Factors Controlling the Enhanced Mechanical and Thermal Properties of Nanodiamond-Reinforced Cross-Linked High Density Polyethylene

A systematic investigation of the factors influencing the notable enhancement of the mechanical and thermal properties of nanodiamonds (NDs)-reinforced cross-linked high density polyethylene (PEX) is presented in this work. The effects of crystal structure and molecular conformation as well as filler dispersion and adhesion with the matrix were found to govern the mechanical properties of the final composites. A considerable increase in the strength, toughness, and elastic modulus of the materials was found for the composites with filler content below 1 wt %. For higher NDs concentrations, the properties degraded. When filler concentration does not exceed 1 wt %, enhanced adhesion with the matrix is achieved, allowing a more successful load transfer between the filler and the matrix, thus enabling an effective reinforcement of the composites. The higher degree of crystallinity along with larger crystal size are also positively influencing the mechanical properties of PEX. Higher filler concentrations, on the other hand, lead to the formation of larger aggregates, which lead to lower adhesion with the matrix, while they also constitute stress concentrators and therefore reduce the positive reinforcement of the matrix. The thermal conductivity of the composites was also found to be significantly increased for low-filler concentrations. This enhancement was less significant for higher NDs concentrations. It is concluded that this reinforcement is due to the heat capacity increase that NDs incorporation causes in PEX. Additionally, a thermal stability enhancement was found for the composite with minimum filler content

Additional file 3: of Estimating the agreement between the metabolic rate calculated from prediction equations and from a portable indirect calorimetry device: an effort to develop a new equation for predicting resting metabolic rate

Table S3 AF. Tabulated statistics between BMI classes and gender, age groups and education level. (DOCX 19 kb

Table_1_Structure Differentiation of Hydrophilic Brass Nanoparticles Using a Polyol Toolbox.DOCX

Nano-brasses are emerging as a new class of composition-dependent applicable materials. It remains a challenge to synthesize hydrophilic brass nanoparticles (NPs) and further exploit them for promising bio-applications. Based on red/ox potential of polyol and nitrate salts precursors, a series of hydrophilic brass formulations of different nanoarchitectures was prepared and characterized. Self-assembly synthesis was performed in the presence of triethylene glycol (TrEG) and nitrate precursors Cu(NO3)2·3H2O and Zn(NO3)2·6H2O in an autoclave system, at different temperatures, conventional or microwave-assisted heating, while a range of precursor ratios was investigated. NPs were thoroughly characterized via X-ray diffraction (XRD), thermogravimetric analysis (TGA), scanning electron microscopy (SEM), transmition electron microscopy (TEM), Fourier-transform infrared (FTIR) spectroscopy, dynamic light scattering (DLS), and ζ-potential to determine the crystal structure, composition, morphology, size, state of polyol coating, and aqueous colloidal stability. Distinct bimetallic α-brasses and γ-brasses, α-Cu40Zn25/γ-Cu11Zn24, α-Cu63Zn37, α-Cu47Zn10/γ-Cu19Zn24, and hierarchical core/shell structures, α-Cu59Zn30@(ZnO)11, Cu35Zn16@(ZnO)49, α-Cu37Zn18@(ZnO)45, Cu@Zinc oxalate, were produced by each synthetic protocol as stoichiometric, copper-rich, and/or zinc-rich nanomaterials. TEM sizes were estimated at 20–40 nm for pure bimetallic particles and at 45–70 nm for hierarchical core/shell structures. Crystallite sizes for the bimetallic nanocrystals were found ca. 30–45 nm, while in the case of the core-shell structures, smaller values around 15–20 nm were calculated for the ZnO shells. Oxidation and/or fragmentation of TrEG was unveiled and attributed to the different fabrication routes and formation mechanisms. All NPs were hydrophilic with 20–30% w/w of polyol coating, non-ionic colloidal stabilization (−5 mV < ζ-potential < −13 mV) and relatively small hydrodynamic sizes (<250 nm). The polyol toolbox proved effective in tailoring the structure and composition of hydrophilic brass NPs while keeping the crystallite and hydrodynamic sizes fixed.</p

Additional file 1: of Estimating the agreement between the metabolic rate calculated from prediction equations and from a portable indirect calorimetry device: an effort to develop a new equation for predicting resting metabolic rate

Table S1 AF. Physical characteristics of the subjects as cross-tabulated by BMI classes, Age group and Gender. (DOCX 16 kb

Additional file 2: of Estimating the agreement between the metabolic rate calculated from prediction equations and from a portable indirect calorimetry device: an effort to develop a new equation for predicting resting metabolic rate

Table S2 AF. Equations for Estimating Energy Expenditure. (DOCX 21 kb

High-Drug-Loading Amorphous Solid Dispersions via <i>In Situ</i> Thermal Cross-Linking: Unraveling the Mechanisms of Stabilization

This article takes a step forward in understanding the mechanisms involved during the preparation and performance of cross-linked high-drug-loading (HDL) amorphous solid dispersions (ASDs). Specifically, ASDs, having 90 wt % poorly water-soluble drug indomethacin (IND), were prepared via in situ thermal cross-linking of poly­(acrylic acid) (PAA) and poly­(vinyl alcohol) (PVA) and thoroughly evaluated in terms of physical stability and in vitro supersaturation. Results showed that HDL ASDs having excellent active pharmaceutical ingredient (API) amorphous stability and prolonged in vitro supersaturation were prepared by fine tuning the cross-linking procedure. Unraveling of the processes involved during ASD’s formation shed light on the significant role of the cross-linking conditions (i.e., temperature and time), the physicochemical properties of the API, and the hydrolysis level of the cross-linker as key factors in modulating ASD’s stability. In-depth analysis of the prepared systems revealed the (1) reduction of API’s molecular motions within the cross-linked polymeric networks (through API’s strong spatial confinement), (2) the structural changes in the prepared cross-linked matrices (induced by the high API drug loading), and (3) the tuning of the cross-linking density via utilization of low-hydrolyzed PVA as the major mechanisms responsible for ASD’s exceptional performance. Complementary analysis by means of molecular dynamics simulations also highlighted the vital role of strong drug–polymer intermolecular interactions evolving among the ASD components. Overall, the impression of the complexity of in situ cross-linked ASDs has been reinforced with the excessive variation of parameters investigated in the current study, offering thus insights up to the submolecular level to lay the groundwork and foundations for the comprehensive assessment of a new emerging class of HDL amorphous API formulations