Your search keyword '"Molecular Chaperones metabolism"' showing total 10,987 results

51. Preserve or destroy: Orphan protein proteostasis and the heat shock response.

Author

Ali A, Paracha S, and Pincus D

Subjects

Humans, Molecular Chaperones metabolism, Molecular Chaperones genetics, Animals, Ribosomes metabolism, Ribosomes genetics, Biomolecular Condensates metabolism, Proteostasis, Heat-Shock Response

Abstract

Most eukaryotic genes encode polypeptides that are either obligate members of hetero-stoichiometric complexes or clients of organelle-targeting pathways. Proteins in these classes can be released from the ribosome as "orphans"-newly synthesized proteins not associated with their stoichiometric binding partner(s) and/or not targeted to their destination organelle. Here we integrate recent findings suggesting that although cells selectively degrade orphan proteins under homeostatic conditions, they can preserve them in chaperone-regulated biomolecular condensates during stress. These orphan protein condensates activate the heat shock response (HSR) and represent subcellular sites where the chaperones induced by the HSR execute their functions. Reversible condensation of orphan proteins may broadly safeguard labile precursors during stress., (© 2024 Ali et al.)

Published

2024

52. Proteostasis is a key driver of the pathogenesis in Apicomplexa.

Author

Mitra P and Deshmukh AS

Subjects

Unfolded Protein Response, Humans, Animals, Protozoan Proteins metabolism, Protozoan Proteins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Protein Folding, Endoplasmic Reticulum metabolism, Proteostasis, Apicomplexa metabolism, Apicomplexa genetics

Abstract

Proteostasis, including protein folding mediated by molecular chaperones, protein degradation, and stress response pathways in organelles like ER (unfolded protein response: UPR), are responsible for cellular protein quality control. This is essential for cell survival as it regulates and reprograms cellular processes. Here, we underscore the role of the proteostasis pathway in Apicomplexan parasites with respect to their well-characterized roles as well as potential roles in many parasite functions, including survival, multiplication, persistence, and emerging drug resistance. In addition to the diverse physiological importance of proteostasis in Apicomplexa, we assess the potential of the pathway's components as chemotherapeutic targets., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

53. Targeting chaperone modifications: Innovative approaches to cancer treatment.

Author

Stewart M and Schisler JC

Subjects

Humans, Molecular Chaperones metabolism, Animals, Heat-Shock Proteins metabolism, Heat-Shock Proteins antagonists & inhibitors, Neoplasms metabolism, Neoplasms drug therapy, Protein Processing, Post-Translational

Abstract

Cancer and other chronic diseases are marked by alterations in the protein quality control system, affecting the posttranslational destiny of various proteins that regulate, structure, and catalyze cellular processes. Cellular chaperones, also known as heat shock proteins (HSPs), are pivotal in this system, performing protein triage that often determines the fate of proteins they bind to. Grasping the regulatory mechanisms of HSPs and their associated cofactors is crucial for understanding protein quality control in both healthy and diseased states. Recent research has shed light on the interactions within the protein quality control system and how post-translational modification govern protein interactions, function, and localization, which can drive or inhibit cell proliferation. This body of work encompasses critical elements of the heat shock response, including heat shock protein 70, heat shock protein 90, carboxyl-terminus of HSC70 interacting protein, and heat shock protein organizing protein. This review aims to synthesize these advancements, offering a holistic understanding of the system and its response when commandeered by diseases like cancer. We focus on the mechanistic shift in co-chaperone engagement-transitioning from heat shock protein organizing protein to carboxyl-terminus of HSC70 interacting protein in association with heat shock protein 70 and heat shock protein 90-which could influence cellular growth and survival pathways. A comprehensive examination of posttranslational modification-driven regulation within the protein quality control network is presented, highlighting the roles of activation factors, chaperones, and co-chaperones. Our insights aim to inform new strategies for therapeutically targeting diseases by considering the entire heat shock response system., Competing Interests: Conflict of interests The authors declare that they have no conflicts of interests with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

54. Redox regulation of proteostasis.

Author

Duong LD, West JD, and Morano KA

Subjects

Humans, Animals, Protein Folding, Molecular Chaperones metabolism, Proteasome Endopeptidase Complex metabolism, Autophagy, Proteostasis, Oxidation-Reduction, Oxidative Stress

Abstract

Oxidants produced through endogenous metabolism or encountered in the environment react directly with reactive sites in biological macromolecules. Many proteins, in particular, are susceptible to oxidative damage, which can lead to their altered structure and function. Such structural and functional changes trigger a cascade of events that influence key components of the proteostasis network. Here, we highlight recent advances in our understanding of how cells respond to the challenges of protein folding and metabolic alterations that occur during oxidative stress. Immediately after an oxidative insult, cells selectively block the translation of most new proteins and shift molecular chaperones from folding to a holding role to prevent wholesale protein aggregation. At the same time, adaptive responses in gene expression are induced, allowing for increased expression of antioxidant enzymes, enzymes that carry out the reduction of oxidized proteins, and molecular chaperones, all of which serve to mitigate oxidative damage and rebalance proteostasis. Likewise, concomitant activation of protein clearance mechanisms, namely proteasomal degradation and particular autophagic pathways, promotes the degradation of irreparably damaged proteins. As oxidative stress is associated with inflammation, aging, and numerous age-related disorders, the molecular events described herein are therefore major determinants of health and disease., Competing Interests: Conflict of interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests. Kevin A. Morano reports financial support was provided by the National Institute of General Medical Sciences. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

55. Functional similarities and differences among subunits of the nascent polypeptide-associated complex (NAC) of Saccharomyces cerevisiae.

Author

Schilke BA, Ziegelhoffer T, Domanski P, Marszalek J, Tomiczek B, and Craig EA

Subjects

Ribosomal Proteins metabolism, Ribosomal Proteins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Protein Subunits metabolism, Protein Binding, Ribosomes metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins metabolism, Saccharomyces cerevisiae Proteins genetics

Abstract

Protein factors bind ribosomes near the tunnel exit, facilitating protein trafficking and folding. In eukaryotes, the heterodimeric nascent polypeptide-associated complex (NAC) is the most abundant-equimolar to ribosomes. Saccharomyces cerevisiae has a minor β-type subunit (Nacβ2) in addition to abundant Nacβ1, and therefore two NAC heterodimers, α/β1 and α/β12. The additional beta NAC gene arose at the time of the whole genome duplication that occurred in the S. cerevisiae lineage. Nacβ2 has been implicated in regulating the fate of messenger RNA encoding ribosomal protein Rpl4 during translation via its interaction with the Caf130 subunit of the regulatory CCR4-Not complex. We found that Nacβ2 residues just C-terminal to the globular domain are required for its interaction with Caf130 and its negative effect on the growth of cells lacking Acl4, the specialized chaperone for Rpl4. Substitution of these Nacβ2 residues at homologous positions in Nacβ1 results in a chimeric protein that interacts with Caf130 and slows the growth of ∆acl4 cells lacking Nacβ2. Furthermore, alteration of residues in the N-terminus of Nacβ2 or chimeric Nacβ1 previously shown to affect ribosome binding overcomes the growth defect of ∆acl4. Our results are consistent with a model in which Nacβ2's ribosome association per se or its precise positioning is necessary for productive recruitment of CCR4-Not via its interaction with the Caf130 subunit to drive Rpl4 messenger RNA degradation., Competing Interests: Declarations of interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

56. The HSP90/R2TP Quaternary Chaperone Scaffolds Assembly of the TSC Complex.

Author

Abéza C, Busse P, Paiva ACF, Chagot ME, Schneider J, Robert MC, Vandermoere F, Schaeffer C, Charpentier B, Sousa PMF, Bandeiras TM, Manival X, Cianferani S, Bertrand E, and Verheggen C

Subjects

Humans, DNA Helicases metabolism, DNA Helicases genetics, DNA Helicases chemistry, Molecular Chaperones metabolism, Molecular Chaperones genetics, Molecular Chaperones chemistry, Protein Binding, RNA Helicases metabolism, RNA Helicases chemistry, RNA Helicases genetics, Carrier Proteins metabolism, Carrier Proteins chemistry, Carrier Proteins genetics, HEK293 Cells, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing chemistry, Apoptosis Regulatory Proteins, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins chemistry, HSP90 Heat-Shock Proteins genetics, Tuberous Sclerosis Complex 1 Protein metabolism, Tuberous Sclerosis Complex 1 Protein genetics, ATPases Associated with Diverse Cellular Activities metabolism, ATPases Associated with Diverse Cellular Activities genetics, ATPases Associated with Diverse Cellular Activities chemistry, Tuberous Sclerosis Complex 2 Protein metabolism, Tuberous Sclerosis Complex 2 Protein genetics, Tuberous Sclerosis Complex 2 Protein chemistry

Abstract

The R2TP chaperone is composed of the RUVBL1/RUVBL2 AAA+ ATPases and two adapter proteins, RPAP3 and PIH1D1. Together with HSP90, it functions in the assembly of macromolecular complexes that are often involved in cell proliferation. Here, proteomic experiments using the isolated PIH domain reveals additional R2TP partners, including the Tuberous Sclerosis Complex (TSC) and many transcriptional complexes. The TSC is a key regulator of mTORC1 and is composed of TSC1, TSC2 and TBC1D7. We show a direct interaction of TSC1 with the PIH phospho-binding domain of PIH1D1, which is, surprisingly, phosphorylation independent. Via the use of mutants and KO cell lines, we observe that TSC2 makes independent interactions with HSP90 and the TPR domains of RPAP3. Moreover, inactivation of PIH1D1 or the RUVBL1/2 ATPase activity inhibits the association of TSC1 with TSC2. Taken together, these data suggest a model in which the R2TP recruits TSC1 via PIH1D1 and TSC2 via RPAP3 and HSP90, and use the chaperone-like activities of RUVBL1/2 to stimulate their assembly., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

57. DNAJB6 is expressed in neurons and oligodendrocytes of the human brain.

Author

Hentze J, Folke J, Aznar S, Nyeng P, Brudek T, and Hansen C

Subjects

Humans, Male, Female, Aged, Middle Aged, Aged, 80 and over, Multiple System Atrophy metabolism, Multiple System Atrophy pathology, alpha-Synuclein metabolism, Parkinson Disease metabolism, Parkinson Disease pathology, Adult, Oligodendroglia metabolism, HSP40 Heat-Shock Proteins metabolism, HSP40 Heat-Shock Proteins genetics, Neurons metabolism, Brain metabolism, Nerve Tissue Proteins metabolism, Molecular Chaperones metabolism

Abstract

DNAJB6 is a suppressor of α-synuclein aggregation in vivo and in vitro. DNAJB6 is strongly expressed in the brain, and its overall protein expression is altered in neurodegenerative conditions such as Parkinson's Disease (PD) and Multiple System Atrophy (MSA). These two diseases are characterized by accumulation of aggregated α-synuclein in neurons and oligodendrocytes, respectively. To further explore this, we employed post-mortem normal human brain material to investigate the regional and cell type specific protein expression of DNAJB6. We found that the DNAJB6 protein is ubiquitously expressed across various regions of the brain. Notably, we demonstrate for the first time that DNAJB6 is present in nearly half (41%-53%) of the oligodendrocyte population and in the majority (68%-80%) of neurons. However, DNAJB6 was only sparsely present in other cell types such as astrocytes and microglia. Given that α-synuclein aggregation in oligodendrocytes is a hallmark of MSA, we investigated DNAJB6 presence in MSA brains compared to control brains. We found no significant difference in the percentage of oligodendrocytes where DNAJB6 was present in MSA brains relative to control brains. In conclusion, our results reveal an expression of the DNAJB6 protein across various regions of the human brain, and that DNAJB6 is almost exclusively present in neurons and oligodendrocytes. Since prior studies have shown that PD and MSA brains have altered levels of DNAJB6 relative to control brains, DNAJB6 may be an interesting target for drug development., (© 2024 Wiley Periodicals LLC.)

