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               <dc:title>Amygdalin analogues inhibit INF-gamma signalling reducing inflammatory response in human keratinocytes (HaCat)</dc:title>
               <dc:creator>Paoletti, Iole</dc:creator>
               <dc:creator>De Gregorio, Vicenza</dc:creator>
               <dc:creator>Baroni, Adone</dc:creator>
               <dc:creator>Tufano, Maria Antonieta</dc:creator>
               <dc:creator>Donnarumma, Giovanna</dc:creator>
               <dc:creator>Pérez González, Juan Jesús</dc:creator>
               <dc:subject>Àrees temàtiques de la UPC::Enginyeria química</dc:subject>
               <dc:subject>Peptides</dc:subject>
               <dc:subject>Psoriasis</dc:subject>
               <dc:subject>peptide T</dc:subject>
               <dc:subject>amygdalin analogues</dc:subject>
               <dc:subject>NHEK cells</dc:subject>
               <dc:subject>psoriasis</dc:subject>
               <dc:subject>Pèptids</dc:subject>
               <dc:subject>Psoriasi</dc:subject>
               <dc:description>Peptide T (PT), an octapeptide fragment located in the V2 region of the HIV-1 gp120-&#xd;
coating protein, appears to be bene&#xd;
fi&#xd;
cial in the treatment of psoriasis. Our previous investigations&#xd;
suggest that keratinocytes play a key role in conditioning the therapeutic effects of PT in psoriasis.&#xd;
The aim of this study was to explore the effects of PT and the peptidomimetic natural products,&#xd;
Dhurrin and Prunasin, on the expression of the IL-6, IL-8, IL-23, HSP70 and ICAM-1 on IFN-&#xd;
γ&#xd;
and TNF-&#xd;
α&#xd;
-NHEK activated cells. Moreover, we analysed the interference of PT and its analogues&#xd;
through STAT-3 activation. Our results show that the analogues tested exhibit the bene&#xd;
fi&#xd;
cial biol-&#xd;
ogical effects of PT, suggesting the primary role of keratinocytes upon which PT and the peptido-&#xd;
mimetics act directly, by reducing proin&#xd;
fl&#xd;
ammatory responses. Its reduction appears to be important&#xd;
for therapeutic approach in psoriasis pathogenesis</dc:description>
               <dc:description>Peer Reviewed</dc:description>
               <dc:description>Postprint (published version)</dc:description>
               <dc:date>2013-12-02</dc:date>
               <dc:type>Article</dc:type>
               <dc:relation>http://link.springer.com/article/10.1007%2Fs10753-013-9670-7</dc:relation>
               <dc:rights>http://creativecommons.org/licenses/by-nc-nd/3.0/es/</dc:rights>
               <dc:rights>Restricted access - publisher's policy</dc:rights>
               <dc:rights>Attribution-NonCommercial-NoDerivs 3.0 Spain</dc:rights>
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