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BD-2 and BD-3 increase skin flap survival in a model of ischemia and Pseudomonas aeruginosa infection.

Sci Rep. 2019-05; 
CasalDiogo,IriaInês,RamalhoJosé S,AlvesSara,Mota-SilvaEduarda,Mascarenhas-LemosLuís,PontinhaCarlos,Guadalupe-CabralMaria,Ferreira-SilvaJosé,Ferraz-OliveiraMário,VassilenkoValentina,Goyri-O'NeillJo?o,PaisDiogo,VideiraPau
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Gene Synthesis The defensin beta 4 A (DEFB4A) and defensin beta 103 A (DEFB103A) cDNA sequences, which code for the BD-2 and BD-3 proteins, respectively, were synthetized by GenScript Corporation® (New Jersey, USA) and cloned into pcDNA ENTR BP, using XhoI/EcoRI (DEFB4A) and SalI/KpnI (DEFB103A). Get A Quote

摘要

The main aim of this work was to study the usefulness of human β-defensins 2 (BD-2) and 3 (BD-3), which are part of the innate immune system, in the treatment of infected ischemic skin flaps. We investigated the effect of transducing rat ischemic skin flaps with lentiviral vectors encoding human BD-2, BD-3, or both BD-2 and BD-3, to increase flap survival in the context of a P. aeruginosa infection associated with a foreign body. The secondary endpoints assessed were: bacterial counts, and biofilm formation on the surface of the foreign body. A local ischemic environment was created by producing arterialized venous flaps in the left epigastric region of rats. Flaps were intentionally infected by pl... More

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