3,646 research outputs found

    A Note on Optimal Effort in the Maldivian Tuna Fishery

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    This note argues that spatial considerations and travel costs should be taken into account in devising tax/subsidy regulations for island-based tuna fisheries. In particular, the effect of a landings tax on distant fishing grounds should be considered when setting the level of the tax. A fuel subsidy is suggested as a means of offsetting the impact of the landings tax on marginal grounds.Environmental Economics and Policy, Research Methods/ Statistical Methods, Resource /Energy Economics and Policy,

    Myelin tetraspan family proteins but no non-tetraspan family proteins are present in the ascidian (Ciona intestinalis) genome

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    Author Posting. © Marine Biological Laboratory, 2005. This article is posted here by permission of Marine Biological Laboratory for personal use, not for redistribution. The definitive version was published in Biological Bulletin 209 (2005): 49-66.Several of the proteins used to form and maintain myelin sheaths in the central nervous system (CNS) and the peripheral nervous system (PNS) are shared among different vertebrate classes. These proteins include one-to-several alternatively spliced myelin basic protein (MBP) isoforms in all sheaths, proteolipid protein (PLP) and DM20 (except in amphibians) in tetrapod CNS sheaths, and one or two protein zero (P0) isoforms in fish CNS and in all vertebrate PNS sheaths. Several other proteins, including 2', 3'-cyclic nucleotide 3'-phosphodiesterase (CNP), myelin and lymphocyte protein (MAL), plasmolipin, and peripheral myelin protein 22 (PMP22; prominent in PNS myelin), are localized to myelin and myelin-associated membranes, though class distributions are less well studied. Databases with known and identified sequences of these proteins from cartilaginous and teleost fishes, amphibians, reptiles, birds, and mammals were prepared and used to search for potential homologs in the basal vertebrate, Ciona intestinalis. Homologs of lipophilin proteins, MAL/plasmolipin, and PMP22 were identified in the Ciona genome. In contrast, no MBP, P0, or CNP homologs were found. These studies provide a framework for understanding how myelin proteins were recruited during evolution and how structural adaptations enabled them to play key roles in myelination.This work was supported by grant IBN-0402188 from the National Science Foundation (RMG)

    Theory of Neutron Diffraction from the Vortex Lattice in UPt3

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    Neutron scattering experiments have recently been performed in the superconducting state of UPt3 to determine the structure of the vortex lattice. The data show anomalous field dependence of the aspect ratio of the unit cell in the B phase. There is apparently also a change in the effective coherence length on the transition from the B to the C phases. Such observations are not consistent with conventional superconductvity. A theory of these results is constructed based on a picture of two-component superconductivity for UPt3. In this way, these unusual observations can be understood. There is a possible discrepancy between theory and experiment in the detailed field dependence of the aspect ratio.Comment: 11 pages; uses REVTEX, APS and PRABIB styles; 2 Postscript figure files include

    Repurposing human PDE4 inhibitors for neglected tropical diseases : design, synthesis and evaluation of cilomilast analogues as Trypanosoma brucei PDEB1 inhibitors

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    Author Posting. © The Author(s), 2014. This is the author's version of the work. It is posted here by permission of Elsevier for personal use, not for redistribution. The definitive version was published in Bioorganic & Medicinal Chemistry Letters 24 (2014): 4084-4089, doi:10.1016/j.bmcl.2014.07.063.A medicinal chemistry exploration of the human phosphodiesterase 4 (hPDE4) inhibitor cilomilast (1) was undertaken in order to identify inhibitors of phosphodiesterase B1 of Trypanosoma brucei (TbrPDEB1). T. brucei is the parasite which causes African sleeping sickness, a neglected tropical disease that affects thousands each year, and TbrPDEB1 has been shown to be an essential target of therapeutic relevance. Noting that 1 is a weak inhibitor of TbrPDEB1, we report the design and synthesis of analogs of this compound, culminating in 12b, a sub-micromolar inhibitor of TbrPDEB1 that shows modest inhibition of T. brucei proliferation.This work was funded by the National Institutes of Health (R01AI082577)

    BIOL-0940E: Precision Medicine or Privileged Medicine?

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    This course proposal and syllabus was conceived and developed by a partnership of the three authors - two undergraduate students and a professor at Brown University. A reflective essay describing our partnership and creative process is in development for publication. This syllabus illustrates many course details that were driven by the student partners' insights and ideas, including the learning outcomes, weekly topics and readings, assignments, active learning elements, and approaches to facilitate agency of the Brown sophomores who subsequently took the course after is was approved in 2018 (BIOL-0940E)
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