gene connections are predicted with a dynamical systems model.Transcription factor induction experiments reveal new regulatory connections as well as transcriptional feedback loops and cascades at a genome‐wide scale.The presented data and modeling results can be explored interactively at https://idea.research.calicolabs.com. [ABSTRACT FROM AUTHOR]

Published

2020

10. Cross-evaluation of E. coli's operon structures via a whole-cell model suggests alternative cellular benefits for low- versus high-expressing operons.

Author

Sun G, DeFelice MM, Gillies TE, Ahn-Horst TA, Andrews CJ, Krummenacker M, Karp PD, Morrison JH, and Covert MW

Subjects

Bacteria genetics, Escherichia coli genetics, Operon genetics

Abstract

Many bacteria use operons to coregulate genes, but it remains unclear how operons benefit bacteria. We integrated E. coli's 788 polycistronic operons and 1,231 transcription units into an existing whole-cell model and found inconsistencies between the proposed operon structures and the RNA-seq read counts that the model was parameterized from. We resolved these inconsistencies through iterative, model-guided corrections to both datasets, including the correction of RNA-seq counts of short genes that were misreported as zero by existing alignment algorithms. The resulting model suggested two main modes by which operons benefit bacteria. For 86% of low-expression operons, adding operons increased the co-expression probabilities of their constituent proteins, whereas for 92% of high-expression operons, adding operons resulted in more stable expression ratios between the proteins. These simulations underscored the need for further experimental work on how operons reduce noise and synchronize both the expression timing and the quantity of constituent genes. A record of this paper's transparent peer review process is included in the supplemental information., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

11. Replicating Chromosomes in Whole-Cell Models of Bacteria.

Author

Gilbert BR and Luthey-Schulten Z

Subjects

DNA, Bacterial genetics, Bacteria genetics, Chromosomes, Bacterial genetics, DNA Replication

Abstract

Computational models of cells cannot be considered complete unless they include the most fundamental process of life, the replication of genetic material. In a recent study, we presented a computational framework to model systems of replicating bacterial chromosomes as polymers at 10 bp resolution with Brownian dynamics. This approach was used to investigate changes in chromosome organization during replication and extend the applicability of an existing whole-cell model (WCM) for a genetically minimal bacterium, JCVI-syn3A, to the entire cell cycle. To achieve cell-scale chromosome structures that are realistic, we modeled the chromosome as a self-avoiding homopolymer with bending and torsional stiffnesses that capture the essential mechanical properties of dsDNA in Syn3A. Additionally, the polymer interacts with ribosomes distributed according to cryo-electron tomograms of Syn3A. The polymer model was further augmented by computational models of loop extrusion by structural maintenance of chromosomes (SMC) protein complexes and topoisomerase action, and the modeling and analysis of multi-fork replication states., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

12. Computer Simulation for Effective Pharmaceutical Kinetics and Dynamics: A Review.

Author

Tiwari G, Shukla A, Singh A, and Tiwari R

Abstract

Computer-based modelling and simulation are developing as effective tools for supplementing biological data processing and interpretation. It helps to accelerate the creation of dosage forms at a lower cost and with the less human effort required to conduct the work. This paper aims to provide a comprehensive description of the different computer simulation models for various drugs along with their outcomes. The data used are taken from different sources, including review papers from Science Direct, Elsevier, NCBI, and Web of Science from 1995-2020. Keywords like - pharmacokinetic, pharmacodynamics, computer simulation, whole-cell model, and cell simulation, were used for the search process. The use of computer simulation helps speed up the creation of new dosage forms at a lower cost and less human effort required to complete the work. It is also widely used as a technique for researching the structure and dynamics of lipids and proteins found in membranes. It also facilitates both the diagnosis and prevention of illness. Conventional data analysis methods cannot assess and comprehend the huge amount, size, and complexity of data collected by in vitro, in vivo, and ex vivo experiments. As a result, numerous in silico computational e-resources, databases, and simulation software are employed to determine pharmacokinetic (PK) and pharmacodynamic (PD) parameters for illness management. These techniques aid in the provision of multiscale representations of biological processes, beginning with proteins and genes and progressing through cells, isolated tissues and organs, and the whole organism., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2024

