The mechanics of epithelial tissues
Lead Research Organisation:
University of Cambridge
Department Name: Engineering
Abstract
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Technical Summary
Exposure to mechanical stresses is a normal part of physiology for epithelial tissues. This mechanical function is particularly apparent in disease when mutations or pathogens affecting the cytoskeleton, adherens junctions, or desmosomes result in increased fragility of tissues. Despite clear physiological relevance, little is known about the mechanics of epithelia and how these relate to the mechanical properties of the tissue's constituent cells.
We have developed a new experimental tool for measuring the mechanical properties of cell monolayers which can be coupled to high magnification optical microscopy to image cellular phenotype and subcellular organization during mechanical testing. To complement this, we have developed a versatile new numerical modeling platform to serve as a means of interpreting and refining our experiments.
We propose to couple mechanical testing with chemical and genetic perturbations to understand what subcellular structures govern tissue mechanics. To do this, we will carry out a limited siRNA screen focusing on proteins that form or regulate subcellular structures thought to be important for tissue mechanics: adherens junctions, desmosomes, the apical actin cortex, intermediate filaments, contractile proteins and proteins identified in pathologies causing fragile epithelia. Statistical methods will be then used to cluster proteins in groups according to the changes their depletion induces on tissue mechanics. We expect that depletion of proteins participating to the assembly of the same substructures should result in similar mechanical phenotypes. These results will then be implemented into our computational model to tailor it for the study of tissues at large deformations. An iterative cycle of mechanical testing and simulations will be used to refine our understanding of how subcellular structures, cellular structures, and multicellular behaviours control the mechanics of epithelia in normal and pathological conditions.
We have developed a new experimental tool for measuring the mechanical properties of cell monolayers which can be coupled to high magnification optical microscopy to image cellular phenotype and subcellular organization during mechanical testing. To complement this, we have developed a versatile new numerical modeling platform to serve as a means of interpreting and refining our experiments.
We propose to couple mechanical testing with chemical and genetic perturbations to understand what subcellular structures govern tissue mechanics. To do this, we will carry out a limited siRNA screen focusing on proteins that form or regulate subcellular structures thought to be important for tissue mechanics: adherens junctions, desmosomes, the apical actin cortex, intermediate filaments, contractile proteins and proteins identified in pathologies causing fragile epithelia. Statistical methods will be then used to cluster proteins in groups according to the changes their depletion induces on tissue mechanics. We expect that depletion of proteins participating to the assembly of the same substructures should result in similar mechanical phenotypes. These results will then be implemented into our computational model to tailor it for the study of tissues at large deformations. An iterative cycle of mechanical testing and simulations will be used to refine our understanding of how subcellular structures, cellular structures, and multicellular behaviours control the mechanics of epithelia in normal and pathological conditions.
Planned Impact
The proposed research will seek to bridge the gap between molecular, cellular, and tissue-scales to understand the molecular and cellular determinants of epithelial tissue mechanics and investigate how tissues adapt to their mechanical environment. This will primarily benefit academics in the fields of tissue and developmental biology but, in the longer term, through comprehension of the determinants of tissue strength, we envisage that it will benefit tissue engineering startups in the UK and clinical medicine.
Academic impact
Academic advancement and innovation:
We expect our research to attract interest from many fields in the global scientific community such as developmental biology, cell biology, biophysics, bioengineering, and clinical medicine.
To ensure our findings have the highest possible impact, we will present our technological developments and preliminary results generated at high profile conferences that cover relevant topics including tissue engineering, biophysics, developmental biology and cell biology throughout the duration of the grant. Where possible we will disseminate our findings in general audience journals.
Training and professional development:
Both GC and AK are actively involved in interdisciplinary training activities at UCL and Cambridge University. GC participates in teaching in the CoMPLEX DTP and is a member of the new interdisciplinary BBSRC DTP. AK is an important contributor to the development of the Bioengineering curriculum in Cambridge, and teaches a number of relevant subjects ranging from material sciences to physiology. The project described here will be used to introduce students from different backgrounds to interdisciplinary research in the life sciences. Elements of the work will be used as exemplar projects for students in the CoMPLEX and BBSRC DTPs. The mechanical aspects of the project will also form the basis of a couple of 4th year engineering projects in Cambridge and are likely to attract students with a Mechanical/Bio Engineering background.
