714 research outputs found
Optimization of the processing of bio based polymer sustainable products
Polylactic Acid (PLA) is processed by injection moulding technology. The main aim of this study is to provide guidelines for mould and part design, namely to cope with the shrinkage effect and the ejection forces related to the use of bio based polymers. Furthermore optimization of the overall process will be investigated as well as the influence of different parameters to the process and product properties. Draft angle, mould temperature and holding pressure will be related to the ejection forces and the level of shrinkage that occurs
An accurate description of quantum size effects in InP nanocrystallites over a wide range of sizes
We obtain an effective parametrization of the bulk electronic structure of
InP within the Tight Binding scheme. Using these parameters, we calculate the
electronic structure of InP clusters with the size ranging upto 7.5 nm. The
calculated variations in the electronic structure as a function of the cluster
size is found to be in excellent agreement with experimental results over the
entire range of sizes, establishing the effectiveness and transferability of
the obtained parameter strengths.Comment: 9 pages, 3 figures, pdf file available at
http://sscu.iisc.ernet.in/~sampan/publications.htm
Photonic crystal carpet: Manipulating wave fronts in the near field at 1550 nm
Ground-plane cloaks, which transform a curved mirror into a flat one, and
recently reported at wavelengths ranging from the optical to the visible
spectrum, bring the realm of optical illusion a step closer to reality.
However, all carpet-cloaking experiments have thus far been carried out in the
far-field. Here, we demonstrate numerically and experimentally that a
dielectric photonic crystal (PC) of a complex shape made of a honeycomb array
of air holes can scatter waves in the near field like a PC with a at boundary
at stop band frequencies. This mirage effect relies upon a specific arrangement
of dielectric pillars placed at the nodes of a quasi-conformal grid dressing
the PC. Our carpet is shown to work throughout the range of wavelengths 1500nm
to 1650nm within the stop band extending from 1280 to 1940 nm. The device has
been fabricated using a single- mask advanced nanoelectronics technique on
III-V semiconductors and the near field measurements have been carried out in
order to image the wave fronts's curvatures around the telecommunication
wavelength 1550 nm.Comment: 6 page
Tight-binding g-Factor Calculations of CdSe Nanostructures
The Lande g-factors for CdSe quantum dots and rods are investigated within
the framework of the semiempirical tight-binding method. We describe methods
for treating both the n-doped and neutral nanostructures, and then apply these
to a selection of nanocrystals of variable size and shape, focusing on
approximately spherical dots and rods of differing aspect ratio. For the
negatively charged n-doped systems, we observe that the g-factors for
near-spherical CdSe dots are approximately independent of size, but show strong
shape dependence as one axis of the quantum dot is extended to form rod-like
structures. In particular, there is a discontinuity in the magnitude of
g-factor and a transition from anisotropic to isotropic g-factor tensor at
aspect ratio ~1.3. For the neutral systems, we analyze the electron g-factor of
both the conduction and valence band electrons. We find that the behavior of
the electron g-factor in the neutral nanocrystals is generally similar to that
in the n-doped case, showing the same strong shape dependence and discontinuity
in magnitude and anisotropy. In smaller systems the g-factor value is dependent
on the details of the surface model. Comparison with recent measurements of
g-factors for CdSe nanocrystals suggests that the shape dependent transition
may be responsible for the observations of anomalous numbers of g-factors at
certain nanocrystal sizes.Comment: 15 pages, 6 figures. Fixed typos to match published versio
Does Pelletizing Catalysts Influence the Efficiency Number of Activity Measurements? Spectrochemical Engineering Considerations for an Accurate Operando Study
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Native-MS analysis of monoclonal antibody conjugates by Fourier transform ion cyclotron resonance mass spectrometry
Antibody drug conjugates (ADCs) are an important class of therapeutic molecule currently being used to treat HER2-positive metastatic breast cancer, relapsed or refractory Hodgkin lymphoma, systemic anaplastic large cell lymphoma, relapsed or refractory B-cell precursor acute lymphoblastic leukemia and acute myeloid leukemia. An ADC typically consists of a small molecule or peptide-based cytotoxic moiety covalently linked, via lysine or cysteine residues, to amonoclonal antibody (mAb) scaffold. Mass spectrometric (MS) characterization of these molecules afford highly accurate molecular weight (MW) and drug-to-antibody ratio (DAR) determination, and is typically performed using orthogonal acceleration time-of-flight (oa-ToF) analysers and more recently Orbitrap instruments. Herein we describe for the first time the use of a 15 Tesla solariX Fourier transform ion cyclotron mass spectrometer to characterize an IgG1 mAb molecule conjugated with biotin via native lysine and cysteine residues, under native-MS and solution conditions. The cysteine biotin conjugates remained fully intact, demonstrating the ability of the FT-ICR to maintain the noncovalent interactions and efficiently transmit labile protein complexes. Native-MS was acquired and is displayed in magnitude mode using a symmetric Hann apodisation function. Baseline separation is achieved on all covalent biotin additions, for each charge state, for both the lysine and cysteine biotin-conjugates. Average DAR values obtained by native-MS for the lysine conjugate are compared to those derived by denaturing reversed phase liquid chromatography using an oa-ToF MS system (1.56 ±0.02 versus 2.24 ±0.02 for a 5-molar equivalent and 3.99 ±0.09 versus 4.43 ±0.01 for a 10-molar equivalent, respectively). Increased DAR value accuracy can be obtained for the higher biotin load, when using standard ESI conditions as opposed to nanoESI native-MS conditions. Both denatured LC-MS and native-MS spectral data were deconvoluted using a parsimonious based algorithm, without the need for parameter adjustment
Matrix elasticity of void-forming hydrogels controls transplanted-stem-cell-mediated bone formation
The effectiveness of stem cell therapies has been hampered by cell death and limited control over fate. These problems can be partially circumvented by using macroporous biomaterials that improve the survival of transplanted stem cells and provide molecular cues to direct cell phenotype. Stem cell behaviour can also be controlled in vitro by manipulating the elasticity of both porous and non-porous materials, yet translation to therapeutic processes in vivo remains elusive. Here, by developing injectable, void-forming hydrogels that decouple pore formation from elasticity, we show that mesenchymal stem cell (MSC) osteogenesis in vitro, and cell deployment in vitro and in vivo, can be controlled by modifying, respectively, the hydrogel’s elastic modulus or its chemistry. When the hydrogels were used to transplant MSCs, the hydrogel’s elasticity regulated bone regeneration, with optimal bone formation at 60 kPa. Our findings show that biophysical cues can be harnessed to direct therapeutic stem cell behaviours in situ
Matrix elasticity of void-forming hydrogels controls transplanted-stem-cell-mediated bone formation
The effectiveness of stem cell therapies has been hampered by cell death and limited control over fate. These problems can be partially circumvented by using macroporous biomaterials that improve the survival of transplanted stem cells and provide molecular cues to direct cell phenotype. Stem cell behaviour can also be controlled in vitro by manipulating the elasticity of both porous and non-porous materials, yet translation to therapeutic processes in vivo remains elusive. Here, by developing injectable, void-forming hydrogels that decouple pore formation from elasticity, we show that mesenchymal stem cell (MSC) osteogenesis in vitro, and cell deployment in vitro and in vivo, can be controlled by modifying, respectively, the hydrogel's elastic modulus or its chemistry. When the hydrogels were used to transplant MSCs, the hydrogel's elasticity regulated bone regeneration, with optimal bone formation at 60 kPa. Our findings show that biophysical cues can be harnessed to direct therapeutic stem cell behaviours in situ
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