Published

2024

58. Chaperone-Mediated Autophagy in Brain Injury: A Double-Edged Sword with Therapeutic Potentials.

Author

Zhang H, Tian Y, Ma S, Ji Y, Wang Z, Xiao P, and Xu Y

Subjects

Humans, Animals, Molecular Chaperones metabolism, Autophagy physiology, Brain Injuries metabolism, Brain Injuries pathology, Chaperone-Mediated Autophagy physiology

Abstract

Autophagy is an intracellular recycling process that maintains cellular homeostasis by degrading excess or defective macromolecules and organelles. Chaperone-mediated autophagy (CMA) is a highly selective form of autophagy in which a substrate containing a KFERQ-like motif is recognized by a chaperone protein, delivered to the lysosomal membrane, and then translocated to the lysosome for degradation with the assistance of lysosomal membrane protein 2A. Normal CMA activity is involved in the regulation of cellular proteostasis, metabolism, differentiation, and survival. CMA dysfunction disturbs cellular homeostasis and directly participates in the pathogenesis of human diseases. Previous investigations on CMA in the central nervous system have primarily focus on neurodegenerative diseases, such as Parkinson's disease and Alzheimer's disease. Recently, mounting evidence suggested that brain injuries involve a wider range of types and severities, making the involvement of CMA in the bidirectional processes of damage and repair even more crucial. In this review, we summarize the basic processes of CMA and its associated regulatory mechanisms and highlight the critical role of CMA in brain injury such as cerebral ischemia, traumatic brain injury, and other specific brain injuries. We also discuss the potential of CMA as a therapeutic target to treat brain injury and provide valuable insights into clinical strategies., Competing Interests: Declarations. Ethics Approval: Not applicable. Consent to Participate: Not applicable. Consent for Publication: Not applicable. Competing Interests: Tha authors declare no competing interests. Research Involving Human Participants and/or Animals: Not applicable., (© 2024. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

59. Identification of a Non-canonical Function of Prefoldin Subunit 5 in Proteasome Assembly.

Author

Shahmoradi Ghahe S, Drabikowski K, Stasiak M, and Topf U

Subjects

Protein Folding, Proteolysis, Adenosine Triphosphatases metabolism, Adenosine Triphosphatases genetics, Proteasome Endopeptidase Complex metabolism, Molecular Chaperones metabolism, Molecular Chaperones genetics, Saccharomyces cerevisiae Proteins metabolism, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae genetics

Abstract

The prefoldin complex is a heterohexameric, evolutionarily conserved co-chaperone that assists in folding of polypeptides downstream of the protein translation machinery. Loss of prefoldin function leads to impaired solubility of cellular proteins. The degradation of proteins by the proteasome is an integral part of protein homeostasis. Failure of regulated protein degradation can lead to the accumulation of misfolded and defective proteins. We show that prefoldin subunit 5 is required for proteasome activity by contributing to the assembly of the 26S proteasome. In particular, we found that absence of the prefoldin subunit 5 impairs formation of the Rpt ring subcomplex of the proteasome. Concomitant deletion of PFD5 and HSM3, a chaperone for assembly of the ATPase subunits comprising the Rpt ring, exacerbates this effect, suggesting a synergistic relationship between the two factors in proteasome assembly. Thus, our findings reveal a regulatory mechanism wherein prefoldin subunit 5 plays a crucial role in maintaining proteasome integrity, thereby influencing the degradation of proteins., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

60. Regulated Proteolysis Induces Aberrant Phase Transition of Biomolecular Condensates into Aggregates: A Protective Role for the Chaperone Clusterin.

Author

Kamps J, Yuste-Checa P, Mamashli F, Schmitz M, Herrera MG, da Silva Correia SM, Gogte K, Bader V, Zerr I, Hartl FU, Bracher A, Winklhofer KF, and Tatzelt J

Subjects

Animals, Protein Folding, Molecular Chaperones metabolism, Molecular Chaperones chemistry, Humans, Amyloid metabolism, Amyloid chemistry, Mice, Prion Proteins metabolism, Prion Proteins chemistry, Prion Diseases metabolism, Prion Diseases pathology, Clusterin metabolism, Clusterin chemistry, Proteolysis, Phase Transition, Protein Aggregates, Biomolecular Condensates metabolism, Biomolecular Condensates chemistry

Abstract

Several proteins associated with neurodegenerative diseases, such as the mammalian prion protein (PrP), undergo liquid-liquid phase separation (LLPS), which led to the hypothesis that condensates represent precursors in the formation of neurotoxic protein aggregates. However, the mechanisms that trigger aberrant phase separation are incompletely understood. In prion diseases, protease-resistant and infectious amyloid fibrils are composed of N-terminally truncated PrP, termed C2-PrP. C2-PrP is generated by regulated proteolysis (β-cleavage) of the cellular prion protein (PrP C ) specifically upon prion infection, suggesting that C2-PrP is a misfolding-prone substrate for the propagation of prions. Here we developed a novel assay to investigate the role of both LLPS and β-cleavage in the formation of C2-PrP aggregates. We show that β-cleavage induces the formation of C2-PrP aggregates, but only when full-length PrP had formed biomolecular condensates via LLPS before proteolysis. In contrast, C2-PrP remains soluble after β-cleavage of non-phase-separated PrP. To investigate whether extracellular molecular chaperones modulate LLPS of PrP and/or misfolding of C2-PrP, we focused on Clusterin. Clusterin does not inhibit LLPS of full-length PrP, however, it prevents aggregation of C2-PrP after β-cleavage of phase-separated PrP. Furthermore, Clusterin interferes with the in vitro amplification of infectious human prions isolated from Creutzfeldt-Jakob disease patients. Our study revealed that regulated proteolysis triggers aberrant phase transition of biomolecular condensates into aggregates and identified Clusterin as a component of the extracellular quality control pathway to prevent the formation and propagation of pathogenic PrP conformers., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

61. Heat shock protein 27 downregulation attenuates isoprenaline-induced myocardial fibrosis and diastolic dysfunction by modulating the endothelial-mesenchymal transition.

Author

Zou Y, Shi H, Li Y, Li T, Liu N, and Liu B

Subjects

Animals, Mice, Male, Mice, Inbred C57BL, Snail Family Transcription Factors metabolism, Snail Family Transcription Factors genetics, Heat-Shock Proteins metabolism, Heat-Shock Proteins genetics, Myocardium pathology, Myocardium metabolism, Molecular Chaperones metabolism, Molecular Chaperones genetics, Humans, Smad3 Protein metabolism, Smad3 Protein genetics, Endothelial-Mesenchymal Transition, Fibrosis, Isoproterenol toxicity, Down-Regulation drug effects, Down-Regulation physiology, Epithelial-Mesenchymal Transition drug effects, Epithelial-Mesenchymal Transition physiology, Mice, Knockout, HSP27 Heat-Shock Proteins metabolism, HSP27 Heat-Shock Proteins genetics

Abstract

Heart failure (HF), an end-stage clinical syndrome secondary to cardiac impairment, significantly affects patients' quality of life and long-term prognosis. Myocardial fibrosis leads to systolic and diastolic dysfunction, and promotes the progression of HF. Several studies involving the modulation of myocardial fibrosis have been conducted in an effort to improve cardiac function. Heat shock protein 27 (HSP27) is a small chaperone protein that is overexpressed in cellular stress states. HSP27 modulates epithelial-mesenchymal transition, playing a crucial role in the pathology of several fibrotic diseases. However, its association with myocardial fibrosis regulation is unknown. This study aimed to investigate the mechanisms by which HSP27 regulates myocardial fibrosis. We created cardiac-specific HSP25 (the murine ortholog of human HSP27) knockout mice and found that HSP25 knockdown inhibited endothelial-mesenchymal transition (EndMT), attenuated myocardial fibrosis, and ameliorated diastolic dysfunction in isoproterenol-induced HF mice via echocardiography, histology, and western bloting. In vitro, HSP27 knockdown attenuated transforming growth factor beta-induced EndMT, whereas HSP27 overexpression promoted EndMT. Furthermore, the SMAD3/SNAIL1 pathway was found to be crucial for HSP27-mediated EndMT regulation. As an essential molecule in EndMT regulation and myocardial fibrosis modulation, HSP27 may hold promise as a therapeutic target for patients with HF., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

62. Boosting extracellular FastPETase production in E. coli: A combined approach of cognate chaperones co-expression and vesicle nucleating peptide tag fusion.

Author

Wu T, Sun H, Wang W, Xie B, Wang Z, Lu J, Xu A, Dong W, Zhou J, and Jiang M

Subjects

Molecular Chaperones genetics, Molecular Chaperones metabolism, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, HSP40 Heat-Shock Proteins genetics, HSP40 Heat-Shock Proteins metabolism, Fermentation, Burkholderiales genetics, Burkholderiales enzymology, Gene Expression, HSP70 Heat-Shock Proteins genetics, HSP70 Heat-Shock Proteins metabolism, Escherichia coli genetics, Escherichia coli metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins biosynthesis

Abstract

Enzymatic PET recycling has emerged as a promising green solution in addition to mechanical recycling, but low soluble expression levels of the inherently hydrophobic PET hydrolases hinder large-scale applications. Here, we propose a novel strategy for enhanced production of FastPETase in Escherichia coli using co-expression of molecular chaperones from Ideonella sakaiensis. Co-expression of cognate DnaK and DnaJ chaperones significantly increased soluble FastPETase expression (up to 2.5-fold), surpassing commercial chaperone plasmids. Furthermore, a combinatorial approach employing co-expression of DnaK/DnaJ chaperones and fusion of FastPETase with the VNp6-tag significantly boosted FastPETase secretion, yielding over 2 g/L of target protein in a 5-l bioreactor. Notably, the crude FastPETase in fermentation broth displayed comparable PET hydrolysis effects to the purified enzyme. This work not only provides new insights into the process of chaperones in protein folding but also suggests a novel and efficient strategy for producing recombinant proteins., Competing Interests: Declaration of competing interest The authors declare that they have no conflicts of interest regarding the contents of this article., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

63. Structural and biochemical insights into FKBP51 as a Hsp90 co-chaperone.

Author

Baischew A, Engel S, Geiger TM, Taubert MC, and Hausch F

Subjects

Humans, Animals, Molecular Chaperones metabolism, Molecular Chaperones chemistry, Receptors, Steroid metabolism, Receptors, Steroid chemistry, Tacrolimus Binding Proteins metabolism, Tacrolimus Binding Proteins chemistry, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins chemistry

Abstract

The FK506-binding protein 51 (FKBP51) is a high-molecular-weight immunophilin that emerged as an important drug target for stress-related disorders, chronic pain, and obesity. It has been implicated in a plethora of molecular pathways but remains best characterized as a co-chaperone of Hsp90 in the steroid hormone receptor (SHR) maturation cycle. However, the mechanistic and structural basis for the regulation of SHRs by FKBP51 and the usually antagonistic function compared with its closest homolog FKBP52 remains enigmatic. Here we review recent structural and biochemical studies of FKBPs as regulators in the Hsp90 machinery. These advances provide important insights into the roles of FKBP51 and FKBP52 in SHR regulation., (© 2023 The Authors. Journal of Cellular Biochemistry published by Wiley Periodicals LLC.)

Published

2024

64. Hyaluronic acid act as drug self-assembly chaperone and co-assembled with celalstrol for ameliorating non-alcoholic steatohepatitis.

