In this study, variations in the thermal diffusivity of PI-clay nanocomposite films prepared by different methods were investigated. The thermal diffusivity of PI-clay nanocomposite film increased at low clay content only when unmodified clay was used, where the clay morphology was a layered structure dispersed on a nanometer scale. Moreover, the thermal diffusivity could be enhanced by controlling the tensile stress induced by spontaneous shrinkage of the film during thermal imidization. These results demonstrated that the thermal diffusivity
of PI-clay nanocomposite films is significantly affected by the dispersion and/or arrangement states of the clay. (C) 2010 Wiley Periodicals, Inc. J Appl Polym Sci 119: 3010-3018, 2011″
“In host and cancer tissues, drug metabolism and susceptibility to drugs vary in a circadian (24 h) manner. In particular, the efficacy of a cell cycle specific (CCS) cytotoxic selleck agent is affected by the daily modulation of cell cycle activity in the target tissues. Anti-cancer chronotherapy, in which treatments are administered at a particular time each day, aims at exploiting these biological rhythms to reduce toxicity and improve efficacy of the treatment. The circadian status, which is the timing of physiological and behavioral activity relative AZD7762 solubility dmso to daily environmental cues, largely determines the best timing of treatments.
However, the influence of variations in tumor kinetics has not been considered in determining appropriate treatment selleck chemicals schedules. We used a simple model for cell populations under chronomodulated treatment to identify which biological parameters are important for
the successful design of a chronotherapy strategy. We show that the duration of the phase of the cell cycle targeted by the treatment and the cell proliferation rate are crucial in determining the best times to administer CCS drugs. Thus, optimal treatment times depend not only on the circadian status of the patient but also on the cell cycle kinetics of the tumor. Then, we developed a theoretical analysis of treatment outcome (TATO) to relate the circadian status and cell cycle kinetic parameters to the treatment outcomes. We show that the best and the worst CCS drug administration schedules are those with 24 h intervals, implying that 24 h chronomodulated treatments can be ineffective or even harmful if administered at wrong circadian times. We show that for certain tumors, administration times at intervals different from 24 h may reduce these risks without compromising overall efficacy.”
“Objectives
This study investigates opioid maintenance treatment (OMT) patients found to have corrected QT (QTc) interval above 500 ms, with particular focus on past medical history, genetic testing and cardiac investigations.
Methods
Detailed medical and cardiac history was obtained, with particular focus upon risk factors.