3,927 research outputs found
Sleep homeostasis, seizures, and cognition in children with focal epilepsy
AIM: To investigate the link between sleep disruption and cognitive impairment in childhood epilepsy by studying the effect of epilepsy on sleep homeostasis, as reflected in slow-wave activity (SWA). METHOD: We examined SWA from overnight EEG-polysomnography in 19 children with focal epilepsy (mean [SD] age 11 years 6 months [3 years], range 6 years 6 months-15 years 6 months; 6 females, 13 males) and 18 age- and sex-matched typically developing controls, correlating this with contemporaneous memory consolidation task scores, full-scale IQ, seizures, and focal interictal discharges. RESULTS: Children with epilepsy did not differ significantly from controls in overnight SWA decline (p = 0.12) or gain in memory performance with sleep (p = 0.27). SWA was lower in patients compared to controls in the first hour of non-rapid eye movement sleep (p = 0.021), although not in those who remained seizure-free (p = 0.26). Full-scale IQ did not correlate with measures of SWA in patients or controls. There was no significant difference in SWA measures between focal and non-focal electrodes. INTERPRETATION: Overnight SWA decline is conserved in children with focal epilepsy and may underpin the preservation of sleep-related memory consolidation in this patient group. Reduced early-night SWA may reflect impaired or immature sleep homeostasis in those with a higher seizure burden
Sleep homeostasis, seizures, and cognition in children with focal epilepsy
AIM
To investigate the link between sleep disruption and cognitive impairment in childhood epilepsy by studying the effect of epilepsy on sleep homeostasis, as reflected in slow-wave activity (SWA).
METHOD
We examined SWA from overnight EEG-polysomnography in 19 children with focal epilepsy (mean [SD] age 11 years 6 months [3 years], range 6 years 6 months-15 years 6 months; 6 females, 13 males) and 18 age- and sex-matched typically developing controls, correlating this with contemporaneous memory consolidation task scores, full-scale IQ, seizures, and focal interictal discharges.
RESULTS
Children with epilepsy did not differ significantly from controls in overnight SWA decline (p = 0.12) or gain in memory performance with sleep (p = 0.27). SWA was lower in patients compared to controls in the first hour of non-rapid eye movement sleep (p = 0.021), although not in those who remained seizure-free (p = 0.26). Full-scale IQ did not correlate with measures of SWA in patients or controls. There was no significant difference in SWA measures between focal and non-focal electrodes.
INTERPRETATION
Overnight SWA decline is conserved in children with focal epilepsy and may underpin the preservation of sleep-related memory consolidation in this patient group. Reduced early-night SWA may reflect impaired or immature sleep homeostasis in those with a higher seizure burden
Cholestatic hepatitis as a possible new side-effect of oxycodone: a case report
<p>Abstract</p> <p>Introduction</p> <p>Oxycodone is a widely-used semisynthetic opioid analgesic that has been used for over eighty years. Oxycodone is known to cause side effects such as nausea, pruritus, dizziness, constipation and somnolence. As far as we are aware cholestatic hepatitis as a result of oxycodone use has not been reported so far in the world literature.</p> <p>Case presentation</p> <p>A 34-year-old male presented with cholestatic jaundice and severe pruritus after receiving oxycodone for analgesia post-T11 vertebrectomy. Extensive laboratory investigations and imaging studies did not reveal any other obvious cause for his jaundice and a liver biopsy confirmed canalicular cholestatis suggestive of drug-induced hepatotoxicity. The patient's symptoms and transaminases normalised on withdrawal of oxycodone confirming that oxycodone was the probable cause of the patient's hepatotoxicity.</p> <p>Conclusion</p> <p>We conclude that cholestatic hepatitis is possibly a rare side effect of oxycodone use. Physicians should be aware of the possibility of this potentially serious picture of drug-induced hepatotoxicity.</p
Testing outer boundary treatments for the Einstein equations
Various methods of treating outer boundaries in numerical relativity are
compared using a simple test problem: a Schwarzschild black hole with an
outgoing gravitational wave perturbation. Numerical solutions computed using
different boundary treatments are compared to a `reference' numerical solution
obtained by placing the outer boundary at a very large radius. For each
boundary treatment, the full solutions including constraint violations and
extracted gravitational waves are compared to those of the reference solution,
thereby assessing the reflections caused by the artificial boundary. These
tests use a first-order generalized harmonic formulation of the Einstein
equations. Constraint-preserving boundary conditions for this system are
reviewed, and an improved boundary condition on the gauge degrees of freedom is
presented. Alternate boundary conditions evaluated here include freezing the
incoming characteristic fields, Sommerfeld boundary conditions, and the
constraint-preserving boundary conditions of Kreiss and Winicour. Rather
different approaches to boundary treatments, such as sponge layers and spatial
compactification, are also tested. Overall the best treatment found here
combines boundary conditions that preserve the constraints, freeze the
Newman-Penrose scalar Psi_0, and control gauge reflections.Comment: Modified to agree with version accepted for publication in Class.
