Lapuhs, Philipp | Heinrich, Eilien | Garcia, Ronald | Goes, Adriely | Frank, Nicolas | Bollenbach, Lukas | Stibane, Veronika | Kuhn, Thomas | Koch, Marcus | Kiemer, Alexandra K. | Müller, Rolf | Fuhrmann, Kathrin | Fuhrmann, Gregor
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Outer membrane vesicles are small, lipid-based vesicles shed from the outer membrane of Gram-negative bacteria. They are becoming increasingly recognised as important factors for resistance gene transfer, bacterial virulence factors and host cell modulation. The presence of pathogenic factors and antimicrobial compounds in bacterial vesicles has been proven in recent years, but it remains unclear, if and how environmental factors, such as light specifically regulate the vesicle composition. We report the first example of autofluorescent vesicles derived from non-pathogenic soil-living myxobacteria. These vesicles additionally showed inherent antibiotic activity, a property that is specifically regulated by light stimulation of the producing bacteria. Our data provide a central basis for better understanding the environmental impact on bacteria-derived vesicles, and design of future therapeutic options.
Metelkina, Olga | Huck, Benedikt | O’Connor, Jonathan S. | Koch, Marcus | Manz, Andreas | Lehr, Claus-Michael | Titz, Alexander
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The antimicrobial resistance crisis requires novel approaches for the therapy of infections especially with Gram-negative pathogens. Pseudomonas aeruginosa is defined as priority 1 pathogen by the WHO and thus of particular interest. Its drug resistance is primarily associated with biofilm formation and essential constituents of its extracellular biofilm matrix are the two lectins, LecA and LecB. Here, we report microbial lectin-specific targeted nanovehicles based on liposomes. LecA- and LecB-targeted phospholipids were synthesized and used for the preparation of liposomes. These liposomes with varying surface ligand density were then analyzed for their competitive and direct lectin binding activity. We have further developed a microfluidic device that allowed the optical detection of the targeting process to the bacterial lectins. Our data showed that the targeted liposomes are specifically binding to their respective lectin and remain firmly attached to surfaces containing these lectins. This synthetic and biophysical study provides the basis for future application in targeted antibiotic delivery to overcome antimicrobial resistance.
Pickering, Edmund | Paxton, Naomi C. | Bo, Arixin | O’Connell, Bridget | King, Mitchell | Woodruff, Maria A
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Melt electrowriting (MEW) is a promising additive manufacturing technique for tissue scaffold biofabrication. Successful application of MEW scaffolds requires strictly controlled mechanical behavior. This requires scaffold geometry be optimized to match native tissue properties while simultaneously supporting cell attachment and proliferation. The objective of this work is to investigate how geometric properties can be exploited to massively tailor the mechanical behavior of tubular crosshatch scaffolds. An experimentally validated finite element (FE) model is developed and 441 scaffold geometries are investigated under tension, compression, bending, and radial loading. A range of pore areas (4–150 mm2) and pore angles (11°–134°) are investigated. It is found that scaffold mechanical behavior is massively tunable through the control of these simple geometric parameters. Across the ranges investigated, scaffold stiffness varies by a factor of 294× for tension, 204× for compression, 231× for bending, and 124× for radial loading. Further, it is discussed how these geometric parameters can be simultaneously tuned for different biomimetic material applications. This work provides critical insights into scaffold design to achieve biomimetic mechanical behavior and provides an important tool in the development of biomimetic tissue engineered constructs.
