Osmotic Concentration-Controlled Particle Uptake and Wrapping-Induced Lysis of Cells and Vesicles.

In vivo, high protein and ion concentrations determine the preferred volumes of cells, organelles, and vesicles. Deformations of their lipid-bilayer membranes by nanoparticle wrapping reduce the interior volumes available to solutes and thus induce large osmotic pressure differences. Osmotic concentration can therefore be an important control parameter for wrapping of nanoparticles. We employ a curvature-elasticity model of the membrane and contact interaction with spherical particles to study their wrapping at initially spherical vesicles. Although the continuous particle-binding transition is independent of the presence of solutes, the discontinuous envelopment transition shifts to higher adhesion strengths and the corresponding energy barrier increases with increasing osmotic concentration. High osmotic concentrations stabilize partial-wrapped, membrane-bound states for both, particle attachment to the inside and the outside. In this regime, wrapping of particles controls membrane tension, with power-law dependencies on osmotic concentration and adhesion strength. For high adhesion strengths, particle wrapping can lead to the opening of mechanosensitive channels in cell membranes and to lysis. Membrane tension-induced stabilization of partial-wrapped states as well as wrapping-induced lysis play important roles not only for desired mechano-bacteriocidal effects of engineered nanomaterials but may also determine viral burst sizes of bacteria and control endocytosis for mammalian cells.

Syncytial germline architecture is actively maintained by contraction of an internal actomyosin corset.

Syncytial architecture is an evolutionarily-conserved feature of the germline of many species and plays a crucial role in their fertility. However, the mechanism supporting syncytial organization is largely unknown. Here, we identify a corset-like actomyosin structure within the syncytial germline of Caenorhabditis elegans, surrounding the common rachis. Using laser microsurgery, we demonstrate that actomyosin contractility within this structure generates tension both in the plane of the rachis surface and perpendicular to it, opposing membrane tension. Genetic and pharmacological perturbations, as well as mathematical modeling, reveal a balance of forces within the gonad and show how changing the tension within the actomyosin corset impinges on syncytial germline structure, leading, in extreme cases, to sterility. Thus, our work highlights a unique tissue-level cytoskeletal structure, and explains the critical role of actomyosin contractility in the preservation of a functional germline.

Fluidization of epithelial sheets by active cell rearrangements.

We theoretically explore fluidization of epithelial tissues by active T1 neighbor exchanges. We show that the geometry of cell-cell junctions encodes important information about the local features of the energy landscape, which we support by an elastic theory of T1 transformations. Using a 3D vertex model, we show that the degree of active noise driving forced cell rearrangements governs the stress-relaxation timescale of the tissue. We study tissue response to in-plane shear at different timescales. At short time, the tissue behaves as a solid, whereas its long-time fluid behavior can be associated with an effective viscosity which scales with the rate of active T1 transformations. Furthermore, we develop a coarse-grained theory, where we treat the tissue as an active fluid and confirm the results of the vertex model. The impact of cell rearrangements on tissue shape is illustrated by studying axial compression of an epithelial tube.

Single-Cell RNA Sequencing: A New Window into Cell Scale Dynamics.

Single-cell genomics has recently emerged as a powerful tool for observing multicellular systems at a much higher level of resolution and depth than previously possible. High-throughput single-cell RNA sequencing techniques are able to simultaneously quantify expression levels of several thousands of genes within individual cells for tens of thousands of cells within a complex tissue. This has led to development of novel computational methods to analyze this high-dimensional data, investigating longstanding and fundamental questions regarding the granularity of cell types, the definition of cell states, and transitions from one cell type to another along developmental trajectories. In this perspective, we outline this emerging field starting from the "input data" (e.g., quantifying transcription levels in single cells), which are analyzed to define "identities" (e.g., cell types, states, and key genes) and to build "interactions" using models that can infer relations and transitions between cells.

Physics of lumen growth.

We model the dynamics of formation of intercellular secretory lumens. Using conservation laws, we quantitatively study the balance between paracellular leaks and the build-up of osmotic pressure in the lumen. Our model predicts a critical pumping threshold to expand stable lumens. Consistently with experimental observations in bile canaliculi, the model also describes a transition between a monotonous and oscillatory regime during luminogenesis as a function of ion and water transport parameters. We finally discuss the possible importance of regulation of paracellular leaks in intercellular tubulogenesis.

Nanoparticle wrapping at small non-spherical vesicles: curvatures at play.

Nanoparticles in biological systems encounter lipid-bilayer membranes as barriers. They interact with plasma membranes, membranous organelles, such as the endoplasmic reticulum and the Golgi apparatus, the nucleus, and intracellular and extracellular vesicles, such as autophagosomes, lysosomes, and exosomes. Extracellular vesicles have recently attracted particular attention, as they are involved in the transmission of biological signals and as regulators for biological processes. For example, exosomes, small vesicles containing proteins, mRNA, and miRNA, that are released by cells into the extracellular environment, have been suggested to participate in tumor metastasis. Furthermore, vesicles can be applied as targeted-drug-delivery systems. We systematically characterize wrapping of spherical nanoparticles that enter and exit vesicles, depending on particle size, vesicle size, vesicle reduced volume, and membrane spontaneous curvature. We predict the complex wrapping behavior, in particular for large particle-to-vesicle size ratios, where the shape changes of the free membrane contribute significantly to the deformation energy and where nanoparticle wrapping transitions and vesicle shape transitions are coupled. Partial-wrapped membrane-bound particles impose boundary conditions on the membrane that stabilise oblates and stomatocytes for particle entry, and prolates and stomatocytes for particle exit. Our results suggest that nanoparticles may stimulate autophagocytic engulfment, which would facilitate transport of the nanoparticles into lysosomes and would lead to subsequent degradation of nanoparticle-attached proteins.

