Your search keyword '"Jiusheng Lin"' showing total 27 results

1. TRAF4 Maintains Deubiquitination of Caveolin-1 to Drive Glioblastoma Stemness and Temozolomide Resistance

Author

Yongxu Li, Tiepeng Wang, Quan Wan, Qing Wang, Zhenzhong Chen, Yuan Gao, Yuchen Ye, Jiusheng Lin, Bihuan Zhao, Huaile Wang, Jinming Yang, Kai Zhao, and Na Lu

Subjects

Cancer Research, TNF Receptor-Associated Factor 4, Brain Neoplasms, Ubiquitin-Protein Ligases, Caveolin 1, Risperidone, Ubiquitin-Specific Peptidase 7, Oncology, Drug Resistance, Neoplasm, Cell Line, Tumor, Neoplastic Stem Cells, Temozolomide, Humans, Glioblastoma, Proto-Oncogene Proteins c-akt, Ubiquitins

Abstract

Glioblastoma (GBM) is the most common type of primary adult brain tumor. Glioma stem cell (GSC) residence and temozolomide (TMZ) resistance in GBM both contribute to poor patient outcome. TRAF4 is a scaffold protein with E3 ubiquitin ligase activity that has recently been discovered to promote invasion and metastasis in several malignancies, but the effects and functions of TRAF4 in GBM remain to be determined. Here, we report that TRAF4 is preferentially overexpressed in GSCs and is required for stem-like properties as well as TMZ sensitivity in GBM cells. TRAF4 specifically interacted with the N-terminal tail of Caveolin-1 (CAV1), an important contributor to the tumorigenicity of GBM cells. TRAF4 regulated CAV1 stability by preventing ZNRF1-mediated ubiquitination and facilitating USP7-mediated deubiquitination independently of its E3 ubiquitin ligase catalytic activity. TRAF4-mediated stabilization of CAV1 activated protumorigenic AKT/ERK1/2 signaling, and disruption of this axis resulted in defects in stemness maintenance. In addition, expression of TRAF4 and CAV1 was positively correlated and predicted poor prognosis in human GBM samples. Screening of common nervous system drugs identified risperidone interaction with TRAF4, and risperidone treatment resulted in the dissociation of TRAF4 and CAV1. Importantly, pharmacologic inhibition of TRAF4 with risperidone potently inhibited self-renewal, abrogated tumorigenicity, and reversed TMZ resistance in GBM. Overall, TRAF4-mediated stabilization of CAV1 promotes stemness and TMZ resistance in GBM, providing a therapeutic strategy that could improve patient outcomes. Significance: The identification of a TRAF4/Caveolin-1 axis that plays a crucial role in malignant progression of glioblastoma provides new insights into the function of TRAF4 in ubiquitin signaling and suggests TRAF4 as a potential therapeutic target.

Published

2022

2. Supplementary Figure from TRAF4 Maintains Deubiquitination of Caveolin-1 to Drive Glioblastoma Stemness and Temozolomide Resistance

Author

Na Lu, Kai Zhao, Jinming Yang, Huaile Wang, Bihuan Zhao, Jiusheng Lin, Yuchen Ye, Yuan Gao, Zhenzhong Chen, Qing Wang, Quan Wan, Tiepeng Wang, and Yongxu Li

Abstract

Supplementary Figure from TRAF4 Maintains Deubiquitination of Caveolin-1 to Drive Glioblastoma Stemness and Temozolomide Resistance

Published

2023

3. Data from TRAF4 Maintains Deubiquitination of Caveolin-1 to Drive Glioblastoma Stemness and Temozolomide Resistance

Author

Na Lu, Kai Zhao, Jinming Yang, Huaile Wang, Bihuan Zhao, Jiusheng Lin, Yuchen Ye, Yuan Gao, Zhenzhong Chen, Qing Wang, Quan Wan, Tiepeng Wang, and Yongxu Li

Abstract

Glioblastoma (GBM) is the most common type of primary adult brain tumor. Glioma stem cell (GSC) residence and temozolomide (TMZ) resistance in GBM both contribute to poor patient outcome. TRAF4 is a scaffold protein with E3 ubiquitin ligase activity that has recently been discovered to promote invasion and metastasis in several malignancies, but the effects and functions of TRAF4 in GBM remain to be determined. Here, we report that TRAF4 is preferentially overexpressed in GSCs and is required for stem-like properties as well as TMZ sensitivity in GBM cells. TRAF4 specifically interacted with the N-terminal tail of Caveolin-1 (CAV1), an important contributor to the tumorigenicity of GBM cells. TRAF4 regulated CAV1 stability by preventing ZNRF1-mediated ubiquitination and facilitating USP7-mediated deubiquitination independently of its E3 ubiquitin ligase catalytic activity. TRAF4-mediated stabilization of CAV1 activated protumorigenic AKT/ERK1/2 signaling, and disruption of this axis resulted in defects in stemness maintenance. In addition, expression of TRAF4 and CAV1 was positively correlated and predicted poor prognosis in human GBM samples. Screening of common nervous system drugs identified risperidone interaction with TRAF4, and risperidone treatment resulted in the dissociation of TRAF4 and CAV1. Importantly, pharmacologic inhibition of TRAF4 with risperidone potently inhibited self-renewal, abrogated tumorigenicity, and reversed TMZ resistance in GBM. Overall, TRAF4-mediated stabilization of CAV1 promotes stemness and TMZ resistance in GBM, providing a therapeutic strategy that could improve patient outcomes.Significance:The identification of a TRAF4/Caveolin-1 axis that plays a crucial role in malignant progression of glioblastoma provides new insights into the function of TRAF4 in ubiquitin signaling and suggests TRAF4 as a potential therapeutic target.