Author

Zheng T, Gan X, Luo J, Shi Z, Zhao Y, Wang Y, Chen J, and Yu C

Subjects

Animals, Mice, Male, Triterpenes pharmacology, Triterpenes chemistry, Molecular Chaperones metabolism, Liver drug effects, Liver metabolism, Liver pathology, Humans, Hyaluronic Acid chemistry, Hyaluronic Acid pharmacology, Pentacyclic Triterpenes pharmacology, Pentacyclic Triterpenes chemistry, Non-alcoholic Fatty Liver Disease drug therapy, Non-alcoholic Fatty Liver Disease metabolism, Nanoparticles chemistry

Abstract

Nanoformulations of therapeutic drugs with diverse chemical structures are often complex to produce and lack a universal synthesis approach. Herein, we demonstrate that hyaluronic acid (HA) can function as an assembly chaperone, facilitating the formulation of various chemical compounds into nanoparticles without necessitating chemical modification. As a proof of concept, celastrol-HA co-assembled nanoparticles (CHNPs) were synthesized and utilized in the multifactorial treatment of non-alcoholic steatohepatitis (NASH). By simply blending an aqueous solution of HA and celastrol, we achieved the formation of homogeneous, stable, and biocompatible nanoparticles, effectively addressing the critical issues associated with celastrol's poor water solubility and high systemic toxicity. of celastrol. Ex vivo and in vivo experiments demonstrated that CHNPs ameliorated NASH by inhibiting macrophage M1 polarization, reducing liver inflammation and lipid deposition, and improving metabolic disorders. Furthermore, CHNPs reduced systemic toxicity and enhanced the bioavailability of celastrol. The simplicity of the HA-based nanoparticles may facilitate the development of translational nanomedicines., Competing Interests: Declaration of competing interest The authors declare no conflict of interests., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

65. A method for producing protease pS273R of the African swine fever virus.

Author

Kalinin DS, Mayorov SG, Zemskova MY, Latypov OR, Shlyapnikov MG, Gorshkova MA, Titova EN, Vlasova NN, Lipkin AV, Fedorov AN, and Granovsky IE

Subjects

Animals, Viral Proteases metabolism, Viral Proteases genetics, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Thioredoxins metabolism, Thioredoxins genetics, Swine, Endopeptidases metabolism, Endopeptidases genetics, Molecular Chaperones genetics, Molecular Chaperones metabolism, African Swine Fever Virus enzymology, African Swine Fever Virus genetics, Escherichia coli genetics, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism

Abstract

The pS273R protease of the African swine fever virus (ASFV) is responsible for the processing of the viral polyproteins pp220 and pp62, precursors of the internal capsid of the virus. The protease is essential for a productive viral infection and is an attractive target for antiviral therapy. This work presents a method for the production of pS273R in E. coli cells by fusing the protease with the SlyD chaperone. The chimeric protein pS273R protease, during expression, is formed in a soluble form possessing enzymatic activity. Subsequently, pS273R separates from SlyD through autocatalytic cleavage at the TEV protease site in vivo. This work devised a straightforward protocol for chromatographic purification, resulting in the production of a highly purified viral protease. Additionally, we suggest using a fluorescence method to assess the activity of pS273R. This method is predicated on a shift in the chimeric protein thioredoxin-EGFP's electrophoretic mobility following its protease cleavage. It was shown that thioredoxin-EGFP substrate is effectively and selectively cleaved by the pS273R protease, even in complex protein mixtures such as mammalian cell lysates., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

66. Generation of four human-derived iPSC TorsinA-3xFLAG reporter lines from a DYT-TOR1A patient.

Author

Tanzer K, Meier B, Vulinovic F, Pawlack H, Klein C, Seibler P, and Rakovic A

Subjects

Humans, Cell Line, CRISPR-Cas Systems, Cell Differentiation, Dystonia genetics, Dystonia metabolism, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells cytology, Molecular Chaperones metabolism, Molecular Chaperones genetics

Abstract

A 3-bp deletion (ΔGAG) in TOR1A is a common cause of early-onset isolated dystonia DYT-TOR1A. The exact disease mechanism remains unknown. Here we describe the generation and characterization of four TorsinA-3xFLAG reporter induced pluripotent cell (iPSC) lines derived from a DYT-TOR1A patient. The cell lines carry either a ΔGAG variant or a corrected allele and a mono- or biallelic 3xFLAG-Tag introduced using CRISPR/Cas9 technology. These cells provide an opportunity to study differential protein stability, subcellular localization, and interactors of endogenous WT or ΔE variants of TorsinA in iPSCs, neural progenitor cells (smNPC), and neurons., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

67. The molecular chaperone ALYREF promotes R-loop resolution and maintains genome stability.

Author

Bhandari J, Guillén-Mendoza C, Banks K, Eliaz L, Southwell S, Eyaa D, Luna R, Aguilera A, and Xue X

Subjects

Humans, Molecular Chaperones metabolism, Molecular Chaperones genetics, DEAD-box RNA Helicases metabolism, DEAD-box RNA Helicases genetics, HeLa Cells, Nuclear Proteins metabolism, Nuclear Proteins genetics, RNA-Binding Proteins metabolism, RNA-Binding Proteins genetics, HEK293 Cells, Genomic Instability, R-Loop Structures

Abstract

Unscheduled R-loops usually cause DNA damage and replication stress, and are therefore a major threat to genome stability. Several RNA processing factors, including the conserved THO complex and its associated RNA and DNA-RNA helicase UAP56, prevent R-loop accumulation in cells. Here, we investigate the function of ALYREF, an RNA export adapter associated with UAP56 and the THO complex, in R-loop regulation. We demonstrate that purified ALYREF promotes UAP56-mediated R-loop dissociation in vitro, and this stimulation is dependent on its interaction with UAP56 and R-loops. Importantly, we show that ALYREF binds DNA-RNA hybrids and R-loops. Consistently, ALYREF depletion causes R-loop accumulation and R-loop-mediated genome instability in cells. We propose that ALYREF, apart from its known role in RNA metabolism and export, is a key cellular R-loop coregulator, which binds R-loops and stimulates UAP56-driven resolution of unscheduled R-loops during transcription., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

68. Resolving chaperone-assisted protein folding on the ribosome at the peptide level.

Author

Wales TE, Pajak A, Roeselová A, Shivakumaraswamy S, Howell S, Kjær S, Hartl FU, Engen JR, and Balchin D

Subjects

Ribosomal Proteins metabolism, Ribosomal Proteins chemistry, Models, Molecular, Peptides metabolism, Peptides chemistry, Protein Conformation, Protein Biosynthesis, Peptidylprolyl Isomerase, Ribosomes metabolism, Protein Folding, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Escherichia coli Proteins chemistry, Molecular Chaperones metabolism, Molecular Chaperones chemistry, Tetrahydrofolate Dehydrogenase metabolism, Tetrahydrofolate Dehydrogenase chemistry

Abstract

Protein folding in vivo begins during synthesis on the ribosome and is modulated by molecular chaperones that engage the nascent polypeptide. How these features of protein biogenesis influence the maturation pathway of nascent proteins is incompletely understood. Here, we use hydrogen-deuterium exchange mass spectrometry to define, at peptide resolution, the cotranslational chaperone-assisted folding pathway of Escherichia coli dihydrofolate reductase. The nascent polypeptide folds along an unanticipated pathway through structured intermediates not populated during refolding from denaturant. Association with the ribosome allows these intermediates to form, as otherwise destabilizing carboxy-terminal sequences remain confined in the ribosome exit tunnel. Trigger factor binds partially folded states without disrupting their structure, and the nascent chain is poised to complete folding immediately upon emergence of the C terminus from the exit tunnel. By mapping interactions between the nascent chain and ribosomal proteins, we trace the path of the emerging polypeptide during synthesis. Our work reveals new mechanisms by which cellular factors shape the conformational search for the native state., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

69. The Hsp90 Molecular Chaperone as a Global Modifier of the Genotype-Phenotype-Fitness Map: An Evolutionary Perspective.

Author

Aguilar-Rodríguez J, Jakobson CM, and Jarosz DF

Subjects

Humans, Animals, Genetic Fitness, Epistasis, Genetic, Evolution, Molecular, Molecular Chaperones metabolism, Molecular Chaperones genetics, Selection, Genetic, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins genetics, Genotype, Phenotype

Abstract

Global modifier genes influence the mapping of genotypes onto phenotypes and fitness through their epistatic interactions with genetic variants on a massive scale. The first such factor to be identified, Hsp90, is a highly conserved molecular chaperone that plays a central role in protein homeostasis. Hsp90 is a "hub of hubs" that chaperones proteins engaged in many key cellular and developmental regulatory networks. These clients, which are enriched in kinases, transcription factors, and E3 ubiquitin ligases, drive diverse cellular functions and are themselves highly connected. By contrast to many other hub proteins, the abundance and activity of Hsp90 changes substantially in response to shifting environmental conditions. As a result, Hsp90 modifies the functional impact of many genetic variants simultaneously in a manner that depends on environmental stress. Studies in diverse organisms suggest that this coupling between Hsp90 function and challenging environments exerts a substantial impact on what parts of the genome are visible to natural selection, expanding adaptive opportunities when most needed. In this Perspective, we explore the multifaceted role of Hsp90 as global modifier of the genotype-phenotype-fitness map as well as its implications for evolution in nature and the clinic., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

70. Spontaneous and chaperone-assisted metal loading in the active site of protein phosphatase-1.

Author

Van der Hoeven G, Lemaire S, Cao X, Claes Z, Karamanou S, and Bollen M

Subjects

Humans, Iron metabolism, Iron chemistry, Manganese metabolism, Manganese chemistry, Hydrogen-Ion Concentration, Protein Phosphatase 1 metabolism, Protein Phosphatase 1 chemistry, Protein Phosphatase 1 genetics, Catalytic Domain, Zinc metabolism, Molecular Chaperones metabolism, Molecular Chaperones genetics, Molecular Chaperones chemistry

Abstract

Protein phosphatase PP1 has two active-site metals (Zn 2+ /Fe 2+ ) that are essential for catalysis. However, when expressed in bacteria, PP1 has two Mn 2+ -ions in its active site, indicating that the incorporation of Zn 2+ /Fe 2+ depends on additional eukaryotic component(s). Here, we used purified, metal-deficient PP1 to study metal incorporation. Fe 2+ was incorporated spontaneously, but Zn 2+ was not. Mn 2+ -incorporation at physiological pH depended on the co-expression of PP1 with PPP1R2 (Inhibitor-2) or PPP1R11 (Inhibitor-3), or a pre-incubation of PP1 at pH 4. We also demonstrate that PPP1R2 and PPP1R11 are Zn 2+ -binding proteins but are, by themselves, not able to load PP1 with Zn 2+ . Our data suggest that PPP1R2 and PPP1R11 function as metal chaperones for PP1 but depend on co-chaperone(s) and/or specific modification(s) for the transfer of associated Zn 2+ to PP1., (© 2024 The Author(s). FEBS Letters published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2024

71. Six induced pluripotent stem cell lines from fibroblasts of individuals with CLN3-related conditions.

Author

Dwojak E, O'Mard D, Zou J, Wassif CA, Burkett S, Eckhaus M, Rueda Faucz F, Padilla C, Villasmil R, Zheng W, and Dang Do AN

Subjects

Humans, Membrane Glycoproteins metabolism, Membrane Glycoproteins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Cell Line, Male, Female, Cell Differentiation, Cellular Reprogramming, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells cytology, Kruppel-Like Factor 4, Fibroblasts metabolism

Abstract

Primary fibroblasts from six individuals with CLN3-related conditions were used to generate induced pluripotent stem cell (iPSC) lines CHDTRi001-B, CHDTRi002-B, CHDTRi003-A, CHDTRi004-B, CHDTRi005-A, and CHDTRi006-E through the expression of four reprogramming factors: human OCT3/4, KLF4, SOX2, and c-MYC. The iPSC lines were characterized to confirm their pluripotency via immunocytochemistry, flow cytometry, and teratoma formation. Genomic stability, cell line identity, and CLN3 genotype were confirmed. These iPSC lines may be used as participant-derived experimental models for further investigation of CLN3, a rare, fatal, pediatric, blindness and neurodegenerative lysosomal disorder with no cure., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: An Ngoc Dang Do reports a relationship with NCL Stiftung that includes: board membership. An Ngoc Dang Do reports a relationship with Our Promise to Nicholas Foundation that includes: travel reimbursement. An Ngoc Dang Do reports a relationship with Beyond Batten Disease Foundation that includes: funding grants. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Published by Elsevier B.V.)

