Absence of effects of short-term fasting on plasma ghrelin and brain expression of ghrelin receptors in the tilapia, Oreochromis mossambicus

Ghrelin is an important endocrine peptide that links the gastrointestinal system and brain in the regulation of food intake and energy expenditure. In human, rat, and goldfish plasma levels of ghrelin and GH are elevated in fasted animals, suggesting that ghrelin is an orexigenic signal and a driving force behind the elevated plasma levels of GH during fasting. Ghrelin's orexigenic action is mediated by the ghrelin receptor (GHS-R1a and GHS-R1b) which is localized on neuropeptide Y (NPY) neurons in the brain. Studies were undertaken to investigate the effect of short-term fasting on plasma ghrelin and brain expression of GHS-R1a, GHS-R1b, and NPY in the tilapia. Fasting for 7 days had no effect on plasma ghrelin concentrations, whereas significant increases in plasma levels of GH were observed on day 3. Fasting significantly reduced plasma levels of IGF-I on days 3 and 7, and of glucose on days 3, 5, and 7. Brain expression of ghrelin and GHS-R1b were significantly elevated in fasted fish on day 3, but were significantly reduced on day 5. This reduction was likely due to a significant increase in the expression in the fed controls on day 5 compared to day 0. No change was detected in the expression of GHS-R1a or NPY in the brain. These results indicate that ghrelin is not acting as a hunger signal in short-term fasted tilapia and is not responsible for the elevated levels of plasma GH.     

Estimating the impact of interactions between bottlenose dolphins and artisanal fisheries around the Balearic Islands

Interactions between marine mammals and fisheries are a growing problem, and effective management requires assessment of the factors driving the interaction and of the impacts on fisheries. We used data from interactions between artisanal fisheries and bottlenose dolphins around the Balearic Islands to assess these factors and impacts. Observers collected data during 1,040 fishing operations over 3 yr. Location and year were important factors affecting interaction probability, with some areas showing large increases over the study period. We estimated the combined cost of catch loss and net damage as 6.5% of the total catch value (95% CI ?12.3%, ?1.6%), and the annual loss to be 3.4% (95% CI ?6.5%, ?0.1%) of the total catch by weight. This weight equates to the dietary needs of ～12 dolphins (95% CI 0.2, 22), suggesting the fishery is not a vital food source for the dolphin population. Two dolphins died through entanglement during the observed fishing operations. We observed 3% of the total fishing activity, by weight, in 2003; scaling up this mortality directly suggests that as many as sixty dolphins may be dying in nets each year. This interaction likely has serious conservation implications for the dolphin population.     

Lewis super-acid catalyzed cyclizations: a new route to fragrance compounds

This review deals with the application of Lewis super acids such as Al(III), In(III), and Sn(IV) triflates and triflimidates as catalysts in the synthesis of fragrance materials. Novel catalytic reactions involving C-C and C-heteroatom bond-forming reactions, as well as cycloisomerization processes are presented. In particular, Sn(IV) and Al(III) triflates were employed as catalysts in the selective cyclization of unsaturated alcohols to cyclic ethers, as well as in the cyclization of unsaturated carboxylic acids to lactones. The addition of thiols and thioacids to non-activated olefins, both in intra- and intermolecular versions, was efficiently catalyzed by In(III) derivatives. Sn(IV) Triflimidates catalyzed the cycloisomerization of highly substituted 1,6-dienes to gem-dimethyl-substituted cyclohexanes bearing an isopropylidene substituent. The hydroformylation of these unsaturated substrates, catalyzed by a Rh(I) complex with a bulky phosphite ligand, selectively afforded the corresponding linear aldehydes. The olfactory evaluation of selected heterocycles, carbocycles, and aldehydes synthesized is also discussed.     

Reproducibility of plantar pressure distribution data in barefoot running

The aim of this study was to provide detailed information on rationales, calculations, and results of common methods used to quantify reproducibility in plantar pressure variables. Recreational runners (N=95) performed multiple barefoot running trials in a laboratory setup, and pressure variables were analyzed in nine distinct subareas of the foot. Reproducibility was assessed by calculating intraclass correlation coefficients (ICC) and the root mean square error (RMSE). Intraclass correlation coefficients ranged from 0.58 to 0.99, depending on the respective variable and type of ICC. Root mean square errors ranged between 2.3 and 3.1% for relative force-time integrals, between 0.07 and 0.23 for maximum force (Fmax), and between 107 and 278 kPa for maximum pressure (Pmax), depending on the subarea of the foot. Force-time integral variables demonstrated the best within-subject reproducibility. Rear-foot data suffered from slightly increased measurement error and reduced reproducibility compared with the forefoot.     