Published

2023

4. DJ-1 is not a deglycase and makes a modest contribution to cellular defense against methylglyoxal damage in neurons

Author

Melissa Conti Mazza, Sarah C. Shuck, Jiusheng Lin, Michael A. Moxley, John Termini, Mark R. Cookson, and Mark A. Wilson

Subjects

Neurons, Cellular and Molecular Neuroscience, Mice, Oxidative Stress, Glycosylation, Guanine, Protein Deglycase DJ-1, Animals, Humans, Pyruvaldehyde, Biochemistry

Abstract

Human DJ-1 is a cytoprotective protein whose absence causes Parkinson's disease and is also associated with other diseases. DJ-1 has an established role as a redox-regulated protein that defends against oxidative stress and mitochondrial dysfunction. Multiple studies have suggested that DJ-1 is also a protein/nucleic acid deglycase that plays a key role in the repair of glycation damage caused by methylglyoxal (MG), a reactive α-keto aldehyde formed by central metabolism. Contradictory reports suggest that DJ-1 is a glyoxalase but not a deglycase and does not play a major role in glycation defense. Resolving this issue is important for understanding how DJ-1 protects cells against insults that can cause disease. We find that DJ-1 reduces levels of reversible adducts of MG with guanine and cysteine in vitro. The steady-state kinetics of DJ-1 acting on reversible hemithioacetal substrates are fitted adequately with a computational kinetic model that requires only a DJ-1 glyoxalase activity, supporting the conclusion that deglycation is an apparent rather than a true activity of DJ-1. Sensitive and quantitative isotope-dilution mass spectrometry shows that DJ-1 modestly reduces the levels of some irreversible guanine and lysine glycation products in primary and cultured neuronal cell lines and whole mouse brain, consistent with a small but measurable effect on total neuronal glycation burden. However, DJ-1 does not improve cultured cell viability in exogenous MG. In total, our results suggest that DJ-1 is not a deglycase and has only a minor role in protecting neurons against methylglyoxal toxicity.

Published

2022

5. A molecular plugin rescues GroEL/ES substrates from pre-folding oxidation

Author

Emile Dupuy, Sander E. Van der Verren, Jiusheng Lin, Mark A. Wilson, Alix Dachsbeck, Felipe Viela, Emmanuelle Latour, Alexandra Gennaris, Didier Vertommen, Yves F. Dufrêne, Bogdan I. Iorga, Camille V. Goemans, Han Remaut, and Jean-François Collet

Abstract

SUMMARYHsp60 chaperonins and their Hsp10 cofactors assist protein folding in all living cells, constituting the paradigmatic example of molecular chaperones. Despite extensive investigations of their structure and mechanism, crucial questions regarding how these chaperonins promote folding remain unsolved. Here, we report that the bacterial Hsp60 chaperonin GroEL forms a stable, functionally relevant complex with the chaperedoxin CnoX, a protein combining a chaperone and a redox function. Binding of GroES (Hsp10) to GroEL induces CnoX release. Cryo-electron microscopy provided crucial structural information on the GroEL-CnoX complex, showing that CnoX binds GroEL outside the substrate-binding site via a highly conserved C-terminal α-helix. Furthermore, the identification of complexes in which CnoX, bound to GroEL, forms mixed-disulfides with GroEL substrates indicates that CnoX likely functions as a redox quality-control plugin for GroEL. Proteins sharing structural features with CnoX exist in eukaryotes, which suggests that Hsp60 molecular plugins have been conserved through evolution.

Published

2022

6. The DUF328 family member YaaA is a DNA-binding protein with a novel fold

Author

Janani Prahlad, Yifeng Yuan, Valérie de Crécy-Lagard, Jiusheng Lin, Mark A. Wilson, Chou Wei Chang, Yilun Liu, and Dirk Iwata-Reuyl

Subjects

DNA, Bacterial, 0301 basic medicine, Protein Folding, DNA Repair, DNA repair, DNA and Chromosomes, Crystallography, X-Ray, Biochemistry, DNA-binding protein, law.invention, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, law, Escherichia coli, Holliday junction, Molecular Biology, Gene, 030102 biochemistry & molecular biology, Escherichia coli Proteins, Binding protein, Cell Biology, DNA-Binding Proteins, Oxidative Stress, 030104 developmental biology, Regulon, chemistry, Recombinant DNA, DNA

Abstract

DUF328 family proteins are present in many prokaryotes, however their molecular activities are unknown. The Escherichia coli DUF328 protein YaaA is a member of the OxyR regulon and is protective against oxidative stress. Because uncharacterized proteins involved in prokaryotic oxidative stress response are rare, we sought to learn more about the DUF328 family. Using comparative genomics, we found a robust association between the DUF328 family and genes involved in DNA recombination and the oxidative stress response. In some proteins, DUF328 domains are fused to other domains involved in DNA binding, recombination, and repair. Co-fitness analysis indicates that DUF328 family genes associate with recombination-mediated DNA repair pathways, particularly the RecFOR pathway. Purified recombinant YaaA binds to double-stranded DNA, duplex DNA containing bubbles of unpaired nucleotides, and Holliday junction constructs in vitro with dissociation equilibrium constants of 200-300 nM. YaaA binds DNA with positive cooperativity, forming multiple shifted species in electrophoretic mobility shift assays. The 1.65 A resolution X-ray crystal structure of YaaA reveals that the protein possesses a new fold that we name the cantaloupe fold. YaaA has a positively charged cleft and a helix-hairpin-helix (HhH) DNA binding motif found in other DNA repair enzymes. Our results demonstrate that YaaA is a new type of DNA-binding protein associated with the oxidative stress response and that this molecular function is likely conserved in other DUF328 family members.