Wang, Yujia | Zhang, Xuan | Li, Zihe | Gao, Huajian | Li, Xiaoyan
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Recent developments in mechanical metamaterials exemplify a new paradigm shift called mechanomaterials, in which mechanical forces and designed geometries are proactively deployed to program material properties at multiple scales. Here, we designed shell-based micro-/nanolattices with I-WP (Schoen’s I-graph–wrapped package) and Neovius minimal surface topologies. Following the designed topologies, polymeric microlattices were fabricated via projection microstereolithography or two-photon lithography, and pyrolytic carbon nanolattices were created through two-photon lithography and subsequent pyrolysis. The shell thickness of created lattice metamaterials varies over three orders of magnitude from a few hundred nanometers to a few hundred micrometers, covering a wider range of relative densities than most plate-based micro-/nanolattices. In situ compression tests showed that the measured modulus and strength of our shell-based micro-/nanolattices with I-WP topology are superior to those of the optimized plate-based lattices with cubic and octet plate unit cells and truss-based lattices. More strikingly, when the density is larger than 0.53 g cm−3, the strength of shell-based pyrolytic carbon nanolattices with I-WP topology was found to achieve its theoretical limit. In addition, our shell-based carbon nanolattices exhibited an ultrahigh strength of 3.52 GPa, an ultralarge fracture strain of 23%, and an ultrahigh specific strength of 4.42 GPa g−1 cm3, surpassing all previous micro-/nanolattices at comparable densities. These unprecedented properties can be attributed to the designed topologies inducing relatively uniform strain energy distributions and avoiding stress concentrations as well as the nanoscale feature size. Our study demonstrates a mechanomaterial route to design and synthesize micro-/nanoarchitected materials.
Zhang, Jingnan | Zhao, Renping | Li, Bin | Farrukh, Aleeza | Hoth, Markus | Qu, Bin | del Campo, Aránzazu
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The analysis of T cell responses to mechanical properties of antigen presenting cells (APC) is experimentally challenging at T cell-APC interfaces. Soft hydrogels with adjustable mechanical properties and biofunctionalization are useful reductionist models to address this problem. Here, we report a methodology to fabricate micropatterned soft hydrogels with defined stiffness to form spatially confined T cell/hydrogel contact interfaces at micrometer scale. Using automatized microcontact printing we prepared arrays of anti-CD3 microdots on poly(acrylamide) hydrogels with Young's Modulus in the range of 2 to 50 kPa. We optimized the printing process to obtain anti-CD3 microdots with constant area (50 µm2, corresponding to 8 µm diameter) and comparable anti-CD3 density on hydrogels of different stiffness. The anti-CD3 arrays were recognized by T cells and restricted cell attachment to the printed areas. To test functionality of the hydrogel-T cell contact, we analyzed several key events downstream of T cell receptor (TCR) activation. Anti-CD3 arrays on hydrogels activated calcium influx, induced rearrangement of the actin cytoskeleton, and led to Zeta-chain-associated protein kinase 70 (ZAP70) phosphorylation. Interestingly, upon increase in the stiffness, ZAP70 phosphorylation was enhanced, whereas the rearrangements of F-actin (F-actin clearance) and phosphorylated ZAP70 (ZAP70/pY centralization) were unaffected. Our results show that micropatterned hydrogels allow tuning of stiffness and receptor presentation to analyze TCR mediated T cell activation as function of mechanical, biochemical, and geometrical parameters.

Rodrigo-Navarro, Aleixandre | Sankaran, Shrikrishnan | Dalby, Matthew J. | del Campo, Aránzazu | Salmeron-Sanchez, Manuel
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Biomaterials have evolved from inert materials that lack interaction with the body to biologically active, instructive materials that host and provide signals to surrounding cells and tissues. Engineered living materials contain living cells (responsive function) and polymeric matrices (scaffolding function) and, thus, can be designed as active and response biomaterials. In this Review, we discuss engineered living materials that incorporate microorganisms as the living, bioactive component. Microorganisms can provide complex responses to environmental stimuli, and they can be genetically engineered to allow user control over responses and integration of numerous inputs. The engineered microorganisms can either generate their own matrix, such as in biofilms, or they can be incorporated in matrices using various technologies, such as coating, 3D printing, spinning and microencapsulation. We highlight biomedical applications of such engineered living materials, including biosensing, wound healing, stem-cell-based tissue engineering and drug delivery, and provide an outlook to the challenges and future applications of engineered living materials.
