622 research outputs found
INFLUENCE OF DIFFERENT ASSEMBLIES ON PRE-HEATING THE HSLA SAR 80T STEEL ON COATED ELECTRODE WELDING
The present work evaluated the influence of assemblies other than preheating in the welding process obtained by coated electrode, using high strength and low alloy steel SAR 80T as the base metal and the AWS E7018 electrode as the addition metal. In order to prevent cracks, preheating and interpassing for low alloy steel was performed. Depending on the way the preheating equipment is installed, it may take more or less time to reach the preheat temperature. Different assembly arrangements for top joints were evaluated, aiming at cost reduction, in addition to evaluations of the mechanical properties of the joint. Visual testing, ultrasound, micrography, macrography and cross-sectional traction were performed. The results obtained were considered acceptable and showed that there was an influence on time, cost of preheating and resistance to impact
Assembly of a Three-Dimensional Multitype Bronchiole Coculture Model Using Magnetic Levitation
A longstanding goal in biomedical research has been to create organotypic cocultures that faithfully represent
native tissue environments. There is presently great interest in representative culture models of the lung, which
is a particularly challenging tissue to recreate in vitro. This study used magnetic levitation in conjunction with
magnetic nanoparticles as a means of creating an organized three-dimensional (3D) coculture of the bronchiole
that sequentially layers cells in a manner similar to native tissue architecture. The 3D coculture model was
assembled from four human cell types in the bronchiole: endothelial cells, smooth muscle cells (SMCs), fibroblasts,
and epithelial cells (EpiCs). This study represents the first effort to combine these particular cell types into
an organized bronchiole coculture. These cell layers were first cultured in 3D by magnetic levitation, and then
manipulated into contact with a custom-made magnetic pen, and again cultured for 48 h. Hematoxylin and eosin
staining of the resulting coculture showed four distinct layers within the 3D coculture. Immunohistochemistry
confirmed the phenotype of each of the four cell types and showed organized extracellular matrix formation,
particularly, with collagen type I. Positive stains for CD31, von Willebrand factor, smooth muscle a-actin,
vimentin, and fibronectin demonstrate the maintenance of the phenotype for endothelial cells, SMCs, and
fibroblasts. Positive stains for mucin-5AC, cytokeratin, and E-cadherin after 7 days with and without 1% fetal
bovine serum showed that EpiCs maintained the phenotype and function. This study validates magnetic levitation
as a method for the rapid creation of organized 3D cocultures that maintain the phenotype and induce
extracellular matrix formation
Free 2-propen-1-amine Derivative And Inclusion Complexes With β-cyclodextrin: Scanning Electron Microscopy, Dissolution, Cytotoxicity And Antimycobacterial Activity
Inclusion complexes and physical mixtures of isomeric mixture of E/Z (50:50) of 3-(4′-bromo-[1,1′-biphenyl]-4-yl)-3-(4-bromophenyl)-N,N- dimethyl-2-propen-1-amine (BBAP) and β-cyclodextrin (β-CD) in the molar proportion of 1:1 and 1:2 were analyzed by scanning electron microscopy. The dissolution behavior of BBAP and of the inclusion complexes were also evaluated for six hours. By scanning electron microscopy (SEM), it was possible to observe an inclusion complex formed between BBAP and β-CD by co-evaporation, either in the molar proportion of 1:1 or 1:2. In the physical mixtures, no complex was observed as previously detected by physicochemical analysis. The dissolution studies showed that the inclusion complexes BBAP/β-CD 1:1 and 1:2 released respectively 49.07 ± 1.48 and 40.26 ± 3.90% of BBAP during six hours. Free BBAP was less soluble than the inclusion complex and reached 9.00 ± 0.75% of dissolution. Biological assays, such as cytotoxicity to J774 macrophages and to a permanent lung fibroblast cell line (V79), indicated that the BBAP does not exhibit any additional toxic effect with the β-CD complexes. However, the complexes were less cytotoxic to V79 cells than the free form. The BBAP/β-CD inclusion complexes were more effective (MIC) than the free compound on several mycobacteria strains. Similar behavior was observed for BBAP/β-CD complexes and rifampicin, a front-line antitubercular drug, on M. tuberculosis H37Rv growing inside J774 macrophages.155682689Bibby, D.C., Davies, N.M., Tucker, I.G., (2000) Int. J. Pharm., 197, p. 1De Souza, A.O., Sato, D.N., Aily, D.C.G., Durán, N., (1998) J. Antimicrob. Chemother., 