Published

2020

7. DJ-1 glyoxalase activity makes a modest contribution to cellular defense against methylglyoxal damage in neurons

Author

Melissa Conti Mazza, Sarah Shuck, Jiusheng Lin, Michael A. Moxley, John Termini, Mark R. Cookson, and Mark A. Wilson

Abstract

Human DJ-1 is a cytoprotective protein whose absence causes Parkinson’s disease and is also associated with other diseases. DJ-1 has an established role as a redox-regulated protein that defends against oxidative stress and mitochondrial dysfunction. Multiple studies have suggested that DJ-1 is also a protein/nucleic acid deglycase that plays a key role in the repair of glycation damage caused by methylglyoxal (MG), a reactive α-keto aldehyde formed by central metabolism. Contradictory reports suggest that DJ-1 is a glyoxalase but not a deglycase and does not play a major role in glycation defense. Resolving this issue is important for understanding how DJ-1 protects cells against insults that can cause disease. We find that DJ-1 reduces levels of reversible adducts of MG with guanine and cysteine in vitro. The steady-state kinetics of DJ-1 acting on reversible hemithioacetal substrates are fitted adequately with a computational kinetic model that requires only a DJ-1 glyoxalase activity, supporting the conclusion that deglycation is an apparent rather than a true activity of DJ-1. Sensitive and quantitative isotope-dilution mass spectrometry shows that DJ-1 modestly reduces the levels of some irreversible guanine and lysine glycation products in primary and cultured neuronal cell lines and whole mouse brain, consistent with a small but measurable effect on total neuronal glycation burden. However, DJ-1 does not improve cultured cell viability in exogenous MG. In total, our results suggest that DJ-1 is not a deglycase and has only a minor role in protecting neurons against methylglyoxal toxicity.

Published

2022

8. A molecular device for the redox quality control of GroEL/ES substrates

Author

Emile Dupuy, Sander Egbert Van der Verren, Jiusheng Lin, Mark Alan Wilson, Alix Vincent Dachsbeck, Felipe Viela, Emmanuelle Latour, Alexandra Gennaris, Didier Vertommen, Yves Frédéric Dufrêne, Bogdan Iuliu Iorga, Camille Véronique Goemans, Han Remaut, Jean-François Collet, Structural Biology Brussels, Department of Bio-engineering Sciences, and UCL - SSS/DDUV/BCHM - Biochimie-Recherche métabolique

Subjects

Protein Folding, chaperonin, proteostasis, Chaperonins, Cryoelectron Microscopy, TPR, Chaperonin 60, thioredoxin, General Biochemistry, Genetics and Molecular Biology, redox, Chaperonin 10, chaperones, Oxidation-Reduction, Molecular Chaperones

Abstract

Hsp60 chaperonins and their Hsp10 cofactors assist protein folding in all living cells, constituting the paradigmatic example of molecular chaperones. Despite extensive investigations of their structure and mechanism, crucial questions regarding how these chaperonins promote folding remain unsolved. Here, we report that the bacterial Hsp60 chaperonin GroEL forms a stable, functionally relevant complex with the chaperedoxin CnoX, a protein combining a chaperone and a redox function. Binding of GroES (Hsp10 cofactor) to GroEL induces CnoX release. Cryoelectron microscopy provided crucial structural information on the GroEL-CnoX complex, showing that CnoX binds GroEL outside the substrate-binding site via a highly conserved C-terminal α-helix. Furthermore, we identified complexes in which CnoX, bound to GroEL, forms mixed disulfides with GroEL substrates, indicating that CnoX likely functions as a redox quality-control plugin for GroEL. Proteins sharing structural features with CnoX exist in eukaryotes, suggesting that Hsp60 molecular plugins have been conserved through evolution.

Published

2023

9. Metabolite Damage and Damage-Control in a Minimal Genome

Author

Steven D. Bruner, Jacob Folz, John I. Glass, I. Inna Kurilyak, D. Haas, Christopher S. Henry, Oliver Fiehn, Alexander F. Yakunin, Jiusheng Lin, Andrew D. Hanson, Kim S. Wise, J. Sun, V. de Crecy-Lagard, Marian Breuer, Antje M. K. Thamm, Zaida Luthey-Schulten, Mark A. Wilson, Claudia Lerma-Ortiz, Lili Huang, Greg Brown, Lijie Sun, and Guillaume A.W. Beaudoin

Subjects

chemistry.chemical_classification, chemistry.chemical_compound, Enzyme, Metabolomics, chemistry, Biochemistry, Metabolite, Hydrolase, Minimal genome, Genome, Gene, Function (biology)

Abstract

Analysis of the genes retained in the minimized Mycoplasma JCVI-Syn3A genome established that systems that repair or preempt metabolite damage are essential to life. Several genes with known metabolite damage repair or preemption functions were identified and experimentally validated, including 5-formyltetrahydrofolate cyclo-ligase, CoA disulfide reductase, and certain hydrolases. Furthermore, we discovered that an enigmatic YqeK hydrolase domain fused to NadD has a novel proofreading function in NAD synthesis and could double as a MutT-like sanitizing enzyme for the nucleotide pool. Finally, we combined metabolomics and cheminformatics approaches to extend the core metabolic map of JCVI-Syn3A to include promiscuous enzymatic reactions and spontaneous side reactions. This extension revealed that several key metabolite damage-control systems remain to be identified in JCVI-Syn3A, such as that for methylglyoxal.

