1,121 research outputs found
Channel Capacities for Different Antenna Arrays with Various Transmitting Angles in Tunnels
[[abstract]]This paper focuses on the research of channel capacity of multiple-input multipleoutput
(MIMO) system with different transmitting angles in straight and curvy tunnels.Araytracing
technique is developed to calculate channel frequency responses for tunnels, and the
channel frequency response is further used to calculate corresponding channel capacity. The
channel capacities are calculated based on the realistic environment. The channel capacities
of MIMO long term evolution system using spatial and polar antenna arrays by different
transmitting angles are computed. Numerical results show that, The channel capacity for
transmitting angle at 15◦ is largest compared to the other angles in the tunnels. Moreover,
the channel capacity of polar array is better than that of spatial array both in the straight and
curvy tunnels. Besides, the channel capacity for the tunnels with traffic is larger than that
without traffic. Finally, it isworth noting that in these cases the presentwork provides not only
comparative information but also quantitative information on the performance reduction.[[notice]]補正完畢[[incitationindex]]SC
Two cold inducible genes encoding lipid transfer protein LTP4 from barley show differential responses to bacterial pathogens
The barley genesHvLtp4.2 andHvLtp4.3 both encode the lipid transfer protein LTP4 and are less than 1 kb apart in tail-to-tail orientation. They differ in their non-coding regions from each other and from the gene corresponding to a previously reportedLtp4 cDNA (nowLtp4.1). Southern blot analysis indicated the existence of three or moreLtp4 genes per haploid genome and showed considerable polymorphism among barley cultivars. We have investigated the transient expression of genesHvLtp4.2 andHvLtp4.3 following transformation by particle bombardment, using promoter fusions to the-glucuronidase reporter sequence. In leaves, activities of the two promoters were of the same order as those of the sucrose synthase (Ss1) and cauliflower mosaic virus 35S promoters used as controls. Their expression patterns were similar, except thatLtp4.2 was more active thanLtp4.3 in endosperm, andLtp4.3 was active in roots, whileLtp4.2 was not. The promoters of both genes were induced by low temperature, both in winter and spring barley cultivars. Northern blot analysis, using theLtp4-specific probe, indicated thatXanthomonas campestris pv.translucens induced an increase over basal levels ofLtp4 mRNA, whilePseudomonas syringae pv.japonica caused a decrease. TheLtp4.3-Gus promoter fusion also responded in opposite ways to these two compatible bacterial pathogens, whereas theLtp4.2-Gus construction did not respond to infectio
Genetics of CM-proteins (A-hordeins) in barley
The CM-proteins, which are the main components of the A-hordeins, include four previously described proteins (CMa-1, CMb-1, CMc-1, CMd-1), plus a new one, CMe-1, which has been tentatively included in this group on the basis of its solubility properties and electrophoretic mobility. The variability of the five proteins has been investigated among 38 Hordeum vulgare cultivars and 17 H. spontaneum accessions. Proteins CMa-1, CMc-1 and CMd-1 were invariant within the cultivated species; CMd was also invariant in the wild one. The inheritance of variants CMb-1/CMb-2 and CMe-1/CMe-2,2 was studied in a cross H. spontaneum x H. vulgare. The first two proteins were inherited as codominantly expressed allelic variations of a single mendelian gene. Components CMe-2,2 were jointly inherited and codominantly expressed with respect to CMe-1. Gene CMb and gene(s) CMe were found to be unlinked. The chromosomal locations of genes encoding CM-proteins were investigated using wheat-barley addition lines. Genes CMa and CMc were associated with chromosome 1, and genes CMb and CMd with chromosome 4. These gene locations further support the proposed homoeology of chromosomes 1 and 4 of barley with chromosomes groups 7 and 4 of wheat, respectively. Gene(s) CMe has been assigned to chromosome 3 of barley. The accumulation of protein CMe-1 is totally blocked in the high lysine mutant Riso 1508 and partially so in the high lysine barley Hiproly
Targeting Angiogenesis with Multitargeted Tyrosine Kinase Inhibitors in the Treatment of Non-Small Cell Lung Cancer
The article reviews the current developmental status of antiangiogenic tyrosine kinase inhibitors (including vandetanib, sunitinib, axitinib, sorafenib, vatalanib, and pazopanib) in non-small cell lung cancer and discusses the need for optimal patient selection and potential future directions
Identification of the occurrence and pattern of masseter muscle activities during sleep using EMG and accelerometer systems
<p>Abstract</p> <p>Background</p> <p>Sleep bruxism has been described as a combination of different orofacial motor activities that include grinding, clenching and tapping, although accurate distribution of the activities still remains to be clarified.</p> <p>Methods</p> <p>We developed a new system for analyzing sleep bruxism to examine the muscle activities and mandibular movement patterns during sleep bruxism. The system consisted of a 2-axis accelerometer, electroencephalography and electromyography. Nineteen healthy volunteers were recruited and screened to evaluate sleep bruxism in the sleep laboratory.</p> <p>Results</p> <p>The new system could easily distinguish the different patterns of bruxism movement of the mandible and the body movement. Results showed that grinding (59.5%) was most common, followed by clenching (35.6%) based on relative activity to maximum voluntary contraction (%MVC), whereas tapping was only (4.9%).</p> <p>Conclusion</p> <p>It was concluded that the tapping, clenching, and grinding movement of the mandible could be effectively differentiated by the new system and sleep bruxism was predominantly perceived as clenching and grinding, which varied between individuals.</p
