Littérature scientifique sur le sujet « L18A »
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Articles de revues sur le sujet "L18A"
Aoyama, Yuji, Yuen-Ling Chan, Oded Meyuhas et Ira G. Wool. « The primary structure of rat ribosomal protein L18a ». FEBS Letters 247, no 2 (24 avril 1989) : 242–46. http://dx.doi.org/10.1016/0014-5793(89)81344-4.
Texte intégralHan, Sun‐Young, et Mieyoung Choi. « Human ribosomal protein L18a interacts with hnRNP E1 ». Animal Cells and Systems 12, no 3 (janvier 2008) : 143–48. http://dx.doi.org/10.1080/19768354.2008.9647167.
Texte intégralSommer, W., C. Arlinde, L. Caberlotto, A. Thorsell, P. Hyytia et M. Heilig. « CNS expression of diacylglycerol kinase iota and L18A mRNAs ». Molecular Psychiatry 6, no 1 (14 décembre 2000) : 5. http://dx.doi.org/10.1038/sj.mp.4000831.
Texte intégralDhar, D., K. Mapa, R. Pudi, P. Srinivasan, K. Bodhinathan et S. Das. « Human ribosomal protein L18a interacts with hepatitis C virus internal ribosome entry site ». Archives of Virology 151, no 3 (30 septembre 2005) : 509–24. http://dx.doi.org/10.1007/s00705-005-0642-6.
Texte intégralNtwasa, Monde, Sean G. S. C. Buchanan et Nicholas J. Gay. « Drosophila ribosomal protein L18a : cDNA sequence, expression and chromosomal localization of the gene ». Biochimica et Biophysica Acta (BBA) - Gene Structure and Expression 1218, no 2 (juin 1994) : 210–12. http://dx.doi.org/10.1016/0167-4781(94)90014-0.
Texte intégralYant, Stephen R., Julie Park, Yong Huang, Jacob Giehm Mikkelsen et Mark A. Kay. « Mutational Analysis of the N-Terminal DNA-Binding Domain of Sleeping Beauty Transposase : Critical Residues for DNA Binding and Hyperactivity in Mammalian Cells ». Molecular and Cellular Biology 24, no 20 (15 octobre 2004) : 9239–47. http://dx.doi.org/10.1128/mcb.24.20.9239-9247.2004.
Texte intégralGazda, Hanna T., Mee Rie Sheen, Natasha Darras, Hal Shneider, Colin A. Sieff, Sarah E. Ball, Edyta Niewiadomska et al. « Mutations of the Genes for Ribosomal Proteins L5 and L11 Are a Common Cause of Diamond-Blackfan Anemia. » Blood 110, no 11 (16 novembre 2007) : 421. http://dx.doi.org/10.1182/blood.v110.11.421.421.
Texte intégralZhang, Yihao, Yuying Jin, Qian Gong, Zhi Li, Lihong Zhao, Xiao Han, Jinglong Zhou, Fuguang Li et Zhaoen Yang. « Mechanismal analysis of resistance to Verticillium dahliae in upland cotton conferred by overexpression of RPL18A-6 (Ribosomal Protein L18A-6) ». Industrial Crops and Products 141 (décembre 2019) : 111742. http://dx.doi.org/10.1016/j.indcrop.2019.111742.
Texte intégralSommer, W., C. Arlinde, L. Caberlotto, A. Thorsell, P. Hyytia et M. Heilig. « Differential expression of diacylglycerol kinase iota and L18A mRNAs in the brains of alcohol-preferring AA and alcohol-avoiding ANA rats ». Molecular Psychiatry 6, no 1 (14 décembre 2000) : 103–8. http://dx.doi.org/10.1038/sj.mp.4000823.
Texte intégralMottaghi-Dastjerdi, N., M. Soltany-Rezaee-Rad, Z. Sepehrizadeh, G. Roshandel, F. Ebrahimifard et N. Setayesh. « Identification of novel genes involved in gastric carcinogenesis by suppression subtractive hybridization ». Human & ; Experimental Toxicology 34, no 1 (8 mai 2014) : 3–11. http://dx.doi.org/10.1177/0960327114532386.