Published

2021

10. The effect of cysteine oxidation on DJ-1 cytoprotective function in human alveolar type II cells

Author

Karim Bahmed, Hsin Yao Tang, Jiusheng Lin, Tessa Andrews, Samia Boukhenouna, Robert John Mason, Loukmane Karim, Elise M. Messier, Gerard J. Criner, Robert Powers, Mark A. Wilson, Roger Powell, Chih-Ru Lin, Beata Kosmider, and Nichole Reisdorph

Subjects

Male, 0301 basic medicine, Cancer Research, Protein Deglycase DJ-1, Immunology, Mitochondrion, Transfection, medicine.disease_cause, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, medicine, Humans, Cysteine, Propidium iodide, lcsh:QH573-671, Cysteine metabolism, Aged, chemistry.chemical_classification, A549 cell, Respiratory tract diseases, Reactive oxygen species, lcsh:Cytology, Cell Biology, Middle Aged, Cell biology, Oxidative Stress, Mechanisms of disease, 030104 developmental biology, chemistry, Cell culture, Alveolar Epithelial Cells, 030220 oncology & carcinogenesis, Female, Oxidation-Reduction, Oxidative stress

Abstract

DJ-1 is a multifunctional protein with cytoprotective functions. It is localized in the cytoplasm, nucleus, and mitochondria. The conserved cysteine residue at position 106 (Cys106) within DJ-1 serves as a sensor of redox state and can be oxidized to both the sulfinate (-SO2−) and sulfonate (-SO3−) forms. DJ-1 with Cys106-SO2− has cytoprotective activity but high levels of reactive oxygen species can induce its overoxidation to Cys106-SO3−. We found increased oxidative stress in alveolar type II (ATII) cells isolated from emphysema patients as determined by 4-HNE expression. DJ-1 with Cys106-SO3− was detected in these cells by mass spectrometry analysis. Moreover, ubiquitination of Cys106-SO3− DJ-1 was identified, which suggests that this oxidized isoform is targeted for proteasomal destruction. Furthermore, we performed controlled oxidation using H2O2 in A549 cells with DJ-1 knockout generated using CRISPR-Cas9 strategy. Lack of DJ-1 sensitized cells to apoptosis induced by H2O2 as detected using Annexin V and propidium iodide by flow cytometry analysis. This treatment also decreased both mitochondrial DNA amount and mitochondrial ND1 (NADH dehydrogenase 1, subunit 1) gene expression, as well as increased mitochondrial DNA damage. Consistent with the decreased cytoprotective function of overoxidized DJ-1, recombinant Cys106-SO3− DJ-1 exhibited a loss of its thermal unfolding transition, mild diminution of secondary structure in CD spectroscopy, and an increase in picosecond–nanosecond timescale dynamics as determined using NMR. Altogether, our data indicate that very high oxidative stress in ATII cells in emphysema patients induces DJ-1 overoxidation to the Cys106-SO3− form, leading to increased protein flexibility and loss of its cytoprotective function, which may contribute to this disease pathogenesis.

Published

2019

11. Regulation of DJ-1 by Glutaredoxin 1 in Vivo: Implications for Parkinson’s Disease

Author

Amy L. Wilson-Delfosse, Shu G. Chen, Nicole M. Milkovic, John J. Mieyal, Mark A. Wilson, Pierce L. Curran, Kyonghwan Choe, Chen Yao, Ajit Ray, Olga Gorelenkova Miller, Vijayalakshmi Ravindranath, Marcin Golczak, Wenzhang Wang, William M. Johnson, Xiongwei Zhu, and Jiusheng Lin

Subjects

0301 basic medicine, Parkinson's disease, Protein Deglycase DJ-1, Substantia nigra, Biology, Biochemistry, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, Glutaredoxin, medicine, Animals, Humans, Amino Acid Sequence, Cysteine, Viability assay, Caenorhabditis elegans, Glutaredoxins, Dopaminergic, PARK7, Parkinson Disease, Glutathione, medicine.disease, Cell biology, 030104 developmental biology, chemistry, Protein Processing, Post-Translational

Abstract

Parkinson's disease (PD) is the second most common neurodegenerative disease worldwide, caused by the degeneration of the dopaminergic neurons in the substantia nigra. Mutations in PARK7 (DJ-1) result in early onset autosomal recessive PD, and oxidative modification of DJ-1 has been reported to regulate the protective activity of DJ-1 in vitro. Glutathionylation is a prevalent redox modification of proteins resulting from the disulfide adduction of the glutathione moiety to a reactive cysteine-SH, and glutathionylation of specific proteins has been implicated in regulation of cell viability. Glutaredoxin 1 (Grx1) is the principal deglutathionylating enzyme within cells, and it has been reported to mediate protection of dopaminergic neurons in Caenorhabditis elegans; however many of the functional downstream targets of Grx1 in vivo remain unknown. Previously, DJ-1 protein content was shown to decrease concomitantly with diminution of Grx1 protein content in cell culture of model neurons (SH-SY5Y and Neuro-2A lines). In the current study we aimed to investigate the regulation of DJ-1 by Grx1 in vivo and characterize its glutathionylation in vitro. Here, with Grx(-/-) mice we provide show that Grx1 regulates protein levels of DJ-1 in vivo. Furthermore, with model neuronal cells (SH-SY5Y) we observed decreased DJ-1 protein content in response to treatment with known glutathionylating agents, and with isolated DJ-1 we identified two distinct sites of glutathionylation. Finally, we found that overexpression of DJ-1 in the dopaminergic neurons partly compensates for the loss of the Grx1 homologue in a C. elegans in vivo model of PD. Therefore, our results reveal a novel redox modification of DJ-1 and suggest a novel regulatory mechanism for DJ-1 content in vivo.