Published

2024

72. Anti-viral defence by an mRNA ADP-ribosyltransferase that blocks translation.

Author

Vassallo CN, Doering CR, and Laub MT

Subjects

Adenine metabolism, Adenine analogs & derivatives, Molecular Chaperones metabolism, Virus Replication, Escherichia coli Proteins metabolism, ADP Ribose Transferases metabolism, Capsid Proteins biosynthesis, Capsid Proteins genetics, Capsid Proteins immunology, Capsid Proteins metabolism, Escherichia coli enzymology, Escherichia coli immunology, Escherichia coli metabolism, Escherichia coli virology, Host-Pathogen Interactions immunology, Protein Biosynthesis, RNA, Messenger chemistry, RNA, Messenger genetics, RNA, Messenger metabolism, T-Phages genetics, T-Phages growth & development, T-Phages immunology, T-Phages metabolism

Abstract

Host-pathogen conflicts are crucibles of molecular innovation 1,2 . Selection for immunity to pathogens has driven the evolution of sophisticated immunity mechanisms throughout biology, including in bacterial defence against bacteriophages 3 . Here we characterize the widely distributed anti-phage defence system CmdTAC, which provides robust defence against infection by the T-even family of phages 4 . Our results support a model in which CmdC detects infection by sensing viral capsid proteins, ultimately leading to the activation of a toxic ADP-ribosyltransferase effector protein, CmdT. We show that newly synthesized capsid protein triggers dissociation of the chaperone CmdC from the CmdTAC complex, leading to destabilization and degradation of the antitoxin CmdA, with consequent liberation of the CmdT ADP-ribosyltransferase. Notably, CmdT does not target a protein, DNA or structured RNA, the known targets of other ADP-ribosyltransferases. Instead, CmdT modifies the N6 position of adenine in GA dinucleotides within single-stranded RNAs, leading to arrest of mRNA translation and inhibition of viral replication. Our work reveals a novel mechanism of anti-viral defence and a previously unknown but broadly distributed class of ADP-ribosyltransferases that target mRNA., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

73. Targeting Ser78 phosphorylation of Hsp27 achieves potent antiviral effects against enterovirus A71 infection.

Author

Wu M, Wan Q, Dan X, Wang Y, Chen P, Chen C, Li Y, Yao X, and He ML

Subjects

Phosphorylation, Humans, Enterovirus Infections virology, Enterovirus Infections metabolism, Antiviral Agents pharmacology, Viral Proteins metabolism, Viral Proteins genetics, Serine metabolism, HeLa Cells, Protein Biosynthesis, Cysteine Endopeptidases metabolism, Cysteine Endopeptidases genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Heat-Shock Proteins, Enterovirus A, Human drug effects, Enterovirus A, Human physiology, Enterovirus A, Human genetics, Virus Replication drug effects, Heterogeneous Nuclear Ribonucleoprotein A1 metabolism, Heterogeneous Nuclear Ribonucleoprotein A1 genetics, HSP27 Heat-Shock Proteins metabolism, HSP27 Heat-Shock Proteins genetics

Abstract

A positive-sense (+) single-stranded RNA (ssRNA) virus (e.g. enterovirus A71, EV-A71) depends on viral polypeptide translation for initiation of virus replication after entry. We reported that EV-A71 hijacks Hsp27 to induce hnRNP A1 cytosol redistribution to initiate viral protein translation, but the underlying mechanism is still elusive. Here, we show that phosphorylation-deficient Hsp27-3A (Hsp27 S15/78/82A ) and Hsp27 S78A fail to translocate into the nucleus and induce hnRNP A1 cytosol redistribution, while Hsp27 S15A and Hsp27 S82A display similar effects to the wild type Hsp27. Furthermore, we demonstrate that the viral 2A protease (2A pro ) activity is a key factor in regulating Hsp27/hnRNP A1 relocalization. Hsp27 S78A dramatically decreases the IRES activity and viral replication, which are partially reduced by Hsp27 S82A . However, Hsp27 S15A displays the same activity as the wild-type Hsp27. Peptide S78 potently suppresses EV-A71 protein translation and reproduction through blockage of EV-A71-induced Hsp27 phosphorylation and Hsp27/hnRNP A1 relocalization. A point mutation (S78A) on S78 impairs its inhibitory functions on Hsp27/hnRNP A1 relocalization and viral replication. Taken together, we demonstrate the importance of Ser78 phosphorylation of Hsp27 regulated by virus infection in nuclear translocation, hnRNP A1 cytosol relocation, and viral replication, suggesting a new path (such as peptide S78) for target-based antiviral strategy.

Published

2024

74. Bombyx mori UFBP1 regulates apoptosis and promotes BmNPV proliferation by affecting the expression of ER chaperone BmBIP.

Author

Meng H, Ai H, Li D, Jiang X, Zhang H, Xu J, and Huang S

Subjects

Animals, Endoplasmic Reticulum metabolism, Gene Expression Regulation, Cell Proliferation genetics, Signal Transduction, Nucleopolyhedroviruses, Bombyx genetics, Bombyx metabolism, Apoptosis genetics, Insect Proteins genetics, Insect Proteins metabolism, Molecular Chaperones metabolism, Molecular Chaperones genetics

Abstract

Ubiquitin-fold modifier 1 (UFM1) is attached to protein substrates through the sequential activity of an E1 (UBA5) - E2 (UFC1) - E3 (UFL1) cascade. UFBP1 is a conserved UFL1-interacting protein in mammals. However, to date, no study has been conducted on UFBP1 in silkworm. In this study, we identified a UFBP1 ortholog in the B. mori genome. Spatiotemporal expression profiles showed that BmUFBP1 expression was high in the midgut and fatbody, and at the moth stage. BmUFBP1 knockdown inhibited ER chaperone BmBIP expression and BmNPV proliferation, while BmUFBP1 overexpression increased BmNPV proliferation, and BmBIP rescued BmUFBP1-regulated BmNPV proliferation. Mechanistically, Apoptosis and ATF6 signaling are involved in BmUFBP1-regulated BmBIP expression and BmNPV proliferation. These results suggest that BmUFBP1 facilitates BmNPV proliferation via ATF6-BIP signaling, and provide a potential molecular target for BmNPV prevention and silkworm breeding., Competing Interests: Declaration of competing interest The authors declare no conflict of interest. The funders had no role in the design of the study, in the collection, analyses, or interpretation of data, in the writing of the manuscript, or in the decision to publish the results., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

75. Heat shock proteins in chronic pain: From molecular chaperones to pain modulators.

Author

Verma N, Chouhan D, Meghana A, and Tiwari V

Subjects

Humans, Animals, Analgesics pharmacology, Analgesics therapeutic use, Neuralgia metabolism, Neuralgia drug therapy, Chronic Pain metabolism, Chronic Pain drug therapy, Molecular Chaperones metabolism, Heat-Shock Proteins metabolism

Abstract

Chronic pain is the most prevalent and complex clinical disorder,affecting approximately 30% of people globally. Various intricate alterations in nociceptive pathways responsible for chronic pain are linked to long-term tissue damage or injury to the peripheral or central nervous systems. These include remolding in the phenotype of cells and fluctuations in the expression of proteins such as ion channels, neurotransmitters, and receptors. Heat shock proteins are important molecular chaperone proteins in cell responses to stress, including inflammation, neurodegeneration, and pain signaling. They play a key role in activating glial and endothelial cells and in the production of inflammatory mediators and excitatory amino acids in both peripheral and central nervous systems. In particular, they contribute to central sensitization and hyperactivation within the dorsal horn of the spinal cord. The expression of some HSPs plays a remarkable role in upregulating pain response by acting as scavengers of ROS, controlling inflammatory cytokines. Different HSPs act by different mechanisms and several important pathways have been implicated in targeting HSPs for the treatment of neuropathic pain including p38-mitogen-activated protein kinases (MAPKs), extracellular signal-regulated kinases (ERKs), brain-derived neurotrophic factors (BDNF). We summarize the role of HSPs in various preclinical and clinical studies and the crosstalk of HSPs with various nociceptors and other pain models. We also highlighted some artificial intelligence tools and machine learning-assisted drug discovery methods for rapid screening of HSPs in various diseases. Focusing on HSPs could lead to the development of new therapeutics that modulate pain responses and enhance our understanding of pain in various pathological conditions and neurological disorders., Competing Interests: Declaration of competing interest The authors declare no conflicts of interest. Also, it is certified that no materials were taken out of the literature verbatim or with minimal revisions., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2025

76. TanGIBLE: A selective probe for evaluating hydrophobicity-exposed defective proteins in live cells.

Author

Iwasa Y, Miyata S, Tomita T, Yokota N, Miyauchi M, Mori R, Matsushita S, Suzuki R, Saeki Y, and Kawahara H

Subjects

Humans, HeLa Cells, HEK293 Cells, Molecular Chaperones metabolism, Molecular Chaperones genetics, Peptides metabolism, Peptides chemistry, Ubiquitination, Protein Domains, Molecular Probes chemistry, Molecular Probes metabolism, Hydrophobic and Hydrophilic Interactions

Abstract

The accumulation of defective polypeptides in cells is a major cause of various diseases. However, probing defective proteins is difficult because no currently available method can retrieve unstable defective translational products in a soluble state. To overcome this issue, there is a need for a molecular device specific to structurally defective polypeptides. In this study, we developed an artificial protein architecture comprising tandemly aligned BAG6 Domain I, a minimum substrate recognition platform responsible for protein quality control. This tandem-aligned entity shows enhanced affinity not only for model defective polypeptides but also for endogenous polyubiquitinated proteins, which are sensitive to translational inhibition. Mass-spectrometry analysis with this probe enabled the identification of endogenous defective proteins, including orphaned subunits derived from multiprotein complexes and misassembled transmembrane proteins. This probe is also useful for the real-time visualization of protein foci derived from defective polypeptides in stressed cells. Therefore, this "new molecular trap" is a versatile tool for evaluating currently "invisible" pools of defective polypeptides as tangible entities., (© 2025 Iwasa et al.)

Published

2025

77. CCDC134 controls TLR biogenesis through the ER chaperone Gp96.

Author

Bernaleau L, Drobek M, Blank F, Walch P, Delacrétaz M, Drobek A, Monguió-Tortajada M, Broz P, Majer O, and Rebsamen M

Subjects

Humans, HEK293 Cells, Molecular Chaperones metabolism, Molecular Chaperones genetics, Animals, Toll-Like Receptors metabolism, Mice, Endoplasmic Reticulum-Associated Degradation, NF-kappa B metabolism, Lysosomes metabolism, Signal Transduction, Inflammation metabolism, Endoplasmic Reticulum metabolism, Membrane Glycoproteins metabolism, Membrane Glycoproteins genetics

Abstract

Toll-like receptors (TLRs) are central to initiate immune responses against invading pathogens. To ensure host defense while avoiding aberrant activation leading to pathogenic inflammation and autoimmune diseases, TLRs are tightly controlled by multilevel regulatory mechanisms. Through a loss-of-function genetic screen in a reporter cell line engineered to undergo cell death upon TLR7-induced IRF5 activation, we identified here CCDC134 as an essential factor for TLR responses. CCDC134 deficiency impaired endolysosomal TLR-induced NF-κB, MAPK, and IRF5 activation, as well as downstream production of proinflammatory cytokines and type I interferons. We further demonstrated that CCDC134 is an endoplasmic reticulum (ER)-resident interactor of Gp96 (HSP90B1/Grp94), an ER chaperone essential for folding and trafficking of plasma membrane and endolysosomal TLRs. CCDC134 controlled Gp96 stability as its loss led to Gp96 hyperglycosylation and ER-associated protein degradation (ERAD)-mediated clearance. Accordingly, CCDC134 deficiency impaired the folding, maturation, and trafficking of TLRs, resulting in blunted inflammatory responses upon stimulation. Altogether, this study reveals CCDC134 as a central regulator of the chaperone Gp96, thereby controlling TLR biogenesis and responses., (© 2024 Bernaleau et al.)

Published

2025

78. The combined effect of the gene copy number and chaperone overexpression on the recombinant bovine chymosin production in Pichia pastoris, with mutant ADH2 promoter.

Author

Ersöz F and İnan M

Subjects

Animals, Cattle, Gene Dosage, Molecular Chaperones genetics, Molecular Chaperones metabolism, Alcohol Dehydrogenase genetics, Alcohol Dehydrogenase metabolism, Protein Disulfide-Isomerases genetics, Protein Disulfide-Isomerases metabolism, Saccharomycetales genetics, Saccharomycetales metabolism, Cloning, Molecular methods, Chymosin genetics, Chymosin metabolism, Chymosin biosynthesis, Promoter Regions, Genetic, Recombinant Proteins genetics, Recombinant Proteins biosynthesis, Recombinant Proteins metabolism

Abstract

Chymosin is an enzyme used to coagulate milk, in the cheese industry. This study aimed to increase recombinant production of the chymosin in Pichia pastoris by determining the optimum copy number and overproduction of a Protein Disulfide Isomerase (PpPDI) chaperon protein. Bos taurus chymosin was expressed under the control of a mutant ADH2 promoter. The clones containing 1-4 gene copy numbers of the chymosin were constructed using the in vitro cloning method, and the effect of chaperone protein on chymosin secretion was investigated. The enzyme production levels are 4, 6.3, 4.5, and 3 IMCU/mL for 1, 2, 3, and 4-copy clones. The secreted chymosin levels increased up to two copies, and increasing the number of copies decreased the secretion level. Therefore, PpPDI was over-expressed in the clones regulated with the ADH2 promoter. The over-expression of PDI gene increased chymosin secretion in clones compared to the counterpart host. However, the highest chymosin level was obtained with C2 (2-copy chymosin containing clone; 6.3 IMCU/mL) and C2P2 (2-copy chymosin/2-copy PDI containing clone; 8.2 IMCU/mL). The maximum production was 39 IMCU/mL with the clone C2P2 in the fermenter scale production. The enzyme activity increased approximately 2-fold by adding two copies of the chaperone protein. The combined effect of gene copy number and chaperone overexpression on chymosin production was investigated. Two copies of the chymosin and PpPDI genes were the optimum among the tested clones., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2025

