215 research outputs found
Framing an independent, integrated and evidence-based evaluation of the state of Australia's biophysical and human environments
© 2015, The Author(s). Published by Taylor & Francis. A new approach was developed for Australia's 2011 national State of the Environment (SoE) report to integrate the assessment of biophysical and human elements of the environment. A Common Assessment and Reporting Framework (CARF) guided design and implementation, responding to jurisdictional complexity, outstanding natural diversity and ecosystem values, high levels of cultural and heritage diversity, and a paucity of national-scale data. The CARF provided a transparent response to the need for an independent, robust and evidence-based national SoE report. We conclude that this framework will be effective for subsequent national SoE assessments and other integrated national-scale assessments in data-poor regions
Functional interaction between Lypd6 and nicotinic acetylcholine receptors
Nicotinic acetylcholine receptors (nAChRs) affect multiple physiological functions in the brain and their functions are modulated by regulatory proteins of the Lynx family. Here, we report for the first time a direct interaction of the Lynx protein LY6/PLAUR domainâcontaining 6 (Lypd6) with nAChRs in human brain extracts, identifying Lypd6 as a novel regulator of nAChR function. Using protein crossâlinking and affinity purification from human temporal cortical extracts, we demonstrate that Lypd6 is a synaptically enriched membraneâbound protein that binds to multiple nAChR subtypes in the human brain. Additionally, soluble recombinant Lypd6 protein attenuates nicotineâinduced hippocampal inward currents in rat brain slices and decreases nicotineâinduced extracellular signalâregulated kinase phosphorylation in PC12 cells, suggesting that binding of Lypd6 is sufficient to inhibit nAChRâmediated intracellular signaling. We further show that perinatal nicotine exposure in rats (4Â mg/kg/day through minipumps to dams from embryonic day 7 to postânatal day 21) significantly increases Lypd6 protein levels in the hippocampus in adulthood, which did not occur after exposure to nicotine in adulthood only. Our findings suggest that Lypd6 is a versatile inhibitor of cholinergic signaling in the brain, and that Lypd6 is dysregulated by nicotine exposure during early development. [Image: see text] Regulatory proteins of the Lynx family modulate the function of nicotinic receptors (nAChRs). We report for the first time that the Lynx protein Lypd6 binds to nAChRs in human brain extracts, and that recombinant Lypd6 decreases nicotineâinduced ERK phosphorylation and attenuates nicotineâinduced hippocampal inward currents. Our findings suggest that Lypd6 is a versatile inhibitor of cholinergic signaling in the brain
Population-based study of diagnostic assays for Borrelia infection: comparison of purified flagella antigen assay (Ideiaâą, Dako Cytomation) and recombinant antigen assay (LiaisonÂź, DiaSorin)
<p>Abstract</p> <p>Background</p> <p>Testing for <it>Borrelia</it>-specific IgM and IgG-antibodies are often performed on a variety of poorly defined symptoms, and isolated IgM results are a frequent finding, which results in diagnostic uncertainty and further testing. We wanted to test the hypothesis that Borrelia-specific assays using recombinant antigens perform differently from assays based on purified flagella antigen.</p> <p>Methods</p> <p>We compared the use of recombinant antigens (LIAISON<sup>Âź </sup>DiaSorin, Saluggia, Italy) and purified flagella antigen (IDEIAâą Borrelia, DakoCytomation, Glostrup, Denmark) in the assay for <it>Borrelia</it>-specific IgM and IgG-antibodies. The assays were tested on an unselected population of serum samples submitted from general practice. A total of 357 consecutive samples for analysis of <it>Borrelia </it>IgM and IgG antibodies. Furthermore, we analysed 540 samples for <it>Borrelia</it>-specific IgM or IgG antibodies first by the IDEIAâą and, if they were positive, the samples were further analysed using the LIAISON<sup>Âź </sup>assay. To verify the correctness of the patient's serological status, discrepant samples were analysed by line blots (EcoLine, Virotech).</p> <p>Results</p> <p>In the consecutive series of 357 samples, the IgM assays detected 308 negative and 3 positive samples with concordant results. Compared with the line blot, the IDEIAâą system produced 21 false-positive IgM results, whereas the LIAISON<sup>Âź </sup>system produced only one false-positive IgM result. The IgG assays showed 1 positive and 328 negative concordant results. The LIAISON<sup>Âź </sup>system produced 9 true IgG-positive samples that were not detected by the IDEIAâą system, but the former produced 4 positive IgG results that were negative by line blot.</p> <p>Conclusion</p> <p>Diagnostic assays based on flagella antigen seem to show more false-positive IgM and false-negative IgG results than assays based on recombinant antigens. The latter may reduce the number of presumably false-positive IgM results and identify more IgG-positive subjects, but this system also produces more false-positive IgG results.</p