Published

2016

12. Transient sampling of aggregation-prone conformations causes pathogenic instability of a parkinsonian mutant of DJ-1 at physiological temperature

Author

Jiusheng Lin, Nicole M. Milkovic, Steven M Halouska, Robert Powers, Ronald L. Cerny, Jonathan Catazaro, James L. Kizziah, Sara B.G. Basiaga, and Mark A. Wilson

Subjects

Circular dichroism, biology, Chemistry, Mutant, PARK7, Nuclear magnetic resonance spectroscopy, Biochemistry, Protein Deglycase DJ-1, Chaperone (protein), biology.protein, Biophysics, Missense mutation, Hydrogen–deuterium exchange, Molecular Biology

Abstract

Various missense mutations in the cytoprotective protein DJ-1 cause rare forms of inherited parkinsonism. One mutation, M26I, diminishes DJ-1 protein levels in the cell but does not result in large changes in the three-dimensional structure or thermal stability of the protein. Therefore, the molecular defect that results in loss of M26I DJ-1 protective function is unclear. Using NMR spectroscopy near physiological temperature, we found that the picosecond–nanosecond dynamics of wild-type and M26I DJ-1 are similar. In contrast, elevated amide hydrogen/deuterium exchange rates indicate that M26I DJ-1 is more flexible than the wild-type protein on longer timescales and that hydrophobic regions of M26I DJ-1 are transiently exposed to solvent. Tryptophan fluorescence spectroscopy and thiol crosslinking analyzed by mass spectrometry also demonstrate that M26I DJ-1 samples conformations that differ from the wild-type protein at 37°C. These transiently sampled conformations are unstable and cause M26I DJ-1 to aggregate in vitro at physiological temperature but not at lower temperatures. M26I DJ-1 aggregation is correlated with pathogenicity, as the structurally similar but non-pathogenic M26L mutation does not aggregate at 37°C. The onset of dynamically driven M26I DJ-1 instability at physiological temperature resolves conflicting literature reports about the behavior of this disease-associated mutant and illustrates the pitfalls of characterizing proteins exclusively at room temperature or below, as key aspects of their behavior may not be apparent.

Published

2015

13. 15N CEST Data and Traditional Model-Free Analysis Capture Fast Internal Dynamics of DJ-1

Author

Nicole M. Milkovic, Jonathan Catazaro, Jiusheng Lin, Tessa Andrews, Austin J. Lowe, Mark A. Wilson, and Robert Powers

Subjects

0301 basic medicine, Chemistry, Protein dynamics, Dynamics (mechanics), Relaxation (NMR), Chemical exchange, Biophysics, Cell Biology, Model free, 010402 general chemistry, 01 natural sciences, Biochemistry, Article, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, Nuclear magnetic resonance, Biological system, Molecular Biology

Abstract

Previous studies have shown that relaxation parameters and fast protein dynamics can be quickly elucidated from 15N-CEST experiments [1]. Longitudinal R1 and transverse R2 values were reliably derived from fitting of CEST profiles. Herein we show that 15N-CEST experiments and traditional modelfree analysis provide the internal dynamics of three states of human protein DJ-1 at physiological temperature. The chemical exchange profiles show the absence of a minor state conformation and, in conjunction with 1H-15N NOEs, show increased mobility. R1 and R2 values remained relatively unchanged at the three naturally occurring oxidation states of DJ-1, but exhibit striking NOE differences. The NOE data was, therefore, essential in determining the internal motions of the DJ-1 proteins. To the authors' knowledge, we present the first study that combines 15N CEST data with traditional model-free analyses in the study of a biological system and affirm that more 'lean' model-free approaches should be used cautiously.

Published

2017

14. Short Carboxylic Acid-Carboxylate Hydrogen Bonds Can Have Fully Localized Protons

Author

Jiusheng Lin, Mark A. Wilson, and Edwin Pozharski

Subjects

0301 basic medicine, Models, Molecular, Ribosomal Proteins, Proton, Carboxylic acid, Low-barrier hydrogen bond, Protein Deglycase DJ-1, Carboxylic Acids, Gene Expression, Glutamic Acid, Protonation, 010402 general chemistry, Crystallography, X-Ray, Hydroxylation, 01 natural sciences, Biochemistry, Protein Structure, Secondary, Article, 03 medical and health sciences, chemistry.chemical_compound, Delocalized electron, Protein Domains, Escherichia coli, Humans, Carboxylate, Cloning, Molecular, chemistry.chemical_classification, Aspartic Acid, Hydrogen bond, Escherichia coli Proteins, Hydrogen Bonding, Recombinant Proteins, 0104 chemical sciences, Bond length, Crystallography, 030104 developmental biology, chemistry, Protons, Protein Processing, Post-Translational

