Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK

Both prokaryotic and eukaryotic cells contain multiple heat shock protein 40 (Hsp40) and heat shock protein 70 (Hsp70) proteins, which cooperate as molecular chaperones to ensure fidelity at all stages of protein biogenesis. The Hsp40 signature domain, the J-domain, is required for binding of an Hsp...

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Autores principales: Nicoll, W.S., Botha, M., McNamara, C., Schlange, M., Pesce, E.-R., Boshoff, A., Ludewig, M.H., Zimmermann, R., Cheetham, M.E., Chapple, J.P., Blatch, G.L.
Formato: Texto
Lenguaje:English
Publicado: Elsevier 2007
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1906734/
https://www.ncbi.nlm.nih.gov/pubmed/17239655
http://dx.doi.org/10.1016/j.biocel.2006.11.006
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author Nicoll, W.S.
Botha, M.
McNamara, C.
Schlange, M.
Pesce, E.-R.
Boshoff, A.
Ludewig, M.H.
Zimmermann, R.
Cheetham, M.E.
Chapple, J.P.
Blatch, G.L.
author_facet Nicoll, W.S.
Botha, M.
McNamara, C.
Schlange, M.
Pesce, E.-R.
Boshoff, A.
Ludewig, M.H.
Zimmermann, R.
Cheetham, M.E.
Chapple, J.P.
Blatch, G.L.
author_sort Nicoll, W.S.
collection PubMed
description Both prokaryotic and eukaryotic cells contain multiple heat shock protein 40 (Hsp40) and heat shock protein 70 (Hsp70) proteins, which cooperate as molecular chaperones to ensure fidelity at all stages of protein biogenesis. The Hsp40 signature domain, the J-domain, is required for binding of an Hsp40 to a partner Hsp70, and may also play a role in the specificity of the association. Through the creation of chimeric Hsp40 proteins by the replacement of the J-domain of a prokaryotic Hsp40 (DnaJ), we have tested the functional equivalence of J-domains from a number of divergent Hsp40s of mammalian and parasitic origin (malarial Pfj1 and Pfj4, trypanosomal Tcj3, human ERj3, ERj5, and Hsj1, and murine ERj1). An in vivo functional assay was used to test the functionality of the chimeric proteins on the basis of their ability to reverse the thermosensitivity of a dnaJ cbpA mutant Escherichia coli strain (OD259). The Hsp40 chimeras containing J-domains originating from soluble (cytosolic or endoplasmic reticulum (ER)-lumenal) Hsp40s were able to reverse the thermosensitivity of E. coli OD259. In all cases, modified derivatives of these chimeric proteins containing an His to Gln substitution in the HPD motif of the J-domain were unable to reverse the thermosensitivity of E. coli OD259. This suggested that these J-domains exerted their in vivo functionality through a specific interaction with E. coli Hsp70, DnaK. Interestingly, a Hsp40 chimera containing the J-domain of ERj1, an integral membrane-bound ER Hsp40, was unable to reverse the thermosensitivity of E. coli OD259, suggesting that this J-domain was unable to functionally interact with DnaK. Substitutions of conserved amino acid residues and motifs were made in all four helices (I–IV) and the loop regions of the J-domains, and the modified chimeric Hsp40s were tested for functionality using the in vivo assay. Substitution of a highly conserved basic residue in helix II of the J-domain was found to disrupt in vivo functionality for all the J-domains tested. We propose that helix II and the HPD motif of the J-domain represent the fundamental elements of a binding surface required for the interaction of Hsp40s with Hsp70s, and that this surface has been conserved in mammalian, parasitic and bacterial systems.
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spelling pubmed-19067342007-08-07 Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK Nicoll, W.S. Botha, M. McNamara, C. Schlange, M. Pesce, E.-R. Boshoff, A. Ludewig, M.H. Zimmermann, R. Cheetham, M.E. Chapple, J.P. Blatch, G.L. Int J Biochem Cell Biol Article Both prokaryotic and eukaryotic cells contain multiple heat shock protein 40 (Hsp40) and heat shock protein 70 (Hsp70) proteins, which cooperate as molecular chaperones to ensure fidelity at all stages of protein biogenesis. The Hsp40 signature domain, the J-domain, is required for binding of an Hsp40 to a partner Hsp70, and may also play a role in the specificity of the association. Through the creation of chimeric Hsp40 proteins by the replacement of the J-domain of a prokaryotic Hsp40 (DnaJ), we have tested the functional equivalence of J-domains from a number of divergent Hsp40s of mammalian and parasitic origin (malarial Pfj1 and Pfj4, trypanosomal Tcj3, human ERj3, ERj5, and Hsj1, and murine ERj1). An in vivo functional assay was used to test the functionality of the chimeric proteins on the basis of their ability to reverse the thermosensitivity of a dnaJ cbpA mutant Escherichia coli strain (OD259). The Hsp40 chimeras containing J-domains originating from soluble (cytosolic or endoplasmic reticulum (ER)-lumenal) Hsp40s were able to reverse the thermosensitivity of E. coli OD259. In all cases, modified derivatives of these chimeric proteins containing an His to Gln substitution in the HPD motif of the J-domain were unable to reverse the thermosensitivity of E. coli OD259. This suggested that these J-domains exerted their in vivo functionality through a specific interaction with E. coli Hsp70, DnaK. Interestingly, a Hsp40 chimera containing the J-domain of ERj1, an integral membrane-bound ER Hsp40, was unable to reverse the thermosensitivity of E. coli OD259, suggesting that this J-domain was unable to functionally interact with DnaK. Substitutions of conserved amino acid residues and motifs were made in all four helices (I–IV) and the loop regions of the J-domains, and the modified chimeric Hsp40s were tested for functionality using the in vivo assay. Substitution of a highly conserved basic residue in helix II of the J-domain was found to disrupt in vivo functionality for all the J-domains tested. We propose that helix II and the HPD motif of the J-domain represent the fundamental elements of a binding surface required for the interaction of Hsp40s with Hsp70s, and that this surface has been conserved in mammalian, parasitic and bacterial systems. Elsevier 2007 /pmc/articles/PMC1906734/ /pubmed/17239655 http://dx.doi.org/10.1016/j.biocel.2006.11.006 Text en . https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Article
Nicoll, W.S.
Botha, M.
McNamara, C.
Schlange, M.
Pesce, E.-R.
Boshoff, A.
Ludewig, M.H.
Zimmermann, R.
Cheetham, M.E.
Chapple, J.P.
Blatch, G.L.
Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title_full Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title_fullStr Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title_full_unstemmed Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title_short Cytosolic and ER J-domains of mammalian and parasitic origin can functionally interact with DnaK
title_sort cytosolic and er j-domains of mammalian and parasitic origin can functionally interact with dnak
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1906734/
https://www.ncbi.nlm.nih.gov/pubmed/17239655
http://dx.doi.org/10.1016/j.biocel.2006.11.006
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