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The objective of the study was to identify key elements of the feeding ecology of the dolphinfish, which is a high tropic predator important for sport and artisanal fishing in the Mexican Pacific. Feeding habits were investigated during the years 2000–2003. This species is seasonal in the southern Gulf of California and probably remains there because of the abundant prey. The contents of 232 dolphinfish stomachs were analyzed, identifying 98 prey species, although only eight of these were well‐represented in the diet. The most important prey by weight was the fish Hemiramphus saltator, however by number and frequency of occurrence was the crustacean Hemisquilla californiensis. No differences in the diet were found between males and females, although there was an ontogenic diet shift between seasons. There was no relationship between dolphinfish size and prey size, because dolphinfish fed preferentially on prey with an average size of 4.7 cm.  相似文献   
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Fundulus heteroclitus maintained under laboratory for more than four weeks showed a significantly lower immunocytoadherence (rosette) response to thymus-dependent antigens (SRBC and DNP-BSA) than newly captured fish. There was no comparable effect on scale allograft rejection nor in the response to a thymus-independent antigen (DNP-Ficoll) as measured by the rosette response. This suggests that captivity has a differential effect on a sub-population of lymphocytes analogous to the T-helper cells of mammals.  相似文献   
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Tripp  Nicole K.  Kabalan  Bana A.  Stoeckel  James  Reisinger  Lindsey S. 《Hydrobiologia》2022,849(16):3565-3579
Hydrobiologia - Species are often exposed to novel thermal regimes as a result of anthropogenic activities. Understanding the extent to which populations are locally adapted to the thermal regime...  相似文献   
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Series of aminopyridinecarboxamide-based inhibitors were synthesized and tested against human recombinant IKK-2 and in IL-1β stimulated synovial fibroblasts. The 2-amino-5-chloropyridine-4-carboxamides were identified as the most potent inhibitors with improved cellular activity.  相似文献   
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The study objective was to characterize the AGS human gastric mucosal cell line as a model for estimating gastrointestinal toxicity of COX-inhibiting compounds. Rofecoxib, celecoxib, nimesulide, ibuprofen, indomethacin, aspirin, salicylic acid, naproxen and acetaminophen were tested for inhibition of COX-2-mediated prostaglandin E2 synthesis in A549 and AGS cells. The IC50 ratio AGS/A549 was calculated as an estimate of the therapeutic index (TI) for gastrointestinal toxicity. Calculated IC50 values of non-steroidal anti-inflammatory drugs (NSAIDs) in A549 cells were in excellent agreement with published values (r = 0.996; P < 0.005). Calcium ionophore induction of arachidonic acid release in AGS cells provided TI similar to those using platelets and A549 cells (r = 0.918; P < 0.01). The AGS/A549 model exhibited lower TI than the platelet/A549 model. Spearman ranking correlated clinical NSAID gastropathy with lower AGS TI values. The AGS cell line has excellent potential to serve as a model for assessing the gastrointestinal effects of COX-inhibiting compounds.  相似文献   
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Human metapneumovirus (HMPV) is a recently discovered pathogen first identified in respiratory specimens from young children suffering from clinical respiratory syndromes ranging from mild to severe lower respiratory tract illness. HMPV has worldwide prevalence, and is a leading cause of respiratory tract infection in the first years of life, with a spectrum of disease similar to respiratory syncytial virus (RSV). The disease burden associated with HMPV infection has not been fully elucidated; however, studies indicate that HMPV may cause upper or lower respiratory tract illness in patients between ages 2 months and 87 years, may co-circulate with RSV, and HMPV infection may be associated with asthma exacerbation. The mechanisms and effector pathways contributing to immunity or disease pathogenesis following infection are not fully understood; however, given the clinical significance of HMPV, there is a need for a fundamental understanding of the immune and pathophysiological processes that occur following infection to provide the foundation necessary for the development of effective vaccine or therapeutic intervention strategies. This review provides a current perspective on the processes associated with HMPV infection, immunity, and disease pathogenesis.  相似文献   
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Human carbonic anhydrase II (CA II), a zinc metalloenzyme, was screened against 960 structurally diverse, biologically active small molecules. The assay monitored CA II esterase activity against the substrate 4-nitrophenyl acetate in a format allowing high-throughput screening. The assay proved to be robust and reproducible with a hit rate of approximately 2%. Potential hits were further characterized by determining their IC(50) and K(d) values and tested for nonspecific, promiscuous inhibition. Three known sulfonamide CA inhibitors were identified: acetazolamide, methazolamide, and celecoxib. Other hits were also found, including diuretics and antibiotics not previously identified as CA inhibitors, for example, furosemide and halazone. These results confirm that many sulfonamide drugs have CA inhibitory properties but also that not all sulfonamides are CA inhibitors. Thus many, but not all, sulfonamide drugs appear to interact with CA II and may target other CA isozymes. The screen also yielded several novel classes of nonsulfonamide inhibitors, including merbromin, thioxolone, and tannic acid. Although these compounds may function by some nonspecific mechanism (merbromin and tannic acid), at least 1 (thioxolone) appears to represent a genuine CA inhibitor. Thus, this study yielded a number of potentially new classes of CA inhibitors and preliminary experiments to characterize their mechanism of action.  相似文献   
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