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1. Stress generation, relaxation and size control in confined tumor growth

   https://doi.org/10.1371/journal.pcbi.1009701  

   Yan, Huaming ; Ramirez-Guerrero, Daniel ; Lowengrub, John ; Wu, Min ( December 2021 , PLOS Computational Biology)

   Maini, Philip K (Ed.)

   Experiments on tumor spheroids have shown that compressive stress from their environment can reversibly decrease tumor expansion rates and final sizes. Stress release experiments show that nonuniform anisotropic elastic stresses can be distributed throughout. The elastic stresses are maintained by structural proteins and adhesive molecules, and can be actively relaxed by a variety of biophysical processes. In this paper, we present a new continuum model to investigate how the growth-induced elastic stresses and active stress relaxation, in conjunction with cell size control feedback machinery, regulate the cell density and stress distributions within growing tumors as well as the tumor sizes in the presence of external physical confinement and gradients of growth-promoting chemical fields. We introduce an adaptive reference map that relates the current position with the reference position but adapts to the current position in the Eulerian frame (lab coordinates) via relaxation. This type of stress relaxation is similar to but simpler than the classical Maxwell model of viscoelasticity in its formulation. By fitting the model to experimental data from two independent studies of tumor spheroid growth and their cell density distributions, treating the tumors as incompressible, neo-Hookean elastic materials, we find that the rates of stress relaxation of tumor tissues can be comparable to volumetric growth rates. Our study provides insight on how the biophysical properties of the tumor and host microenvironment, mechanical feedback control and diffusion-limited differential growth act in concert to regulate spatial patterns of stress and growth. When the tumor is stiffer than the host, our model predicts tumors are more able to change their size and mechanical state autonomously, which may help to explain why increased tumor stiffness is an established hallmark of malignant tumors. 

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2. Epithelial multicellular clustering enabled by polarized macrophages on soft matrices

   https://doi.org/10.1096/fj.202300120RR  

   Zmuda, Hannah ; Pathak, Amit ( June 2023 , The FASEB Journal)

   Formation of epithelial structures of variegated geometries and sizes is essential for organogenesis, tumor growth, and wound repair. Although epithelial cells are predisposed with potential for multicellular clustering, it remains unclear whether immune cells and mechanical cues from their microenvironment influence this process. To explore this possibility, we cocultured human mammary epithelial cells with prepolarized macrophages on soft or stiff hydrogels. In the presence of M1 (proinflammatory) macrophages on soft matrices, epithelial cells migrated faster and subsequently formed larger multicellular clusters compared to cocultures with M0 (unpolarized) or M2 (anti‐inflammatory) macrophages. By contrast, stiff matrices disabled active clustering of epithelial cells due to their enhanced migration and cell–ECM adhesion, regardless of macrophage polarization. We found that the copresence of soft matrices and M1 macrophages reduced focal adhesions, but enhanced fibronectin deposition and nonmuscle myosin‐IIA expression, which altogether optimize conditions for epithelial clustering. Upon ROCK inhibition, epithelial clustering was abrogated, indicating a requirement for optimized cellular forces. In these cocultures, TNF‐α secretion was the highest with M1 macrophages and TGF‐β secretion was exclusively detectable in case of M2 macrophages on soft gels, which indicated potential role of macrophage secreted factors in the observed epithelial clustering. Indeed, exogenous addition of TGF‐β promoted epithelial clustering with M1 coculture on soft gels. According to our findings, optimization of both mechanical and immune factors can tune epithelial clustering responses, which could have implications in tumor growth, fibrosis, and would healing.

    

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3. Mechanical behavior of bio‐inspired composites made of co‐continuous geopolymer and 3D‐printed polymer

   https://doi.org/10.1002/appl.202300097  

   Pang, Siyuan ; Mahrous, Mahmoud A. ; Trindade, Ana Carolina Constancio ; Kozych, Andrij ; Kale, Nupur ; Kriven, Waltraud M. ; Jasiuk, Iwona ( March 2024 , Applied Research)

