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Targeting intrinsically disordered regions facilitates discovery of CaV3.2 inhibitory peptides for AAV-mediated peripheral analgesia

Pain. 2022-04; 
Seung Min Shin , Justas Lauzadis , Brandon Itson-Zoske , Yongsong Cai 1 , Fan Fan , Gayathri Natarajan , Wai-Meng Kwok , Michelino Puopolo , Quinn H Hogan , Hongwei Yu
Products/Services Used Details Operation
Gene Synthesis To construct the AAV vector encoding a chimeric monomer GFP (hereafter referred to as GFP) CaV3.2iPA expression cassette, the DNA fragments encoding the CaV3.2iPA peptides were synthesized and subcloned into BsrG I/Sal I sites (Genscript, Piscataway, NJ) of a single-strand AAV expressing plasmid pAAVchicken b-actin (CBA)-GFP. Get A Quote

摘要

Ample data support a prominent role of peripheral T-type calcium channels 3.2 (CaV3.2) in generating pain states. Development of primary sensory neuron-specific inhibitors of CaV3.2 channels is an opportunity for achieving effective analgesic therapeutics, but success has been elusive. Small peptides, especially those derived from the natural proteins as inhibitory peptide aptamers (iPAs), can produce highly effective and selective blockade of specific nociceptive molecular pathways to reduce pain with minimal off-target effects. Here, we report the engineering of the potent and selective iPAs of CaV3.2 from the intrinsically disordered regions (IDR) of CaV3.2 intracellular segments. Using established predictio... More

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