Cutaneous nociception and neurogenic inflammation evoked by PACAP38 and VIP
Pituitary adenylate cyclase-activating peptide-38 (PACAP38) and vasoactive intestinal peptide (VIP) belong to the same secretinâglucagon superfamily and are present in nerve fibers in dura and skin. Using a model of acute cutaneous pain we explored differences in pain perception and vasomotor responses between PACAP38 and VIP in 16 healthy volunteers in a double-blind, placebo-controlled, crossover study. All participants received intradermal injections of 200Â pmol PACAP38, 200Â pmol VIP and placebo into the volar forearm. Measurements included pain intensity on a visual analog scale (VAS), blood flow by laser Doppler flowmetry, visual flare and wheal. Pain intensities after PACAP38 and VIP were mild and limited to a short time of about 100Â s after injection. The area under the VAS-time curve was larger following PACAP38 (PÂ =Â 0.004) and VIP (PÂ =Â 0.01) compared to placebo. We found no statistical difference in pain perception between PACAP38 and VIP. Skin blood flow increase, flare and wheal were larger after both PACAP38 (PÂ =Â 0.011) and VIP (PÂ =Â 0.001) compared to placebo. VIP induced a considerably larger increase in skin blood flow, flare and wheal than PACAP38 (PÂ =Â 0.002). In conclusion, we found that peripheral nociceptive cutaneous responses elicited by PACAP38 and VIP are similar in healthy volunteers. This suggests that acute pain and vasomotor responses following intradermal injections of PACAP38 and VIP are primarily mediated by VPAC receptors
Contrasting phylogeographic pattern among Eudyptes penguins around the Southern Ocean
Since at least the middle-Miocene, the Antarctic Polar Front (APF) and the Subtropical Front (STF) appear to have been the main drivers of diversification of marine biota in the Southern Ocean. However, highly migratory marine birds and mammals challenge this paradigm and the importance of oceanographic barriers. Eudyptes penguins range from the Antarctic Peninsula to subantarctic islands and some of the southernmost subtropical islands. Because of recent diversification, the number of species remains uncertain. Here we analyze two mtDNA (HVRI, COI) and two nuclear (ODC, AK1) markers from 13 locations of five putative Eudyptes species: rockhopper (E. filholi, E. chrysocome, and E. moseleyi), macaroni (E. chrysolophus) and royal penguins (E. schlegeli). Our results show a strong phylogeographic structure among rockhopper penguins from South America, subantarctic and subtropical islands supporting the recognition of three separated species of rockhopper penguins. Although genetic divergence was neither observed among macaroni penguins from the Antarctic Peninsula and sub-Antarctic islands nor between macaroni and royal penguins, population genetic analyses revealed population genetic structure in both cases. We suggest that the APF and STF can act as barriers for these species. While the geographic distance between colonies might play a role, their impact/incidence on gene flow may vary between species and colonies
Convergence of marine megafauna movement patterns in coastal and open oceans
The extent of increasing anthropogenic impacts on large marine vertebrates partly depends on the animalsâ movement patterns. Effective conservation requires identification of the key drivers of movement including intrinsic properties and extrinsic constraints associated with the dynamic nature of the environments the animals inhabit. However, the relative importance of intrinsic versus extrinsic factors remains elusive. We analyze a global dataset of âŒ2.8 million locations from >2,600 tracked individuals across 50 marine vertebrates evolutionarily separated by millions of years and using different locomotion modes (fly, swim, walk/paddle). Strikingly, movement patterns show a remarkable convergence, being strongly conserved across species and independent of body length and mass, despite these traits ranging over 10 orders of magnitude among the species studied. This represents a fundamental difference between marine and terrestrial vertebrates not previously identified, likely linked to the reduced costs of locomotion in water. Movement patterns were primarily explained by the interaction between species-specific traits and the habitat(s) they move through, resulting in complex movement patterns when moving close to coasts compared with more predictable patterns when moving in open oceans. This distinct difference may be associated with greater complexity within coastal microhabitats, highlighting a critical role of preferred habitat in shaping marine vertebrate global movements. Efforts to develop understanding of the characteristics of vertebrate movement should consider the habitat(s) through which they move to identify how movement patterns will alter with forecasted severe ocean changes, such as reduced Arctic sea ice cover, sea level rise, and declining oxygen content