Throughout the course of the project, the post-docs involved will receive cross-disciplinary mentoring and benefit from regular interactions both in Cambridge and London. In addition, they will be involved in mentoring students and develop their own mentoring and leadership skills. This will aid their progression towards an independent group leader position.
Societal and economic impact
Commercialisation and exploitation:
We envisage that, in the longer term, our integrated mechanical testing and computational modeling approach will be of interest to clinical medicine, bioengineering startups, and the pharmaceutical industry. Indeed, we anticipate that our approach could be utilized to study the effect of pathologic genetic mutations on tissue mechanical properties and test the efficacy of palliative treatments in restoring the mechanical properties of diseased tissues. Should there be industrial interest, we will study the possibility of designing a new prototype in a format suited to high throughput screening.
Both the UCL and Cambridge University have efficient mechanisms to assist academics in the development of commercial applications of their research outputs and in the management of intellectual property rights (see for instance Cambridge Enterprise or UCL Business).
Increasing public engagement and understanding:
Previously members of the team have been involved in interactions with the wider community through public discussions and school visits. Through this type of outreach we expect this work to reach a wide audience, giving the public a better understanding of multidisciplinary research and an appreciation of the remarkable natural world in which we live. The co-Is each expect to participate in one public engagement event per year during the course of this project. We will use these opportunities to stress the important role played by basic research in driving societal advances.
Academic impact
Academic advancement and innovation:
We expect our research to attract interest from many fields in the global scientific community such as developmental biology, cell biology, biophysics, bioengineering, and clinical medicine.
To ensure our findings have the highest possible impact, we will present our technological developments and preliminary results generated at high profile conferences that cover relevant topics including tissue engineering, biophysics, developmental biology and cell biology throughout the duration of the grant. Where possible we will disseminate our findings in general audience journals.
Training and professional development:
Both GC and AK are actively involved in interdisciplinary training activities at UCL and Cambridge University. GC participates in teaching in the CoMPLEX DTP and is a member of the new interdisciplinary BBSRC DTP. AK is an important contributor to the development of the Bioengineering curriculum in Cambridge, and teaches a number of relevant subjects ranging from material sciences to physiology. The project described here will be used to introduce students from different backgrounds to interdisciplinary research in the life sciences. Elements of the work will be used as exemplar projects for students in the CoMPLEX and BBSRC DTPs. The mechanical aspects of the project will also form the basis of a couple of 4th year engineering projects in Cambridge and are likely to attract students with a Mechanical/Bio Engineering background.
Throughout the course of the project, the post-docs involved will receive cross-disciplinary mentoring and benefit from regular interactions both in Cambridge and London. In addition, they will be involved in mentoring students and develop their own mentoring and leadership skills. This will aid their progression towards an independent group leader position.
Societal and economic impact
Commercialisation and exploitation:
We envisage that, in the longer term, our integrated mechanical testing and computational modeling approach will be of interest to clinical medicine, bioengineering startups, and the pharmaceutical industry. Indeed, we anticipate that our approach could be utilized to study the effect of pathologic genetic mutations on tissue mechanical properties and test the efficacy of palliative treatments in restoring the mechanical properties of diseased tissues. Should there be industrial interest, we will study the possibility of designing a new prototype in a format suited to high throughput screening.
Both the UCL and Cambridge University have efficient mechanisms to assist academics in the development of commercial applications of their research outputs and in the management of intellectual property rights (see for instance Cambridge Enterprise or UCL Business).
Increasing public engagement and understanding:
Previously members of the team have been involved in interactions with the wider community through public discussions and school visits. Through this type of outreach we expect this work to reach a wide audience, giving the public a better understanding of multidisciplinary research and an appreciation of the remarkable natural world in which we live. The co-Is each expect to participate in one public engagement event per year during the course of this project. We will use these opportunities to stress the important role played by basic research in driving societal advances.
