2011
DOI: 10.1002/mds.23611
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Truncating mutations in THAP1 define the nuclear localization signal

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Cited by 14 publications
(13 citation statements)
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“…THAP1 contains a bipartite NLS spanning 16 amino acids (aa 146-162) in the C-terminal part of THAP1. 18 Although the frameshift mutation Asp191Thrfs*9 does not affect the NLS itself, we demonstrated an impaired nuclear import of mutant THAP1 in vitro. This altered intracellular distribution of THAP1 may be explained by a protein misfolding affecting at least the C-terminal region of THAP1, which disturbs the formation of the bipartite NLS and results in a reduced interaction with nuclear importing proteins.…”
Section: Discussionmentioning
confidence: 56%
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“…THAP1 contains a bipartite NLS spanning 16 amino acids (aa 146-162) in the C-terminal part of THAP1. 18 Although the frameshift mutation Asp191Thrfs*9 does not affect the NLS itself, we demonstrated an impaired nuclear import of mutant THAP1 in vitro. This altered intracellular distribution of THAP1 may be explained by a protein misfolding affecting at least the C-terminal region of THAP1, which disturbs the formation of the bipartite NLS and results in a reduced interaction with nuclear importing proteins.…”
Section: Discussionmentioning
confidence: 56%
“…These GFP-labeled constructs were transiently expressed for 48 h in OVCAR-3 cells and localization was determined using confocal laser scanning microscopy as described. 18 OVCAR-3 cells are well suited for immunocytochemistry experiments due to their size and handling.…”
Section: Subcellular Localization Of Truncated Thap1mentioning
confidence: 99%
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“…Both mutations affect distinct domains of the THAP1 protein: While the missense mutation p.Arg13His is localized in the THAP domain, the frameshift mutation p.Lys158Asnfs*23 disrupts the nuclear localization signal. It has been shown that this mutation impairs the nuclear import of THAP1 preventing DNA binding of cytoplasm-located THAP1 [19]. Thus, both mutations are considered to result in reduced THAP1 promoter binding leading to decreased transcription factor activity and subsequently resulting in reduced repression of THAP1 expression.…”
Section: Discussionmentioning
confidence: 97%
“…Therefore, we also aimed to investigate endogenous expression levels in patient-derived neurons. Since primary neurons are not available from living individuals, we generated iPS cells from primary human dermal fibroblasts taken from two dystonia patients harboring a heterozygous missense mutation (p.Arg13His) within the THAP DNA-binding domain or a frameshift mutation (p.Lys158Asnfs*23) disrupting the nuclear localization signal of THAP1 [19] as well as two healthy individuals as controls. One iPS cell line per individual was established and the expression of pluripotency markers in these cells was confirmed by immunostaining (Fig.…”
Section: Thap1 and Tor1a Expression Levels In Ips-derived Neuronsmentioning
confidence: 99%