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Transient capture of cells or model microspheres from flow over substrates sparsely coated with adhesive ligands has provided significant insight into the unbinding kinetics of leukocyte:endothelium adhesion complexes under external force. Whenever a cell is stopped by a point attachment, the full hydrodynamic load is applied to the adhesion site within an exceptionally short time-less than the reciprocal of the hydrodynamic shear rate (e.g., typically <0.01 s). The decay in numbers of cells or beads that remain attached to a surface has been used as a measure of the kinetics of molecular bond dissociation under constant force, revealing a modest increase in detachment rate at growing applied shear stresses. On the other hand, when detached under steady ramps of force with mechanical probes (e.g., the atomic force microscope and biomembrane force probe), P-selectin:PSGL-1 adhesion bonds break at rates that increase enormously under rising force, yielding 100-fold faster off rates at force levels comparable to high shear. The comparatively weak effect of force on tether survival in flow chamber experiments could be explained by a possible partition of the load amongst several bonds. However, a comprehensive understanding of the difference in kinetic behavior requires us to also inspect other factors affecting the dynamics of attachment-force buildup, such as the interfacial compliance of all linkages supporting the adhesion complex. Here, combining the mechanical properties of the leukocyte interface measured in probe tests with single-bond kinetics and the kinetics of cytoskeletal dissociation, we show that for the leukocyte adhesion complex P-selectin:PSGL-1, a detailed adhesive dynamics simulation accurately reproduces the tethering behavior of cells observed in flow chambers. Surprisingly, a mixture of 10% single bonds and 90% dimeric bonds is sufficient to fully match the data of the P-selectin:PSGL-1 experiments, with the calculated decay in fraction of attached cells still appearing exponential.
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http://dx.doi.org/10.1529/biophysj.104.051805 | DOI Listing |
Angew Chem Int Ed Engl
August 2025
State Key Laboratory of Natural Medicines, Jiangsu Key Laboratory of Drug Discovery for Metabolic Diseases and Jiangsu Key Laboratory of Drug Design and Optimization, Center of Advanced Pharmaceuticals and Biomaterials, School of Life Science and Technology, China Pharmaceutical University, Nanjing,
Controlled self-organization of amphiphilic phospholipid camptothecin (CPT) conjugates (named PCCs) selectively forms supramolecular nanotubes with varying lengths and polydispersity. Our study elucidates the underlying mechanisms governing PCC assembly, demonstrating that π-π stacking interactions derived from the planar, conjugated structure of CPT play a pivotal role in nanotube formation. Precise modulation of the hydrophobic characteristics of PCC linkers enables fine-tuning of π-stacking strength, thereby controlling the length of the nanotubes, ranging from the nano- to micro-scale.
View Article and Find Full Text PDFSci Rep
August 2025
Department of Pathological Analyzes, Al Manara College for Medical Sciences, Maysan, Iraq.
In this paper, the influence of surface energy (SE) on the linear and nonlinear frequencies of anodic aluminum micro beams with [100] and [111] crystalline orientations resting on an elastic substrate are analyzed based on the Timoshenko beam (TB) and Euler-Bernoulli (EB) models, spanning Nano- to micro-scale dimensions. Given the high ratio of surface-to-volume the studied micro beams, the proposed model incorporates SE effects. To extract the micro beam frequencies, the governing the Galerkin method with trigonometric and polynomial shape functions corresponding to clamped-clamped, clamped-simply supported, and simply supported boundary conditions are used.
View Article and Find Full Text PDFObes Rev
August 2025
Department of Inflammation and Ageing, MRC-Versus Arthritis Centre for Musculoskeletal Ageing Research, College of Medicine and Health, University of Birmingham, Birmingham, UK.
Sarcopenic obesity, characterized by the concurrent presence of excess adiposity and diminished skeletal muscle mass and function, is closely linked to frailty, chronic inflammation, and insulin resistance. The increasing prevalence of sarcopenic obesity is driven by the global aging population, widespread adoption of sedentary lifestyles, and the ongoing obesity epidemic. Existing research describes a role for dysregulated crosstalk between adipose tissue and skeletal muscle tissue in driving sarcopenic obesity pathology, with recent evidence implying that extracellular vesicles (EVs, nano- to micro-scale, lipid bilayer membrane-delimited particles) have a significant role in facilitating intercellular communication to mediate critical tissue crosstalk.
View Article and Find Full Text PDFRSC Adv
June 2025
Linnaeus University Centre for Biomaterials Chemistry, Linnaeus University SE-391 82 Kalmar Sweden
A series of nanostructured polysulfobetaine (PSB) hydrogel-coated surfaces were fabricated and tested for hemocompatibility in contact with human blood. PSB films were grafted onto SiO-coated silicon wafers or Au/quartz photochemically induced polymerization of a sulfobetaine-based monomer (SBMA, [2-(methacryloylamino)propyl]dimethyl(3-sulfopropyl)ammonium hydroxide). An anodized aluminum oxide (AAO) membrane and latex beads (LB) were used as sacrificial template structures to synthesize polysulfobetaine nanowires (PSB) and hyperporous (PSB) networks, respectively.
View Article and Find Full Text PDFNanotechnology
February 2025
Energy and Environment Unit, Institute of Nano Science and Technology, Knowledge City, Sector 81, Mohali, Punjab 140306, India.
This study investigates simple acetylenes substituted with phenylurea as a constant H-bonding unit () and varied hydrophobic units (R = H, Phenyl (Ph), phenylacetylene (PA), Ph-NMe) to understand self-assembly properties driven by synergistic non-covalent interactions. Our observations reveal hierarchical self-assembled fibrillar networks with luminescent needles, fibers, and flowers on nano- to micro-meter scales. Subtle changes in substituents led to significant differences: H, Ph, PA, and Ph-NMeproduced needle-like crystals, dendritic nanofibers, microflakes, and no self-assembly, respectively.
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