Texte intégralThèses sur le sujet "L18A"
Das, Priyanka. « Study of the L13a residues required for ribosomal function ». Cleveland State University / OhioLINK, 2012. http://rave.ohiolink.edu/etdc/view?acc_num=csu1331762160.
Texte intégralPoddar, Darshana Ph D. « Study of Role of Ribosomal Protein L13a in Resolving Inflammation ». Cleveland State University / OhioLINK, 2014. http://rave.ohiolink.edu/etdc/view?acc_num=csu1400587453.
Texte intégralKour, Ravinder. « Insights into the ribosomal, extra-ribosomal and developmental role of RP L13a in mammalian model ». Cleveland State University / OhioLINK, 2019. http://rave.ohiolink.edu/etdc/view?acc_num=csu1572548728931568.
Texte intégralVon, Hagen William J. « Analysis of the L1A, L1M, L2A, and L2F Low-Pressure Turbine Blades Using Large-Eddy Simulation ». University of Cincinnati / OhioLINK, 2016. http://rave.ohiolink.edu/etdc/view?acc_num=ucin1470045392.
Texte intégralViegas, Taisa Giordano [UNESP]. « Interação do peptídeo antimicrobiano L1A com membrana modelo : efeito do pH e carga da vesícula ». Universidade Estadual Paulista (UNESP), 2014. http://hdl.handle.net/11449/127655.
Texte intégralCoordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)
Peptdeos antimicrobianos possuem em geral cadeias curtas, carga líquida positiva devido ao excesso dos res duos b asicos e são ricos em amino acidos hidrof obicos. Possuem um grande potencial farmacológico, com atividade antimicrobiana modulada por interações eletrost aticas e hidrof obicas. Neste trabalho utilizou-se o pept deo sintético L1A (IDGLKAIWKKV ADLLKNT NH2), que devido aos res duos de acido asp artico e lisinas constituintes de sua cadeia, possui carga liquida +3, em pH neutro. Foram analisadas as insuficiências do pH e da carga de ves culas aniônicas na adsorçãao do pept deo. Este estudo utilizou medidas de potencial eletrocin etico de ves culas e experimentos de titulação monitorados por dicro smo circular (CD). A adsorção do L1A a LUVs de POPC e misturas POPC/POPG em diferentes proporções de POPG, foi medida nos pHs 4, 7 e 10. Os espectros de dicro smo circular dos peptídeos, na presença de vesícula, apresentaram caracter sticas de estruturas helicoidais, enquanto apresentaram estruturas desordenadas em tampão. As frações de hélices obtidas são maiores quando o pept deo adsorve em ves culas com maiores quantidades de POPG, indicando forte contribuição eletrost atica. As constantes aparentes de adsorção dos pept deos as membranas modelo foram calculadas atrav es da elipticidade de CD normalizada em 222 nm, obtidas por titulações de pept deo com ves culas. A a - nidade do pept deo a ves culas aniônicas e signi cativamente maior do que a ves culas zwitteriônicas, o que refor ca a import ancia das interçõeoes eletrost aticas no processo de adsorção do pept deo na bicamada. O efeito conjunto de carga das ves culas e de pH resultaram em signi cativa regulação de carga do pept deo resultando em valores de carga efetiva alta em pH 4,0 devido a protonação dos res duos de asp artico. Em pH 10,0 a pequena carga efetiva calculada deve-se as desprotona ações do N-terminal e das lisinas...
