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抗髓磷脂酶CNPase的纳米抗体作为结构和功能研究的工具。

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

作者信息

Markusson Sigurbjörn, Raasakka Arne, 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 Felipe, Kursula Petri

机构信息

Department of Biomedicine, University of Bergen, Bergen, Norway.

Neurosurgery Department, Stanford University School of Medicine, Stanford, California, USA.

出版信息

J Neurochem. 2025 Jan;169(1):e16274. doi: 10.1111/jnc.16274.

Abstract

2',3'-Cyclic nucleotide 3'-phosphodiesterase (CNPase) is an abundant constituent of central nervous system non-compact myelin, and its loss in mice and humans causes neurodegeneration. Additionally, CNPase is frequently used as a marker antigen for myelinating cells. The catalytic activity of CNPase, the 3'-hydrolysis of 2',3'-cyclic nucleotides, is well characterised in vitro, but the in vivo function 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 recognising 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 fibres and whole brain tissue sections, as well as super-resolution microscopy. These anti-CNPase nanobodies provide new tools for structural and functional studies on myelin formation, dynamics, and disease, including high-resolution imaging of nerve tissue.

摘要

2',3'-环核苷酸3'-磷酸二酯酶(CNPase)是中枢神经系统非致密髓鞘的一种丰富成分,其在小鼠和人类体内的缺失会导致神经退行性变。此外,CNPase经常被用作髓鞘形成细胞的标记抗原。CNPase的催化活性,即2',3'-环核苷酸的3'-水解作用,在体外已得到充分表征,但其在体内的功能仍不清楚。CNPase与肌动蛋白细胞骨架相互作用,以对抗穿过致密髓鞘的细胞质通道的发育性闭合;其酶活性可能参与腺苷代谢和RNA降解。我们开发了一组识别CNPase磷酸二酯酶结构域的高亲和力纳米抗体,每个复合物的晶体结构表明这五个纳米抗体具有不同的表位。其中一个纳米抗体深入结合到CNPase活性位点并起抑制剂作用。此外,这些纳米抗体在成像应用中以及作为在哺乳动物细胞(如原代少突胶质细胞)中表达的胞内抗体进行了表征。荧光标记的纳米抗体在 teased 神经纤维和全脑组织切片成像以及超分辨率显微镜检查中发挥作用。这些抗CNPase纳米抗体为髓鞘形成、动力学和疾病的结构和功能研究提供了新工具,包括神经组织的高分辨率成像。

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