Quantum Gra
Model independent results for and at order
Exclusive semileptonic B decays into and mesons are
investigated including order corrections using the
heavy quark effective theory. At zero recoil, the
corrections can be written in terms of the leading Isgur-Wise function for
these transitions, , and known meson mass splittings. We obtain an almost
model independent prediction for the shape of the spectrum near zero recoil,
including order corrections. We determine
from the measured branching ratio. Implications for B
decay sum rules are discussed.Comment: 11 pages, revte
B --> pi and B --> K transitions in partially quenched chiral perturbation theory
We study the properties of the B-->pi and B-->K transition form factors in
partially quenched QCD by using the approach of partially quenched chiral
perturbation theory combined with the static heavy quark limit. We show that
the form factors change almost linearly when varying the value of the sea quark
mass, whereas the dependence on the valence quark mass contains both the
standard and chirally divergent (quenched) logarithms. A simple strategy for
the chiral extrapolations in the lattice studies with Nsea=2 is suggested. It
consists of the linear extrapolations from the realistically accessible quark
masses, first in the sea and then in the valence quark mass. From the present
approach, we estimate the uncertainty induced by such extrapolations to be
within 5%.Comment: Published versio
The Rare Decay D^0 -> gamma gamma
We present a calculation of the rare decay mode D^0 -> gamma gamma, in which
the long distance contributions are expected to be dominant. Using the Heavy
Quark Chiral Perturbation Theory Lagrangian with a strong g coupling as
recently determined by CLEO from the D^* -> D pi width, we consider both the
anomaly contribution which relates to the annihilation part of the weak
Lagrangian and the one-loop pi, K diagrams. The loop contributions which are
proportional to g and contain the a_1 Wilson coefficient are found to dominate
the decay amplitude, which turns out to be mainly parity violating. The
branching ratio is then calculated to be (1.0+-0.5)x10^(-8). Observation of an
order of magnitude larger branching ratio could be indicative of new physics.Comment: 16 pages, 5 figures, additional reference and several remarks added,
results unchange
Angiogenic Factors Stimulate Growth of Adult Neural Stem Cells
The ability to grow a uniform cell type from the adult central nervous system (CNS) is valuable for developing cell therapies and new strategies for drug discovery. The adult mammalian brain is a source of neural stem cells (NSC) found in both neurogenic and non-neurogenic zones but difficulties in culturing these hinders their use as research tools.Here we show that NSCs can be efficiently grown in adherent cell cultures when angiogenic signals are included in the medium. These signals include both anti-angiogenic factors (the soluble form of the Notch receptor ligand, Dll4) and pro-angiogenic factors (the Tie-2 receptor ligand, Angiopoietin 2). These treatments support the self renewal state of cultured NSCs and expression of the transcription factor Hes3, which also identifies the cancer stem cell population in human tumors. In an organotypic slice model, angiogenic factors maintain vascular structure and increase the density of dopamine neuron processes.We demonstrate new properties of adult NSCs and a method to generate efficient adult NSC cultures from various central nervous system areas. These findings will help establish cellular models relevant to cancer and regeneration
B-->pi and B-->K transitions in standard and quenched chiral perturbation theory
We study the effects of chiral logs on the heavy-->light pseudoscalar meson
transition form factors by using standard and quenched chiral perturbation
theory combined with the static heavy quark limit. The resulting expressions
are used to indicate the size of uncertainties due to the use of the quenched
approximation in the current lattice studies. They may also be used to assess
the size of systematic uncertainties induced by missing chiral log terms in
extrapolating toward the physical pion mass. We also provide the coefficient
multiplying the quenched chiral log, which may be useful if the quenched
lattice studies are performed with very light mesons.Comment: 33 pages, 8 PostScript figures, version to appear in PR
Persistence of anticancer activity in berry extracts after simulated gastrointestinal digestion and colonic fermentation
Fruit and vegetable consumption is associated at the population level with a protective effect against colorectal cancer. Phenolic compounds, especially abundant in berries, are of interest due to their putative anticancer activity. After consumption, however, phenolic compounds are subject to digestive conditions within the gastrointestinal tract that alter their structures and potentially their function. However, the majority of phenolic compounds are not efficiently absorbed in the small intestine and a substantial portion pass into the colon. We characterized berry extracts (raspberries, strawberries, blackcurrants) produced by in vitro-simulated upper intestinal tract digestion and subsequent fecal fermentation. These extracts and selected individual colonic metabolites were then evaluated for their putative anticancer activities using in vitro models of colorectal cancer, representing the key stages of initiation, promotion and invasion. Over a physiologically-relevant dose range (0–50 µg/ml gallic acid equivalents), the digested and fermented extracts demonstrated significant anti-genotoxic, anti-mutagenic and anti-invasive activity on colonocytes. This work indicates that phenolic compounds from berries undergo considerable structural modifications during their passage through the gastrointestinal tract but their breakdown products and metabolites retain biological activity and can modulate cellular processes associated with colon cancer
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