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  • Vilstrup Johnsen posted an update 15 hours, 22 minutes ago

    The aim of this work was to show the evolution over time of the dynamic moduli in components made of Polybutylene Terephthalate reinforced with glass fiber when they are held to temperatures close to the glass transition temperature over time. For this purpose, PBT samples reinforced with short, glass fibers of Ultradur® material with 0%, 20%, and 50% in weight content were tested. Dynamic moduli showed an increment with glass fiber content showing a nonlinear behavior with the temperature. The evolution of storage modulus was depicted by means of a modified law of mixtures with an effectiveness factor depending on temperature and fiber content, whereas the evolution over time was obtained with a time-temperature transformation generated with the TTS Data Analysis software of TA-instruments for a given temperature. Storage modulus showed a linear relationship with glass fiber content when components were held to temperatures near to their respective glass transition temperature, obtained from the maximum of loss modulus curve with temperature. In summary, the value and evolution of dynamic moduli of PBT samples improved with glass fiber content, allowing us to increase the durability of components when they are submitted to high-temperature environments.In this study, we analyzed microbial community composition and the functional capacities of degraded sites and restored/natural sites in two typical wetlands of Northeast China-the Phragmites marsh and the Carex marsh, respectively. The degradation of these wetlands, caused by grazing or land drainage for irrigation, alters microbial community components and functional structures, in addition to changing the aboveground vegetation and soil geochemical properties. Bacterial and fungal diversity at the degraded sites were significantly lower than those at restored/natural sites, indicating that soil microbial groups were sensitive to disturbances in wetland ecosystems. Further, a combined analysis using high-throughput sequencing and GeoChip arrays showed that the abundance of carbon fixation and degradation, and ~95% genes involved in nitrogen cycling were increased in abundance at grazed Phragmites sites, likely due to the stimulating impact of urine and dung deposition. In contrast, the abundance of genes involved in methane cycling was significantly increased in restored wetlands. Particularly, we found that microbial composition and activity gradually shifts according to the hierarchical marsh sites. Altogether, this study demonstrated that microbial communities as a whole could respond to wetland changes and revealed the functional potential of microbes in regulating biogeochemical cycles.Gynaecological cancers are attributed to the second most diagnosed cancers in women after breast cancer. On a global scale, cervical cancer is the fourth most common cancer and the most common cancer in developing countries with rapidly increasing mortality rates. Human papillomavirus (HPV) infection is a major contributor to the disease. HPV infections cause prominent cellular changes including alternative splicing to drive malignant transformation. A fundamental characteristic attributed to cancer is the dysregulation of cellular transcription. Alternative splicing is regulated by several splicing factors and molecular changes in these factors lead to cancer mechanisms such as tumour development and progression and drug resistance. The serine/arginine-rich (SR) proteins and heterogeneous ribonucleoproteins (hnRNPs) have prominent roles in modulating alternative splicing. Evidence shows molecular alteration and expression levels in these splicing factors in cervical cancer. Furthermore, aberrant splicing events in cancer-related genes lead to chemo- and radioresistance. read more Identifying clinically relevant modifications in alternative splicing events and splicing variants, in cervical cancer, as potential biomarkers for their role in cancer progression and therapy resistance is scrutinised. This review will focus on the molecular mechanisms underlying the aberrant splicing events in cervical cancer that may serve as potential biomarkers for diagnosis, prognosis, and novel drug targets.In this review on spin exchanges, written to provide guidelines useful for finding the spin lattice relevant for any given magnetic solid, we discuss how the values of spin exchanges in transition metal magnetic compounds are quantitatively determined from electronic structure calculations, which electronic factors control whether a spin exchange is antiferromagnetic or ferromagnetic, and how these factors are related to the geometrical parameters of the spin exchange path. In an extended solid containing transition metal magnetic ions, each metal ion M is surrounded with main-group ligands L to form an MLn polyhedron (typically, n = 3-6), and the unpaired spins of M are represented by the singly-occupied d-states (i.e., the magnetic orbitals) of MLn. Each magnetic orbital has the metal d-orbital combined out-of-phase with the ligand p-orbitals; therefore, the spin exchanges between adjacent metal ions M lead not only to the M-L-M-type exchanges, but also to the M-L…L-M-type exchanges in which the two metal ions do not share a common ligand. The latter can be further modified by d0 cations A such as V5+ and W6+ to bridge the L…L contact generating M-L…A…L-M-type exchanges. We describe several qualitative rules for predicting whether the M-L…L-M and M-L…A…L-M-type exchanges are antiferromagnetic or ferromagnetic by analyzing how the ligand p-orbitals in their magnetic orbitals (the ligand p-orbital tails, for short) are arranged in the exchange paths. Finally, we illustrate how these rules work by analyzing the crystal structures and magnetic properties of four cuprates of current interest -CuV2O6, LiCuVO4, (CuCl)LaNb2O7, and Cu3(CO3)2(OH)2.The advancement of knowledge on tumor biology over the past decades has demonstrated a close link between tumor cells and cells of the immune system. In this context, cytokines have a major role because they act as intermediaries in the communication into the tumor bed. Cytokines play an important role in the homeostasis of innate and adaptive immunity. In particular, they participate in the differentiation of CD4 T lymphocytes. These cells play essential functions in the anti-tumor immune response but can also be corrupted by tumors. The differentiation of naïve CD4 T cells depends on the cytokine environment in which they are activated. Additionally, at the tumor site, their activity can also be modulated according to the cytokines of the tumor microenvironment. Thus, polarized CD4 T lymphocytes can see their phenotype evolve, demonstrating functional plasticity. Knowledge of the impact of these cytokines on the functions of CD4 T cells is currently a source of innovation, for therapeutic purposes. In this review, we discuss the impact of the major cytokines present in tumors on CD4 T cells.

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