Antimicrobial peptides have in general short chains, positive net charge due to the excess of basic residues and are rich in hydrophobic amino acids. They have pharmacological potential as antimicrobial agents and their activity is modulated by electrostatic and hydrophobic interactions. In this work, we used the synthetic peptide L1A (IDGLKAIWKKV ADLLKNT NH2) that due to its acid and basic residues have an net charge +3, at neutral pH. The e ects of the pH and of the charges of anionic vesicles on the adsorption of L1A were analized. This study used measurement of electrokinetic potential of vesicles and titration experiments monitored by circular dichroism spectroscopy (CD). Adsorption of L1A to POPC and POPC/POPG LUVs in di erent POPG contents were assessed in the pH 4.0, 7.0 and 10.0. Circular dichroism spectra of the peptides in the presence of vesicles showed to features of helical structures; while random coil structures were observed at bu er for all the used pHs. The helical content was evaluated and showed to increase when the peptide adsorbs into vesicles with increasing amounts of POPG, indicating that there is a strong electrostatic contribution. Partition coe cients were calculated through the normalized CD ellipticities at 222 nm and showed that the a nity of the peptide for anionic model membranes is e ectively higher than those found for zwitterionic ones. It reinforces the importance of the electrostatic contribution to the process of peptide-lipid interaction. The coupled e ect of the vesicle charge and pH lead to signi cant charge regulation of the peptide resulting in high values of e ective charge at pH 4.0 due to the deprotonation of aspartic acid residues. At pH 10.0 the estimated e ective charge is small as a consequence of the deprotonation of both N-terminus and the lysines. The electrostatic and interfatial free energies seems to be additive only at pH 4.0, especially for the bilayers with higher content...
Viegas, Taisa Giordano. « Interação do peptídeo antimicrobiano L1A com membrana modelo : efeito do pH e carga da vesícula / ». São José do Rio Preto, 2014. http://hdl.handle.net/11449/127655.
Texte intégralBanca: Alexandre Suman de Araujo
Banca: Fernando Luis Barroso da Silva
Resumo: Peptdeos antimicrobianos possuem em geral cadeias curtas, carga líquida positiva devido ao excesso dos res duos b asicos e são ricos em amino acidos hidrof obicos. Possuem um grande potencial farmacológico, com atividade antimicrobiana modulada por interações eletrost aticas e hidrof obicas. Neste trabalho utilizou-se o pept deo sintético L1A (IDGLKAIWKKV ADLLKNT ���� NH2), que devido aos res duos de acido asp artico e lisinas constituintes de sua cadeia, possui carga liquida +3, em pH neutro. Foram analisadas as insuficiências do pH e da carga de ves culas aniônicas na adsorçãao do pept deo. Este estudo utilizou medidas de potencial eletrocin etico de ves culas e experimentos de titulação monitorados por dicro smo circular (CD). A adsorção do L1A a LUVs de POPC e misturas POPC/POPG em diferentes proporções de POPG, foi medida nos pHs 4, 7 e 10. Os espectros de dicro smo circular dos peptídeos, na presença de vesícula, apresentaram caracter sticas de estruturas helicoidais, enquanto apresentaram estruturas desordenadas em tampão. As frações de hélices obtidas são maiores quando o pept deo adsorve em ves culas com maiores quantidades de POPG, indicando forte contribuição eletrost atica. As constantes aparentes de adsorção dos pept deos as membranas modelo foram calculadas atrav es da elipticidade de CD normalizada em 222 nm, obtidas por titulações de pept deo com ves culas. A a - nidade do pept deo a ves culas aniônicas e signi cativamente maior do que a ves culas zwitteriônicas, o que refor ca a import^ancia das interçõeoes eletrost aticas no processo de adsorção do pept deo na bicamada. O efeito conjunto de carga das ves culas e de pH resultaram em signi cativa regulação de carga do pept deo resultando em valores de carga efetiva alta em pH 4,0 devido a protonação dos res duos de asp artico. Em pH 10,0 a pequena carga efetiva calculada deve-se as desprotona ações do N-terminal e das lisinas...