13. An energetic reformulation of kinetic rate laws enables scalable parameter estimation for biochemical networks.

Author

C. Mason, John and W. Covert, Markus

Subjects

*DYNAMICS, *DATA acquisition systems, *METABOLIC disorders, *PERTURBATION theory, *BIOCHEMISTRY

Abstract

Highlights • Standard kinetic rate laws can be reformulated to an energetic basis. • The energetic reformulation readily links data availability to model parameters. • A novel perturbation approach leads to more successful parameter estimation. • Estimated parameters compare well with validation data, and yield biological insight. Abstract The technology for building functionally complete or 'whole-cell' biological simulations is rapidly developing. However, the predictive capabilities of these simulations are hindered by the availability of parameter values, which are often difficult or even impossible to obtain experimentally and must therefore be estimated. Using E. coli 's glycolytic network as a model system, we describe and apply a new method which can estimate the values of all the system's 102 parameters – fit to observations from studies of proteomics, metabolomics, enzyme kinetics and chemical energetics – and find that the resulting metabolic models are not only well-fit, but also dynamically stable. An analysis of how well parameter values in the network were determined by the training data revealed that over 80% of the parameter values were not well-specified. Moreover, the distribution of well-determined values was biased to a specific part of the network and against certain types of experimental data. Our results also suggest that perturbing the functional, energetic space of parameters (rather than traditional metabolic parameters) is a superior strategy for exploring the space of biological dynamics. The estimated parameter values matched both training data and previously withheld validation data within an order of magnitude for over 85% of the data points; notably, the area of greatest frustration in the network was also the most fully determined. Finally, our estimation method showed that fidelity to physiological observations such as network response time is enforced at the cost of fit to molecular parameter values. In summary, our reformulation enables estimation of accurate, biologically relevant parameters, generates insight into the biology of the simulated network, and appears generalizable to any biochemical network – potentially including whole-cell models. [ABSTRACT FROM AUTHOR]

Published

2019

14. Multi-scale models of whole cells: progress and challenges.

Author

Georgouli K, Yeom JS, Blake RC, and Navid A

Abstract

Whole-cell modeling is "the ultimate goal" of computational systems biology and "a grand challenge for 21st century" (Tomita, Trends in Biotechnology, 2001, 19(6), 205-10). These complex, highly detailed models account for the activity of every molecule in a cell and serve as comprehensive knowledgebases for the modeled system. Their scope and utility far surpass those of other systems models. In fact, whole-cell models (WCMs) are an amalgam of several types of "system" models. The models are simulated using a hybrid modeling method where the appropriate mathematical methods for each biological process are used to simulate their behavior. Given the complexity of the models, the process of developing and curating these models is labor-intensive and to date only a handful of these models have been developed. While whole-cell models provide valuable and novel biological insights, and to date have identified some novel biological phenomena, their most important contribution has been to highlight the discrepancy between available data and observations that are used for the parametrization and validation of complex biological models. Another realization has been that current whole-cell modeling simulators are slow and to run models that mimic more complex (e.g., multi-cellular) biosystems, those need to be executed in an accelerated fashion on high-performance computing platforms. In this manuscript, we review the progress of whole-cell modeling to date and discuss some of the ways that they can be improved., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Georgouli, Yeom, Blake and Navid.)

Published

2023

15. The Sum of the Parts: Large-Scale Modeling in Systems Biology.

Author

Gross, Fridolin and Greeny, Sara

Published

2017

16. Dynamics of chromosome organization in a minimal bacterial cell.

Author

Gilbert BR, Thornburg ZR, Brier TA, Stevens JA, Grünewald F, Stone JE, Marrink SJ, and Luthey-Schulten Z