42, p. 407Pereira, D.G., De Castro, S.L., Durán, N., (1998) Acta Tropica, 69, p. 205De Souza, A.O., Santos Júnior, R.R., Ferreira-Júlio, J.F., Rodrigues, J.A., Melo, P.S., Haun, M., Sato, D.N., Durán, N., (2001) Eur. J. Med. Chem., 36, p. 843De Souza, A.O., Hemerly, F.P., Busollo, A.C., Melo, P.S., Machado, G.M.C., Miranda, C.C., Santa-Rita, R.M., Durán, N., (2002) J. Antimicrob. Chemother., 50, p. 629De Conti, R., Gimenez, S.M.N., Haun, M., Pilli, R.A., De Castro, S.L., Durán, N., (1996) Eur. J. Med. Chem., 31, p. 915De Souza, A.O., Santos Jr., R.R., Sato, D.N., Lima, H.O.S., Andrade-Santana, M.H., Alderete, J.B., Faljoni-Alario, A., Durán, N., (2000) Abstracts of the 29 a Reunião Anual Da Sociedade Brasileira de Bioquímica, , Caxambu, BrazilHiguchi, T., Connors, K.A., (1965) Adv. Anal. Chem. Instrum., 4, p. 117Collins, L.A., Franzblau, S.G., (1997) Antimicrob. Agents Chemother., 41, p. 1004Oh, Y.K., Nix, D.E., Straubinger, R.M., (1995) Antimicrob Agents Chemother., 39, p. 2104Cingi, M.R., De Angelis, I., Fortunati, E., Reggiani, D., Bianchi, V., Tiozzo, R., Zucco, F., (1991) Toxicol. In Vitro, 5, p. 119Denizot, F., Lang, R., (1986) J. Immun. Methods, 89, p. 271Borenfreund, E., Puerner, J.A., (1984) J. Tiss. Cult. Meth., 9, p. 7Melo, P.S., Maria, S.S., Vidal, B.C., Haun, M., Durán, N., (2000) In Vitro Cell Rev. Biol. Animal, 36, p. 539Melo, P.S., Durán, N., Haun, M., (2001) Toxicology, 159, p. 135Shrivastava, R., John, G.W., Rispat, G., Chevalier, A., Massingham, R., (1991) ATLA - Alt. Lab. Anim., 19, p. 39
Quasiparticle Interactions in Fractional Quantum Hall Systems: Justification of Different Hierarchy Schemes
The pseudopotentials describing the interactions of quasiparticles in
fractional quantum Hall (FQH) states are studied. Rules for the identification
of incompressible quantum fluid ground states are found, based upon the form of
the pseudopotentials. States belonging to the Jain sequence nu=n/(1+2pn), where
n and p are integers, appear to be the only incompressible states in the
thermodynamic limit, although other FQH hierarchy states occur for finite size
systems. This explains the success of the composite Fermion picture.Comment: RevTeX, 10 pages, 7 EPS figures, submitted fo Phys.Rev.
Some exact solutions of F(R) gravity with charged (a)dS black hole interpretation
In this paper we obtain topological static solutions of some kind of pure
gravity. The present solutions are two kind: first type is uncharged
solution which corresponds with the topological (a)dS Schwarzschild solution
and second type has electric charge and is equivalent to the
Einstein--conformally invariant Maxwell solution. In other word,
starting from pure gravity leads to (charged) Einstein- solutions
which we interpreted them as (charged) (a)dS black hole solutions of pure
gravity. Calculating the Ricci and Kreschmann scalars show that there is
a curvature singularity at . We should note that the Kreschmann scalar of
charged solutions goes to infinity as , but with a rate slower
than that of uncharged solutions.Comment: 21 pages, 4 figures, generalization to higher dimensions, references
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Pre-M Phase-promoting Factor Associates with Annulate Lamellae in Xenopus Oocytes and Egg Extracts
We have used complementary biochemical and in vivo approaches to study the compartmentalization of M phase-promoting factor (MPF) in prophase Xenopus eggs and oocytes. We first examined the distribution of MPF (Cdc2/CyclinB2) and membranous organelles in high-speed extracts of Xenopus eggs made during mitotic prophase. These extracts were found to lack mitochondria, Golgi membranes, and most endoplasmic reticulum (ER) but to contain the bulk of the pre-MPF pool. This pre-MPF could be pelleted by further centrifugation along with components necessary to activate it. On activation, Cdc2/CyclinB2 moved into the soluble fraction. Electron microscopy and Western blot analysis showed that the pre-MPF pellet contained a specific ER subdomain comprising "annulate lamellae" (AL): stacked ER membranes highly enriched in nuclear pores. Colocalization of pre-MPF with AL was demonstrated by anti-CyclinB2 immunofluorescence in prophase oocytes, in which AL are positioned close to the vegetal surface. Green fluorescent protein-CyclinB2 expressed in oocytes also localized at AL. These data suggest that inactive MPF associates with nuclear envelope components just before activation. This association may explain why nuclei and centrosomes stimulate MPF activation and provide a mechanism for targeting of MPF to some of its key substrates
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