Abstract: Antimicrobial peptides have in general short chains, positive net charge due to the excess of basic residues and are rich in hydrophobic amino acids. They have pharmacological potential as antimicrobial agents and their activity is modulated by electrostatic and hydrophobic interactions. In this work, we used the synthetic peptide L1A (IDGLKAIWKKV ADLLKNT ���� NH2) that due to its acid and basic residues have an net charge +3, at neutral pH. The e ects of the pH and of the charges of anionic vesicles on the adsorption of L1A were analized. This study used measurement of electrokinetic potential of vesicles and titration experiments monitored by circular dichroism spectroscopy (CD). Adsorption of L1A to POPC and POPC/POPG LUVs in di erent POPG contents were assessed in the pH 4.0, 7.0 and 10.0. Circular dichroism spectra of the peptides in the presence of vesicles showed to features of helical structures; while random coil structures were observed at bu er for all the used pHs. The helical content was evaluated and showed to increase when the peptide adsorbs into vesicles with increasing amounts of POPG, indicating that there is a strong electrostatic contribution. Partition coe cients were calculated through the normalized CD ellipticities at 222 nm and showed that the a nity of the peptide for anionic model membranes is e ectively higher than those found for zwitterionic ones. It reinforces the importance of the electrostatic contribution to the process of peptide-lipid interaction. The coupled e ect of the vesicle charge and pH lead to signi cant charge regulation of the peptide resulting in high values of e ective charge at pH 4.0 due to the deprotonation of aspartic acid residues. At pH 10.0 the estimated e ective charge is small as a consequence of the deprotonation of both N-terminus and the lysines. The electrostatic and interfatial free energies seems to be additive only at pH 4.0, especially for the bilayers with higher content...
Mestre
Kapasi, Purvi. « An Insight into GAIT Complex Mediated Translational Silencing ». Cleveland State University / OhioLINK, 2008. http://rave.ohiolink.edu/etdc/view?acc_num=csu1232567504.
Texte intégralRocha, Carolina da Silva. « Identificação de componentes da via de sinalização mediada pela proteína NIK, um receptor que interage com a proteína NSP de geminivírus ». Universidade Federal de Viçosa, 2007. http://locus.ufv.br/handle/123456789/4824.
Texte intégralCoordenação de Aperfeiçoamento de Pessoal de Nível Superior
Proteins of the family of LRR-RLKs (receptor-like-kinases with leucine-rich repeats) have a conceptual relevance in signaling events but in plants information regarding function is limited to a few members of this family. The receptors NIK1, NIK2 and NIK3 of Arabidopsis thaliana belong to the sub-family LRRII-RLK and were initially identified by their capacity to interact with the geminivirus NSP protein. In response to an unknown stimulus, NSP-interacting kinases (NIKs) are activated after the formation of dimmers and intermolecular autophosphorylation. The inhibition of autophosphorylation of NIK by NSP and the activation of NIK genes increase the susceptibility to viral infection, suggesting that this protein is involved in a defense pathway against geminivirus infection. The downstream components of this pathway, mediated by the protein NIK, have yet to be identified. In the present study, the biochemical and functional characterization of two ribosomal proteins, L10 and L18 were described, these being capable of interacting with the protein NIK via the yeast two-hybrid system. In vitro studies demonstrated that the protein NIK is capable of phosphorylating the protein L10, but not L18. Of the members of the LRRIIRLK family, the protein NIK2 phosphorylates L10, while NIK3 presents a low capacity for phosphorylation of the substrate. However, the development protein SERK1 does not use L10 as a substrate. Assays of transient expression in tobacco plants, revealed that the L18 protein is located in the cytoplasm, as well as around the nucleus and the nucleoli of some cells. In turn, in 97% of the cells, L10 was localized only in the cytoplasm, although it was also found in the nucleus, in approximately 3% of the observed cells. The transient expression of NIK1 and NIK2 redirects the L10 protein to the nucleus in approximately 30% of the cells. In contrast, NIK3 does not relocalize the L10 protein to the nucleus, and L18 does not change its localization in the presence of the NIKs. In plants infected with TGMV, a change only in the cytoplasmic localization of L10 was observed, accumulating in points of the cytoplasm when not co-localized with NIK. To prove genetically the interactions of L10-NIK and L18-NIK, null alleles for the genes L10 and L18 de Arabidopsis, containing T-DNA insertion, were obtained and inoculated with CaLCuV. The inactivation of the genes L10 and L18 restored the elevated susceptibility phenotype of nik1 and the knockout plants, principally l10, presented severe symptoms and high rates of infection when compared with the wild columbia plants. The results of this work are consistent with a model that places the ribosomal proteins L10 and L18 as functional components of the defense signaling pathway mediated by the protein NIK, L10 being a component immediately downstream of the transmembrane receptor.