79. Thioredoxin 1 moonlights as a chaperone for an interbacterial ADP-ribosyltransferase toxin.

Author

Dumont B, Terradot L, Cascales E, Van Melderen L, and Jurėnas D

Subjects

Oxidation-Reduction, Protein Binding, Disulfides metabolism, Disulfides chemistry, Binding Sites, Cysteine metabolism, Cysteine chemistry, Models, Molecular, Escherichia coli metabolism, Escherichia coli genetics, Thioredoxins metabolism, Thioredoxins chemistry, Thioredoxins genetics, ADP Ribose Transferases metabolism, ADP Ribose Transferases chemistry, ADP Ribose Transferases genetics, Molecular Chaperones metabolism, Molecular Chaperones chemistry, Molecular Chaperones genetics, Bacterial Toxins metabolism, Bacterial Toxins chemistry

Abstract

Formation and breakage of disulfide bridges strongly impacts folding and activity of proteins. Thioredoxin 1 (TrxA) is a small, conserved enzyme that reduces disulfide bonds in the bacterial cytosol. In this study, we provide an example of the emergence of a chaperone role for TrxA, which is independent of redox catalysis. We show that the activity of the secreted bacterial ADP-ribosyltransferase (ART) toxin TreX, which does not contain any cysteines, is dependent on TrxA. TreX binds to the reduced form of TrxA via its carboxy-terminal extension to form a soluble and active complex. Structural studies revealed that TreX-like toxins are homologous to Scabin-like ART toxins which possess cysteine residues and form disulfide bridges at the position that superimposes the TrxA binding site in TreX. Our study therefore suggests that thioredoxin 1 evolved alternative functions by maintaining the interaction with cysteine-free substrates., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

80. The promiscuous biotin ligase TurboID reveals the proxisome of the T3SS chaperone IpgC in Shigella flexneri .

Author

Haidar-Ahmad N, Tomaro K, Lavallée-Adam M, and Campbell-Valois F-X

Subjects

Biotin metabolism, Carbon-Nitrogen Ligases metabolism, Carbon-Nitrogen Ligases genetics, Escherichia coli Proteins metabolism, Escherichia coli Proteins genetics, Repressor Proteins metabolism, Repressor Proteins genetics, Shigella flexneri genetics, Shigella flexneri metabolism, Shigella flexneri enzymology, Type III Secretion Systems metabolism, Type III Secretion Systems genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Bacterial Proteins metabolism, Bacterial Proteins genetics

Abstract

Promiscuous biotin ligases derived from the bacterial enzyme BirA are used to identify proteins vicinal to a bait protein, thereby defining its proxisome. Despite the popularity of this approach, surprisingly little is known about its use in prokaryotes. Here, we compared the activity of four widely used promiscuous biotin ligases in the cytoplasm of Shigella flexneri , a pathogenic subgroup of Escherichia coli . Our data indicate that the kinetics of TurboID's biotinylating activity is the highest of those tested. In addition, TurboID showed reduced interaction with the natural BirA binding partners, BccP and the biotin operator, when compared to its ancestor BioID. We therefore evaluated the ability of TurboID to probe the proxisome of the type III secretion system (T3SS) chaperone IpgC and the transcriptional activator MxiE. When the T3SS is inactive (off-state), these proteins are inhibited by forming complexes with the T3SS substrates OspD1 and IpaBC, respectively. In contrast, when the T3SS is active (on-state), OspD1 and IpaBC are secreted allowing MxiE and IpgC to interact together and activate their target genes. The results obtained with the IpgC and TurboID fusions capture a good fraction of these known interactions. It also suggests that the availability of IpgC increases in the on-state, resulting in a greater number of proteins detected in its vicinity. Among these is the T3SS ATPase SpaL (also known as Spa47 or SctN), further supporting the notion that chaperones escort their substrate to the T3SS. Interestingly, a specific subset of proteins conserved in E. coli completes the IpgC proxisome in the on-state.IMPORTANCEPromiscuous biotin ligases are widely used to study protein function in eukaryotes. Strikingly, their use in prokaryotes has been rare. Indeed, the small volume and the cytoplasmic location of the biotin ligase's natural binding partners in these organisms pose unique challenges that can interfere with the study of the proxisome of proteins of interest. Here, we evaluated four of the most common promiscuous biotin ligases and found TurboID was best suited for use in the cytoplasm of Shigella flexneri . Using this method, we extended the proxisome of IpgC beyond its known direct binding partners involved in the regulation of the type III secretion system (T3SS) signaling cascade. Of particular interest for further study are transcription factors and housekeeping proteins that are enriched around IpgC when the T3SS is active. We propose a model in which the increased availability of IpgC in the on-state may allow cross-talk of the T3SS with other cellular processes., Competing Interests: The authors declare no conflict of interest.

Published

2024

81. Threonine-rich carboxyl-terminal extension drives aggregation of stalled polypeptides.

Author

Chang WD, Yoon MJ, Yeo KH, and Choe YJ

Subjects

Protein Biosynthesis, Alanine metabolism, Alanine chemistry, Alanine genetics, Proteostasis, Heat-Shock Response, Molecular Chaperones metabolism, Molecular Chaperones genetics, Molecular Chaperones chemistry, RNA-Binding Proteins, Threonine metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae Proteins chemistry, Protein Aggregates, Ribosomes metabolism, Ribosomes genetics, Peptides metabolism, Peptides chemistry, Peptides genetics

Abstract

Ribosomes translating damaged mRNAs may stall and prematurely split into their large and small subunits. The split large ribosome subunits can continue elongating stalled polypeptides. In yeast, this mRNA-independent translation appends the C-terminal alanine/threonine tail (CAT tail) to stalled polypeptides. If not degraded by the ribosome-associated quality control (RQC), CAT-tailed stalled polypeptides form aggregates. How the CAT tail, a low-complexity region composed of alanine and threonine, drives protein aggregation remains unknown. In this study, we demonstrate that C-terminal polythreonine or threonine-enriched tails form detergent-resistant aggregates. These aggregates exhibit a robust seeding effect on shorter tails with lower threonine content, elucidating how heterogeneous CAT tails co-aggregate. Polythreonine aggregates sequester molecular chaperones, disturbing proteostasis and provoking the heat shock response. Furthermore, polythreonine cross-seeds detergent-resistant polyserine aggregation, indicating structural similarity between the two aggregates. This study identifies polythreonine and polyserine as a distinct group of aggregation-prone protein motifs., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

82. The inhibitory action of the chaperone BRICHOS against the α-Synuclein secondary nucleation pathway.

Author

Ghosh D, Torres F, Schneider MM, Ashkinadze D, Kadavath H, Fleischmann Y, Mergenthal S, Güntert P, Krainer G, Andrzejewska EA, Lin L, Wei J, Klotzsch E, Knowles T, and Riek R

Subjects

Humans, Amyloid metabolism, Amyloid chemistry, Protein Binding, Pulmonary Surfactant-Associated Protein C metabolism, Pulmonary Surfactant-Associated Protein C chemistry, Pulmonary Surfactant-Associated Protein C genetics, Kinetics, Magnetic Resonance Spectroscopy, Protein Domains, alpha-Synuclein metabolism, alpha-Synuclein chemistry, alpha-Synuclein genetics, Molecular Chaperones metabolism, Molecular Chaperones chemistry

Abstract

The complex kinetics of disease-related amyloid aggregation of proteins such as α-Synuclein (α-Syn) in Parkinson's disease and Aβ42 in Alzheimer's disease include primary nucleation, amyloid fibril elongation and secondary nucleation. The latter can be a key accelerator of the aggregation process. It has been demonstrated that the chaperone domain BRICHOS can interfere with the secondary nucleation process of Aβ42. Here, we explore the mechanism of secondary nucleation inhibition of the BRICHOS domain of the lung surfactant protein (proSP-C) against α-Syn aggregation and amyloid formation. We determine the 3D NMR structure of an inactive trimer of proSP-C BRICHOS and its active monomer using a designed mutant. Furthermore, the interaction between the proSP-C BRICHOS chaperone and a substrate peptide has been studied. NMR-based interaction studies of proSP-C BRICHOS with α-Syn fibrils show that proSP-C BRICHOS binds to the C-terminal flexible fuzzy coat of the fibrils, which is the secondary nucleation site on the fibrils. Super-resolution fluorescence microscopy demonstrates that proSP-C BRICHOS runs along the fibrillar axis diffusion-dependently sweeping off monomeric α-Syn from the fibrils. The observed mechanism explains how a weakly binding chaperone can inhibit the α-Syn secondary nucleation pathway via avidity where a single proSP-C BRICHOS molecule is sufficient against up to ~7-40 α-Syn molecules embedded within the fibrils., Competing Interests: Competing interests: The authors declare no competing interest., (© 2024. The Author(s).)

Published

2024

83. Mutation of CRYAB encoding a conserved mitochondrial chaperone and antiapoptotic protein causes hereditary optic atrophy.

Author

Wang C, Zhang L, Nie Z, Liang M, Liu H, Yi Q, Wang C, Ai C, Zhang J, Gao Y, Ji Y, and Guan MX

Subjects

Animals, Humans, Mice, Male, Female, Pedigree, Retinal Ganglion Cells pathology, Retinal Ganglion Cells metabolism, Mutation, Adult, Optic Atrophy, Autosomal Dominant genetics, Optic Atrophy, Autosomal Dominant pathology, Optic Atrophy, Autosomal Dominant metabolism, Molecular Chaperones genetics, Molecular Chaperones metabolism, Optic Atrophy genetics, Optic Atrophy pathology, Apoptosis genetics, alpha-Crystallin B Chain genetics, alpha-Crystallin B Chain metabolism, Mitochondria metabolism, Mitochondria genetics, Mitochondria pathology

Abstract

The degeneration of retinal ganglion cells (RGC) due to mitochondrial dysfunctions manifests optic neuropathy. However, the molecular components of RGC linked to optic neuropathy manifestations remain largely unknown. Here, we identified a potentially novel optic atrophy-causative CRYAB gene encoding a highly conserved major lens protein acting as mitochondrial chaperone and possessing antiapoptotic activities. The heterozygous CRYAB mutation (c.313G>A, p. Glu105Lys) was cosegregated with autosomal dominant inheritance of optic atrophy in 3 Chinese families. The p.E105K mutation altered the structure and function of CRYAB, including decreased stability, reduced formation of oligomers, and decreased chaperone activity. Coimmunoprecipitation indicated that the p.E105K mutation reduced the interaction of CRYAB with apoptosis-associated cytochrome c and voltage-dependent anion channel protein. The cell lines carrying the p.E105K mutation displayed promotion of apoptosis and defective assembly, stability, and activities of oxidative phosphorylation system as well as imbalance of mitochondrial dynamics. Involvement of CRYAB in optic atrophy was confirmed by phenotypic evaluations of Cryabp.E105K-knockin mice. These mutant mice exhibited ocular lesions that included alteration of intraretinal layers, degeneration of RGCs, photoreceptor deficits, and abnormal retinal vasculature. Furthermore, Cryab-deficient mice displayed elevated apoptosis and mitochondrial dysfunctions. Our findings provide insight of pathophysiology of optic atrophy arising from RGC degeneration caused by CRYAB deficiency-induced elevated apoptosis and mitochondrial dysfunctions.

Published

2024

84. Identification of phosphatases that dephosphorylate the co-chaperone BAG3.

Author

Kokot T, Zimmermann JP, Chand Y, Krier F, Reimann L, Scheinost L, Höfflin N, Esch A, Höhfeld J, Warscheid B, and Köhn M

Subjects

Humans, Phosphorylation, HEK293 Cells, 14-3-3 Proteins metabolism, Protein Phosphatase 1 metabolism, Molecular Chaperones metabolism, Protein Binding, Proteolysis, Proteostasis, Nuclear Proteins, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Apoptosis Regulatory Proteins metabolism, Phosphoprotein Phosphatases metabolism

Abstract

The co-chaperone BAG3 plays critical roles in maintaining cellular proteostasis. It associates with 14-3-3 proteins during the trafficking of aggregation-prone proteins and facilitates their degradation through chaperone-assisted selective autophagy in cooperation with small heat shock proteins. Although reversible phosphorylation regulates BAG3 function, the involved phosphatases remain unknown. Here, we used affinity purification mass spectrometry to identify phosphatases that target BAG3. Of the hits, we evaluated the involvement of protein phosphatase-1 (PP1) using chemical inhibitors and activators in in vitro and cellular approaches. Our results demonstrate that PP1 can dephosphorylate BAG3-pS136 in cells and counteract 14-3-3γ association with BAG3 at this motif. Furthermore, protein phosphatase-5 (PP5) co-enriched with proteostasis-related proteins, and it has the capacity to dephosphorylate a BAG3 phosphorylation-site cluster regulating the interaction of BAG3 with small heat shock proteins and BAG3-mediated protein degradation. Our findings provide new insights into the regulation of BAG3 by phosphatases. This paves the way for future research focused on the precise control of BAG3 function through its regulatory proteins, potentially holding therapeutic promise for diseases characterized by disrupted proteostasis., (© 2024 Kokot et al.)

