Interaction between importin 13 and myopodin suggests a nuclear import pathway for myopodin

被引:0
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作者
Jie Liang
Guifen Ke
Wenjun You
Zi Peng
Jie Lan
Markus Kalesse
Alan M. Tartakoff
Feige Kaplan
Tao Tao
机构
[1] Xiamen University,School of Life Sciences and Key Laboratory for Cell Biology and Tumor Cell Engineering, The Ministry of Education of China
[2] Xiamen University,Xiamen Zhong Shan Hospital
[3] No. 1 Hospital of Xiamen,Montreal Children’s Hospital Research Institute
[4] McGill University,Institut für Organische Chemie
[5] Universität Hannover,Department of Pathology and Cell Biology Program
[6] Case Western Reserve University,undefined
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关键词
Importin 13; Myopodin; Interaction; Nuclear import;
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摘要
Importin 13 is a member of the importin β superfamily of nuclear transport proteins and is expressed in multiple tissues at high levels both in humans and rodents, including fetal lung, brain, and heart. In order to elucidate potential functions of imp13 in the heart, we have used rat imp13 as bait to screen a human heart cDNA library and identified an interaction with the C-terminal peptide of myopodin (a.a. 360–698), an actin-bundling protein, associated with tumor–suppressor activity that localizes to both the cytoplasm and the nucleus. We have used GST-pull down assays and co-immunoprecipitation experiments to demonstrate an interaction between imp13 and full-length myopodin and observed that RanGTP dissociates the myopodin–imp13 complex. In studies of cultured cells, we show that both imp13 siRNA and a C-terminal fragment of imp13 protein prevent nuclear localization of myopodin. We, therefore, conclude that imp13 functions in myopodin import and we suggest that the regulation of these events is critical for normal and abnormal cellular differentiation.
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页码:93 / 100
页数:7
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