As proteínas da família das LRR-RLKs (receptor-like-quinases com repetições ricas em leucina) possuem uma relevância conceitual em eventos de sinalização mas, em plantas, a informação funcional ainda é restrita a alguns membros desta família. Os receptores NIK1, NIK2 e NIK3 de Arabidopsis thaliana pertecem à sub-familia LRRII-RLK e foram inicialmente identificados pela sua capacidade de interagir com a proteína NSP de geminivírus. Em resposta a um estímulo desconhecido, NSP-interacting kinases (NIKs) são ativadas após a formação de dímeros e autofosforilação intermolecular. A inibição da autofosforilação de NIK por NSP e a inativação de genes NIKs aumenta a suscetibilidade à infecção viral, sugerindo que esta proteína estaria envolvida em uma via de defesa contra a infecção por geminivírus. Os componentes downstream dessa via de sinalização, mediada pela proteína NIK, ainda não foram identificados. No presente estudo foi descrita a caracterização bioquímica e funcional de duas proteínas ribossomais, L10 e L18, as quais foram capazes de interagir com a proteína NIK através do sistema de duplo híbrido de leveduras. Estudos in vitro demonstraram que a proteína NIK é capaz de fosforilar a proteína L10, mas não L18. Entre os membros da família LRRII-RLK, a proteína NIK2 fosforila L10, enquanto NIK3 apresenta uma baixa capacidade de fosforilação do substrato. No entanto, a proteína de desenvolvimento SERK1 não utiliza L10 como substrato. Ensaios de expressão transiente, em plantas de tabaco, revelaram que a proteína L18 está localizada no citoplasma, bem como ao redor do núcleo e no nucléolo de algumas células. Por sua vez, em 97% das células, L10 foi localizada apenas no citoplasma, embora tenha sido encontrada no núcleo, em aproximadamente 3% das células observadas. A expressão transiente de NIK1 e NIK2 redireciona a proteína L10 para o núcleo em aproximadamente 30% das células. Em contraste, NIK3 não relocaliza a proteína L10 para o núcleo, e L18 não muda sua localização na presença das NIKs. Em plantas infectadas com TGMV, observou-se mudança apenas na localização citoplasmática de L10, acumulando-se em pontos do citoplasma quando não colocalizada com NIK. Para se comprovar geneticamente as interações de L10-NIK e L18- NIK, alelos nulos para os genes L10 e L18 de Arabidopsis, contendo inserção de T-DNA, foram obtidos e inoculados com o CaLCuV. A inativação dos genes L10 e L18 recapitulou o fenótipo de suscetibilidade aumentada de nik1 e as plantas knockout, principalmente l10, apresentaram sintomas severos e taxa de infecção alta quanto comparados com as plantas selvagens columbia. Os resultados deste trabalho são consistentes com um modelo que posiciona as proteínas ribossomais L10 e L18 como componentes funcionais da via de sinalização de defesa mediada pela proteína NIK, sendo L10 um componente imediatamente downstream ao receptor transmembrana.
Lefèvre, Charlène. « Coreshine, un phénomène et un outil ». Thesis, Paris 6, 2015. http://www.theses.fr/2015PA066460/document.
