99 research outputs found

    Introduction to Maxxam All-Season Passive Sampling System and Principles of Proper Use of Passive Samplers in the Field Study

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    Maxxam all-season passive sampling system (PASS) is introduced in this paper. The PASS can be used to quantitatively and accurately monitor SO2 , NO2, O 3, and H2 S in air in all weather conditions with flexible exposure times from several hours to several months. The air pollution detection limits of PASS are very low. They can be from sub ppb to ppt levels. The principles of proper use of passive samplers in the field study are discussed by using the PASS as an example

    Research on Urban Logistics Competitiveness in Fujian Province Based on Factor Analysis and Cluster Analysis

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    As an important province in the southeast coastal area, Fujian is composed of 9 cities. Due to various economic, political and geographical influences, the logistics development of these cities is uneven. Based on the analysis of the factors affecting the competitiveness of urban logistics, this paper establishes the evaluation index system of urban logistics competitiveness. Factor analysis is used to evaluate the logistics competitiveness index of each city in Fujian Province, and the comprehensive score and ranking of the logistics competitiveness of each city are obtained. Cluster analysis is used to divide 9 cities in Fujian into 4 categories, and the reasons for the results are analyzed

    Research on Urban Logistics Competitiveness in Fujian Province Based on Factor Analysis and Cluster Analysis

    Get PDF
    As an important province in the southeast coastal area, Fujian is composed of 9 cities. Due to various economic, political and geographical influences, the logistics development of these cities is uneven. Based on the analysis of the factors affecting the competitiveness of urban logistics, this paper establishes the evaluation index system of urban logistics competitiveness. Factor analysis is used to evaluate the logistics competitiveness index of each city in Fujian Province, and the comprehensive score and ranking of the logistics competitiveness of each city are obtained. Cluster analysis is used to divide 9 cities in Fujian into 4 categories, and the reasons for the results are analyzed. Document type: Articl

    Genomic and protein expression analysis reveals flap endonuclease 1 (FEN1) as a key biomarker in breast and ovarian cancer

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    FEN1 has key roles in Okazaki fragment maturation during replication, long patch base excision repair, rescue of stalled replication forks, maintenance of telomere stability and apoptosis. FEN1 may be dysregulated in breast and ovarian cancers and have clinicopathological significance in patients. We comprehensively investigated FEN1 mRNA expression in multiple cohorts of breast cancer [training set (128), test set (249), external validation (1952)]. FEN1 protein expression was evaluated in 568 oestrogen receptor (ER) negative breast cancers, 894 ER positive breast cancers and 156 ovarian epithelial cancers. FEN1 mRNA overexpression was highly significantly associated with high grade (p= 4.89 x 10 - 57) , high mitotic index (p= 5.25 x 10 - 28), pleomorphism (p= 6.31 x 10-19), ER negative (p= 9.02 x 10-35 ), PR negative (p= 9.24 x 10-24 ), triple negative phenotype (p= 6.67 x 10-21) , PAM50.Her2 (p=5.19 x 10-13 ), PAM50.Basal (p=2.7 x 10-41), PAM50.LumB (p=1.56 x 10-26), integrative molecular cluster 1 (intClust.1) ( p=7.47 x 10-12), intClust.5 (p=4.05 x 10-12) and intClust. 10 (p=7.59 x 10-38 ) breast cancers. FEN1 mRNA overexpression is associated with poor breast cancer specific survival in univariate (p=4.4 x 10-16) and multivariate analysis (p=9.19 x 10-7). At the protein level, in ER positive tumours , FEN1 overexpression remains significantly linked to high grade, high mitotic index and pleomorphism (ps< 0.01). In ER negative tumours, high FEN1 is significantly associated with pleomorphism, tumour type, lymphovascular invasion, triple negative phenotype, EGFR and HER2 expression (ps<0.05). In ER positive as well as in ER negative tumours, FEN1 protein over expression is associated with poor survival in univariate and multivariate analysis (ps<0.01). In ovarian epithelial cancers , similarly, FEN1 overexpression is associated with high grade, high stage and poor survival (ps<0.05). We conclude that FEN1 is a promising biomarker in breast and ovarian epithelial cancer

    Quantitative high-throughput phenotypic screening of pediatric cancer cell lines identifies multiple opportunities for drug repurposing

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    Drug repurposing approaches have the potential advantage of facilitating rapid and cost-effective development of new therapies. Particularly, the repurposing of drugs with known safety profiles in children could bypass or streamline toxicity studies. We employed a phenotypic screening paradigm on a panel of well-characterized cell lines derived from pediatric solid tumors against a collection of ∼3,800 compounds spanning approved drugs and investigational agents. Specifically, we employed titration-based screening where compounds were tested at multiple concentrations for their effect on cell viability. Molecular and cellular target enrichment analysis indicated that numerous agents across different therapeutic categories and modes of action had an antiproliferative effect, notably antiparasitic/protozoal drugs with non-classic antineoplastic activity. Focusing on active compounds with dosing and safety information in children according to the Children's Pharmacy Collaborative database, we identified compounds with therapeutic potential through further validation using 3D tumor spheroid models. Moreover, we show that antiparasitic agents induce cell death via apoptosis induction. This study demonstrates that our screening platform enables the identification of chemical agents with cytotoxic activity in pediatric cancer cell lines of which many have known safety/toxicity profiles in children. These agents constitute attractive candidates for efficacy studies in pre-clinical models of pediatric solid tumors