Zheng, Yijun | Han, Mitchell K. L. | Zhao, Renping | Blass, Johanna | Zhang, Jingnan | Zhou, Dennis W. | Colard-Itté, Jean-Rémy | Dattler, Damien | Çolak, Arzu | Hoth, Markus | García, Andrés J. | Qu, Bin | Bennewitz, Roland | Giuseppone, Nicolas | del Campo, Aránzazu
DOI:
Progress in our understanding of mechanotransduction events requires noninvasive methods for the manipulation of forces at molecular scale in physiological environments. Inspired by cellular mechanisms for force application (i.e. motor proteins pulling on cytoskeletal fibers), we present a unique molecular machine that can apply forces at cell-matrix and cell-cell junctions using light as an energy source. The key actuator is a light-driven rotatory molecular motor linked to polymer chains, which is intercalated between a membrane receptor and an engineered biointerface. The light-driven actuation of the molecular motor is converted in mechanical twisting of the entangled polymer chains, which will in turn effectively “pull” on engaged cell membrane receptors (e.g., integrins, T cell receptors) within the illuminated area. Applied forces have physiologically-relevant magnitude and occur at time scales within the relevant ranges for mechanotransduction at cell-friendly exposure conditions, as demonstrated in force-dependent focal adhesion maturation and T cell activation experiments. Our results reveal the potential of nanomotors for the manipulation of living cells at the molecular scale and demonstrate a functionality which at the moment cannot be achieved by other technologies for force application.
Wang, Lei | Zhang, Yuan | Moh, Karsten | Presser, Volker
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The considerable growth of the world population, concomitant with an increase in environmental pollution, aggravates the antinomy between supply and demand for drinking water. Various desalination technologies have been developed to address this issue, allowing for abundant saltwater as a source for drinking water. Electrochemical desalination attracts more and more attention due to its high energy efficiency, facile operation, and low cost. Especially within the last decade, tremendous scientific progress on electrochemical desalination technologies has been made. This paper reviews the development of electrochemical desalination technologies and introduces a facile classification into three generations according to the different working principles. The cell architecture, metrics, advantages, and disadvantages of other electrochemical desalination technologies are introduced and compared.
Sukhomlinov, Sergey | Müser, Martin H.
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The viscous dissipation between rigid, randomly rough indenters and linearly elastic counter bodies sliding past them is investigated using Green’s function molecular dynamics. The study encompasses a variety of models differing in the height spectra properties of the rigid indenter, in the viscoelasticity of the elastomer, and in their interaction. All systems reveal the expected damping linear in sliding velocity v at small v and a pronounced maximum at intermediate v. Persson’s theory of rubber friction, which is adopted to the studied model systems, reflects all observed trends. However, close quantitative agreement is only found up to intermediate sliding velocities. Relative errors in the friction force become significant once the contact area is substantially reduced by sliding.
Tavernaro, Isabella | Dekkers, Susan | Soeteman-Hernandez, Lya G. | Herbeck-Engel, Petra | Noorlander, Cornelle W. | Kraegeloh, Annette
DOI:
Manufactured nanomaterials have the potential to impact an exceedingly wide number of industries and markets ranging from energy storage, electronic and optical devices, light-weight construction to innovative medical approaches for diagnostics and therapy. In order to foster the development of safer nanomaterial-containing products, two main aspects are of major interest: their functional performance as well as their safety towards human health and the environment. In this paper a first proposal for a strategy is presented to link the functionality of nanomaterials with safety aspects. This strategy first combines information on the functionality and safety early during the innovation process and onwards, and then identifies Safe-by-Design (SbD) actions that allow for optimisation of both aspects throughout the innovation process. The strategy encompasses suggestions for the type of information needed to balance functionality and safety to support decision making in the innovation process. The applicability of the strategy is illustrated using a literature-based case study on carbon nanotube-based transparent conductive films. This is a first attempt to identify information that can be used for balancing functionality and safety in a structured way during innovation processes.
