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Number of Pages: 5Integrative BiologyGeological Science
Temperature perturbation model of the opto-galvanic effect in CO2-laser discharges
A detailed discharge model of the opto-galvanic effect in molecular laser gas mixtures is developed based on the temperature perturbation or discharge cooling mechanism of Smith and Brooks (1979). Excellent agreement between the model and experimental results in CO2 laser gas mixtures is obtained. The model should be applicable to other molecular systems where the OGE is being used for laser stabilisation and as a spectroscopic tool
Artemisinin-based combination therapy does not measurably reduce human infectiousness to vectors in a setting of intense malaria transmission
<p>Background:
Artemisinin-based combination therapy (ACT) for treating malaria has activity against immature gametocytes. In theory, this property may complement the effect of terminating otherwise lengthy malaria infections and reducing the parasite reservoir in the human population that can infect vector mosquitoes. However, this has never been verified at a population level in a setting with intense transmission, where chronically infectious
asymptomatic carriers are common and cured patients are rapidly and repeatedly re-infected.</p>
<p>Methods:
From 2001 to 2004, malaria vector densities were monitored using light traps in three Tanzanian districts. Mosquitoes were dissected to determine parous and oocyst rates.
Plasmodium falciparum sporozoite rates were determined by ELISA. Sulphadoxinepyrimethamine(SP) monotherapy was used for treatment of uncomplicated malaria in the
contiguous districts of Kilombero and Ulanga throughout this period. In Rufiji district, the standard drug was changed to artesunate co-administered with SP (AS + SP) in March 2003. The effects of this change in case management on malaria parasite infection in the vectors were analysed.</p>
<p>Results:
Plasmodium falciparum entomological inoculation rates exceeded 300 infective bites per person per year at both sites over the whole period. The introduction of AS + SP in Rufiji was associated with increased oocyst prevalence (OR [95%CI] = 3.9 [2.9-5.3], p < 0.001), but had no consistent effect on sporozoite prevalence (OR [95%CI] = 0.9 [0.7-1.2], p = 0.5). The estimated infectiousness of the human population in Rufiji was very low prior to the change
in drug policy. Emergence rates and parous rates of the vectors varied substantially throughout the study period, which affected estimates of infectiousness. The latter
consequently cannot be explained by the change in drug policy.</p>
<p>Conclusions:
In high perennial transmission settings, only a small proportion of infections in humans are symptomatic or treated, so case management with ACT may have little impact on overall infectiousness of the human population. Variations in infection levels in vectors largely
depend on the age distribution of the mosquito population. Benefits of ACT in suppressingtransmission are more likely to be evident where transmission is already low or effective
vector control is widely implemented.</p>
Deep UV Luminosity Functions at the Infall Region of the Coma Cluster
We have used deep GALEX observations at the infall region of the Coma cluster
to measure the faintest UV luminosity functions (LFs) presented for a rich
galaxy cluster thus far. The Coma UV LFs are measured to M_UV = -10.5 in the
GALEX FUV and NUV bands, or 3.5 mag fainter than previous studies, and reach
the dwarf early-type galaxy population in Coma for the first time. The
Schechter faint-end slopes (alpha = -1.39 in both GALEX bands) are shallower
than reported in previous Coma UV LF studies owing to a flatter LF at faint
magnitudes. A Gaussian-plus-Schechter model provides a slightly better
parametrization of the UV LFs resulting in a faint-end slope of ~ -1.15 in both
GALEX bands. The two-component model gives faint-end slopes shallower than -1
(a turnover) for the LFs constructed separately for passive and star forming
galaxies. The UV LFs for star forming galaxies show a turnover at M_UV ~ -14
owing to a deficit of dwarf star forming galaxies in Coma with stellar masses
below M*=10^8 Msun. A similar turnover is identified in recent UV LFs measured
for the Virgo cluster suggesting this may be a common feature of local galaxy
clusters, whereas the field UV LFs continue to rise at faint magnitudes. We did
not identify an excess of passive galaxies as would be expected if the missing
dwarf star forming galaxies were quenched inside the cluster. In fact, the LFs
for both dwarf passive and star forming galaxies show the same turnover at
faint magnitudes. We discuss the possible origin of the missing dwarf star
forming galaxies in Coma and their expected properties based on comparisons to
local field galaxies.Comment: accepted for publication in Ap
Afrotheria genome; overestimation of genome size and distinct chromosome GC content revealed by flow karyotyping
AbstractAfrotheria genome size is reported to be over 50% larger than that of human, but we show that this is a gross overestimate. Although genome sequencing in Afrotheria is not complete, extensive homology with human has been revealed by chromosome painting. We provide new data on chromosome size and GC content in four Afrotherian species using flow karyotyping. Genome sizes are 4.13Gb in aardvark, 4.01Gb in African elephant, 3.69Gb in golden mole and 3.31Gb in manatee, whereas published results show a mean of 5.18Gb for Afrotheria. Genome GC content shows a negative correlation with size, indicating that this is due to differences in the amount of AT-rich sequences. Low genome GC content and small variance in chromosome GC content are characteristic of aardvark and elephant and may be associated with the high degree of conserved synteny, suggesting that these are features of the Afrotherian ancestral genome
Preventing childhood malaria in Africa by protecting adults from mosquitoes with insecticide-treated nets
Malaria prevention in Africa merits particular attention as the world strives toward a better life for the poorest. Insecticide-treated nets (ITNs) represent a practical means to prevent malaria in Africa, so scaling up coverage to at least 80% of young children and pregnant women by 2010 is integral to the Millennium Development Goals (MDG). Targeting individual protection to vulnerable groups is an accepted priority, but community-level impacts of broader population coverage are largely ignored even though they may be just as important. We therefore estimated coverage thresholds for entire populations at which individual- and community-level protection are equivalent, representing rational targets for ITN coverage beyond vulnerable groups
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The evolution of imprinting: chromosomal mapping of orthologues of mammalian imprinted domains in monotreme and marsupial mammals.