Abstract

Computational models of cells cannot be considered complete unless they include the most fundamental process of life, the replication and inheritance of genetic material. By creating a computational framework to model systems of replicating bacterial chromosomes as polymers at 10 bp resolution with Brownian dynamics, we investigate changes in chromosome organization during replication and extend the applicability of an existing whole-cell model (WCM) for a genetically minimal bacterium, JCVI-syn3A, to the entire cell-cycle. To achieve cell-scale chromosome structures that are realistic, we model the chromosome as a self-avoiding homopolymer with bending and torsional stiffnesses that capture the essential mechanical properties of dsDNA in Syn3A. In addition, the conformations of the circular DNA must avoid overlapping with ribosomes identitied in cryo-electron tomograms. While Syn3A lacks the complex regulatory systems known to orchestrate chromosome segregation in other bacteria, its minimized genome retains essential loop-extruding structural maintenance of chromosomes (SMC) protein complexes (SMC-scpAB) and topoisomerases. Through implementing the effects of these proteins in our simulations of replicating chromosomes, we find that they alone are sufficient for simultaneous chromosome segregation across all generations within nested theta structures. This supports previous studies suggesting loop-extrusion serves as a near-universal mechanism for chromosome organization within bacterial and eukaryotic cells. Furthermore, we analyze ribosome diffusion under the influence of the chromosome and calculate in silico chromosome contact maps that capture inter-daughter interactions. Finally, we present a methodology to map the polymer model of the chromosome to a Martini coarse-grained representation to prepare molecular dynamics models of entire Syn3A cells, which serves as an ultimate means of validation for cell states predicted by the WCM., Competing Interests: JES was employed by the company NVIDIA Corporation. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Gilbert, Thornburg, Brier, Stevens, Grünewald, Stone, Marrink and Luthey-Schulten.)

Published

2023

17. Biomolecular interactions modulate macromolecular structure and dynamics in atomistic model of a bacterial cytoplasm

Author

Isseki Yu, Takaharu Mori, Tadashi Ando, Ryuhei Harada, Jaewoon Jung, Yuji Sugita, and Michael Feig

Subjects

crowding effects, metabolite dynamics, whole-cell modeling, native state stability, diffusion, quinary interactions, Medicine, Science, Biology (General), QH301-705.5

Abstract

Biological macromolecules function in highly crowded cellular environments. The structure and dynamics of proteins and nucleic acids are well characterized in vitro, but in vivo crowding effects remain unclear. Using molecular dynamics simulations of a comprehensive atomistic model cytoplasm we found that protein-protein interactions may destabilize native protein structures, whereas metabolite interactions may induce more compact states due to electrostatic screening. Protein-protein interactions also resulted in significant variations in reduced macromolecular diffusion under crowded conditions, while metabolites exhibited significant two-dimensional surface diffusion and altered protein-ligand binding that may reduce the effective concentration of metabolites and ligands in vivo. Metabolic enzymes showed weak non-specific association in cellular environments attributed to solvation and entropic effects. These effects are expected to have broad implications for the in vivo functioning of biomolecules. This work is a first step towards physically realistic in silico whole-cell models that connect molecular with cellular biology.

Published

2016

18. Why Build Whole-Cell Models?

Author

Carrera, Javier and Covert, Markus W.

Subjects

*CELL physiology, *COMPUTATIONAL biology, *CYTOGENETICS, *CELL morphology, *BIOLOGICAL research

Abstract

Our ability to build computational models that account for all known gene functions in a cell has increased dramatically. But why build whole-cell models, and how can they best be used? In this forum, we enumerate several areas in which whole-cell modeling can significantly impact research and technology. [ABSTRACT FROM AUTHOR]

Published

2015

19. A new visual design language for biological structures in a cell.

Author

Singla, Jitin, Burdsall, Kylie, Cantrell, Brian, Halsey, Jordan R., McDowell, Alex, McGregor, Colleen, Mittal, Sanraj, Stevens, Raymond C., Su, Shaoyu, Thomopoulos, Alexandra, Vaillant, Theotime, White, Kate L., Zhang, Bryan, and Berman, Helen M.

