1,221 research outputs found
Zonal flow generation through four wave interaction in reduced models of fusion plasma turbulence
In tokamaks, turbulence is a key contributor to cross field transport. However,
it is also responsible for the spontaneous generation of large scale structures
such as zonal
ows. These are of relevance to fusion plasmas as they can create transport
barriers which aid plasma confinement. The interaction between drift waves
and zonal
ows can be investigated using reduced models such as the Hasegawa-
Mima and Hasegawa-Wakatani equations.
A four-wave truncated model is developed for the Extended-Hasegawa-Mima
(EHM) equation. This produces a set of four ordinary differential equations (ODEs)
that are used to investigate the modulational instability (MI), a mechanism by which
drift waves can produce a zonal
ow. These equations are linearised to produce a
dispersion relation for the MI which is used to produce a set of maps of the linear
growth rate of the MI. These show how additional modes become unstable as the
gyroradius is increased. The truncated model and dispersion relation are then compared
to measurements taken from simulations of the full EHM partial differential
equation (PDE) which has been seeded with an appropriate initial condition. Good
agreement is found when the pump wave has no component in the direction of the
density gradient.
A similar truncated model is derived for the Extended-Hasegawa-Wakatani
(EHW) equations. As the EHW system has separate equations for density and
potential this leads to a set of eight ODEs. The linearisation technique used for the
EHM system cannot be applied here. Instead, approximations based on the built in
EHW instability are made to calculate a linear growth rate for the zonal
ow using
the ODEs describing it. These analytical predictions are then compared to a full
PDE simulation of the system, which is initialised using random noise. It is found
that for particular sets of waves the ODEs provide a good prediction of the linear
growth rate.
A driving term is added to the EHM equation to reproduce the effect of
the built in instability of the EHW equations. This causes a drift wave spectrum to
grow when full EHW PDE simulations are seeded with random noise. The four-wave
ODE model is updated to include this driving. The ODE model again produces good
predictions for the growth rate of the zonal
flow
Making It Last: Storage Time and Temperature Have Differential Impacts on Metabolite Profiles of Airway Samples from Cystic Fibrosis Patients.
Metabolites of human or microbial origin have the potential to be important biomarkers of the disease state in cystic fibrosis (CF). Clinical sample collection and storage conditions may impact metabolite abundances with clinical relevance. We measured the change in metabolite composition based on untargeted gas chromatography-mass spectrometry (GC-MS) when CF sputum samples were stored at 4°C, -20°C, or -80°C with one or two freeze-thaw cycles. Daily measurements were taken for 1 week and then weekly for 4 weeks (4°C) and 8 weeks (-20°C). The metabolites in samples stored at -20°C maintained abundances similar to those found at-80°C over the course of 8 weeks (average change in Bray-Curtis distance, 0.06 ± 0.04) and were also stable after one or two freeze-thaw cycles. However, the metabolite profiles of samples stored at 4°C shifted after 1 day and continued to change over the course of 4 weeks (average change in Bray-Curtis distance, 0.31 ± 0.12). The abundances of several amino acids and other metabolites increased with time of storage at 4°C but remained constant at -20°C. Storage temperature was a significant factor driving the metabolite composition (permutational multivariate analysis of variance: r2 = 0.32 to 0.49, P < 0.001). CF sputum samples stored at -20°C at the time of sampling maintain a relatively stable untargeted GC-MS profile. Samples should be frozen on the day of collection, as more than 1 day at 4°C impacts the global composition of the metabolites in the sample. IMPORTANCE Metabolomics has great potential for uncovering biomarkers of the disease state in CF and many other contexts. However, sample storage timing and temperature may alter the abundance of clinically relevant metabolites. To assess whether existing samples are stable and to direct future study design, we conducted untargeted GC-MS metabolomic analysis of CF sputum samples after one or two freeze-thaw cycles and storage at 4°C and -20°C for 4 to 8 weeks. Overall, storage at -20°C and freeze-thaw cycles had little impact on metabolite profiles; however, storage at 4°C shifted metabolite abundances significantly. GC-MS profiling will aid in our understanding of the CF lung, but care should be taken in studies using sputum samples to ensure that samples are properly stored
Portfolio Concentration and Investment Performance
This study examines the relationship between investment performance and concentration in
active equity portfolios. Active management is dependent on the success of two important
components in the investment process â stock selection skill and portfolio management. Our
study documents a positive relationship between fund performance and portfolio concentration.