   Geopolymers (GPs) are emerging, low‐density ceramic materials that are simple to manufacture, with high elastic modulus and strength, albeit with low toughness. Fiber reinforcements have been used to achieve varied ductile behaviors, but little is known about the GP addition to polymeric frame structures. Thus, drawing inspiration from the nanostructure of bones, this paper investigated an interpenetrating, co‐continuous composite consisting of a GP as the stiff but brittle phase, and a 3D‐printed polymer (PA12 White) as the soft and deformable phase. The composite mechanical properties and failure modes were studied experimentally using uniaxial compression and four‐point bending tests. The co‐continuous network constrained brittle cracking within the GP and reduced strain localization in the polymer. The results showed that the composite had higher strength (56.11 ± 2.12 MPa) and elastic modulus (6.08 ± 1.37 GPa) than the 3D‐printed polymer and had higher toughness (5.98 ± 0.24 MJ/mm³) than the GP for the specific geometries examined. The shape effect study demonstrated that cubic structures had higher elastic modulus and strength but at the expense of lower toughness when compared to rectangular prism structures. The study of scale effects indicated that increasing the number of periodic unit cells while maintaining consistent bulk dimensions led to augmented strength and toughness, albeit without statistically significant alterations in elastic modulus. Thus, this paper presents an experimental realization of a novel, bio‐inspired, interpenetrating, GP–polymer composite design, offering improved strength and toughness. It also provides valuable insights into the shape and size effects on the mechanical properties of this new composite.

    

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4. Rigid tumours contain soft cancer cells

   https://doi.org/10.1038/s41567-022-01755-0  

   Fuhs, Thomas ; Wetzel, Franziska ; Fritsch, Anatol W. ; Li, Xinzhi ; Stange, Roland ; Pawlizak, Steve ; Kießling, Tobias R. ; Morawetz, Erik ; Grosser, Steffen ; Sauer, Frank ; et al ( September 2022 , Nature Physics)

   Palpation utilizes the fact that solid breast tumours are stiffer than the surrounding tissue. However, cancer cells tend to soften, which may enhance their ability to squeeze through dense tissue. This apparent paradox proposes two contradicting hypotheses: either softness emerges from adaptation to the tumour’s microenvironment or soft cancer cells are already present inside a rigid primary tumour mass giving rise to cancer cell motility. We investigate primary tumour explants from patients with breast and cervix carcinomas on multiple length scales. We find that primary tumours are highly heterogeneous in their mechanical properties on all scales from the tissue level down to individual cells. This results in a broad rigidity distribution—from very stiff cells to cells softer than those found in healthy tissue—that is shifted towards a higher fraction of softer cells. Atomic-force-microscopy-based tissue rheology reveals that islands of rigid cells are surrounded by soft cells. The tracking of vital cells confirms the coexistence of jammed and unjammed areas in tumour explants. Despite the absence of a percolated backbone of stiff cells and a large fraction of unjammed, motile cells, cancer cell clusters show a heterogeneous solid behaviour with a finite elastic modulus providing mechanical stability. 

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5. Morphogenesis and cell ordering in confined bacterial biofilms

   https://doi.org/10.1073/pnas.2107107118  

   Zhang, Qiuting ; Li, Jian ; Nijjer, Japinder ; Lu, Haoran ; Kothari, Mrityunjay ; Alert, Ricard ; Cohen, Tal ; Yan, Jing ( July 2021 , Proceedings of the National Academy of Sciences)

   Biofilms are aggregates of bacterial cells surrounded by an extracellular matrix. Much progress has been made in studying biofilm growth on solid substrates; however, little is known about the biophysical mechanisms underlying biofilm development in three-dimensional confined environments in which the biofilm-dwelling cells must push against and even damage the surrounding environment to proliferate. Here, combining single-cell imaging, mutagenesis, and rheological measurement, we reveal the key morphogenesis steps ofVibrio choleraebiofilms embedded in hydrogels as they grow by four orders of magnitude from their initial size. We show that the morphodynamics and cell ordering in embedded biofilms are fundamentally different from those of biofilms on flat surfaces. Treating embedded biofilms as inclusions growing in an elastic medium, we quantitatively show that the stiffness contrast between the biofilm and its environment determines biofilm morphology and internal architecture, selecting between spherical biofilms with no cell ordering and oblate ellipsoidal biofilms with high cell ordering. When embedded in stiff gels, cells self-organize into a bipolar structure that resembles the molecular ordering in nematic liquid crystal droplets. In vitro biomechanical analysis shows that cell ordering arises from stress transmission across the biofilm–environment interface, mediated by specific matrix components. Our imaging technique and theoretical approach are generalizable to other biofilm-forming species and potentially to biofilms embedded in mucus or host tissues as during infection. Our results open an avenue to understand how confined cell communities grow by means of a compromise between their inherent developmental program and the mechanical constraints imposed by the environment.

    

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