Texte intégralEven though dust grains contribute only to 1% of the interstellar medium mass, their study is crucial to understand both the structure and content of interstellar clouds. Dust grains leave their birth places, spread out into the diffuse medium before being gathered together again when dense molecular clouds form. During this last stage, they grow, by coagulation especially, and they acquire ice mantles composed mainly of water. These morphological changes also modify their optical properties (absorption, scattering, and emission). However, it remains a highly degenerate issue to determine their composition, size, and shape from observations. In particular, I will highlight that using wavelengths associated to dust emission is not sufficient to investigate the dense cores, where stars and planets will form. I will show that scattering can dominate the absorption at 3.6 and 4.5 μm, and that this phenomenon called coreshine is a powerful tool to investigate the densest parts of molecular clouds. The coreshine detection in more than one hundred clouds of our Galaxy allows us to eliminate a large number of dust models. Multi–wavelength 3D modeling is mandatory to characterize the balance between the absorption and the scattering of the radiation field. While most of the work about dust focus on absorption and re–emission of the radiation, I will present how scattering, often neglected, brings a complete picture of the radiative transfer inside dense clouds
Vinci, Samuel J. « CFD SIMULATIONS FOR THE EFFECT OF UNSTEADY WAKES ON THE BOUNDARY LAYER OF A HIGHLY LOADED LOW PRESSURE TURBINE AIRFOIL (L1A) ». Cleveland State University / OhioLINK, 2011. http://rave.ohiolink.edu/etdc/view?acc_num=csu1307111386.
Texte intégralLivres sur le sujet "L18A"
The Building Regulations 2000 : Conservation of fuel and power in new dwellings : approved document L1A. [Norwich] : TSO, 2010.
Trouver le texte intégralA, Freeman Kerry, Rivele Richard J et Chilton Book Company, dir. Chilton's repair & tune-up guide, Datsun Nissan pick-ups, 1970-84 : All U.S. and Canadian models of L16, L18, L20B, Z20, Z22, Z24 gasoline engines, SD22, SD25 diesel engines, including 4-wheel drive. Radnor, Pa : Chilton Book Co., 1985.
Trouver le texte intégralCommunities and Local Government Staff. Approved Document L1A : Conservation of Fuel and Power. Taylor & Francis Group, 2010.
Trouver le texte intégralHidalgo, Álvaro. El valor del medicamento desde una perspectiva social. Actualización 2020. Fundación Weber, 2021. http://dx.doi.org/10.37666/l18-2020.
Texte intégralAt Your Request : Grades K-3 (Accelerated Reader Book Set L18). Renaissance Learning Inc, 2002.
Trouver le texte intégralCorporation, Intertec Publishing. Kubota Shop Manual Models L185, L235, L245, L275, L285, L295, L305,Ll345, L355 (K-3). Primedia Business Directories & Books, 1987.
Trouver le texte intégralBuilding Regulations Approved Document L1a : Conservation of Fuel And Power-new Dwellings. Stationery Office, 2006.
Trouver le texte intégralCournane, Ailís. In defence of the child innovator. Oxford University Press, 2017. http://dx.doi.org/10.1093/oso/9780198747840.003.0002.
Texte intégralDomestic heating compliance guide : Compliance with approved documents L1A : New dwellings and L1B : Existing dwellings : the Building Regulations 2000 as amended 2006. London : TSO, 2006.
Trouver le texte intégralGreat Britain : Department for Communities and Local Government. Building Act 1984 : The Building Regulations and the Building Regulations 2000, Building Regulations 2000, schedule 1, part L, approved documents L1A, L1B, L2A, L2B, multi-foil Insulation. Stationery Office, The, 2009.
Trouver le texte intégralChapitres de livres sur le sujet "L18A"
Bühlmann, Albert A., Ernst B. Völlm et Peter Nussberger. « Das Rechenmodell ZH-L16A ». Dans Tauchmedizin, 127–32. Berlin, Heidelberg : Springer Berlin Heidelberg, 2002. http://dx.doi.org/10.1007/978-3-642-55939-6_7.
Texte intégralBühlmann, Albert A. « Das Rechenmodell ZH-L16A ». Dans Tauchmedizin, 85–88. Berlin, Heidelberg : Springer Berlin Heidelberg, 1993. http://dx.doi.org/10.1007/978-3-642-97413-7_7.