Carbon Pools and Emissions from Deforestation in Extra-Tropical Forests of Northern Argentina Between 1900 and 2005

We estimated carbon pools and emissions from deforestation in northern Argentine forests between 1900 and 2005, based on forest inventories, deforestation estimates from satellite images and historical data on forests and agriculture. Carbon fluxes were calculated using a book-keeping model. We ran 1000 simulations for a 105-year period with different combinations of values of carbon stocks (Mg C ha⁻¹), soil carbon in the top 0.2 m, and annual deforestation series. The 1000 combinations of parameters were performed as a sensitivity analysis that for each run, randomly selected the values of each variable within a predefined range of values and probability distributions. Using the simulation outputs, we calculated the accumulated C emissions due to deforestation from 1900 to 2005 and the annual emission as the average of the 1000 simulations, and uncertainties of our estimates as the standard deviation. We found that northern Argentine forests contain an estimated 4.54 Pg C (2.312 Pg C in biomass and 2.233 Pg C in soil). Between 1900 and 2005 approximately 30% of the forests were deforested, yielding carbon emissions of 0.945 (SD = 0.270) Pg C. Estimated average annual carbon emissions between 1996 and 2005, mostly from deforestation of the Chaco dry forests, were 20,875 (SD = 6,156) Gg C y⁻¹ (1 Gg = 10⁻⁶ Pg). These values represent the largest source of carbon from land-cover change in the extra-tropical southern hemisphere, between 0.9 and 2.7% of the global carbon emissions from deforestation, and approximately 10% of carbon emissions from the Brazilian Amazon. Deforestation, which has accelerated during the last decades as a result of modern agriculture expansion, represents a major national source of greenhouse gases and the second emission source, after fossil fuel consumption by fixed sources. We conclude that Argentine forests are an important carbon pool and emission source that need more attention for accurate global estimates, and seasonally dry forest deforestation is a key component of the Argentine carbon cycle. Electronic supplementary material  The online version of this article (doi:) contains supplementary material, which is available to authorized users.     

Hexavalent chromium is cytotoxic and genotoxic to the North Atlantic right whale (Eubalaena glacialis) lung and testes fibroblasts

Although hexavalent chromium is a known genotoxic agent in human and terrestrial mammals and is present in seawater and air, its effects on marine mammals including the endangered North Atlantic right whale are unknown and untested. The present study investigated the cytotoxic and genotoxic effects of hexavalent chromium in primary cultured North Atlantic right whale lung and testes fibroblasts and levels of total chromium in skin biopsies from North Atlantic right whales. Cytotoxicity was measured by clonogenic survival assay. Genotoxicity was measured as production of chromosome aberrations. Tissue chromium levels were determined from skin biopsies of healthy free-ranging whales in the Bay of Fundy using inductively coupled plasma optical emission spectroscopy. Hexavalent chromium-induced concentration-dependent increases in right whale lung and testes fibroblast cytotoxicity with the testes more sensitive to the cytotoxic effects. It also induced concentration-dependent increases in chromosomal aberrations in both cell types with no significant difference in sensitivity. Skin biopsy data indicate that North Atlantic right whales are exposed to chromium and accumulate a range of 4.9-10 microg Cr/g tissue with a mean of 7.1 microg/g. Hexavalent chromium is cytotoxic and genotoxic to North Atlantic right whale cells. The whales have tissue chromium levels that are concerning. These data support a hypothesis that chromium may be a concern for the health of the North Atlantic right whales. Considering these data with chromium chemistry, whale physiology and atmospheric chromium levels further suggest that inhalation may be an important exposure route.     