Published

2024

85. Cotranslational molecular condensation of cochaperones and assembly factors facilitates axonemal dynein biogenesis.

Author

Li Y, Xu W, Cheng Y, Djenoune L, Zhuang C, Cox AL, Britto CJ, Yuan S, Wang S, and Sun Z

Subjects

Molecular Chaperones metabolism, Molecular Chaperones genetics, RNA, Messenger metabolism, RNA, Messenger genetics, Axoneme metabolism, Protein Biosynthesis, Chlamydomonas reinhardtii metabolism, Chlamydomonas reinhardtii genetics, Axonemal Dyneins metabolism, Axonemal Dyneins genetics

Abstract

Axonemal dynein, the macromolecular machine that powers ciliary motility, assembles in the cytosol with the help of dynein axonemal assembly factors (DNAAFs). These DNAAFs localize in cytosolic foci thought to form via liquid-liquid phase separation. However, the functional significance of DNAAF foci formation and how the production and assembly of multiple components are so efficiently coordinated, at such enormous scale, remain unclear. Here, we unveil an axonemal dynein production and assembly hub enriched with translating heavy chains (HCs) and DNAAFs. We show that mRNAs encoding interacting HCs of outer dynein arms colocalize in cytosolic foci, along with nascent HCs. The formation of these mRNA foci and their colocalization relies on HC translation. We observe that a previously identified DNAAF assembly, containing the DNAAF Lrrc6 and cochaperones Ruvbl1 and Ruvbl2, colocalizes with these HC foci, and is also dependent on HC translation. We additionally show that Ruvbl1 is required for the recruitment of Lrrc6 into the HC foci and that both proteins function cotranslationally. We propose that these DNAAF foci are anchored by stable interactions between translating HCs, ribosomes, and encoding mRNAs, followed by cotranslational molecular condensation of cochaperones and assembly factors, providing a potential mechanism that coordinates HC translation, folding, and assembly at scale., Competing Interests: Competing interests statement:S.W. is a shareholder and consultant of Translura, Inc. The remaining authors declare no competing interests.

Published

2024

86. TSG101 depletion dysregulates mitochondria and PML NBs, triggering MAD2-overexpressing interphase cell death (MOID) through AIFM1-PML-DAXX pathway.

Author

Xi Y, Xu R, Chen S, Fang J, Duan X, Zhang Y, Zhong G, He Z, Guo Y, Li X, Tao W, Li Y, Li Y, Fang L, and Niikura Y

Subjects

Humans, Molecular Chaperones metabolism, Molecular Chaperones genetics, Promyelocytic Leukemia Protein metabolism, Promyelocytic Leukemia Protein genetics, Interphase, Phosphorylation, Cell Death, Signal Transduction, HeLa Cells, Tumor Suppressor Proteins metabolism, Tumor Suppressor Proteins genetics, Autophagy, Transcription Factors metabolism, Transcription Factors genetics, DNA-Binding Proteins metabolism, DNA-Binding Proteins genetics, Mitochondria metabolism, Nuclear Proteins metabolism, Nuclear Proteins genetics, Co-Repressor Proteins metabolism, Co-Repressor Proteins genetics, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Endosomal Sorting Complexes Required for Transport metabolism, Endosomal Sorting Complexes Required for Transport genetics, Mad2 Proteins metabolism, Mad2 Proteins genetics

Abstract

Overexpression of mitotic arrest deficiency 2 (MAD2/MAD2L1), a pivotal component of the spindle assembly checkpoint (SAC), resulted in many types of cancer. Here we show that the depletion of tumor susceptibility gene 101 (TSG101), causes synthetic dosage lethality (SDL) in MAD2-overexpressing cells, and we term this cell death MAD2-overexpressing interphase cell death (MOID). The induction of MOID depends on PML and DAXX mediating mitochondrial AIFM1-release. MAD2, TSG101, and AIF-PML-DAXX axis regulate mitochondria, PML nuclear bodies (NBs), and autophagy with close inter-dependent protein stability in survival cells. Loss of C-terminal phosphorylation(s) of TSG101 and closed (C-)MAD2-overexpression contribute to induce MOID. In survival cells, both MAD2 and TSG101 localize at PML NBs in interphase, and TSG101 Y390 phosphorylation is required for localization of TSG101 to PML NBs. PML release from PML NBs through PML deSUMOylation contributes to induce MOID. The post-transcriptional/translational cell death machinery and the non-canonical transcriptional regulation are intricately linked to MOID, and ER-MAM, may serve as a crucial intersection for MOID signaling., Competing Interests: Competing interests The authors declare no competing interests. Ethics approval and consent to participate All methods were performed in accordance with the relevant guidelines and regulations. The Ethics Committee at Model Animal Research Center of Nanjing University approved the animal protocols used in this study (reference/registration number: IACUC-D2108001). No human research participants are involved in this study., (© 2024. The Author(s).)

Published

2024

87. Modification of Regulatory Tyrosine Residues Biases Human Hsp90α in its Interactions with Cochaperones and Clients.

Author

Huo Y, Karnawat R, Liu L, Knieß RA, Groß M, Chen X, and Mayer MP

Subjects

Humans, Phosphorylation, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae genetics, Chaperonins metabolism, Chaperonins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Hep G2 Cells, Cell Cycle Proteins metabolism, Cell Cycle Proteins genetics, Prostaglandin-E Synthases metabolism, Prostaglandin-E Synthases genetics, Heat-Shock Proteins metabolism, Heat-Shock Proteins genetics, Homeodomain Proteins, Tumor Suppressor Proteins, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins genetics, Tyrosine metabolism, Tyrosine genetics, Protein Processing, Post-Translational, Protein Binding

Abstract

The highly conserved Hsp90 chaperones control stability and activity of many essential signaling and regulatory proteins including many protein kinases, E3 ligases and transcription factors. Thereby, Hsp90s couple cellular homeostasis of the proteome to cell fate decisions. High-throughput mass spectrometry revealed 178 and 169 posttranslational modifications (PTMs) for human cytosolic Hsp90α and Hsp90β, but for only a few of the modifications the physiological consequences are investigated in some detail. In this study, we explored the suitability of the yeast model system for the identification of key regulatory residues in human Hsp90α. Replacement of three tyrosine residues known to be phosphorylated by phosphomimetic glutamate and by non-phosphorylatable phenylalanine individually and in combination influenced yeast growth and the maturation of 7 different Hsp90 clients in distinct ways. Furthermore, wild-type and mutant Hsp90 differed in their ability to stabilize known clients when expressed in HepG2 HSP90AA1 -/- cells. The purified mutant proteins differed in their interaction with the cochaperones Aha1, Cdc37, Hop and p23 and in their support of the maturation of glucocorticoid receptor ligand binding domain in vitro. In vivo and in vitro data correspond well to each other confirming that the yeast system is suitable for the identification of key regulatory sites in human Hsp90s. Our findings indicate that even closely related clients are affected differently by the amino acid replacements in the investigated positions, suggesting that PTMs could bias Hsp90s client specificity., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

88. The role of the co-chaperone DNAJB11 in polycystic kidney disease: Molecular mechanisms and cellular origin of cyst formation.

Author

Busch T, Neubauer B, Schmitt L, Cascante I, Knoblich L, Wegehaupt O, Schöler F, Tholen S, Hofherr A, Schell C, Schilling O, Westermann L, and Köttgen M

Subjects

Animals, Mice, TRPP Cation Channels metabolism, TRPP Cation Channels genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Humans, Polycystic Kidney Diseases metabolism, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases pathology, Endoplasmic Reticulum metabolism, Male, Female, Mice, Inbred C57BL, Mice, Knockout, Cysts metabolism, Cysts pathology, Cysts genetics, HSP40 Heat-Shock Proteins metabolism, HSP40 Heat-Shock Proteins genetics, Polycystic Kidney, Autosomal Dominant metabolism, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant pathology

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is caused by mutations in PKD1 and PKD2, encoding polycystin-1 (PC1) and polycystin-2 (PC2), which are required for the regulation of the renal tubular diameter. Loss of polycystin function results in cyst formation. Atypical forms of ADPKD are caused by mutations in genes encoding endoplasmic reticulum (ER)-resident proteins through mechanisms that are not well understood. Here, we investigate the function of DNAJB11, an ER co-chaperone associated with atypical ADPKD. We generated mouse models with constitutive and conditional Dnajb11 inactivation and Dnajb11-deficient renal epithelial cells to investigate the mechanism underlying autosomal dominant inheritance, the specific cell types driving cyst formation, and molecular mechanisms underlying DNAJB11-dependent polycystic kidney disease. We show that biallelic loss of Dnajb11 causes cystic kidney disease and fibrosis, mirroring human disease characteristics. In contrast to classical ADPKD, cysts predominantly originate from proximal tubules. Cyst formation begins in utero and the timing of Dnajb11 inactivation strongly influences disease severity. Furthermore, we identify impaired PC1 cleavage as a potential mechanism underlying DNAJB11-dependent cyst formation. Proteomic analysis of Dnajb11- and Pkd1-deficient cells reveals common and distinct pathways and dysregulated proteins, providing a foundation to better understand phenotypic differences between different forms of ADPKD., (© 2024 The Author(s). The FASEB Journal published by Wiley Periodicals LLC on behalf of Federation of American Societies for Experimental Biology.)

Published

2024

89. Chaperoning system: Intriguing target to modulate the expression of CFTR in cystic fibrosis.

Author

Scalia F, Culletta G, Barreca M, Caruso Bavisotto C, Bivacqua R, D'Amico G, Alberti G, Spanò V, Tutone M, Almerico AM, Cappello F, Montalbano A, and Barraja P

Subjects

Humans, Molecular Chaperones metabolism, Protein Folding drug effects, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins antagonists & inhibitors, Animals, Chaperonin 60 metabolism, Chaperonin 60 chemistry, Chaperonin 60 antagonists & inhibitors, HSP70 Heat-Shock Proteins metabolism, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Cystic Fibrosis drug therapy, Cystic Fibrosis metabolism, Cystic Fibrosis genetics

Abstract

The correction of protein folding is fundamental for cellular functionality and its failure can lead to severe diseases. In this context, molecular chaperones are crucial players involved in the tricky process of assisting in protein folding, stabilization, and degradation. Chaperones, such as heat shock proteins (HSP) 90, 70, and 60, operate within complex systems, interacting with co-chaperones both to prevent protein misfolding and direct to the correct folding. Chaperone targeting drugs could represent a challenging approach for the treatment of cystic fibrosis (CF), an autosomal recessive genetic disease caused by mutations in the CFTR gene, encoding for the CFTR chloride channel. In this review, we discuss the potential role of molecular chaperones as proteostasis modulators affecting CFTR biogenesis. In particular, we focused on HSP90 and HSP70, for their key role in CFTR folding and trafficking, as well as on HSP60 for its involvement in the inflammation process., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Masson SAS. All rights reserved.)

Published

2024

90. Dosage constraint of the ribosome-associated molecular chaperone drives the evolution and fates of its duplicates in bacteria.

