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Why Does Knocking Out NACHO, But Not RIC3, Completely Block Expression of α7 Nicotinic Receptors in Mouse Brain?

Biomolecules. 2020-03; 
Anish Deshpande , Remitha M. Vinayakamoorthy , Brijesh K. Garg , Jaya Prakash Thummapudi , Gauri Oza , Ketaki Adhikari, Aayush Agarwal , Parnika Dalvi , Swetha Iyer , Sarulatha Thulasi Raman , Vijay Ramesh , Akshitha Rameshbabu, Alexandra Rezvaya , Sneha Sukumaran , Sweta Swaminathan , Bhargav Tilak , Zhiyuan Wang, Phu V. Tran , and Ralph H. Loring
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Gene Synthesis … August 2011. Xenopus xric3(S+) in pcDNA3.1+/C-(K)DYK was synthesized by Genscript (#OAf03325) and used as supplied. Rat ric3(S-) in Invitrogen pRep4 plasmid (without a DDK tag) was used as described [11]. Human … Get A Quote

摘要

Alpha7 nicotinic acetylcholine receptors (α7nAChRs) are interesting not only because of their physiological effects, but because this receptor requires chaperones to traffic to cell surfaces (measured by alpha-bungarotoxin [αBGT] binding). While knockout (KO) animals and antibodies that react across species exist for tmem35a encoding the protein chaperone NACHO, commercially available antibodies against the chaperone RIC3 that allow Western blots across species have not been generally available. Further, no effects of deleting RIC3 function (ric3 KO) on α7nAChR expression are reported. Finally, antibodies against α7nAChRs have shown various deficiencies. We find mouse macrophages bind αBGT but lack NACHO. ... More

关键词

Protein folding; multi-subunit membrane protein assembly; receptor chaperone; alternate splice variants; antibody specificity; in vitro vs. in vivo effects