Subjects

*CELL anatomy, *CELLULAR recognition, *BIOMOLECULES, *LANGUAGE & languages

Abstract

As part of a project to build a spatiotemporal model of the pancreatic β-cell, we are creating an immersive experience called "World in a Cell" that can be used to integrate and create new educational tools. To do this, we have developed a new visual design language that uses tetrahedral building blocks to express the structural features of biological molecules and organelles in crowded cellular environments. The tetrahedral language enables more efficient animation and user interaction in an immersive environment. [Display omitted] • Biological structures are represented with tetrahedral building blocks • The tetrahedral representation facilitates recognition of the cellular components • The representation is compatible with immersive environments Singla et al. present a design language to represent biological structures using tetrahedral building blocks. The proposed design language in this article enables more efficient animation and user interaction in an immersive environment for building crowded cellular environments. [ABSTRACT FROM AUTHOR]

Published

2022

20. WholeCellViz: data visualization for whole-cell models.

Author

Lee, Ruby, Karr, Jonathan R., and Covert, Markus W.

Subjects

*COMPUTER software, *COMPUTER simulation, *BIOINFORMATICS

Abstract

Background: Whole-cell models promise to accelerate biomedical science and engineering. However, discovering new biology from whole-cell models and other high-throughput technologies requires novel tools for exploring and analyzing complex, high-dimensional data. Results: We developed WholeCellViz, a web-based software program for visually exploring and analyzing whole-cell simulations. WholeCellViz provides 14 animated visualizations, including metabolic and chromosome maps. These visualizations help researchers analyze model predictions by displaying predictions in their biological context. Furthermore, WholeCellViz enables researchers to compare predictions within and across simulations by allowing users to simultaneously display multiple visualizations. Conclusion: WholeCellViz was designed to facilitate exploration, analysis, and communication of whole-cell model data. Taken together, WholeCellViz helps researchers use whole-cell model simulations to drive advances in biology and bioengineering. [ABSTRACT FROM AUTHOR]

Published

2013

21. A Petri nets-based framework for whole-cell modeling.

Author

Liu, Fei, Assaf, George, Chen, Ming, and Heiner, Monika

Subjects

*SYSTEMS biology, *PETRI nets, *CELL anatomy

Abstract

Whole-cell modeling aims to incorporate all main genes and processes, and their interactions of a cell in one model. Whole-cell modeling has been regarded as the central aim of systems biology but also as a grand challenge, which plays essential roles in current and future systems biology. In this paper, we analyze whole-cell modeling challenges and requirements and classify them into three aspects (or dimensions): heterogeneous biochemical networks, uncertainties in components, and representation of cell structure. We then explore how to use different Petri net classes to address different aspects of whole-cell modeling requirements. Based on these analyses, we present a Petri nets-based framework for whole-cell modeling, which not only addresses many whole-cell modeling requirements, but also offers a graphical, modular, and hierarchical modeling tool. We think this framework can offer a feasible modeling approach for whole-cell model construction. [ABSTRACT FROM AUTHOR]

Published

2021

22. The E. coli Whole-Cell Modeling Project.

Author

Sun G, Ahn-Horst TA, and Covert MW

Subjects

Escherichia coli genetics

Abstract

The Escherichia coli whole-cell modeling project seeks to create the most detailed computational model of an E. coli cell in order to better understand and predict the behavior of this model organism. Details about the approach, framework, and current version of the model are discussed. Currently, the model includes the functions of 43% of characterized genes, with ongoing efforts to include additional data and mechanisms. As additional information is incorporated in the model, its utility and predictive power will continue to increase, which means that discovery efforts can be accelerated by community involvement in the generation and inclusion of data. This project will be an invaluable resource to the E. coli community that could be used to verify expected physiological behavior, to predict new outcomes and testable hypotheses for more efficient experimental design iterations, and to evaluate heterogeneous data sets in the context of each other through deep curation.