Genomic Expression Libraries for the Identification of Cross-Reactive Orthopoxvirus Antigens
Increasing numbers of human cowpox virus infections that are being observed and that particularly affect young non-vaccinated persons have renewed interest in this zoonotic disease. Usually causing a self-limiting local infection, human cowpox can in fact be fatal for immunocompromised individuals. Conventional smallpox vaccination presumably protects an individual from infections with other Orthopoxviruses, including cowpox virus. However, available live vaccines are causing severe adverse reactions especially in individuals with impaired immunity. Because of a decrease in protective immunity against Orthopoxviruses and a coincident increase in the proportion of immunodeficient individuals in today's population, safer vaccines need to be developed. Recombinant subunit vaccines containing cross-reactive antigens are promising candidates, which avoid the application of infectious virus. However, subunit vaccines should contain carefully selected antigens to confer a solid cross-protection against different Orthopoxvirus species. Little is known about the cross-reactivity of antibodies elicited to cowpox virus proteins. Here, we first identified 21 immunogenic proteins of cowpox and vaccinia virus by serological screenings of genomic Orthopoxvirus expression libraries. Screenings were performed using sera from vaccinated humans and animals as well as clinical sera from patients and animals with a naturally acquired cowpox virus infection. We further analyzed the cross-reactivity of the identified immunogenic proteins. Out of 21 identified proteins 16 were found to be cross-reactive between cowpox and vaccinia virus. The presented findings provide important indications for the design of new-generation recombinant subunit vaccines
Convergence of marine megafauna movement patterns in coastal and open oceans
Author Posting. © The Author(s), 2017. This is the author's version of the work. It is posted here for personal use, not for redistribution. The definitive version was published in Proceedings of the National Academy of Sciences of the United States of America 115 (2018): 3072-3077, doi:10.1073/pnas.1716137115.The extent of increasing anthropogenic impacts on large marine
vertebrates partly depends on the animalsâ movement patterns.
Effective conservation requires identification of the key drivers of
movement including intrinsic properties and extrinsic constraints
associated with the dynamic nature of the environments the animals
inhabit. However, the relative importance of intrinsic versus
extrinsic factors remains elusive. We analyse a global dataset of
2.8 million locations from > 2,600 tracked individuals across 50
marine vertebrates evolutionarily separated by millions of years
and using different locomotion modes (fly, swim, walk/paddle).
Strikingly, movement patterns show a remarkable convergence,
being strongly conserved across species and independent of body
length and mass, despite these traits ranging over 10 orders of
magnitude among the species studied. This represents a fundamental
difference between marine and terrestrial vertebrates not
previously identified, likely linked to the reduced costs of locomotion
in water. Movement patterns were primarily explained by the
interaction between species-specific traits and the habitat(s) they
move through, resulting in complex movement patterns when
moving close to coasts compared to more predictable patterns
when moving in open oceans. This distinct difference may be
associated with greater complexity within coastal micro-habitats,
highlighting a critical role of preferred habitat in shaping marine
vertebrate global movements. Efforts to develop understanding
of the characteristics of vertebrate movement should consider the
habitat(s) through which they move to identify how movement
patterns will alter with forecasted severe ocean changes, such as
reduced Arctic sea ice cover, sea level rise and declining oxygen
content.Workshops funding granted by the UWA Oceans Institute, AIMS, and
KAUST. AMMS was supported by an ARC Grant DE170100841 and an IOMRC
(UWA, AIMS, CSIRO) fellowship; JPR by MEDC (FPU program, Spain); DWS by
UK NERC and Save Our Seas Foundation; NQ by FCT (Portugal); MMCM by
a CAPES fellowship (Ministry of Education)
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