    Correlation between acoustic velocity and physical parameters of sea floor sediments: a case study of the northern South China Sea

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    As the interface between seawater and the seabed, superficial sediments on the seabed are an important part of the marine acoustic field environment and are indispensable for marine resource investigations. Studying sediments several meters to hundreds of meters below the seafloor is highly valuable and important. This study processes and analyses the water depth, topography and bottom data and obtains the shallow bottom profile and topographic map of the northern continental slope of the South China Sea (SCS). The study analyzes the influence of physical parameter (including density, porosity, and grain size) on the acoustic velocity in sediments. Single-parameter and dual-parameter models are established to further examine this influence. The results show that porosity and density have greater influences on the acoustic velocity of sediments than does grain size. Finally, the acoustic properties of several typical stations with water depths are tested to analyze the variations in the acoustic properties of the shallow sediments in the northern SCS. The results show that the influence of each parameter on the prediction of the acoustic velocity of the sediment is in the following order: porosity&gt;density&gt;grain size. This study analyses and reveals the reason why the seafloor sediments in the local area cause the acoustic properties to change greatly. It may be caused by changes in the sediment type, lithology along with the depth. And the other reason is the development of interlayer in the land slope of the northern SCS

    Disrupting malaria parasite AMA1-RON2 interaction with a small molecule prevents erythrocyte invasion

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    Plasmodium falciparumresistance to artemisinin derivatives, the first-line anti-malarial drug, drives the search for new classes of chemotherapeutic agents. Current discovery is primarily directed against the intracellular forms of the parasite. However, late schizont-infected red blood cells (RBCs) may still rupture and cause disease by sequestration; consequently targeting invasion may reduce disease severity. Merozoite invasion of RBCs requires interaction between two parasite proteins AMA1 and RON2. Here we identify the first inhibitor of this interaction that also blocks merozoite invasion in genetically distinct parasites by screening a library of over 21,000 compounds. We demonstrate that this inhibition is mediated by the small molecule binding to AMA1 and blocking the formation of AMA1-RON complex. Electron microscopy confirms that the inhibitor prevents junction formation, a critical step in invasion that results from AMA1-RON2 binding. This study uncovers a strategy that will allow for highly effective combination therapies alongside existing anti-malarial drugs

    Human GPR17 missense variants identified in metabolic disease patients have distinct downstream signaling profiles

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    GPR17 is a G-protein-coupled receptor (GPCR) implicated in the regulation of glucose metabolism and energy homeostasis. Such evidence is primarily drawn from mouse knockout studies and suggests GPR17 as a potential novel therapeutic target for the treatment of metabolic diseases. However, links between human GPR17 genetic variants, downstream cellular signaling, and metabolic diseases have yet to be reported. Here, we analyzed GPR17 coding sequences from control and disease cohorts consisting of individuals with adverse clinical metabolic deficits including severe insulin resistance, hypercholesterolemia, and obesity. We identified 18 nonsynonymous GPR17 variants, including eight variants that were exclusive to the disease cohort. We characterized the protein expression levels, membrane localization, and downstream signaling profiles of nine GPR17 variants (F43L, V96M, V103M, D105N, A131T, G136S, R248Q, R301H, and G354V). These nine GPR17 variants had similar protein expression and subcellular localization as wild-type GPR17; however, they showed diverse downstream signaling profiles. GPR17-G136S lost the capacity for agonist-mediated cAMP, Ca2+, and β-arrestin signaling. GPR17-V96M retained cAMP inhibition similar to GPR17-WT, but showed impaired Ca2+ and β-arrestin signaling. GPR17-D105N displayed impaired cAMP and Ca2+ signaling, but unaffected agonist-stimulated β-arrestin recruitment. The identification and functional profiling of naturally occurring human GPR17 variants from individuals with metabolic diseases revealed receptor variants with diverse signaling profiles, including differential signaling perturbations that resulted in GPCR signaling bias. Our findings provide a framework for structure-function relationship studies of GPR17 signaling and metabolic disease

    Identification of floR Variants Associated With a Novel Tn4371-Like Integrative and Conjugative Element in Clinical Pseudomonas aeruginosa Isolates

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    Florfenicol is widely used to control respiratory diseases and intestinal infections in food animals. However, there are increasing reports about florfenicol resistance of various clinical pathogens. floR is a key resistance gene that mediates resistance to florfenicol and could spread among different bacteria. Here, we investigated the prevalence of floR in 430 Pseudomonas aeruginosa isolates from human clinical samples and identified three types of floR genes (designated floR, floR-T1 and floR-T2) in these isolates, with floR-T1 the most prevalent (5.3%, 23/430). FloR-T2 was a novel floR variant identified in this study, and exhibited less identity with other FloR proteins than FloRv. Moreover, floR-T1 and floR-T2 identified in P. aeruginosa strain TL1285 were functionally active and located on multi-drug resistance region of a novel incomplete Tn4371-like integrative and conjugative elements (ICE) in the chromosome. The expression of the two floR variants could be induced by florfenicol or chloramphenicol. These results indicated that the two floR variants played an essential role in the host’s resistance to amphenicol and the spreading of these floR variants might be related with the Tn4371 family ICE
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