BACKGROUND: The evolution of genomic imprinting, the parental-origin specific expression of genes, is the subject of much debate. There are several theories to account for how the mechanism evolved including the hypothesis that it was driven by the evolution of X-inactivation, or that it arose from an ancestrally imprinted chromosome. RESULTS: Here we demonstrate that mammalian orthologues of imprinted genes are dispersed amongst autosomes in both monotreme and marsupial karyotypes. CONCLUSION: These data, along with the similar distribution seen in birds, suggest that imprinted genes were not located on an ancestrally imprinted chromosome or associated with a sex chromosome. Our results suggest imprinting evolution was a stepwise, adaptive process, with each gene/cluster independently becoming imprinted as the need arose.RIGHTS : This article is licensed under the BioMed Central licence at http://www.biomedcentral.com/about/license which is similar to the 'Creative Commons Attribution Licence'. In brief you may : copy, distribute, and display the work; make derivative works; or make commercial use of the work - under the following conditions: the original author must be given credit; for any reuse or distribution, it must be made clear to others what the license terms of this work are
Perturbations to the IGF1 growth pathway and adult energy homeostasis following disruption of mouse chromosome 12 imprinting
AIM: Disruption to insulin-like growth factor (IGF) signalling pathways during early life causes growth retardation and defects of developing metabolic organs that can alter set points of energy homeostasis for a lifetime. Inheritance of two maternal copies of human chromosome 14q32.2 (Temple syndrome) causes severe foetal growth retardation and post-natal failure to thrive. Disruption of imprinted gene dosage in the orthologous region on mouse chromosome 12 also affects growth. Here, we investigated whether altering chromosome 12-imprinted gene dosage can affect IGF signalling. METHODS: We investigated mice with a transgene insertion at the imprinted domain of chromosome 12. This lesion causes misexpression of neighbouring genes such that the expression of non-coding RNAs is elevated, and levels of delta-like homologue 1 (Dlk1), retrotransposon-like 1 (Rtl1) and deiodinase 3 (Dio3) transcripts are reduced. RESULTS: We observed three key phenotypes in these mice: (i) embryonic growth retardation associated with altered expression of IGF1 binding proteins, (ii) peri-natal failure to thrive accompanied by hypothyroidism and low serum IGF1. Unexpectedly this phenotype was growth hormone independent. (iii) Adult animals had reduced glucose tolerance as a result of endocrine pancreatic insufficiency. CONCLUSIONS: We propose that all of these phenotypes are attributable to impaired IGF action and show for the first time that the chromosome 12 cluster in the mouse is an imprinted locus that modulates the IGF signalling pathway. We propose that growth retardation observed in human Temple syndrome might have a similar cause
Age Constraints for an M31 Globular Cluster from Main Sequence Photometry
We present a color-magnitude diagram (CMD) of the globular cluster SKHB-312
in the Andromeda galaxy (M31), obtained with the Advanced Camera for Surveys on
the Hubble Space Telescope. The cluster was included in deep observations taken
to measure the star formation history of the M31 halo. Overcoming a very
crowded field, our photometry of SKHB-312 reaches V ~ 30.5 mag, more than 1 mag
below the main sequence turnoff. These are the first observations to allow a
direct age estimate from the turnoff in an old M31 cluster. We analyze its CMD
and luminosity function using a finely-spaced grid of isochrones that have been
calibrated using observations of Galactic clusters taken with the same camera
and filters. The luminosity difference between the subgiant and horizontal
branches is ~0.2 mag smaller in SKHB-312 than in the Galactic clusters 47 Tuc
and NGC 5927, implying SKHB-312 is 2-3 Gyr younger. A quantitative comparison
to isochrones yields an age of 10 +2.5/-1 Gyr
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