Impact and ecosystem service of forest and sacred grove as saviour of water quantity and quality in Garhwal Himalaya, India.

The present study was conducted in environs of the sacred grove of Garhwal Himalaya, India, with a view to assess the impacts of sacred groves and forests on the quality and quantity of water and also to assess the effect of seasonality on perennial stream quality. Water samples were collected from three randomly selected stream spots of both the sacred grove dominated by deodar (Cedrus deodara) and the non-sacred patch dominated by oak (Quercus leucotrichophora). Water samples from both patches were within the World Health Organization (WHO) standard limits. Based on an already established water quality index, water quality of both patches was safe for domestic and irrigation purposes but needs treatment for drinking purposes. Results of the present study also showed a very prominent impact of forest type as well as management condition on water quality and quantity. The water discharge from an oak forest shows more consistency than the discharge from a deodar forest. Due to the presence of the sacred grove, the area has become the source of good quality water supply during lean season for the surrounding villages. Water quality and quantity differed along with the change in season. The sacred grove and the existing forest leave a great impression on local dwellers, as due to its presence, local dwellers never run out of water supply during the dry season. As a result, the villagers sincerely want to protect the area for the sake of their own well-being.

Capillary assembly of microscale ellipsoidal, cuboidal, and spherical particles at interfaces.

Micron-sized anisotropic particles with homogeneous surface properties at a fluid interface can deform the interface due to their shape. The particles thereby create excess interfacial area and interact in order to minimize this area, which lowers the total interfacial energy. We present a systematic investigation of the interface deformations around single ellipsoidal particles and cuboidal particles with rounded edges in the near field for various contact angles and particle aspect ratios. The correlation of these deformations with capillary bond energies-the interaction energies of two particles at contact-quantifies the relation between the interactions and the near-field deformations. We characterize the interactions using effective power laws and investigate how anisotropic particles self-assemble by capillary forces. Interface deformations and particle interactions for cuboidal particles are weaker compared with those for ellipsoidal particles with the same aspect ratios. For both particle shapes, the bound state in side-by-side orientation is most stable, while the interaction in tip-to-side orientation is repulsive. Furthermore, we find capillary attraction between spherical and ellipsoidal particles. Our calculations therefore suggest cluster formation of spherical and ellipsoidal particles, which elucidates the role of spherical particles as stoppers for the growth of worm-like chains of ellipsoidal particles. The interaction between spherical and ellipsoidal particles might also explain the suppression of the "coffee-ring effect" that has been observed for evaporating droplets with mixtures of spherical and ellipsoidal particles. In general, our calculations of the near-field interactions complement previous calculations in the far field and help to predict colloidal assembly and rheological properties of particle-laden interfaces.

Membrane-wrapping contributions to malaria parasite invasion of the human erythrocyte.

The blood stage malaria parasite, the merozoite, has a small window of opportunity during which it must successfully target and invade a human erythrocyte. The process of invasion is nonetheless remarkably rapid. To date, mechanistic models of invasion have focused predominantly on the parasite actomyosin motor contribution to the energetics of entry. Here, we have conducted a numerical analysis using dimensions for an archetypal merozoite to predict the respective contributions of the host-parasite interactions to invasion, in particular the role of membrane wrapping. Our theoretical modeling demonstrates that erythrocyte membrane wrapping alone, as a function of merozoite adhesive and shape properties, is sufficient to entirely account for the first key step of the invasion process, that of merozoite reorientation to its apex and tight adhesive linkage between the two cells. Next, parasite-induced reorganization of the erythrocyte cytoskeleton and release of parasite-derived membrane can also account for a considerable energetic portion of actual invasion itself, through membrane wrapping. Thus, contrary to the prevailing dogma, wrapping by the erythrocyte combined with parasite-derived membrane release can markedly reduce the expected contributions of the merozoite actomyosin motor to invasion. We therefore propose that invasion is a balance between parasite and host cell contributions, evolved toward maximal efficient use of biophysical forces between the two cells.

Interfacing electrogenic cells with 3D nanoelectrodes: position, shape, and size matter.

An in-depth understanding of the interface between cells and nanostructures is one of the key challenges for coupling electrically excitable cells and electronic devices. Recently, various 3D nanostructures have been introduced to stimulate and record electrical signals emanating from inside of the cell. Even though such approaches are highly sensitive and scalable, it remains an open question how cells couple to 3D structures, in particular how the engulfment-like processes of nanostructures work. Here, we present a profound study of the cell interface with two widely used nanostructure types, cylindrical pillars with and without a cap. While basic functionality was shown for these approaches before, a systematic investigation linking experimental data with membrane properties was not presented so far. The combination of electron microscopy investigations with a theoretical membrane deformation model allows us to predict the optimal shape and dimensions of 3D nanostructures for cell-chip coupling.

Shape and orientation matter for the cellular uptake of nonspherical particles.

Recent advances in nanotechnology have made a whole zoo of particles of different shapes available for applications, but their interaction with biological cells and their toxicity is often not well understood. Experiments have shown that particle uptake by cells is determined by an intricate interplay between physicochemical particle properties like shape, size, and surface functionalization, but also by membrane properties and particle orientation. Our work provides systematic understanding, based on a mechanical description, for membrane wrapping of nanoparticles, viruses, and bacterial forms. For rod-like particles, we find stable endocytotic states with small and high wrapping fraction; an increased aspect ratio is unfavorable for complete wrapping. For high aspect ratios and round tips, the particles enter via a submarine mode, side-first with their long edge parallel to the membrane. For small aspect ratios and flat tips, the particles enter tip-first via a rocket mode.