Organisations
People |
ORCID iD |
| Alexandre Kabla (Principal Investigator) |
Publications
Bonfanti A
(2020)
A unified rheological model for cells and cellularised materials
in Royal Society Open Science
Bonfanti A
(2019)
A unified rheological model for cells and cellularised materials
Bonfanti A
(2020)
Fractional viscoelastic models for power-law materials.
in Soft matter
Fouchard J
(2020)
Curling of epithelial monolayers reveals coupling between active bending and tissue tension.
in Proceedings of the National Academy of Sciences of the United States of America
Kaplan J
(2019)
RHEOS.jl -- A Julia Package for Rheology Data Analysis
in Journal of Open Source Software
Khalilgharibi N
(2019)
Stress relaxation in epithelial monolayers is controlled by the actomyosin cortex.
in Nature physics
Khalilgharibi N
(2016)
The dynamic mechanical properties of cellularised aggregates.
in Current opinion in cell biology
Lisica A
(2022)
Tension at intercellular junctions is necessary for accurate orientation of cell division in the epithelium plane.
in Proceedings of the National Academy of Sciences of the United States of America
Recho P
(2020)
Tug-of-war between stretching and bending in living cell sheets.
in Physical review. E
| Description | Epithelial monolayers are one-cell thick tissue sheets that separate internal and external environments. As part of their function, they withstand extrinsic mechanical stresses applied at high strain rate. However, little is known about how monolayers respond to mechanical deformations. In stress relaxation tests, monolayers respond in a biphasic manner and stress dissipation is accompanied by an increase in monolayer resting length, pointing to active remodelling of cell architecture during relaxation. Consistent with this, actomyosin remodels at a rate commensurate with mechanical relaxation and governs the rate of monolayer stress relaxation - as in single cells. By contrast, junctional complexes and intermediate filaments form stable connections between cells, enabling monolayers to behave rheologically as single cells. Together, these data show actomyosin cytoskeletal dynamics govern the rheological properties of monolayers by enabling active, ATP-dependent changes in the resting length. These findings have far-reaching consequences for our understanding of developmental morphogenesis and tissue response to mechanical stress. In another study, we examined the response of epithelial tissues to shortening in length. Epithelial tissues are subject to mechanical perturbations that vary greatly in magnitude and timescale during development, normal physiological function and regeneration. At timescales of hours to days, their response to perturbations involves cell proliferation and oriented cell division following a stretch (ref) and cell extrusion in response to tissue compression (Marinari and Baum, 2012; Eisenhoffer and Rosenblatt, 2012). While the response of epithelia to stretch has been widely studied, little is known about their response to compressive strain and the molecular mechanisms enabling it despite clear physiological relevance. Here, using monolayers devoid of a substrate, we probe the response of epithelia to compressive strains. When subjected to rapid application of significant (~50%) uniaxial compressive strains, monolayers first buckle as expected from their viscoelastic properties but remarkably, in the following seconds, autonomously driven cell-shape changes return the tissue to a flat configuration. When subjected to slower rate compressive strain, monolayers can retain their flat planar configuration without buckling by accommodating the reduction in surface area through an increase in apico-basal height. A combination of experiment and modelling (performed by Dr Pierre Recho RA funded on this grant in Cambridge) reveals that these behaviours are driven by intrinsic tension generated by the actomyosin cytoskeleton. In physiological conditions, the generation of a resting tension enables epithelia to withstand both compressive and tensile strains while maintaining a planar shape. We also studied a particular aspect of epithelial monolayer, which is the asymmetry of contractility between their apical and basal sides. This leads to spontaneous curvature, and link the in-plane properties of the monolayer with three-dimensional aspects such as curling at the free edges. This has strong implications for the analysis of tissue morphology when the tissue cracks and fails. |
| Exploitation Route | Better fundamental understanding of embryonic development and diseases linked to epithelial fragility. |
| Sectors | Manufacturing, including Industrial Biotechology,Pharmaceuticals and Medical Biotechnology,Other |
| Title | RHEOS |