Texte intégralBühlmann, Albert A. « Das Rechenmodell ZH-L16A ». Dans Tauchmedizin, 85–87. Berlin, Heidelberg : Springer Berlin Heidelberg, 1995. http://dx.doi.org/10.1007/978-3-642-97623-0_7.
Texte intégralBühlmann, Albert A. « Das Rechenmodell ZH-L16A ». Dans Tauchmedizin, 84–87. Berlin, Heidelberg : Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-97256-0_7.
Texte intégralPagani, L., A. J. Apponi, A. Bacmann, L. Cambrésy, M. Fich, G. Lagache, M. A. Miville-Deschênes, F. Motte et J. R. Pardo. « L183 (134N) Dust, Gas and Depletion ». Dans Springer Proceedings in Physics, 439–42. Berlin, Heidelberg : Springer Berlin Heidelberg, 1997. http://dx.doi.org/10.1007/978-3-642-18902-9_78.
Texte intégralChristiansen, J., et R. A. Garrett. « How Do Protein L18 and 5S RNA Interact ? » Dans Springer Series in Molecular Biology, 253–69. New York, NY : Springer New York, 1986. http://dx.doi.org/10.1007/978-1-4612-4884-2_15.
Texte intégralNabedryk, E., J. Breton, J. Wachtveitl, K. A. Gray et D. Oesterhelt. « FTIR Spectroscopy of The P+Q A - /PQA State in Met L248→Thr, Ser L244→Gly, Phe M197→Tyr, Tyr M210→Phe, Tyr M210→Leu, Phe L181—Tyr and Phe L181—Tyr M210→Tyr L181—Phe M210 Mutants of RB. Shaeroides ». Dans The Photosynthetic Bacterial Reaction Center II, 147–53. Boston, MA : Springer US, 1992. http://dx.doi.org/10.1007/978-1-4615-3050-3_18.
Texte intégralYuan, Huadong, Jing Lv, Yong Yu et Jiang Chang. « A Fast Acquisition Algorithm for L1C Based on L1CA and L1C Combined Detection ». Dans Lecture Notes in Electrical Engineering, 689–98. Berlin, Heidelberg : Springer Berlin Heidelberg, 2012. http://dx.doi.org/10.1007/978-3-642-29193-7_65.
Texte intégralVos, Marten H., Michael R. Jones, C. Neil Hunter, Jacques Breton, Jean-Christophe Lambry et Jean-Louis Martin. « Femtosecond spectroscopy and vibrational coherence of membrane-bound RCs of Rhodobacter sphaeroides genetically modified at Positions M210 and L181 ». Dans The Reaction Center of Photosynthetic Bacteria, 271–80. Berlin, Heidelberg : Springer Berlin Heidelberg, 1996. http://dx.doi.org/10.1007/978-3-642-61157-5_21.
Texte intégralSalavaravu, Laxmana Raju, et Lingaraju Dumpala. « Multi-objective Optimization of Submerged Friction Stir Welding Process Parameters for Improved Mechanical Strength of AA6061 Weld Bead by Using Taguchi-L18-Based Gray Relational Analysis ». Dans Advances in Applied Mechanical Engineering, 965–73. Singapore : Springer Singapore, 2020. http://dx.doi.org/10.1007/978-981-15-1201-8_103.
Texte intégralActes de conférences sur le sujet "L18A"
Su, Xiulan, Yiling Hou, Shibin Yuan, Maojie Tian, Bing Sun, Jun Li, Guangfu Wu, Yan Song et Wanru Hou. « cDNA, genomic sequence cloning and sequence analysis of ribosomal protein L18A gene( RPL18A ) from the Giant Panda (Ailuropoda melanoleuca) ». Dans 2010 3rd International Conference on Biomedical Engineering and Informatics (BMEI). IEEE, 2010. http://dx.doi.org/10.1109/bmei.2010.5639805.