Enhancing preschoolers' executive functions through embedding cognitive activities in shared book reading
Given evidence that early executive functioning sets the stage for a broad range of subsequent
outcomes, researchers have sought to identify ways to foster these cognitive capacities. An
increasingly common approach involves computerized ‘brain training’ programs, yet there are
questions about whether these are well suited for fostering the early development of executive
functions (EFs). The current series of studies sought to design, develop, and provide evidence for the
efficacy of embedding cognitive activities in a commonplace activity – shared reading of a children’s
book. The book, Quincey Quokka’s Quest, required children to control their thinking and behaviour to
help the story’s main character through a series of obstacles. The first study investigated effects of
reading with embedded cognitive activities in individual and group contexts on young children’s
executive functions (EFs). The second study compared reading with embedded cognitive activities
against a more-active control condition (dialogic reading) that similarly engaged children in the
reading process yet lacked clear engagement of EFs. The third study sought to investigate whether the
effect of reading the story with embedded EF activities changed across differing doses of the
intervention and whether effects persisted 2 months post-intervention. Findings provide converging
evidence of intervention effects on working memory and shifting in as little as 3 weeks (compared to
more traditional reading) and maintenance of these gains 2 months later. This suggests the efficacy of
embedding cognitive activities in the context of everyday activities, thereby extending the range of
users and contexts in which this approach can be used
Methodological standards in non-inferiority AIDS trials: moving from adherence to compliance
BACKGROUND: The interpretation of the results of active-control trials regarding the efficacy and safety of a new drug is important for drug registration and following clinical use. It has been suggested that non-inferiority and equivalence studies are not reported with the same quantitative rigor as superiority studies. METHODS: Standard methodological criteria for non-inferiority and equivalence trials including design, analysis and interpretation issues were applied to 18 recently conducted large non-inferiority (15) and equivalence (3) randomized trials in the field of AIDS antiretroviral therapy. We used the continuity-corrected non-inferiority chi-square to test 95% confidence interval treatment difference against the predefined non-inferiority margin. RESULTS: The pre-specified non-inferiority margin ranged from 10% to 15%. Only 4 studies provided justification for their choice. 39% of the studies (7/18) reported only intent-to-treat (ITT) analysis for the primary endpoint. When on-treatment (OT) and ITT statistical analyses were provided, ITT was favoured over OT for results interpretation for all but one study, inappropriately in this statistical context. All but two of the studies concluded there was "similar" efficacy of the experimental group. However, 9/18 had inconclusive results for non-inferiority. CONCLUSION: Conclusions about non-inferiority should be drawn on the basis of the confidence interval analysis of an appropriate primary endpoint, using the predefined criteria for non-inferiority, in both OT and ITT, in compliance with the non-inferiority and equivalence CONSORT statement. We suggest that the use of the non-inferiority chi-square test may provide additional useful information
Alcohol and HIV Disease Progression: Weighing the Evidence
Heavy alcohol use is commonplace among HIV-infected individuals; however, the extent that alcohol use adversely impacts HIV disease progression has not been fully elucidated. Fairly strong evidence suggests that heavy alcohol consumption results in behavioral and biological processes that likely increase HIV disease progression, and experimental evidence of the biological effect of heavy alcohol on simian immunodeficiency virus in macaques is quite suggestive. However, several observational studies of the effect of heavy alcohol consumption on HIV progression conducted in the 1990s found no association of heavy alcohol consumption with time to AIDS diagnosis, while some more recent studies showed associations of heavy alcohol consumption with declines of CD4 cell counts and nonsuppression of HIV viral load. We discuss several plausible biological and behavioral mechanisms by which alcohol may cause HIV disease progression, evidence from prospective observational human studies, and suggest future research to further illuminate this important issue
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