Abstract

Short hydrogen bonds (H-bonds) have been proposed to play key functional roles in several proteins. The location of the proton in short H-bonds is of central importance, as proton delocalization is a defining feature of low barrier hydrogen bonds (LBHBs). Experimentally determining proton location in H-bonds is challenging. Here, bond length analysis of atomic (1.15–0.98 Å) resolution X-ray crystal structures of the human protein DJ-1 and its bacterial homolog YajL was used to determine the protonation states of H-bonded carboxylic acids. DJ-1 contains a buried, dimer-spanning 2.49 Å H-bond between Glu15 and Asp23 that satisfies standard donor-acceptor distance criteria for a LBHB. Bond length analysis indicates that the proton is localized on Asp24, excluding a LBHB at this location. However, similar analysis of the E. coli homolog YajL shows both residues may be protonated at the H-bonded oxygen atoms, potentially consistent with an LBHB. A PDB-wide screen identifies candidate carboxylic acid H-bonds in approximately 14% of proteins, which are typically short (=2.542(2) Å). Chemically similar H-bonds between hydroxylated residues (Ser/Thr/Tyr) and carboxylates show a trend of lengthening O-O distance with increasing H-bond donor pKa. This trend suggests that conventional electronic effects provide an adequate explanation for short, charge-assisted carboxylic acid-carboxylate H-bonds in proteins, without the need to invoke LBHBs in general. This study demonstrates that bond length analysis of atomic resolution X-ray crystal structures provides a useful experimental test of certain candidate LBHBs.

Published

2016

15. Atomic resolution experimental phase information reveals extensive disorder and bound 2-methyl-2,4-pentanediol in Ca(2+)-calmodulin

Author

Mark A. Wilson, Axel T. Brunger, Jiusheng Lin, and Henry van den Bedem

Subjects

0301 basic medicine, Models, Molecular, Electron density, Calmodulin, Protein Conformation, Protozoan Proteins, Ciliophora Infections, Crystal structure, Plasma protein binding, Crystallography, X-Ray, Crystal, 03 medical and health sciences, chemistry.chemical_compound, Glycols, Protein structure, Structural Biology, hemic and lymphatic diseases, Humans, Binding site, EF Hand Motifs, Selenomethionine, Binding Sites, biology, Chemistry, Research Papers, Crystallography, 030104 developmental biology, biology.protein, 2-Methyl-2,4-pentanediol, Calcium, Paramecium tetraurelia, Hydrophobic and Hydrophilic Interactions, Protein Binding

Abstract

Calmodulin (CaM) is the primary calcium signaling protein in eukaryotes and has been extensively studied using various biophysical techniques. Prior crystal structures have noted the presence of ambiguous electron density in both hydrophobic binding pockets of Ca2+-CaM, but no assignment of these features has been made. In addition, Ca2+-CaM samples many conformational substates in the crystal and accurately modeling the full range of this functionally important disorder is challenging. In order to characterize these features in a minimally biased manner, a 1.0 Å resolution single-wavelength anomalous diffraction data set was measured for selenomethionine-substituted Ca2+-CaM. Density-modified electron-density maps enabled the accurate assignment of Ca2+-CaM main-chain and side-chain disorder. These experimental maps also substantiate complex disorder models that were automatically built using low-contour features of model-phased electron density. Furthermore, experimental electron-density maps reveal that 2-methyl-2,4-pentanediol (MPD) is present in the C-terminal domain, mediates a lattice contact between N-terminal domains and may occupy the N-terminal binding pocket. The majority of the crystal structures of target-free Ca2+-CaM have been derived from crystals grown using MPD as a precipitant, and thus MPD is likely to be bound in functionally critical regions of Ca2+-CaM in most of these structures. The adventitious binding of MPD helps to explain differences between the Ca2+-CaM crystal and solution structures and is likely to favor more open conformations of the EF-hands in the crystal.

Published

2015

16. A Chemical Approach for the Detection of Protein Sulfinylation

Author

Jiusheng Lin, Kate S. Carroll, Mark A. Wilson, and Mauro Lo Conte

Subjects

Proteomics, Lung Neoplasms, Sulfinic acid, medicine.disease_cause, Biochemistry, Redox, Article, chemistry.chemical_compound, medicine, Humans, Cysteine, Lung, Cysteine metabolism, chemistry.chemical_classification, Staining and Labeling, Proteins, General Medicine, Sulfinic Acids, Sulfiredoxin, Oxidative Stress, chemistry, Molecular Medicine, Cysteine sulfinic acid, Indicators and Reagents, Oxidation-Reduction, Oxidative stress, HeLa Cells, Nitroso Compounds

Abstract

Protein sulfinic acids are formed by the reaction of reactive oxygen species with protein thiols. Sulfinic acid formation has long been considered an irreversible state of oxidation and is associated with high cellular oxidative stress. Increasing evidence, however, indicates that cysteine is oxidized to sulfinic acid in cells to a greater extent, and is more controlled, than first thought. The discovery of sulfiredoxin has demonstrated that cysteine sulfinic acid can be reversed, pointing to a vast array of potential implications for redox biology. Identification of the site of protein sulfinylation is crucial in clarifying the physiological and pathological effects of post-translational modifications. Currently, the only methods for detection of sulfinic acids involve mass spectroscopy and the use of specific antibodies. However, these methodologies are not suitable for proteomic studies. Herein, we report the first probe for detection of protein sulfinylation, NO-Bio, which combines a C-nitroso warhead for rapid labeling of sulfinic acid with a biotin handle. Based on this new tool, we developed a selective two-step approach. In the first, a sulfhydryl-reactive compound is introduced to selectively block free cysteine residues. Thereafter, the sample is treated with NO-Bio to label sulfinic acids. This new technology represents a rapid, selective, and general technology for sulfinic acid detection in biological samples. As proof of our concept, we also evaluated protein sulfinylation levels in various human lung tumor tissue lysates. Our preliminary results suggest that cancer tissues generally have higher levels of sulfinylation in comparison to matched normal tissues. A new ability to monitor protein sulfinylation directly should greatly expand the impact of sulfinic acid as a post-translational modification.

