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Using AAV vectors expressing the β2-adrenoceptor or associated Gα proteins to modulate skeletal muscle mass and muscle fibre size.

Sci Rep . 2016 Mar; 
Hagg A,, Colgan TD,, Thomson RE, Qian H, Lynch GS, Gregorevic P,,,.
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PCR Cloning and Subcloning Traditional cloning techniques were used to gen- erate cDNA constructs encoding Adrb2 (β 2-AR), Gnai2 (Gα i2), GnasL (Gα sL) and GnasXL (Gα sXL) (synthe- sized by GenScript) which were cloned into an AAV expression plasmid consisting of a cytomegalovirus (CMV) promoter and SV40 poly-A region f lanked by AAV2 terminal repeats. Get A Quote

摘要

Anabolic β2-adrenoceptor (β2-AR) agonists have been proposed as therapeutics for treating muscle wasting but concerns regarding possible off-target effects have hampered their use. We investigated whether β2-AR-mediated signalling could be modulated in skeletal muscle via gene delivery to the target tissue, thereby avoiding the risks of β2-AR agonists. In mice, intramuscular administration of a recombinant adeno-associated virus-based vector (rAAV vector) expressing the β2-AR increased muscle mass by >20% within 4 weeks. This hypertrophic response was comparable to that of 4 weeks' treatment with the β2-AR agonist formoterol, and was not ablated by mTOR inhibition. Increasing expression of inhibitory (Gα... More

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