Nanocavity electrode array for recording from electrogenic cells

We present a new nanocavity device for highly localized on-chip recordings of action potentials from individual cells in a network. Microelectrode recordings have become the method of choice for recording extracellular action potentials from high density cultures or slices. Nevertheless, interfacing individual cells of a network with high resolution still remains challenging due to an insufficient coupling of the signal to small electrodes, exhibiting diameters below 10 μm. We show that this problem can be overcome by a new type of sensor that features an electrode, which is accessed via a small aperture and a nanosized cavity. Thus, the properties of large electrodes are combined with a high local resolution and a good seal resistance at the interface. Fabrication of the device can be performed with state-of-the-art clean room technology and sacrificial layer etching allowing integration of the devices into sensor arrays. We demonstrate the capability of such an array by recording the propagation of action potentials in a network of cardiomyocyte-like cells.     

Evaluating alternative electrostatic potential models for polyacrylamide-co-acrylate in aqueous solution

The capabilities of three simplified analytical equations to accurately model electrostatic interactions during proton binding and release by linear anionic polyelectrolytes in aqueous solution were evaluated. The impermeable sphere (IS), Donnan (DN), and cylindrical (CY) electrostatic models were fit to experimental acid-base titration curves of linear polyacrylamide-co-acrylate having ionizable site densities ranging from ca. 10-35%. The titrations were conducted in 0.003-0.12M NaCl solutions and the sum of squared errors from modeled and experimental data was used as a comparative index of each model's capability. In addition, the relative size of each polyelectrolyte was estimated from its measured specific viscosity and then compared against the values obtained from the fitting procedure for the size parameter that each model contained. Although the IS and DN electrostatic models could be used to obtain reasonably good fits to each titration curve, the size parameter values obtained by each model were not reflective of the actual polyelectrolyte sizes, indicating that the models had limited physical meaning and that the size parameter was essentially just an additional fitting parameter in each model. In contrast, the CY model was not only more effective in its ability to fit the titration data but also provided a better physical representation of the polyelectrolyte size. Therefore, for polyelectrolytes that remain essentially linear or are only loosely coiled such that counter ions are free to travel throughout the polymer structure, we conclude that the CY model and its morphological representation of a cylindrical polyelectrolyte are more valid and realistic than the IS and DN models and their representation of polyelectrolytes as spheres.     

Effect of Holoptelea integrifolia (Roxb.) Planch. n-Hexane Extract and Its Bioactive Compounds on Wound Healing and Anti-Inflammatory Activity

The stem bark of Holoptelea integrifolia (Roxb.) Planch. has been applied for the treatment of human cutaneous diseases as well as canine demodicosis in several countries. However, no detailed mechanistic studies have been reported to support their use. In this study, thin-layer chromatography and gas chromatography were used to screen phytochemicals from the fresh stem bark extract of H. integrifolia. We found the two major bioactive compounds, friedelin and lupeol, and their activity on wound healing was further investigated in keratinocytes. Both bioactive compounds significantly reduced wound area and increased keratinocyte migration by increasing matrix metalloproteinases-9 production. Subsequently, we found that the mRNA gene expressions of cadherin 1 and desmoglobin 1 significantly decreased, whereas the gene expression involved in keratinocyte proliferation and homeostasis (keratin-17) increased in compound-treated human immortalized keratinocytes cells. The expression of inflammatory genes (cyclooxygenase-2 and inducible nitric oxide synthase) and pro-inflammatory cytokine genes (tumor necrosis factor-alpha and interleukin-6) was reduced by treatment with n-hexane extract of H. integrifolia and its bioactive compounds. Our results revealed that H. integrifolia extract and its bioactive compounds, friedelin and lupeol, exhibit wound-healing activity with anti-inflammatory properties, mediated by regulating the gene expression involved in skin re-epithelialization.     

An Fc variant with two mutations confers prolonged serum half-life and enhanced effector functions on IgG antibodies