Published

2021

23. A forecast for large-scale, predictive biology: Lessons from meteorology.

Author

Covert MW, Gillies TE, Kudo T, and Agmon E

Subjects

Models, Theoretical, Systems Biology, Meteorology, Models, Biological

Abstract

Quantitative systems biology, in which predictive mathematical models are constructed to guide the design of experiments and predict experimental outcomes, is at an exciting transition point, where the foundational scientific principles are becoming established, but the impact is not yet global. The next steps necessary for mathematical modeling to transform biological research and applications, in the same way it has already transformed other fields, is not completely clear. The purpose of this perspective is to forecast possible answers to this question-what needs to happen next-by drawing on the experience gained in another field, specifically meteorology. We review here a number of lessons learned in weather prediction that are directly relevant to biological systems modeling, and that we believe can enable the same kinds of global impact in our field as atmospheric modeling makes today., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

24. Prediction of Cellular Burden with Host-Circuit Models.

Author

Nikolados EM, Weiße AY, and Oyarzún DA

Subjects

Bacterial Physiological Phenomena, Bacterial Proteins genetics, Gene Expression, Genes, Synthetic, Models, Biological, Synthetic Biology, Bacteria genetics, Gene Regulatory Networks, Systems Biology methods

Abstract

Heterologous gene expression draws resources from host cells. These resources include vital components to sustain growth and replication, and the resulting cellular burden is a widely recognized bottleneck in the design of robust circuits. In this tutorial we discuss the use of computational models that integrate gene circuits and the physiology of host cells. Through various use cases, we illustrate the power of host-circuit models to predict the impact of design parameters on both burden and circuit functionality. Our approach relies on a new generation of computational models for microbial growth that can flexibly accommodate resource bottlenecks encountered in gene circuit design. Adoption of this modeling paradigm can facilitate fast and robust design cycles in synthetic biology.

Published

2021

25. Biomolecular interactions modulate macromolecular structure and dynamics in atomistic model of a bacterial cytoplasm.

Author

Yu I, Mori T, Ando T, Harada R, Jung J, Sugita Y, and Feig M

Subjects

Molecular Dynamics Simulation, Spatio-Temporal Analysis, Cytoplasm chemistry, Macromolecular Substances analysis, Mycoplasma genitalium chemistry

Abstract

Biological macromolecules function in highly crowded cellular environments. The structure and dynamics of proteins and nucleic acids are well characterized in vitro, but in vivo crowding effects remain unclear. Using molecular dynamics simulations of a comprehensive atomistic model cytoplasm we found that protein-protein interactions may destabilize native protein structures, whereas metabolite interactions may induce more compact states due to electrostatic screening. Protein-protein interactions also resulted in significant variations in reduced macromolecular diffusion under crowded conditions, while metabolites exhibited significant two-dimensional surface diffusion and altered protein-ligand binding that may reduce the effective concentration of metabolites and ligands in vivo. Metabolic enzymes showed weak non-specific association in cellular environments attributed to solvation and entropic effects. These effects are expected to have broad implications for the in vivo functioning of biomolecules. This work is a first step towards physically realistic in silico whole-cell models that connect molecular with cellular biology., Competing Interests: The authors declare that no competing interests exist.

Published

2016

26. Efficient Analysis of Systems Biology Markup Language Models of Cellular Populations Using Arrays.

Author

Watanabe L and Myers CJ

Subjects

Models, Biological, Software, Programming Languages, Systems Biology methods

Abstract

The Systems Biology Markup Language (SBML) has been widely used for modeling biological systems. Although SBML has been successful in representing a wide variety of biochemical models, the core standard lacks the structure for representing large complex regular systems in a standard way, such as whole-cell and cellular population models. These models require a large number of variables to represent certain aspects of these types of models, such as the chromosome in the whole-cell model and the many identical cell models in a cellular population. While SBML core is not designed to handle these types of models efficiently, the proposed SBML arrays package can represent such regular structures more easily. However, in order to take full advantage of the package, analysis needs to be aware of the arrays structure. When expanding the array constructs within a model, some of the advantages of using arrays are lost. This paper describes a more efficient way to simulate arrayed models. To illustrate the proposed method, this paper uses a population of repressilator and genetic toggle switch circuits as examples. Results show that there are memory benefits using this approach with a modest cost in runtime.

Published

2016