Nanobodies against the myelin enzyme CNPase as tools for structural and functional studies

Author:

Markusson Sigurbjörn,Raasakka ArneORCID,Schröder Marcel,Sograte-Idrissi Shama,Rahimi Amir Mohammad,Asadpour Ommolbanin,Körner Henrike,Lodygin Dmitri,Eichel-Vogel Maria A.,Chowdhury Risha,Sutinen Aleksi,Muruganandam Gopinath,Iyer Manasi,Cooper Madeline H.,Weigel Maya K.,Ambiel Nicholas,Werner Hauke B.,Zuchero J. Bradley,Opazo FelipeORCID,Kursula PetriORCID

Abstract

Abstract2’,3’-cyclic nucleotide 3’-phosphodiesterase (CNPase) is an abundant constituent of central nervous system non-compact myelin, frequently used as a marker antigen for myelinating cells. The catalytic activity of CNPase, the 3’-hydrolysis of 2’,3’-cyclic nucleotides, is well characterisedin vitro, but thein vivofunction of CNPase remains unclear. CNPase interacts with the actin cytoskeleton to counteract the developmental closure of cytoplasmic channels that travel through compact myelin; its enzymatic activity may be involved in adenosine metabolism and RNA degradation. We developed a set of high-affinity nanobodies recognizing the phosphodiesterase domain of CNPase, and the crystal structures of each complex show that the five nanobodies have distinct epitopes. One of the nanobodies bound deep into the CNPase active site and acted as an inhibitor. Moreover, the nanobodies were characterised in imaging applications and as intrabodies, expressed in mammalian cells, such as primary oligodendrocytes. Fluorescently labelled nanobodies functioned in imaging of teased nerve fibers and whole brain tissue sections, as well as super-resolution microscopy. These anti-CNPase nanobodies provide new tools for structural and functional biology of myelination, including high-resolution imaging of nerve tissue.

Publisher

Cold Spring Harbor Laboratory

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