Texte intégralLattanzi, Valerio, Paola Caselli et Luca Bizzocchi. « A PRESTELLAR CORE 3MM LINE SURVEY : MOLECULAR COMPLEXITY IN L183 ». Dans 72nd International Symposium on Molecular Spectroscopy. Urbana, Illinois : University of Illinois at Urbana-Champaign, 2017. http://dx.doi.org/10.15278/isms.2017.wf06.
Texte intégralSanders, Darius D., Chase A. Nessler, Rolf Sondergaard, Marc D. Polanka, Christopher Marks, Mitch Wolff et Walter F. O’Brien. « A CFD and Experimental Investigation of Unsteady Wake Effects on a Highly Loaded Low Pressure Turbine Blade at Low Reynolds Number ». Dans ASME Turbo Expo 2010 : Power for Land, Sea, and Air. ASMEDC, 2010. http://dx.doi.org/10.1115/gt2010-22977.
Texte intégralChen, Xin, Yu Jade Morton et Di He. « GPS L1CA/BDS B1I NLOS Signal Measurements and Modeling in Dense Urban Area ». Dans 2020 International Technical Meeting of The Institute of Navigation. Institute of Navigation, 2020. http://dx.doi.org/10.33012/2020.17139.
Texte intégralFreciozzi, J., P. Muse, A. Almansa, S. Durand, A. Khazaal et B. Rouge. « SMOS images restoration from L1A data : A sparsity-based variational approach ». Dans IGARSS 2014 - 2014 IEEE International Geoscience and Remote Sensing Symposium. IEEE, 2014. http://dx.doi.org/10.1109/igarss.2014.6946977.
Texte intégralZi-Mao Liu, Yi-Ling Hou, Xiang Ding, Wan-Ru Hou, Jun Yang et Zheng-Song Peng. « CDNA and genomic sequence clonging and analysis of ribosomal protein L10A gene (RPL10A) from giant panda ». Dans 2012 International Conference on Computer Science and Information Processing (CSIP). IEEE, 2012. http://dx.doi.org/10.1109/csip.2012.6308912.
Texte intégralYang Hu, Jun Yang, Yi-Ling Hou, Xiang Ding, Zheng-Song Peng et Wan-Ru Hou. « Cloning and sequence analysis of ribosomal protein L18 gene (rpl18) from Ailuropoda melanoleuca ». Dans 2012 International Conference on Computer Science and Information Processing (CSIP). IEEE, 2012. http://dx.doi.org/10.1109/csip.2012.6308909.
Texte intégralSalehuddin, F., I. Ahmad, F. A. Hamid, A. Zaharim, Afifah Maheran A. Hamid, P. Susthitha Menon, H. A. Elgomati, B. Yeop Majlis et P. R. Apte. « Optimization of process parameter variation in 45nm p-channel MOSFET using L18 orthogonal array ». Dans 2012 10th IEEE International Conference on Semiconductor Electronics (ICSE). IEEE, 2012. http://dx.doi.org/10.1109/smelec.2012.6417127.
Texte intégralGutkin, Gregory, Geoffrey Whitener, Young Wu et Kurt P. Rouser. « L1A Turbine Flow Characterization in a Cascade Facility with a T-Bar Turbulence Generator ». Dans 54th AIAA Aerospace Sciences Meeting. Reston, Virginia : American Institute of Aeronautics and Astronautics, 2016. http://dx.doi.org/10.2514/6.2016-0405.
Texte intégralIbrahim, Mounir B., Samuel Vinci, Olga Kartuzova et Ralph J. Volino. « CFD Simulations of Unsteady Wakes on a Highly Loaded Low Pressure Turbine Airfoil (L1A) ». Dans ASME Turbo Expo 2012 : Turbine Technical Conference and Exposition. American Society of Mechanical Engineers, 2012. http://dx.doi.org/10.1115/gt2012-69770.
Texte intégralRapports d'organisations sur le sujet "L18A"
Rieu, Pierre, Samira Amraoui et Marco Restano. Standalone Multi-mission Altimetry Processor (SMAP). European Space Agency, juin 2021. http://dx.doi.org/10.5270/esa-cnes.sentinel-3.smap.
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