Published

2015

17. Transient sampling of aggregation-prone conformations causes pathogenic instability of a parkinsonian mutant of DJ-1 at physiological temperature

Author

Nicole M, Milkovic, Jonathan, Catazaro, Jiusheng, Lin, Steven, Halouska, James L, Kizziah, Sara, Basiaga, Ronald L, Cerny, Robert, Powers, and Mark A, Wilson

Subjects

Magnetic Resonance Spectroscopy, Circular Dichroism, Mutation, Protein Deglycase DJ-1, Molecular Conformation, Temperature, Humans, Parkinson Disease, Amino Acid Sequence, Articles

Abstract

Various missense mutations in the cytoprotective protein DJ-1 cause rare forms of inherited parkinsonism. One mutation, M26I, diminishes DJ-1 protein levels in the cell but does not result in large changes in the three-dimensional structure or thermal stability of the protein. Therefore, the molecular defect that results in loss of M26I DJ-1 protective function is unclear. Using NMR spectroscopy near physiological temperature, we found that the picosecond–nanosecond dynamics of wild-type and M26I DJ-1 are similar. In contrast, elevated amide hydrogen/deuterium exchange rates indicate that M26I DJ-1 is more flexible than the wild-type protein on longer timescales and that hydrophobic regions of M26I DJ-1 are transiently exposed to solvent. Tryptophan fluorescence spectroscopy and thiol crosslinking analyzed by mass spectrometry also demonstrate that M26I DJ-1 samples conformations that differ from the wild-type protein at 37°C. These transiently sampled conformations are unstable and cause M26I DJ-1 to aggregate in vitro at physiological temperature but not at lower temperatures. M26I DJ-1 aggregation is correlated with pathogenicity, as the structurally similar but non-pathogenic M26L mutation does not aggregate at 37°C. The onset of dynamically driven M26I DJ-1 instability at physiological temperature resolves conflicting literature reports about the behavior of this disease-associated mutant and illustrates the pitfalls of characterizing proteins exclusively at room temperature or below, as key aspects of their behavior may not be apparent.

Published

2015

18. Exploring the Importance of Dimerization for DJ‐1 Function through Engineered Domain Fusions

Author

Mark A. Wilson, Sierra Hansen, and Jiusheng Lin

Subjects

Chemistry, Genetics, Function (mathematics), Computational biology, Molecular Biology, Biochemistry, Biotechnology, Domain (software engineering)

Published

2015

19. Salt stress-induced programmed cell death in tobacco protoplasts is mediated by reactive oxygen species and mitochondrial permeability transition pore status

Author

Gen-Xuan Wang, Jiusheng Lin, and Yuan Wang

Subjects

Programmed cell death, Time Factors, animal structures, DNA, Plant, Physiology, Nicotiana tabacum, Apoptosis, Plant Science, Sodium Chloride, Mitochondrial Membrane Transport Proteins, Cyclosporin a, Tobacco, otorhinolaryngologic diseases, Membrane Potential, Mitochondrial, chemistry.chemical_classification, Membrane potential, Reactive oxygen species, biology, Mitochondrial Permeability Transition Pore, Protoplasts, Hydrogen Peroxide, biology.organism_classification, Ascorbic acid, Cell biology, Oxidative Stress, chemistry, Biochemistry, Mitochondrial permeability transition pore, Cyclosporine, Reactive Oxygen Species, Agronomy and Crop Science

Abstract

The status of mitochondrial permeability transition pore (PTP) and levels of reactive oxygen species (ROS) play key roles in regulating apoptosis in animal cells. To investigate if the PTP and cellular oxidation-reduction state are also involved in salt stress-induced programmed cell death (PCD) in tobacco (Nicotiana tabacum, cultivar BY-2) protoplasts, flow cytometry was used to simultaneously monitor ROS levels, PTP status and PCD. Increased ROS and decreased mitochondrial membrane potential (delta psi(m)) were observed before the appearance of PCD. Pre-treatment with an inhibitor of the PTP opening, cyclosporin A (CsA), effectively retarded the onset of PCD, the delta psi(m) decrease and the ROS content increase. Addition of ascorbic acid (AsA) during the salt stress significantly decreased the percentage of protoplasts undergoing PCD and ROS levels but increased delta psi(m). Hydrogen peroxide effectively induced the appearance of PCD and caused an increase in ROS and a decrease in delta psi(m). Pre-treatment of protoplasts with CsA weakened the effects of H2O2. All these results suggest that the open state of PTP and ROS are necessary elements for salt stress-induced PCD in tobacco protoplasts. The open states of PTP and ROS could promote each other suggesting that ROS could lead to a self-amplifying process. This positive feedback loop may act as an all-or-nothing switch, which is in good accordance with the hypothesis that PTP is an important coordinator and executioner of PCD in both animals and plants.

