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Enhancing arginase 2 expression using target site blockers as a strategy to modulate macrophage phenotype

Mol Ther Nucleic Acids. 2022-08; 
Chiara De Santi, Frances K Nally, Remsha Afzal, Conor P Duffy, Stephen Fitzsimons, Stephanie L Annett, Tracy Robson, Jennifer K Dowling, Sally-Ann Cryan, Claire E McCoy
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Recombinant Proteins … injected with NC TSB and LPS were set at 1. (B) Arg2 and β-actin in spleen. Blot representative of seven mice from each TSB injection (three of which were then injected … Kit (Genscript). … Get A Quote

摘要

Macrophages are plastic cells playing a crucial role in innate immunity. While fundamental in responding to infections, when persistently maintained in a pro-inflammatory state they can initiate and sustain inflammatory diseases. Therefore, a strategy that reprograms pro-inflammatory macrophages toward an anti-inflammatory phenotype could hold therapeutic potential in that context. We have recently shown that arginase 2 (Arg2), a mitochondrial enzyme involved in arginine metabolism, promotes the resolution of inflammation in macrophages and it is targeted by miR-155. Here, we designed and tested a target site blocker (TSB) that specifically interferes and blocks the interaction between miR-155 and mRNA, leadin... More

關鍵詞

MT: non-coding RNAs, PLGA, arginase 2, macrophages, miR-155, microRNAs, target site blocker, transfection
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