The relationship is stronger for stocks in which active managers hold overweight positions, as well as for stocks outside the largest 50 stocks listed on the Australian Stock Exchange (ASX). We find more concentrated funds tend to be those implementing growth styles, having smaller
aggregate assets under management, being institutions which are not affiliated with a bank or life-office entity, whose funds experience past period outflows, and who are benchmarked to narrower indexes than the S&P/ASX 300
Clustering of solutions in the random satisfiability problem
Using elementary rigorous methods we prove the existence of a clustered phase
in the random -SAT problem, for . In this phase the solutions are
grouped into clusters which are far away from each other. The results are in
agreement with previous predictions of the cavity method and give a rigorous
confirmation to one of its main building blocks. It can be generalized to other
systems of both physical and computational interest.Comment: 4 pages, 1 figur
Potentially inappropriate medications defined by STOPP criteria and the risk of adverse drug events in older hospitalized patients
Background: Previous studies have not demonstrated a consistent association between potentially inappropriate medicines (PIMs) in older patients as defined by Beers criteria and avoidable adverse drug events (ADEs). This study aimed to assess whether PIMs defined by new STOPP (Screening Tool of Older Persons' potentially inappropriate Prescriptions) criteria are significantly associated with ADEs in older people with acute illness. Methods: We prospectively studied 600 consecutive patients 65 years or older who were admitted with acute illness to a university teaching hospital over a 4-month interval. Potentially inappropriate medicines were defined by both Beers and STOPP criteria. Adverse drug events were defined by World Health Organization- Uppsala Monitoring Centre criteria and verified by a local expert consensus panel, which also assessed whether ADEs were causal or contributory to current hospitalization. Hallas criteria defined ADE avoidability. We compared the proportions of patients taking Beers criteria PIMs and STOPP criteria PIMs with avoidable ADEs that were causal or contributory to admission. Results: A total of 329 ADEs were detected in 158 of 600 patients (26.3%); 219 of 329 ADEs (66.6%) were considered causal or contributory to admission. Of the 219 ADEs, 151(68.9%) considered causal or contributory to admission were avoidable or potentially avoidable. After adjusting for age, sex, comorbidity, dementia, baseline activities of daily living function, and number of medications, the likelihood of a serious avoidable ADE increased significantly when STOPP PIMs were prescribed (odds ratio, 1.847; 95% confidence interval [CI], 1.506-2.264;P<.001);prescription of Beers criteria PIMs did not significantly increase ADE risk (odds ratio, 1.276; 95% CI, 0.945-1.722; P=.11). Conclusion: STOPP criteria PIMs, unlike Beers criteria PIMs, are significantly associated with avoidable ADEs in older people that cause or contribute to urgent hospitalization
Adipose depot gene expression identifies intelectin-1 as potential mediator of the metabolic response to cancer and cachexia
Background Cancer cachexia is a poorly understood metabolic consequence of cancer. During cachexia, different adipose depots demonstrate differential wasting rates. Animal models suggest adipose tissue may be a key driver of muscle wasting through fatâmuscle crosstalk, but human studies in this area are lacking. We performed global gene expression profiling of visceral (VAT) and subcutaneous (SAT) adipose from weight stable and cachectic cancer patients and healthy controls. Methods Cachexia was defined as >2% weight loss plus low computed tomographyâmuscularity. Biopsies of SAT and VAT were taken from patients undergoing resection for oesophagoâgastric cancer, and healthy controls (n = 16 and 8 respectively). RNA was isolated and reverse transcribed. cDNA was hybridised to the Affymetrix Clariom S microarray and data analysed using R/Bioconductor. Differential expression of genes was assessed using empirical Bayes and moderatedâtâstatistic approaches. Category enrichment analysis was used with a tissueâspecific background to examine the biological context of differentially expressed genes. Selected differentially regulated genes were validated by qPCR. Enzymeâlinked immunosorbent assay (ELISA) for intelectinâ1 was performed on all VAT samples. The previouslyâdescribed cohort plus 12 additional patients from each group also had plasma I = intelectinâ1 ELISA carried out. Results In VAT vs. SAT comparisons, there were 2101, 1722, and 1659 significantly regulated genes in the cachectic, weight stable, and control groups, respectively. There were 2200 significantly regulated genes from VAT in cachectic patients compared with controls. Genes involving inflammation were enriched in cancer and control VAT vs. SAT, although different genes contributed to enrichment in each group. Energy metabolism, fat browning (e.g. uncoupling protein 1), and adipogenesis genes were downâregulated in cancer VAT (P = 0.043, P = 5.4 Ă 10â6 and P = 1 Ă 10â6 respectively). The gene showing the largest difference in expression was ITLN1, the gene that encodes for intelectinâ1 (false discovery rateâcorrected P = 0.0001), a novel adipocytokine associated with weight loss in other contexts. Conclusions SAT and VAT have unique gene expression signatures in cancer and cachexia. VAT is metabolically active in cancer, and intelectinâ1 may be a target for therapeutic manipulation. VAT may play a fundamental role in cachexia, but the downâregulation of energy metabolism genes implies a limited role for fat browning in cachectic patients, in contrast to preâclinical models
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