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A Dynactin Subunit with a Highly Conserved Cysteine-rich Motif Interacts Directly with Arp1

Dynactin is a multisubunit complex and a required cofactor for most, or all, of the cellular processes powered by the microtubule-based motor cytoplasmic dynein. Using a dynein affinity column, the previously uncharacterized p62 subunit of dynactin was isolated and microsequenced. Two peptide sequen...

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Published in:	The Journal of biological chemistry 2000-02, Vol.275 (7), p.4834-4839
Main Authors:	Karki, Sher, Tokito, Mariko K., Holzbaur, Erika L.F.
Format:	Article
Language:	English
Subjects:	Amino Acid Motifs Amino Acid Sequence Animals Arp1 protein Cell Line Cloning, Molecular Conserved Sequence COUP Transcription Factor II COUP Transcription Factors Cysteine - analysis DNA, Complementary DNA-Binding Proteins - metabolism dynactin Dynactin Complex Humans Microtubule-Associated Proteins - chemistry Microtubule-Associated Proteins - genetics Microtubule-Associated Proteins - metabolism p62 protein Protein Binding Receptors, Steroid Sequence Homology, Amino Acid Transcription Factors - metabolism Transfection
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description	Dynactin is a multisubunit complex and a required cofactor for most, or all, of the cellular processes powered by the microtubule-based motor cytoplasmic dynein. Using a dynein affinity column, the previously uncharacterized p62 subunit of dynactin was isolated and microsequenced. Two peptide sequences were used to clone human cDNAs encoding p62. Sequence analysis of the predicted human polypeptide of 53 kDa revealed a highly conserved pattern of eleven cysteine residues, eight of which fit the consensus sequence for a Zn2+-binding RING domain. We have characterized p62 as an integral component of 20 S dynactin by biochemical and immunocytochemical methods. Affinity chromatography experiments demonstrate that p62 binds directly to the Arp1 subunit of dynactin. Immunocytochemistry with antibodies to p62 demonstrates that this polypeptide has a punctate cytoplasmic distribution as well as centrosomal distribution typical of dynactin. In transfected cells, overexpression of p62 did not disrupt microtubule organization or the integrity of the Golgi but did cause both cytosolic and nuclear distribution of the protein, suggesting that this polypeptide may be targeted to the nucleus at very high expression levels.
doi_str_mv	10.1074/jbc.275.7.4834
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Using a dynein affinity column, the previously uncharacterized p62 subunit of dynactin was isolated and microsequenced. Two peptide sequences were used to clone human cDNAs encoding p62. Sequence analysis of the predicted human polypeptide of 53 kDa revealed a highly conserved pattern of eleven cysteine residues, eight of which fit the consensus sequence for a Zn2+-binding RING domain. We have characterized p62 as an integral component of 20 S dynactin by biochemical and immunocytochemical methods. Affinity chromatography experiments demonstrate that p62 binds directly to the Arp1 subunit of dynactin. Immunocytochemistry with antibodies to p62 demonstrates that this polypeptide has a punctate cytoplasmic distribution as well as centrosomal distribution typical of dynactin. 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Using a dynein affinity column, the previously uncharacterized p62 subunit of dynactin was isolated and microsequenced. Two peptide sequences were used to clone human cDNAs encoding p62. Sequence analysis of the predicted human polypeptide of 53 kDa revealed a highly conserved pattern of eleven cysteine residues, eight of which fit the consensus sequence for a Zn2+-binding RING domain. We have characterized p62 as an integral component of 20 S dynactin by biochemical and immunocytochemical methods. Affinity chromatography experiments demonstrate that p62 binds directly to the Arp1 subunit of dynactin. Immunocytochemistry with antibodies to p62 demonstrates that this polypeptide has a punctate cytoplasmic distribution as well as centrosomal distribution typical of dynactin. 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subjects	Amino Acid Motifs Amino Acid Sequence Animals Arp1 protein Cell Line Cloning, Molecular Conserved Sequence COUP Transcription Factor II COUP Transcription Factors Cysteine - analysis DNA, Complementary DNA-Binding Proteins - metabolism dynactin Dynactin Complex Humans Microtubule-Associated Proteins - chemistry Microtubule-Associated Proteins - genetics Microtubule-Associated Proteins - metabolism p62 protein Protein Binding Receptors, Steroid Sequence Homology, Amino Acid Transcription Factors - metabolism Transfection
title	A Dynactin Subunit with a Highly Conserved Cysteine-rich Motif Interacts Directly with Arp1
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