Author

Wan T, Zhuo L, Pan Z, Chen R-y, Ma H, Cao Y, Wang J, Wang J-j, Hu W-f, Lai Y-j, Hayat M, and Li Y-z

Subjects

Bacteria metabolism, Bacteria genetics, Bacterial Proteins metabolism, Bacterial Proteins genetics, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, Gene Dosage, Escherichia coli genetics, Escherichia coli metabolism, Peptidylprolyl Isomerase, Ribosomes metabolism, Ribosomes genetics, Gene Duplication, Evolution, Molecular, Molecular Chaperones metabolism, Molecular Chaperones genetics

Abstract

Gene duplication events happen prevalently during evolution, and the mechanisms governing the loss or retention of duplicated genes are mostly elusive. Our genome scanning analysis revealed that trigger factor (TF), the one and only bacterial ribosome-associated molecular chaperone, is singly copied in virtually every bacterium except for a very few that possess two or more copies. However, even in these exceptions, only one complete TF copy exists, while other homologs lack the N-terminal domain that contains the conserved ribosome binding site (RBS) motif. Consistently, we demonstrated that the overproduction of the N-terminal complete TF proteins is detrimental to the cell, which can be rescued by removing the N-terminal domain. Our findings also indicated that TF overproduction leads to a decrease in protein productivity and profile changes in proteome due to its characteristic ribosome binding and holdase activities. Additionally, these N-terminal deficient TF homologs in bacteria with multiple TF homologs partition the function of TF via subfunctionalization. Our results revealed that TF is subjected to a dosage constraint that originates from its own intrinsic functions, which may drive the evolution and fates of duplicated TFs in bacteria., Importance: Gene duplication events presumably occur in tig , which encodes the ribosome-associated molecular chaperone trigger factor (TF). However, TF is singly copied in virtually every bacterium, and these exceptions with multiple TF homologs always retain only one complete copy while other homologs lack the N-terminal domain. Here, we reveal the manner and mechanism underlying the evolution and fates of TF duplicates in bacteria. We discovered that the mutation-to-loss or retention-to-sub/neofunctionalization of TF duplicates is associated with the dosage constraint of N-terminal complete TF. The dosage constraint of TF is attributed to its characteristic ribosome binding and substrate-holding activities, causing a decrease in protein productivity and profile changes in cellular proteome., Competing Interests: The authors declare no conflict of interest.

Published

2024

91. STAP2 promotes the progression of renal fibrosis via HSP27.

Author

Yuan Y, Wei X, Xiong X, Wang X, Jiang W, Kuang Q, Zhu K, Chen C, Gan J, Li J, Yang J, Li L, and Luo P

Subjects

Animals, Humans, Male, Proto-Oncogene Proteins c-akt metabolism, Mice, Epithelial-Mesenchymal Transition, Adaptor Proteins, Signal Transducing metabolism, Phosphatidylinositol 3-Kinases metabolism, Disease Models, Animal, Reperfusion Injury pathology, Reperfusion Injury metabolism, Mice, Knockout, Kidney Diseases pathology, Kidney Diseases metabolism, Molecular Chaperones metabolism, Fibrosis, HSP27 Heat-Shock Proteins metabolism, HSP27 Heat-Shock Proteins genetics, Disease Progression, Mice, Inbred C57BL, Kidney pathology, Kidney metabolism, Signal Transduction

Abstract

Background: Renal fibrosis is a key process in the progression from acute kidney injury (AKI) to chronic kidney disease (CKD), while the intricate mechanisms of renal fibrosis remain obscure. While the signal-transducing adaptor protein 2 (STAP2) was well-studied for its notable function in inflammation and immune-related disorders, its specific implication in renal fibrosis remains unclear. This study assessed the mechanism by which STAP2 could promote the progression of renal fibrosis., Methods: The expression level of STAP2 in fibrotic human samples, murine fibrosis models, and cellular fibrosis models was measured, respectively. Subsequently, immunoprecipitation (IP), mass spectrometry, and RNA sequencing (RNA-seq) were employed to identify HSP27 as an interacting protein and the PI3K-AKT signaling pathway. STAP2 was thereafter knocked down or overexpressed in both in vivo and in vitro models to assess the expression levels of pathway-related and fibrosis-related proteins. Finally, the important role of STAP2 in the fibrosis process in animal models induced by ischemia-reperfusion injury (IRI) and cisplatin was validated., Results: Functionally, in vivo assays demonstrated that the genetic knockout of STAP2 could remarkably mitigate epithelial-mesenchymal transition (EMT), diminish inflammatory cell infiltration, and reduce collagen deposition in mice with renal fibrosis. Conversely, in vitro assays employing STAP2-overexpressing cell models exacerbated the expression levels of fibrosis markers. The outcomes uncovered a potential mechanism by which STAP2 could modulate renal fibrosis through its impact on the expression level of phosphorylated HSP27, as well as modulating the PI3K/AKT signaling pathway., Conclusions: This comprehensive investigation delineated the noticeable function of STAP2 in the advancement of renal fibrosis, and the outcomes might contribute to the development of targeted therapies concentrated on STAP2 to mitigate renal fibrosis., Competing Interests: Declarations Ethical approval Animal experiments were approved by Experimental Animal Ethics Committee of Wuhan Third Hospital (WuSanYiShiLun SY2023-003). Collected clinical samples and conducted clinical research were approved by Ethics Committee of Wuhan Third Hospital (WuSanYiLun KY2023-057) and Ethics Committee of Huangshi Central Hospital (2024-17). Conflict of interest The authors confirmed the absence of conflict of interest., (© 2024. The Author(s).)

Published

2024

92. Regulated N-glycosylation controls chaperone function and receptor trafficking.

Author

Ma M, Dubey R, Jen A, Pusapati GV, Singal B, Shishkova E, Overmyer KA, Cormier-Daire V, Fedry J, Aravind L, Coon JJ, and Rohatgi R

Subjects

Glycosylation, Humans, Receptor, IGF Type 1 metabolism, HSP90 Heat-Shock Proteins metabolism, HSP90 Heat-Shock Proteins genetics, Animals, Wnt Signaling Pathway, Mice, Protein Folding, HEK293 Cells, Endoplasmic Reticulum metabolism, Protein Transport, Hexosyltransferases metabolism, Hexosyltransferases genetics, Membrane Proteins metabolism, Membrane Proteins genetics, Molecular Chaperones metabolism

Abstract

One-fifth of human proteins are N-glycosylated in the endoplasmic reticulum (ER) by two oligosaccharyltransferases, OST-A and OST-B. Contrary to the prevailing view of N-glycosylation as a housekeeping function, we identified an ER pathway that modulates the activity of OST-A. Genetic analyses linked OST-A to HSP90B1, an ER chaperone for membrane receptors, and CCDC134, an ER luminal protein. During its translocation into the ER, an N-terminal peptide in HSP90B1 templates the assembly of a translocon complex containing CCDC134 and OST-A that protects HSP90B1 during folding, preventing its hyperglycosylation and degradation. Disruption of this pathway impairs WNT and IGF1R signaling and causes the bone developmental disorder osteogenesis imperfecta. Thus, N-glycosylation can be regulated by specificity factors in the ER to control cell surface receptor signaling and tissue development.

Published

2024

93. Modulating metal-centered dimerization of a lanthanide chaperone protein for separation of light lanthanides.

Author

Larrinaga WB, Jung JJ, Lin CY, Boal AK, and Cotruvo JA Jr

Subjects

Protein Multimerization, Molecular Chaperones metabolism, Molecular Chaperones chemistry, Methylobacterium extorquens metabolism, Methylobacterium extorquens genetics, Binding Sites, Lanthanoid Series Elements chemistry, Lanthanoid Series Elements metabolism, Bacterial Proteins metabolism, Bacterial Proteins chemistry, Bacterial Proteins genetics

Abstract

Elucidating details of biology's selective uptake and trafficking of rare earth elements, particularly the lanthanides, has the potential to inspire sustainable biomolecular separations of these essential metals for myriad modern technologies. Here, we biochemically and structurally characterize Methylobacterium ( Methylorubrum ) extorquens LanD, a periplasmic protein from a bacterial gene cluster for lanthanide uptake. This protein provides only four ligands at its surface-exposed lanthanide-binding site, allowing for metal-centered protein dimerization that favors the largest lanthanide, La III . However, the monomer prefers Nd III and Sm III , which are disfavored lanthanides for cellular utilization. Structure-guided mutagenesis of a metal-ligand and an outer-sphere residue weakens metal binding to the LanD monomer and enhances dimerization for Pr III and Nd III by 100-fold. Selective dimerization enriches high-value Pr III and Nd III relative to low-value La III and Ce III in an all-aqueous process, achieving higher separation factors than lanmodulins and comparable or better separation factors than common industrial extractants. Finally, we show that LanD interacts with lanmodulin (LanM), a previously characterized periplasmic protein that shares LanD's preference for Nd III and Sm III . Our results suggest that LanD's unusual metal-binding site transfers less-desirable lanthanides to LanM to siphon them away from the pathway for cytosolic import. The properties of LanD show how relatively weak chelators can achieve high selectivity, and they form the basis for the design of protein dimers for separation of adjacent lanthanide pairs and other metal ions., Competing Interests: Competing interests statement:J.A.C. has a financial interest in REETerra, Inc. W.B.L., J.J.J., C.-Y.L., A.K.B., and J.A.C. are inventors on patent applications filed by the Pennsylvania State University related to this work.

Published

2024

94. Genetic and Cellular Basis of Impaired Phagocytosis and Photoreceptor Degeneration in CLN3 Disease.

Author

Han J, Chear S, Talbot J, Swier V, Booth C, Reuben-Thomas C, Dalvi S, Weimer JM, Hewitt AW, Cook AL, and Singh R

Subjects

Humans, Animals, Retinal Degeneration genetics, Retinal Degeneration metabolism, Retinal Degeneration pathology, Retinal Degeneration physiopathology, Mutation, Retinal Pigment Epithelium pathology, Retinal Pigment Epithelium metabolism, Blotting, Western, Induced Pluripotent Stem Cells metabolism, Retinal Photoreceptor Cell Outer Segment pathology, Retinal Photoreceptor Cell Outer Segment metabolism, Cells, Cultured, Immunohistochemistry, Phagocytosis physiology, Neuronal Ceroid-Lipofuscinoses genetics, Neuronal Ceroid-Lipofuscinoses pathology, Electroretinography, Membrane Glycoproteins genetics, Membrane Glycoproteins metabolism, Molecular Chaperones genetics, Molecular Chaperones metabolism, Tomography, Optical Coherence

Abstract

Purpose: CLN3 Batten disease (also known as juvenile neuronal ceroid lipofuscinosis) is a lysosomal storage disorder that typically initiates with retinal degeneration but is followed by seizure onset, motor decline and premature death. Patient-derived CLN3 disease induced pluripotent stem cell-RPE cells show defective phagocytosis of photoreceptor outer segment (POS). Because modifier genes are implicated in CLN3 disease, our goal here was to investigate a direct link between CLN3 mutation and POS phagocytosis defect., Methods: Isogenic control and CLN3 mutant stem cell lines were generated by CRISPR-Cas9-mediated biallelic deletion of exons 7 and 8. A transgenic CLN3Δ7-8/Δ7-8 (CLN3) Yucatan miniswine was also used to study the impact of CLN3Δ7-8/Δ7-8 mutation on POS phagocytosis. POS phagocytosis by cultured RPE cells was analyzed by Western blotting and immunohistochemistry. Electroretinogram, optical coherence tomography and histological analysis of CLN3Δ7-8/Δ7-8 and wild-type miniswine eyes were carried out at 6, 36, or 48 months of age., Results: CLN3Δ7-8/Δ7-8 RPE (CLN3 RPE) displayed decreased POS binding and consequently decreased uptake of POS compared with isogenic control RPE cells. Furthermore, wild-type miniswine RPE cells phagocytosed CLN3Δ7-8/Δ7-8 POS less efficiently than wild-type POS. Consistent with decreased POS phagocytosis, lipofuscin/autofluorescence was decreased in CLN3 miniswine RPE at 36 months of age and was followed by almost complete loss of photoreceptors at 48 months of age., Conclusions: CLN3Δ7-8/Δ7-8 mutation (which affects ≤85% of patients) affects both RPE and POS and leads to photoreceptor cell loss in CLN3 disease. Furthermore, both primary RPE dysfunction and mutant POS independently contribute to impaired POS phagocytosis in CLN3 disease.

Published

2024

95. Molecular interactions of the chaperone CcmS and carboxysome shell protein CcmK1 that mediate β-carboxysome assembly.

