186 research outputs found
Unc-51/ATG1 Controls Axonal and Dendritic Development via Kinesin-Mediated Vesicle Transport in the Drosophila Brain
Background:Members of the evolutionary conserved Ser/Thr kinase Unc-51 family are key regulatory proteins that control neural development in both vertebrates and invertebrates. Previous studies have suggested diverse functions for the Unc-51 protein, including axonal elongation, growth cone guidance, and synaptic vesicle transport.Methodology/Principal Findings:In this work, we have investigated the functional significance of Unc-51-mediated vesicle transport in the development of complex brain structures in Drosophila. We show that Unc-51 preferentially accumulates in newly elongating axons of the mushroom body, a center of olfactory learning in flies. Mutations in unc-51 cause disintegration of the core of the developing mushroom body, with mislocalization of Fasciclin II (Fas II), an IgG-family cell adhesion molecule important for axonal guidance and fasciculation. In unc-51 mutants, Fas II accumulates in the cell bodies, calyx, and the proximal peduncle. Furthermore, we show that mutations in unc-51 cause aberrant overshooting of dendrites in the mushroom body and the antennal lobe. Loss of unc-51 function leads to marked accumulation of Rab5 and Golgi components, whereas the localization of dendrite-specific proteins, such as Down syndrome cell adhesion molecule (DSCAM) and No distributive disjunction (Nod), remains unaltered. Genetic analyses of kinesin light chain (Klc) and unc-51 double heterozygotes suggest the importance of kinesin-mediated membrane transport for axonal and dendritic development. Moreover, our data demonstrate that loss of Klc activity causes similar axonal and dendritic defects in mushroom body neurons, recapitulating the salient feature of the developmental abnormalities caused by unc-51 mutations.Conclusions/Significance:Unc-51 plays pivotal roles in the axonal and dendritic development of the Drosophila brain. Unc-51-mediated membrane vesicle transport is important in targeted localization of guidance molecules and organelles that regulate elongation and compartmentalization of developing neurons
Compatibilization of polypropylene/poly(3-hydroxybutyrate) blends
Blending polypropylene (PP) with biodegradable poly(3-hydroxybutyrate) (PHB) can be a nice alternative to minimize the disposal problem of PP and the intrinsic brittleness that restricts PHB applications. However, to achieve acceptable engineering properties, the blend needs to be compatibilized because of the immiscibility between PP and PHB. In this work, PP/PHB blends were prepared with different types of copolymers as possible compatibilizers: poly(propylene-g-maleic anhydride) (PPMAH), poly (ethylene-co-methyl acrylate) [P(EMA)], poly(ethylene-co-glycidyl methacrylate) [P(EGMA)], and poly(ethylene-co-methyl acrylate-co-glycidyl methacrylate) [P(EMAGMA)]. The effect of each copolymer on the morphology and mechanical properties of the blends was investigated. The results show that the compatibilizers efficiency decreased in this order: P(EMAGMA) > P(EMA) > P(EGMA) > PP-MAH; we explained this by taking into consideration the affinity degree of the compatibilizers with the PP matrix, the compatibilizers properties, and their ability to provide physical and/or reactive compatibilization with PHB. (C) 2011 Wiley Periodicals, Inc. J Appl Polym Sci 123: 3511-3519, 2012Fundacao de Amparo a Pesquisa do Estado de Sao PauloCoordenacao de Aperfeicoamento de Pessoal de Nivel SuperiorConselho Nacional de Desenvolvimento Cientifico e Tecnologico (Brazil
The Drosophila neural lineages: a model system to study brain development and circuitry
In Drosophila, neurons of the central nervous system are grouped into units called lineages. Each lineage contains cells derived from a single neuroblast. Due to its clonal nature, the Drosophila brain is a valuable model system to study neuron development and circuit formation. To better understand the mechanisms underlying brain development, genetic manipulation tools can be utilized within lineages to visualize, knock down, or over-express proteins. Here, we will introduce the formation and development of lineages, discuss how one can utilize this model system, offer a comprehensive list of known lineages and their respective markers, and then briefly review studies that have utilized Drosophila neural lineages with a look at how this model system can benefit future endeavors
Calibration and Physics with ARA Station 1: A Unique Askaryan Radio Array Detector
The Askaryan Radio Array Station 1 (A1), the first among five autonomous
stations deployed for the ARA experiment at the South Pole, is a unique
ultra-high energy neutrino (UHEN) detector based on the Askaryan effect that
uses Antarctic ice as the detector medium. Its 16 radio antennas (distributed
across 4 strings, each with 2 Vertically Polarized (VPol), 2 Horizontally
Polarized (HPol) receivers), and 2 strings of transmitting antennas
(calibration pulsers, CPs), each with 1 VPol and 1 HPol channel, are deployed
at depths less than 100 m within the shallow firn zone of the 2.8 km thick
South Pole (SP) ice. We apply different methods to calibrate its Ice Ray
Sampler second generation (IRS2) chip for timing offset and ADC-to-Voltage
conversion factors using a known continuous wave input signal to the digitizer,
and achieve a precision of sub-nanoseconds. We achieve better calibration for
odd, compared to even samples, and also find that the HPols under-perform
relative to the VPol channels. Our timing calibrated data is subsequently used
to calibrate the ADC-to-Voltage conversion as well as precise antenna
locations, as a precursor to vertex reconstruction. The calibrated data will
then be analyzed for UHEN signals in the final step of data compression. The
ability of A1 to scan the firn region of SP ice sheet will contribute greatly
towards a 5-station analysis and will inform the design of the planned IceCube
Gen-2 radio array.Comment: 10 page
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