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Class-specific interactions between Sis1 J-domain protein and Hsp70 chaperone potentiate disaggregation of misfolded proteins
by
Obuchowski, Igor
, Chamera, Tomasz
, Kłosowska, Agnieszka
, Liberek, Krzysztof
, Janta, Anna
, Sztangierska, Wiktoria
, Wyszkowski, Hubert
in
Binding
/ Biochemistry
/ Biological Sciences
/ Disaggregation
/ Eukaryotes
/ Heat-Shock Proteins - metabolism
/ Homeostasis
/ HSP40 Heat-Shock Proteins - genetics
/ HSP40 Heat-Shock Proteins - metabolism
/ HSP70 Heat-Shock Proteins - metabolism
/ Hsp70 protein
/ Molecular Chaperones - metabolism
/ Polypeptides
/ Protein Aggregates - physiology
/ Protein Binding - physiology
/ Protein Domains - physiology
/ Protein Folding
/ Proteins
/ Proteostasis - physiology
/ Proteostasis Deficiencies - metabolism
/ Proteostasis Deficiencies - physiopathology
/ Saccharomyces cerevisiae - metabolism
/ Saccharomyces cerevisiae Proteins - genetics
/ Saccharomyces cerevisiae Proteins - metabolism
/ Substrate Specificity
/ Substrates
/ Yeast
2021
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Class-specific interactions between Sis1 J-domain protein and Hsp70 chaperone potentiate disaggregation of misfolded proteins
by
Obuchowski, Igor
, Chamera, Tomasz
, Kłosowska, Agnieszka
, Liberek, Krzysztof
, Janta, Anna
, Sztangierska, Wiktoria
, Wyszkowski, Hubert
in
Binding
/ Biochemistry
/ Biological Sciences
/ Disaggregation
/ Eukaryotes
/ Heat-Shock Proteins - metabolism
/ Homeostasis
/ HSP40 Heat-Shock Proteins - genetics
/ HSP40 Heat-Shock Proteins - metabolism
/ HSP70 Heat-Shock Proteins - metabolism
/ Hsp70 protein
/ Molecular Chaperones - metabolism
/ Polypeptides
/ Protein Aggregates - physiology
/ Protein Binding - physiology
/ Protein Domains - physiology
/ Protein Folding
/ Proteins
/ Proteostasis - physiology
/ Proteostasis Deficiencies - metabolism
/ Proteostasis Deficiencies - physiopathology
/ Saccharomyces cerevisiae - metabolism
/ Saccharomyces cerevisiae Proteins - genetics
/ Saccharomyces cerevisiae Proteins - metabolism
/ Substrate Specificity
/ Substrates
/ Yeast
2021
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Class-specific interactions between Sis1 J-domain protein and Hsp70 chaperone potentiate disaggregation of misfolded proteins
by
Obuchowski, Igor
, Chamera, Tomasz
, Kłosowska, Agnieszka
, Liberek, Krzysztof
, Janta, Anna
, Sztangierska, Wiktoria
, Wyszkowski, Hubert
in
Binding
/ Biochemistry
/ Biological Sciences
/ Disaggregation
/ Eukaryotes
/ Heat-Shock Proteins - metabolism
/ Homeostasis
/ HSP40 Heat-Shock Proteins - genetics
/ HSP40 Heat-Shock Proteins - metabolism
/ HSP70 Heat-Shock Proteins - metabolism
/ Hsp70 protein
/ Molecular Chaperones - metabolism
/ Polypeptides
/ Protein Aggregates - physiology
/ Protein Binding - physiology
/ Protein Domains - physiology
/ Protein Folding
/ Proteins
/ Proteostasis - physiology
/ Proteostasis Deficiencies - metabolism
/ Proteostasis Deficiencies - physiopathology
/ Saccharomyces cerevisiae - metabolism
/ Saccharomyces cerevisiae Proteins - genetics
/ Saccharomyces cerevisiae Proteins - metabolism
/ Substrate Specificity
/ Substrates
/ Yeast
2021
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Class-specific interactions between Sis1 J-domain protein and Hsp70 chaperone potentiate disaggregation of misfolded proteins
Journal Article
Class-specific interactions between Sis1 J-domain protein and Hsp70 chaperone potentiate disaggregation of misfolded proteins
2021
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Overview
Protein homeostasis is constantly being challenged with protein misfolding that leads to aggregation. Hsp70 is one of the versatile chaperones that interact with misfolded proteins and actively support their folding. Multifunctional Hsp70s are harnessed to specific roles by J-domain proteins (JDPs, also known as Hsp40s). Interaction with the J-domain of these cochaperones stimulates ATP hydrolysis in Hsp70, which stabilizes substrate binding. In eukaryotes, two classes of JDPs, Class A and Class B, engage Hsp70 in the reactivation of aggregated proteins. In most species, excluding metazoans, protein recovery also relies on an Hsp100 disaggregase. Although intensely studied, many mechanistic details of how the two JDP classes regulate protein disaggregation are still unknown. Here, we explore functional differences between the yeast Class A (Ydj1) and Class B (Sis1) JDPs at the individual stages of protein disaggregation. With real-time biochemical tools, we show that Ydj1 alone is superior to Sis1 in aggregate binding, yet it is Sis1 that recruits more Ssa1 molecules to the substrate. This advantage of Sis1 depends on its ability to bind to the EEVD motif of Hsp70, a quality specific to most of Class B JDPs. This second interaction also conditions the Hsp70-induced aggregate modification that boosts its subsequent dissolution by the Hsp104 disaggregase. Our results suggest that the Sis1-mediated chaperone assembly at the aggregate surface potentiates the entropic pulling, driven polypeptide disentanglement, while Ydj1 binding favors the refolding of the solubilized proteins. Such subspecialization of the JDPs across protein reactivation improves the robustness and efficiency of the disaggregation machinery.
Publisher
National Academy of Sciences
Subject
/ Heat-Shock Proteins - metabolism
/ HSP40 Heat-Shock Proteins - genetics
/ HSP40 Heat-Shock Proteins - metabolism
/ HSP70 Heat-Shock Proteins - metabolism
/ Molecular Chaperones - metabolism
/ Protein Aggregates - physiology
/ Protein Binding - physiology
/ Protein Domains - physiology
/ Proteins
/ Proteostasis Deficiencies - metabolism
/ Proteostasis Deficiencies - physiopathology
/ Saccharomyces cerevisiae - metabolism
/ Saccharomyces cerevisiae Proteins - genetics
/ Saccharomyces cerevisiae Proteins - metabolism
/ Yeast
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