Missense mutation of SPAST protein (I344K) results in loss of ATPase activity and prolonged the half-life, implicated in autosomal dominant hereditary spastic paraplegia

Missense mutation of SPAST protein (I344K) results in loss of ATPase activity and prolonged the half-life, implicated in autosomal dominant hereditary spastic paraplegia

The spastin protein (SPAST) contains an ATPase with diverse cellular activities (AAA) domain and regulates microtubule dynamics. Missense mutations of the SPAST gene are frequently detected in patients with hereditary spastic paraplegias (HSPs) and represent the main reason of loss of SPAST function...

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Veröffentlicht in:Biochimica et biophysica acta. Molecular basis of disease 2018-10, Vol.1864 (10), p.3221-3233
Hauptverfasser: Lim, Jung Hwa, Kang, Hyun Mi, Jung, Hong-Ryul, Kim, Dae-Soo, Noh, Kyung Hee, Chang, Tae Kyung, Kim, Byoung Joon, Sung, Duk Hyun, Cho, Hyun-Soo, Chung, Kyung-Sook, Kim, Nam-Soon, Jung, Cho-Rok
Format: Artikel
Sprache:eng
Schlagworte:
Animals
ATPase activity
Axonal abnormality
Cell Line, Tumor
Female
Gene therapy
Half-Life
HEK293 Cells
HeLa Cells
Hereditary spastic paraplegia
Humans
Male
Mice
Missense mutation
Models, Molecular
Mutation, Missense
Pedigree
Spastic Paraplegia, Hereditary - genetics
Spastic Paraplegia, Hereditary - metabolism
Spastin
Spastin - chemistry
Spastin - genetics
Spastin - metabolism
Whole Exome Sequencing
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Zusammenfassung:The spastin protein (SPAST) contains an ATPase with diverse cellular activities (AAA) domain and regulates microtubule dynamics. Missense mutations of the SPAST gene are frequently detected in patients with hereditary spastic paraplegias (HSPs) and represent the main reason of loss of SPAST function; however, the pathogenicity of mutant SPAST is heterogeneous. Here, SPAST variant with an I344K mutation (I344K-SPAST) was identified in a Korean family with autosomal dominant-type HSP. We investigated the role of the I344K-SPAST in HSP to provide a therapeutic mechanism. The I344K-SPAST mutation prolonged the half-life of the protein compared to wild-type SPAST (WT-SPAST) in cells by modulating post-translational modifications for proteasomal degradation. I344K-SPAST was localized in microtubule but defective in microtubule severing and ATPase activity compared to WT-SPAST in vitro and in cells. Mutant M87 isoform harboring the same mutation with I344K-M1 SPAST also increased protein stability and loss of MT severing activity, but the pathogenicity was not stronger than I344K-M1 SPAST in neurite outgrowth. Overexpression of I344K-SPAST resulted in microtubule accumulation following inhibited neurite growth in neuroblastoma, neural progenitor cells and mouse primary cortical neurons. Conversely, these pathogenic effects of I344K-SPAST were reduced by overexpression of WT-M1 SPAST in a dose dependent manner since WT-SPAST could interact with I344K-SPAST. Our data therefore provide proof-of-concept that gene transfer of WT-M1 SPAST may serve as a valid therapeutic option for HSPs. •I344K-SPAST, was identified in a Korean family with autosomal dominant-type HSP.•The half-life of I344K-SPAST protein is significantly prolonged against WT-SPAST.•I344K-SPAST was reduced the MT-severing activity compared to WT-SPAST.•Gene transfer of WT-M1 SPAST restored WT functionality in HSP caused by reduced SPAST activity.
ISSN:0925-4439
1879-260X
DOI:10.1016/j.bbadis.2018.07.009