| Description | We created and published a software package to analyse rheological datasets using advanced mathematical methods. The tools was developed and used as part of our RCUK funded research programs, and then released in the public domain following good software engineering practice. The package is supported by a publication in the Journal of Open Source Software. |
| Type Of Material | Improvements to research infrastructure |
| Year Produced | 2019 |
| Provided To Others? | Yes |
| Impact | This research tool has facilitated our own research (doi:10.1098/rsos.190920), and is already used by other groups, see for instance doi:10.1039/C9SM02158B, published early in 2020. |
| URL | https://github.com/JuliaRheology/RHEOS.jl |
| Title | Research data supporting "Tumour heterogeneity promotes collective invasion and cancer metastatic dissemination" |
| Description | The dataset contains: - the source code used for the simulations, - the raw data of the plots included in the paper, - supplementary videos |
| Type Of Material | Database/Collection of data |
| Year Produced | 2017 |
| Provided To Others? | Yes |
| Title | Rheos |
| Description | The software library provides a computational framework to model the rheological response of materials presenting a power law behaviour. Such behaviour has been observed across a broad range of biological materials. |
| Type Of Technology | Software |
| Year Produced | 2018 |
| Open Source License? | Yes |
| Impact | It has provided us with a reliable mechanism to extract material parameters in monolayers and embryo tissues. This has allowed the prediction of complex behaviours in monolayers, as recently reported in https://www.biorxiv.org/content/10.1101/543330v1. |
| URL | https://github.com/JuliaRheology/RHEOS.jl |
| Description | American Physical Society March Meeting 2016 |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | International |
| Primary Audience | Postgraduate students |
| Results and Impact | The APS March meeting is the main annual meeting of the American Physical Society where recent research findings are presented to the scientific and wider community. |
| Year(s) Of Engagement Activity | 2016 |
| URL | https://meetings.aps.org/Meeting/MAR16/Session/P55.1 |
| Description | Cell Mechanics Workshop, Curie Institute - Invited contribution |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | International |
| Primary Audience | Postgraduate students |
| Results and Impact | The goal of this workshop was to bring together biologists and experimental and theoretical physicists to discuss current topics in cell motility from different perspectives. A strong focus is made on the interaction during the talks and in between sessions. We aim at a mixed audience with a diverse scientific background and different levels of professional experience from students to leading scientists in the field. |
| Year(s) Of Engagement Activity | 2015 |
| URL | http://www.labex-celtisphybio.fr/cell-motility-workshop-2015/ |
| Description | FOR1756 DFG meeting in Cassis |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | International |
| Primary Audience | Postgraduate students |
| Results and Impact | This event was a research focused meeting to share with recent progress and unpublished work with colleagues, including a significant proportion of PhD students and early career researchers. |
| Year(s) Of Engagement Activity | 2018 |
| Description | INSERM Workshop 241 - Live imaging of morphogenesis in 4D: probes, microscopy techniques and quantification, Bordeaux |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | International |
| Primary Audience | Postgraduate students |
| Results and Impact | This workshop consisted in a series of talk/lectures to graduate students to introduce the latest development in the field imaging applied to developmental biology. |
| Year(s) Of Engagement Activity | 2016 |
| Description | World congress in Biomechanics - Invited contribution |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | International |
| Primary Audience | Other audiences |
| Results and Impact | The World Congress of Biomechanics is an international meeting held once every four years, rotating among Europe, Asia and the Americas. This, the 7th WCB, will once again bring together engineers, scientists from various disciplines including biology, physics, mathematics, computer science, chemistry and various clinical specialities. Applications range from basic biology to medical devices to the latest technologies. Researchers, engineers from industry, medical doctors, academics, and students are all welcome. Vendor exhibitions will highlight the latest technologies, publications, and medical devices. Current research was presented at the meeting, reaching international audience. |
| Year(s) Of Engagement Activity | 2014 |
| URL | https://esbiomech.org/newsletter/esbiomech-newsletter-autumn-2013/7th-world-congress-of-biomechanics... |