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  4. Reversal of neuroinflammation in novel GS model mice by single i.c.v. administration of CHO-derived rhCTSA precursor protein

Reversal of neuroinflammation in novel GS model mice by single i.c.v. administration of CHO-derived rhCTSA precursor protein

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Use this link to cite this item : https://repo.lib.tokushima-u.ac.jp/117739
ID 117739
Author
Horii, Yuto Tokushima University
Iniwa, Toshiki Tokushima University
Onitsuka, Masayoshi Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Tsukimoto, Jun Tokushima University
Tanaka, Yuki Tokushima University
Ike, Hironobu Tokushima University
Fukushi, Yuri Tokushima University
Ando, Haruna Tokushima University
Takeuchi, Yoshie Tokushima University
Nishioka, So-ichiro Tokushima University
Tsuji, Daisuke Tokushima University KAKEN Search Researchers
Ikuo, Mariko Tokushima University KAKEN Search Researchers
Yamazaki, Naoshi Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Takiguchi, Yoshiharu Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Ishimaru, Naozumi Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Itoh, Kohji Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Content Type
Journal Article
Description
Galactosialidosis (GS) is a lysosomal cathepsin A (CTSA) deficiency. It associates with a simultaneous decrease of neuraminidase 1 (NEU1) activity and sialylglycan storage. Central nervous system (CNS) symptoms reduce the quality of life of juvenile/adult-type GS patients, but there is no effective therapy. Here, we established a novel GS model mouse carrying homozygotic Ctsa IVS6+1g→a mutation causing partial exon 6 skipping with concomitant deficiency of Ctsa/Neu1. The GS mice developed juvenile/adult GS-like symptoms, such as gargoyle-like face, edema, proctoprosia due to sialylglycan accumulation, and neurovisceral inflammation, including activated microglia/macrophage appearance and increase of inflammatory chemokines. We produced human CTSA precursor proteins (proCTSA), a homodimer carrying terminal mannose 6-phosphate (M6P)-type N-glycans. The CHO-derived proCTSA was taken up by GS patient-derived fibroblasts via M6P receptors and delivered to lysosomes. Catalytically active mature CTSA showed a shorter half-life due to intralysosomal proteolytic degradation. Following single i.c.v. administration, proCTSA was widely distributed, restored the Neu1 activity, and reduced the sialylglycans accumulated in brain regions. Moreover, proCTSA suppressed neuroinflammation associated with reduction of activated microglia/macrophage and up-regulated Mip1α. The results show therapeutic effects of intracerebrospinal enzyme replacement utilizing CHO-derived proCTSA and suggest suppression of CNS symptoms.
Journal Title
Molecular Therapy - Methods and Clinical Development
ISSN
23290501
Publisher
The American Society of Gene and Cell Therapy|Elsevier
Volume
25
Start Page
297
End Page
310
Published Date
2022-04-15
Rights
This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
EDB ID
385877
DOI (Published Version)
10.1016/j.omtm.2022.04.001
URL ( Publisher's Version )
https://doi.org/10.1016/j.omtm.2022.04.001
FullText File
mtmcd_25_297.pdf 3.2 MB
language
eng
TextVersion
Publisher
departments
Bioscience and Bioindustry
Pharmaceutical Sciences
Oral Sciences
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