From coffee beans flowing in a chute to cells remodelling in a living tissue, a wide variety of close-packed collective systems— both inert and living—have the potential to jam. The collective can sometimes flow like a fluid or jam and rigidify like a solid. The unjammed-to-jammed transition remains poorly understood, however, and structural properties characterizing these phases remain unknown. Using primary human bronchial epithelial cells, we show that the jamming transition in asthma is linked to cell shape, thus establishing in that system a structural criterion for cell jamming. Surprisingly, the collapse of critical scaling predicts a counter-intuitive relationship between jamming, cell shape and cell–cell adhesive stresses that is borne out by direct experimental observations. Cell shape thus provides a rigorous structural signature for classification and investigation of bronchial epithelial layer jamming in asthma, and potentially in any process in disease or development in which epithelial dynamics play a prominent role.
Our traditional physical picture holds with the intuitive notion that each individual cell comprising the cellular collective senses signals or gradients and then mobilizes physical forces in response. Those forces, in turn, drive local cellular motions from which collective cellular migrations emerge. Although it does not account for spontaneous noisy fluctuations that can be quite large, the tacit assumption has been one of linear causality in which systematic local motions, on average, are the shadow of local forces, and these local forces are the shadow of the local signals. New lines of evidence now suggest a rather different physical picture in which dominant mechanical events may not be local, the cascade of mechanical causality may be not so linear, and, surprisingly, the fluctuations may not be noise as much as they are an essential feature of mechanism. Here we argue for a novel synthesis in which fluctuations and non-local cooperative events that typify the cellular collective might be illuminated by the unifying concept of cell jamming. Jamming has the potential to pull together diverse factors that are already known to contribute but previously had been considered for the most part as acting separately and independently. These include cellular crowding, intercellular force transmission, cadherin-dependent cell-cell adhesion, integrin-dependent cell-substrate adhesion, myosin-dependent motile force and contractility, actin-dependent deformability, proliferation, compression and stretch.
Effective bone tissue
engineering can restore bone and skeletal functions that are impaired
by traumas and/or certain medical conditions. Bone is a complex tissue
and functions through orchestrated interactions between cells, biomechanical
forces, and biofactors. To identify ideal scaffold materials for effective
mesenchymal stem cell (MSC)-based bone tissue regeneration, here we
develop and characterize a composite nanoparticle hydrogel by combining
carboxymethyl chitosan (CMCh) and amorphous calcium phosphate (ACP)
(designated as CMCh-ACP hydrogel). We demonstrate that the CMCh-ACP
hydrogel is readily prepared by incorporating glucono δ-lactone
(GDL) into an aqueous dispersion or rehydrating the acidic freeze-dried
nanoparticles in a pH-triggered controlled-assembly fashion. The CMCh-ACP
hydrogel exhibits excellent biocompatibility and effectively supports
MSC proliferation and cell adhesion. Moreover, while augmenting BMP9-induced
osteogenic differentiation, the CMCh-ACP hydrogel itself is osteoinductive
and induces the expression of osteoblastic regulators and bone markers
in MSCs in vitro. The CMCh-ACP scaffold markedly enhances the efficiency
and maturity of BMP9-induced bone formation in vivo, while suppressing
bone resorption occurred in long-term ectopic osteogenesis. Thus,
these results suggest that the pH-responsive self-assembled CMCh-ACP
injectable and bioprintable hydrogel may be further exploited as a
novel scaffold for osteoprogenitor-cell-based bone tissue regeneration.
Gelatin-graphene conductive biopolymer nanocomposites (CPCs) with ultralow percolation threshold are designed by reducing in situ graphene oxide nanosheets with ascorbic acid and suppressing the aggregation of the graphene nanosheets. The resulting conductive nanocomposites show a record-low electrical percolation threshold of 3.3 × 10(-2) vol%, which arises from the homogeneous dispersion of the graphene nanosheets within the gelatin matrix.
In this research, influence of incorporating LiClO 4 salt on the crystallization, conformation, and ionic conductivity of poly(ethylene oxide) (PEO) in its miscible blend with poly(methyl methacrylate) (PMMA) is studied. Differential scanning calorimetry showed that the incorporation of salt ions into the blend suppresses the crystallinity of PEO. The X-ray diffraction revealed that the unit-cell parameters of the crystals are independent of the LiClO 4 concentration despite of the existence of ionic interactions between PEO and Li cations. In addition, the complexation of the Li þ ions by oxygen atoms of PEO is investigated via Fourier transform infrared spectroscopy. The conformational changes of PEO segments in the presence of salt ions are studied via Raman spectroscopy. It is found that PEO chains in the blend possess a crown-ether like conformation because of their particular complexation with the Li þ ions. This coordination of PEO with lithium cations amorphize the PEO and is accounted for suppressed crystallinity of PEO in the presence of salt ions. Finally, electrochemical impedance spectroscopy is used to characterize the ionic conductivity of PEO in the PEO/PMMA/LiClO 4 ternary mixture at various temperatures.
Effective bone tissue engineering is important to overcome the unmet clinical challenges as more than 1.6 million bone grafts are done annually in the United States. Successful bone tissue engineering needs minimally three critical constituents: osteoprogenitor cells, osteogenic factors, and osteoinductive/osteoconductive scaffolds. Osteogenic progenitors are derived from multipotent mesenchymal stem cells (MSCs), which can be prepared from numerous tissue sources, including adipose tissue. We previously showed that BMP9 is the most osteogenic BMP and induces robust bone formation of immortalized mouse adipose-derived MSCs entrapped in a citrate-based thermoresponsive hydrogel referred to as PPCNg. As graphene and its derivatives emerge as promising biomaterials, here we develop a novel thermosensitive and injectable hybrid material by combining graphene oxide (GO) with PPCNg (designated as GO-P) and characterize its ability to promote bone formation. We demonstrate that the thermoresponsive behavior of the hybrid material is maintained while effectively supporting MSC survival and proliferation. Furthermore, GO-P induces early bone-forming marker alkaline phosphatase (ALP) and potentiates BMP9-induced expression of osteogenic regulators and bone markers as well as angiogenic factor VEGF in MSCs. In vivo studies show BMP9-transduced MSCs entrapped in the GO-P scaffold form well-mineralized and highly vascularized trabecular bone. Thus, these results indicate that GO-P hybrid material may function as a new biocompatible, injectable scaffold with osteoinductive and osteoconductive activities for bone regeneration.
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.