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200 1 $aAnalysis and design of shallow and deep foundations$bRisorsa elettronica$fLymon C. Reese, William M. Isenhower, Shin-Tower Wang
210   $aHoboken, N. J.$cWiley$d2005
230   $aDocumento elettronico
306   $aPublished Online: 12 DEC 2007
336   $aTesto
337   $aFormato pdf
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700  1$aReese,$bLymon C.$f<1917- >$0518353
702  1$aIsenhower,$bWilliam M.
702  1$aWang,$bShin-Tower
801  0$aIT$bUNINA$gREICAT$2UNIMARC
856 4 $zFull text per gli utenti Federico II$uhttp://onlinelibrary.wiley.com/book/10.1002/9780470172773
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912   $a990009814510403321
961   $aFoundations$aDesign and construction
996   $aAnalysis and design of shallow and deep foundations$9835315
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100   $a20160829d2015      uy             |
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182   $cc
183   $acr
200 00$aCD4+ T cell differentiation in infection$b[electronic resource] $eamendments to the Th1/Th2 axiom /$fedited by Dragana Jankovic and Carl G. Feng
210   $cFrontiers Media SA$d2015
210 31$aFrance :$cFrontiers Media SA,$d2015
215   $a1 online resource (111 pages) $ccolour illustrations
225 0 $aFrontiers Research Topics
300   $aBibliographic Level Mode of Issuance: Monograph
320   $aIncludes bibliographical references.
330   $aCD4+ T lymphocytes play an essential role in host defense against bacterial, parasitic and viral infections. During infection, under the influence of intrinsic signals received through peptide-MHC/TCR interactions and extrinsic signals provided by pathogen-conditioned dendritic and other accessory cells, CD4+ T cells proliferate and differentiate into specialized T helper (Th) effectors, which produce distinct sets of cytokines tailored to combat a specific class of microbes. The concept of CD4+ T cell multi-functionality was developed after the seminal discovery of Th1 and Th2 cells nearly 30 years ago. Although the Th1/Th2 paradigm has successfully withstood the test of time, in the past decade additional Th subsets (Th17, Tfh, Th22, Th9) have been identified. Similarly, single cell analyses of cytokines and master transcriptional factors have revealed that, at the population level, CD4+ T cell responses are far more heterogeneous than initially anticipated. While some of the checkpoints in Th cell specification have been identified, recent studies of transcriptional and epigenetic regulation have uncovered a significant flexibility during the course CD4+ T lymphocyte polarization. In addition, Th cells expressing cytokines with counteracting functions, as a measure of self-regulation, display yet another level of diversity. Understanding the mechanisms that control the balance between stability vs. plasticity of Th effectors both at the time of initiation of immune response and during development of CD4 T cell memory is critical for the rational design of better vaccines and new immunotherapeutic strategies. This research topic will cover current views on Th cell development, with a focus on the mechanisms that govern differentiation, function and regulation of effector Th cells in the context of microbial infections.
606   $aClinical Immunology$2HILCC
606   $aMedicine$2HILCC
606   $aHealth & Biological Sciences$2HILCC
610   $aInfection
610   $aDendritic Cells
610   $aCytokines
610   $aImmunoregulation
610   $aCD4 lymphocytes
610   $aMemory
610   $along noncoding RNA
610   $aMacrophages
610   $aMetabolism
610   $aTh1 Th2
615  7$aClinical Immunology
615  7$aMedicine
615  7$aHealth & Biological Sciences
700   $aCarl G Feng$4auth$01366255
702   $aFeng$b Carl G
702   $aJankovic$b Dragana
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