Dissociation between mature phenotype and impaired transmigration in dendritic cells from heparanase-deficient mice

To reach the lymphatics, migrating dendritic cells (DCs) need to interact with the extracellular matrix (ECM). Heparanase, a mammalian endo-β-D-glucuronidase, specifically degrades heparan sulfate proteoglycans ubiquitously associated with the cell surface and ECM. The role of heparanase in the physiology of bone marrow-derived DCs was studied in mutant heparanase knock-out (Hpse-KO) mice. Immature DCs from Hpse-KO mice exhibited a more mature phenotype; however their transmigration was significantly delayed, but not completely abolished, most probably due to the observed upregulation of MMP-14 and CCR7. Despite their mature phenotype, uptake of beads was comparable and uptake of apoptotic cells was more efficient in DCs from Hpse-KO mice. Heparanase is an important enzyme for DC transmigration. Together with CCR7 and its ligands, and probably MMP-14, heparanase controls DC trafficking.     

Synthesis of alpha-fetoprotein (AFP) and cell proliferation in regenerating livers of NMRI mice after partial hepatectomy. An immunohistochemical and autoradiographic study with 3H-thymidine

To get more information concerning the relation between cell proliferation and the synthesis of alpha-fetoprotein (AFP), liver regeneration and AFP production was followed simultaneously in short intervals in NMRI mice after two-thirds hepatectomy using autoradiographic and immunohistochemical methods. The results indicate that AFP synthesis is not linked closely to cell proliferation in the sense that each proliferating hepatocyte synthesizes AFP during a definite phase of the cell cycle. However, AFP production, as measured by the index of anti-AFP positive hepatocytes, occurs in a very small population of parenchymal cells when the bulk of the hepatocytes has just passed the S-phase and is considered to be in the G2-, M or early G1-phase of the cell cycle when the cells are still in an undifferentiate state.     

The segment polarity gene costal-2 in Drosophila. I. The organization of both primary and secondary embryonic fields may be affected

A series of loss of function alleles at the costal-2 locus is described. Embryos mutant for lethal alleles that are derived from a mutant female germ line display polarity defects on the larval segments. A posterior part of the segmental denticle belt is missing and in its place is a mirror-image duplication of the anterior part including the segment boundary. Maternally rescued embryos are lethal but have normal morphology. Hypomorphic alleles escape to adults that display pattern duplications on the wings and halteres. Dominant gain of function alleles at the Costal-1 locus are also described and data are presented that argue that these are neomorphic and act in trans to impair functioning of costal-2. Some wild-type isoalleles of costal-2 are particularly sensitive to interference from Costal-1 mutations and different combinations of these alleles with Costal-1 can lead to embryos in which the primary embryonic field is disrupted (bicaudal phenotype) and adults with pattern duplications on the anterior compartment of most body segments.     

Identification of a cDNA Coding for a Ca-Binding Phosphoprotein (p90), Calnexin, on Melanosomes in Normal and Malignant Human Melanocytes

In order to have a proper biosynthesis and secretion of the melanin-pigment granules (melanosomes) the melanocyte may require a melanosome-associated molecule that provides a signal for assembly and organization of melanogenic enzymes and proteins within the compartment of melanosomes. This study reports the presence of a Ca²⁺-binding phosphoprotein, p90, which can be engaged in such melanogenic function, located on the melanosomal membrane of human melanocytes. A human melanoma cDNA expression library in λ Zap II was screened with a rabbit polyclonal antibody raised against human melanosomes isolated from cultured human melanoma cells, SK MEL 23. A cDNA encoding a melanosomal protein, M_r 90 kDa, was identified through this immunoscreening. A partial sequencing of nucleotides (822 bp from the N-terminal domain) of this clone (3.8 kb) and predicted amino acids showed more than 90% homology with dog calnexin, a previously reported endoplasmic reticulum (ER) transmembrane protein. A fusion protein of this p90 with β-galactosidase expressed in Escherichia coli revealed both the immuno-cross-reactivity with anti-dog calnexin and anti-human melanosome antibodies and the Ca²⁺-binding property. Upon immunohistochemistry, the anti-dog calnexin antibody revealed the positive immunoreactivities with both normal and malignant human melanocytes, showing a much higher expression of antigenic epitope than nonmelanocytic human cells. The laser scanning confocal immunofluorescence, using an anti-body against a human melanosome-specific antigen (HMSA-5), and immunoelectron microscopy, using immunogold, confirmed the major localization of anti-dog calnexin antibody epitope on the melanosomes and ER.