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Calaxin is required for cilia-driven determination of vertebrate laterality

Authors :
Sasaki, Keita
Shiba, Kogiku
Nakamura, Akihiro
Kawano, Natsuko
Satouh, Yuhkoh
Yamaguchi, Hiroshi
Morikawa, Motohiro
Shibata, Daisuke
Yanase, Ryuji
Jokura, Kei
Nomura, Mami
Miyado, Mami
Takada, Shuji
Ueno, Hironori
Nonaka, Shigenori
Baba, Tadashi
Ikawa, Masahito
Kikkawa, Masahide
Miyado, Kenji
Inaba, Kazuo
Sasaki, Keita
Shiba, Kogiku
Nakamura, Akihiro
Kawano, Natsuko
Satouh, Yuhkoh
Yamaguchi, Hiroshi
Morikawa, Motohiro
Shibata, Daisuke
Yanase, Ryuji
Jokura, Kei
Nomura, Mami
Miyado, Mami
Takada, Shuji
Ueno, Hironori
Nonaka, Shigenori
Baba, Tadashi
Ikawa, Masahito
Kikkawa, Masahide
Miyado, Kenji
Inaba, Kazuo

Abstract

Sasaki, K., Shiba, K., Nakamura, A. et al. Calaxin is required for cilia-driven determination of vertebrate laterality. Commun Biol 2, 226 (2019). https://doi.org/10.1038/s42003-019-0462-y<br />Calaxin is a Ca2+-binding dynein-associated protein that regulates flagellar and ciliary movement. In ascidians, calaxin plays essential roles in chemotaxis of sperm. However, nothing has been known for the function of calaxin in vertebrates. Here we show that the mice with a null mutation in Efcab1, which encodes calaxin, display typical phenotypes of primary ciliary dyskinesia, including hydrocephalus, situs inversus, and abnormal motility of trachea cilia and sperm flagella. Strikingly, both males and females are viable and fertile, indicating that calaxin is not essential for fertilization in mice. The 9 + 2 axonemal structures of epithelial multicilia and sperm flagella are normal, but the formation of 9 + 0 nodal cilia is significantly disrupted. Knockout of calaxin in zebrafish also causes situs inversus due to the irregular ciliary beating of Kupffer's vesicle cilia, although the 9 + 2 axonemal structure appears to remain normal.

Details

Database :
OAIster
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1248902255
Document Type :
Electronic Resource

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