The pH-selective interaction between the immunoglobulin G (IgG) fragment crystallizable region (Fc region) and the neonatal Fc receptor (FcRn) is critical for prolonging the circulating half-lives of IgG molecules through intracellular trafficking and recycling. By using directed evolution, we successfully identified Fc mutations that improve the pH-dependent binding of human FcRn and prolong the serum persistence of a model IgG antibody and an Fc-fusion protein. Strikingly, trastuzumab-PFc29 and aflibercept-PFc29, a model therapeutic IgG antibody and an Fc-fusion protein, respectively, when combined with our engineered Fc (Q311R/M428L), both exhibited significantly higher serum half-lives in human FcRn transgenic mice than their counterparts with wild-type Fc. Moreover, in a cynomolgus monkey model, trastuzumab-PFc29 displayed a superior pharmacokinetic profile to that of both trastuzumab-YTE and trastuzumab-LS, which contain the well-validated serum half-life extension Fcs YTE (M252Y/S254T/T256E) and LS (M428L/N434S), respectively. Furthermore, the introduction of two identified mutations of PFc29 (Q311R/M428L) into the model antibodies enhanced both complement-dependent cytotoxicity and antibody-dependent cell-mediated cytotoxicity activity, which are triggered by the association between IgG Fc and Fc binding ligands and are critical for clearing cancer cells. In addition, the effector functions could be turned off by combining the two mutations of PFc29 with effector function-silencing mutations, but the antibodies maintained their excellent pH-dependent human FcRn binding profile. We expect our Fc variants to be an excellent tool for enhancing the pharmacokinetic profiles and potencies of various therapeutic antibodies and Fc-fusion proteins.Subject terms: Antibody therapy, Molecularly targeted therapy, Drug development     

Novel crystalline supramolecular assemblies of amorphous polypyrrole nanoparticles through surfactant templating

A lamellar-structured crystalline polypyrrole (PPy) supramolecular assembly was prepared by surfactant templating, and the regularly linked amorphous PPy nanoparticles with tunable window sizes could play the role of crystalline lattices in the supramolecular assembly.     

Hydroxoundecahydro-closo-dodecaborate(2-) as a Nucleophile. Preparation and Structural Characterization of O-Alkyl and O-Acyl Derivatives of Hydroxoundecahydro-closo-dodecaborate(2-)

The syntheses, solid state structures, and spectral properties of O-alkyl and O-acyl derivatives of hydroxoundecahydro-closo-dodecaborate(2-), 1, are described. Alkylation of 1 with ethyl iodide was achieved in dimethyl sulfoxide using potassium hydroxide as a base, leading to [N(n-C(4)H(9))(4)](2)[CH(3)CH(2)O-B(12)H(11)(2-)], 2, bis(tetrabutylammonium) ethoxyundecahydro-closo-dodecaborate(2-) [monoclinic P2(1)/n, a = 1192.4(9) pm, b = 1253.9(4) pm, c = 3049.1(10) pm, beta = 92.69(4) degrees, Z = 4, R1 = 0.0693, wR(2) = 0.1517]. Alkylation with 1,5-dibromopentane afforded the cyclic oxonium salt [PPN][C(5)H(10)O-B(12)H(11)(1-)], 3, (&mgr;-nitrido)bis(triphenylphosphorus)(1+) tetrahydropyrane-undecahydro-closo-dodecaborate(1-) [monoclinic P2(1)/c, a = 1938.1(2) pm, b = 1329.7(10) pm, c = 1944.0(2) pm, beta = 108.82(10) degrees, Z = 4, R1 = 0.0484, wR(2) = 0.0833]. Acylation of 1 in acetonitrile with acyl chlorides in the presence of pyridine yielded [N(n-C(4)H(9))(4)](2)[C(6)H(5)CO(2)-B(12)H(11)(2-)], 4, bis(tetrabutylammonium) undecahydrobenzoyl-closo-dodecaborate(2-) [monoclinic P2(1)/c, a = 1812.0(4) pm, b = 1711.9(3) pm, c = 1685.0(3) pm, beta = 114.03(3) degrees, Z = 4, R1 = 0.0915, wR(2) = 0.2093], and [N(n-C(4)H(9))(4)](2)[CH(3)CO(2)-B(12)H(11)(2-)], 5, bis(tetrabutylammonium) acetoxyundecahydro-closo-dodecaborate(2-) [monoclinic P2(1)/n, a = 1190.5(2) pm, b = 1243.0(10) pm, c = 3078.4(4) pm, beta = 92.76(10) degrees, Z = 4, R1 = 0.0642, wR(2) = 0.1462]. All crystal structures showed distortion of the pseudoicosahedral geometry of the boron cluster. The boron-oxygen distances varied from 144.2(5) pm for 2, 148.5(3) pm for 5, 149.4(12) pm for 4, to 152.8(4) pm for 3. The 3-fold coordinated oxygen of oxonium salt 3 is nearly planar.     

Fixed charge and interface traps at heterovalent interfaces between Si(1 0 0) and non-crystalline Al2O3–Ta2O5 alloys

Characterization by Auger electron spectroscopy (AES) and Fourier transformation infrared spectroscopy (FTIR) confirms (Ta₂O₅)_x(Al₂O₃)_1−x alloys are homogeneous pseudo-binary alloys with increased thermal stability with respect to end member oxides, Ta₂O₅ and Al₂O₃. Capacitance–voltage (C–V) and current density–voltage (J–V) data as a function of temperate show that the Ta d-states of the alloys act as localized electron traps, and are at an energy approximately equal to the conduction band offset of Ta₂O₅ with respect to Si.