Author

Cheng J, Li CY, Meng M, Li JX, Liu SJ, Cao HY, Wang N, Zhang YZ, and Liu LN

Subjects

Ribulose-Bisphosphate Carboxylase metabolism, Ribulose-Bisphosphate Carboxylase chemistry, Ribulose-Bisphosphate Carboxylase genetics, Nostoc metabolism, Nostoc genetics, Crystallography, X-Ray, Organelles metabolism, Models, Molecular, Bacterial Proteins metabolism, Bacterial Proteins chemistry, Bacterial Proteins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Molecular Chaperones chemistry

Abstract

The carboxysome is a natural proteinaceous organelle for carbon fixation in cyanobacteria and chemoautotrophs. It comprises hundreds of protein homologs that self-assemble to form a polyhedral shell structure to sequester cargo enzymes, ribulose 1,5-bisphosphate carboxylase/oxygenase (Rubisco), and carbonic anhydrases. How these protein components assemble to construct a functional carboxysome is a central question in not only understanding carboxysome structure and function but also synthetic engineering of carboxysomes for biotechnological applications. Here, we determined the structure of the chaperone protein CcmS, which has recently been identified to be involved in β-carboxysome assembly, and its interactions with β-carboxysome proteins. The crystal structure at 1.99 Å resolution reveals CcmS from Nostoc sp. PCC 7120 forms a homodimer, and each CcmS monomer consists of five α-helices and four β-sheets. Biochemical assays indicate that CcmS specifically interacts with the C-terminal extension of the carboxysome shell protein CcmK1, but not the shell protein homolog CcmK2 or the carboxysome scaffolding protein CcmM. Moreover, we solved the structure of a stable complex of CcmS and the C-terminus of CcmK1 at 1.67 Å resolution and unveiled how the CcmS dimer interacts with the C-terminus of CcmK1. These findings allowed us to propose a model to illustrate CcmS-mediated β-carboxysome assembly by interacting with CcmK1 at the outer shell surface. Collectively, our study provides detailed insights into the accessory factors that drive and regulate carboxysome assembly, thereby improving our knowledge of carboxysome structure, function, and bioengineering., Competing Interests: Conflict of interest statement. None declared., (© The Author(s) 2024. Published by Oxford University Press on behalf of American Society of Plant Biologists.)

Published

2024

96. The chloroplast protease system degrades stromal DUF760-1 and DUF760-2 domain-containing proteins at different rates.

Author

Yuan B and van Wijk KJ

Subjects

Endopeptidase Clp metabolism, Endopeptidase Clp genetics, Proteolysis, Plants, Genetically Modified, Mutation genetics, Protein Domains, Molecular Chaperones metabolism, Molecular Chaperones genetics, Chloroplast Proteins metabolism, Chloroplast Proteins genetics, Arabidopsis genetics, Arabidopsis metabolism, Arabidopsis Proteins metabolism, Arabidopsis Proteins genetics, Chloroplasts metabolism

Abstract

The chloroplast chaperone CLPC1 aids to select, unfold, and deliver hundreds of proteins to the CLP protease for degradation. Through in vivo CLPC1, trapping we previously identified dozens of proteins that are (potential) substrate adaptors or substrates for the CLP chaperone-protease system. In this study, we show that two of these highly trapped proteins, DUF760-1 and DUF760-2, are substrates for the CLP protease in Arabidopsis (Arabidopsis thaliana). Loss-of-function mutants and transgenic plants were created for phenotyping, protein expression, and localization using immunoblotting and confocal microscopy. In planta BiFC, cycloheximide chase assays, and yeast 2-hybrid analyses were conducted to determine protein interactions and protein half-life. Both DUF760 proteins directly interacted with the N-domain of CLPC1 and both were highly enriched in clpc1-1 and clpr2-1 mutants. Accordingly, in vivo cycloheximide chase assays demonstrated that both DUF760 proteins are degraded by the CLP protease. The half-life of DUF760-1 was 4 to 6 h, whereas DUF760-2 was highly unstable and difficult to detect unless CLP proteolysis was inhibited. Null mutants for DUF760-1 and DUF760-2 showed weak but differential pigment phenotypes and differential sensitivity to protein translation inhibitors. This study demonstrates that DUF760-1 and DUF760-2 are substrates of the CLP chaperone-protease system and excellent candidates for the determination of CLP substrate degrons., Competing Interests: Conflict of interest statement. None declared., (© The Author(s) 2024. Published by Oxford University Press on behalf of American Society of Plant Biologists. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published

2024

97. Periplasmic Chaperones: Outer Membrane Biogenesis and Envelope Stress.

Author

Combs AN and Silhavy TJ

Subjects

Bacterial Outer Membrane metabolism, Bacterial Outer Membrane Proteins metabolism, Bacterial Outer Membrane Proteins genetics, Cell Membrane metabolism, Escherichia coli Proteins metabolism, Escherichia coli Proteins genetics, Homeostasis, Stress, Physiological, Escherichia coli cytology, Escherichia coli genetics, Escherichia coli metabolism, Molecular Chaperones metabolism, Molecular Chaperones genetics, Periplasm metabolism

Abstract

Envelope biogenesis and homeostasis in gram-negative bacteria are exceptionally intricate processes that require a multitude of periplasmic chaperones to ensure cellular survival. Remarkably, these chaperones perform diverse yet specialized functions entirely in the absence of external energy such as ATP, and as such have evolved sophisticated mechanisms by which their activities are regulated. In this article, we provide an overview of the predominant periplasmic chaperones that enable efficient outer membrane biogenesis and envelope homeostasis in Escherichia coli . We also discuss stress responses that act to combat unfolded protein stress within the cell envelope, highlighting the periplasmic chaperones involved and the mechanisms by which envelope homeostasis is restored.

Published

2024

98. Artemin molecular chaperone from Artemia urmiana improves tolerance of Arabidopsis thaliana to abiotic stress.

Author

Fallahi-Pashaki T, Shirzadian-Khoramabad R, and Sohani MM

Subjects

Animals, Stress, Physiological, Arthropod Proteins genetics, Arthropod Proteins metabolism, Gene Expression Regulation, Plant, Germination, Heat-Shock Response, RNA-Binding Proteins, Iron-Binding Proteins, Arabidopsis genetics, Arabidopsis metabolism, Arabidopsis physiology, Artemia genetics, Plants, Genetically Modified genetics, Molecular Chaperones genetics, Molecular Chaperones metabolism

Abstract

Artemia is a genus of aquatic microcrustaceans that belong to the class Branchiopoda. Encysted Artemia urmiana embryos are resistant to harsh environmental stressors, including repeated desiccation, prolonged anoxia, extreme temperatures, and high levels of UV radiation. The protein artemin has a chaperone activity and is believed to play a crucial role in protecting the organism against such stresses. To elucidate the potential functional roles of artemin in plants, the cDNA sequence of artemin was cloned into the pZPY122 binary plant expression vector. Agrobacterium -mediated transformation and the floral-dip technique were used to introduce this construct into Arabidopsis thaliana . Three independent transgenic lines (art1 , art2 , art3 ) were generated and subjected to heat stress at 45°C. Results showed a significant interaction between heat stress and genotype for germination rate, germination speed, vigor index, and seedling and root length. The transgenic lines with the artemin transgene (ART ) exhibited remarkable heat stress tolerance compared with wild-type plants. They also had markedly lower levels of electrolyte leakage, hydrogen peroxide content, higher activities of catalase, superoxide dismutase and peroxidase, greater total protien content, and increased accumulation of proline. Under heat stress conditions, the expression of two key abiotic stress-responsive genes, DREB2A and HSFA3 , was significantly upregulated in the ART lines compared to the wild-type . These findings suggest that the ART gene from A. urmiana may act as molecular chaperone when expressed in Arabidopsis , thereby enhancing the plant's tolerance to heat stress.

Published

2024

99. crVDAC3 alleviates ferroptosis by impeding HSPB1 ubiquitination and confers trastuzumab deruxtecan resistance in HER2-low breast cancer.

Author

Zou Y, Yang A, Chen B, Deng X, Xie J, Dai D, Zhang J, Tang H, Wu T, Zhou Z, Xie X, and Wang J

Subjects

Humans, Female, Animals, Mice, RNA, Circular genetics, HSP27 Heat-Shock Proteins metabolism, HSP27 Heat-Shock Proteins genetics, Molecular Chaperones metabolism, Cell Line, Tumor, Xenograft Model Antitumor Assays, Molecular Docking Simulation, Heat-Shock Proteins, Ferroptosis drug effects, Breast Neoplasms drug therapy, Breast Neoplasms pathology, Breast Neoplasms genetics, Breast Neoplasms metabolism, Ubiquitination drug effects, Trastuzumab pharmacology, Trastuzumab therapeutic use, Drug Resistance, Neoplasm drug effects, Receptor, ErbB-2 metabolism

Abstract

Aims: With the wide application of trastuzumab deruxtecan (T-DXd), the survival of HER2-low breast cancer patients is dramatically improved. However, resistance to T-DXd still exists in a subset of patients, and the molecular mechanism remains unclear., Methods: An in vivo shRNA lentiviral library functional screening was performed to identify potential circular RNA (crRNA) that mediates T-DXd resistance. RNA pull-down, mass spectrometry, RNA immunoprecipitation, and co-immunoprecipitation assays were conducted to investigate the molecular mechanism. Ferroptosis was detected using C11-BODIPY, Liperfluo, FerroOrange staining, glutathione quantification, malondialdehyde quantification, and transmission electron microscopy. Molecular docking, virtual screening, and patient-derived xenograft (PDX) models were used to validate therapeutic agents., Results: VDAC3-derived crRNA (crVDAC3) ranked first in functional shRNA library screening. Knockdown of crVDAC3 increased the sensitivity of HER2-low breast cancer cells to T-DXd treatment. Further mechanistic research revealed that crVDAC3 specifically binds to HSPB1 protein and inhibits its ubiquitination degradation, leading to intracellular accumulation and increased levels of HSPB1 protein. Notably, suppression of crVDAC3 dramatically increases excessive ROS levels and labile iron pool accumulation. Inhibition of crVDAC3 induces ferroptosis in breast cancer cells by reducing HSPB1 expression, thereby mediating T-DXd resistance. Through virtual screening and experimental validation, we identified that paritaprevir could effectively bind to crVDAC3 and prevent its interaction with HSPB1 protein, thereby increasing ubiquitination degradation of HSPB1 protein to overcome T-DXd resistance. Finally, we validated the enhanced therapeutic efficacy of T-DXd by paritaprevir in a HER2-low PDX model., Conclusion: This finding reveals the molecular mechanisms underlying T-DXd resistance in HER2-low breast cancer. Our study provides a new strategy to overcome T-DXd resistance by inhibiting the interaction between crVDAC3 and HSPB1 protein., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

100. GRAIL1 Stabilizes Misfolded Mutant p53 through a Ubiquitin Ligase-Independent, Chaperone Regulatory Function.

Author

Ray P, Jaiswal S, Ferrer-Torres D, Wang Z, Nancarrow D, Curtin M, Martinho MS, Lacy SM, Kasturirangan S, Thomas D, Spence JR, Truttmann MC, Lagisetty KH, Lawrence TS, Wang TD, Beer DG, and Ray D

Subjects

Humans, Adenocarcinoma genetics, Adenocarcinoma metabolism, Adenocarcinoma pathology, Cell Line, Tumor, Esophageal Neoplasms genetics, Esophageal Neoplasms metabolism, Esophageal Neoplasms pathology, HSP40 Heat-Shock Proteins metabolism, HSP40 Heat-Shock Proteins genetics, Molecular Chaperones metabolism, Molecular Chaperones genetics, Mutation, Protein Folding, Protein Stability, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Protein p53 genetics, Ubiquitin-Protein Ligases metabolism, Ubiquitin-Protein Ligases genetics

Abstract

Frequent (>70%) TP53 mutations often promote its protein stabilization, driving esophageal adenocarcinoma (EAC) development linked to poor survival and therapy resistance. We previously reported that during Barrett's esophagus progression to EAC, an isoform switch occurs in the E3 ubiquitin ligase RNF128 (aka GRAIL-gene related to anergy in lymphocytes), enriching isoform 1 (hereby GRAIL1) and stabilizing the mutant p53 protein. Consequently, GRAIL1 knockdown degrades mutant p53. But, how GRAIL1 stabilizes the mutant p53 protein remains unclear. In search for a mechanism, here, we performed biochemical and cell biology studies to identify that GRAIL has a binding domain (315-PMCKCDILKA-325) for heat shock protein 40/DNAJ. This interaction can influence DNAJ chaperone activity to modulate misfolded mutant p53 stability. As predicted, either the overexpression of a GRAIL fragment (Frag-J) encompassing the DNAJ binding domain or a cell-permeable peptide (Pep-J) encoding the above 10 amino acids can bind and inhibit DNAJ-Hsp70 co-chaperone activity, thus degrading misfolded mutant p53. Consequently, either Frag-J or Pep-J can reduce the survival of mutant p53 containing dysplastic Barrett's esophagus and EAC cells and inhibit the growth of patient-derived organoids of dysplastic Barrett's esophagus in 3D cultures. The misfolded mutant p53 targeting and growth inhibitory effects of Pep-J are comparable with simvastatin, a cholesterol-lowering drug that can degrade misfolded mutant p53 also via inhibiting DNAJA1, although by a distinct mechanism. Implications: We identified a novel ubiquitin ligase-independent, chaperone-regulating domain in GRAIL and further synthesized a first-in-class novel misfolded mutant p53 degrading peptide having future translational potential., (©2024 American Association for Cancer Research.)

Published

2024