Published

2006

20. Salt stress-induced programmed cell death via Ca2+-mediated mitochondrial permeability transition in tobacco protoplasts

Author

Gen-Xuan Wang, Yuan Wang, and Jiusheng Lin

Subjects

Membrane potential, Programmed cell death, Physiology, chemistry.chemical_element, Plant Science, Mitochondrion, Biology, Calcium, Cell biology, EGTA, chemistry.chemical_compound, Cytosol, chemistry, Mitochondrial permeability transition pore, Biochemistry, Apoptosis, Agronomy and Crop Science

Abstract

The change in cytosolic free concentration of calcium ([Ca2+]cyt) plays a key role in regulating apoptosis in animal cells. In our experiment, we tried to investigate the function of Ca2+ in programmed cell death (PCD) in tobacco (Nicotiana tobacum, cultivar BY-2) protoplasts induced by salt stress. An obvious increase in [Ca2+]cyt was observed a few minutes after treatment and the onset of a decrease in mitochondrial membrane potential (ΔΨm) was also observed before the appearance of PCD, pre-treatment of protoplasts with EGTA or LaCl3 effectively retarded the increase in [Ca2+]cyt, which was concomitant with the decrease in the percentage of cell death and higher ΔΨm, pre-treatment with cyclosporine A (CsA) also effectively retarded the increase in [Ca2+]cyt, the decrease in ΔΨm and the onset of PCD. All these results suggest that Ca2+ is a necessary element in regulating PCD and the increase in [Ca2+]cyt and the opening of mitochondrial permeability transition pore (MPTP) could promote each other in regulating PCD in tobacco protoplasts induced by salt stress.

Published

2005

21. Converter transformer valve winding DC field analysis of nonlinear anisotropic

Author

Guangsheng Cheng, Jiusheng Lin, Haiying Yang, and Wei Li

Subjects

Forward converter, Leakage inductance, Materials science, business.industry, Flyback converter, Electrical engineering, law.invention, Nonlinear system, law, Electronic engineering, Delta-wye transformer, Rotary variable differential transformer, Anisotropy, Transformer, business

Published

2014

22. Simulation Analysis for GIS Internal UHF Partial Discharge Signal Propagation Characteristics

Author

Guangsheng Cheng, Jiusheng Lin, Haiying Yang, and Wei Li

Subjects

Radio propagation, Engineering, business.industry, Acoustics, Electric field, Partial discharge, Finite-difference time-domain method, Electrical engineering, Insulator (electricity), Flange, business, Electromagnetic radiation, Magnetic field

Abstract

This paper researches on the propagation characteristics of partial discharge in internal GIS. Through the external UHF sensor to receive the electromagnetic wave signals emitted from the surface of the insulator metal pouring hole flange and using the finite difference time domain method, by means of XFDTD modeling, simulation and analysis the propagation characteristics of partial discharge signals in GIS cavity. The result shows that the UHF partial discharge signal along the GIS cavity axis direction emitted from the metal flange pouring hole has the maximum electric field component; electric field strength modulus value in the center is greater than the modulus of both sides, and both sides are symmetrical distribution; the direction of the magnetic field is parallel to long edge and the strength of magnetic field modulus value in the short- side is greater than the midline of long side.

Published

2014

23. Activity of the Arabidopsis RD29A and RD29B promoter elements in soybean under water stress

Author

Jiusheng Lin, Saadia Bihmidine, James E. Specht, Julie M. Stone, Tala Awada, and Thomas E. Clemente

Subjects

Transgene, Plant Science, Gene Expression Regulation, Plant, Arabidopsis, Botany, Genetics, Arabidopsis thaliana, Fluorometry, Promoter Regions, Genetic, Gene, Glucuronidase, biology, Abiotic stress, Arabidopsis Proteins, Histocytochemistry, fungi, food and beverages, Water, Promoter, Agrobacterium tumefaciens, biology.organism_classification, Plants, Genetically Modified, Droughts, Blotting, Southern, Glycine, Soybeans

Abstract

The constitutive and drought-induced activities of the Arabidopsis thaliana RD29A and RD29B promoters were monitored in soybean (Glycine max (L.) Merr.] via fusions with the visual marker gene β-glucuronidase (GUS). Physiological responses of soybean plants were monitored over 9 days of water deprivation under greenhouse conditions. Data were used to select appropriate time points to monitor the activities of the respective promoter elements. Qualitative and quantitative assays for GUS expression were conducted in root and leaf tissues, from plants under well-watered and dry-down conditions. Both RD29A and RD29B promoters were significantly activated in soybean plants subjected to dry-down conditions. However, a low level of constitutive promoter activity was also observed in both root and leaves of plants under well-watered conditions. GUS expression was notably higher in roots than in leaves. These observations suggest that the respective drought-responsive regulatory elements present in the RD29X promoters may be useful in controlling targeted transgenes to mitigate abiotic stress in soybean, provided the transgene under control of these promoters does not invoke agronomic penalties with leaky expression when no abiotic stress is imposed.

Published

2012

24. Conservation of oxidative protein stabilization in an insect homologue of the parkinsonism-associated protein DJ-1

Author

Jiusheng Lin, Janani Prahlad, and Mark A. Wilson

Subjects

Models, Molecular, Protein DJ-1, Protein Deglycase DJ-1, Nerve Tissue Proteins, Crystallography, X-Ray, Biochemistry, Article, Melanogaster, Animals, Drosophila Proteins, Humans, Cysteine, Tyrosine, Oncogene Proteins, biology, Protein Stability, Intracellular Signaling Peptides and Proteins, biology.organism_classification, Drosophila melanogaster, Protein stabilization, Oxidation-Reduction, Drosophila Protein

Abstract

DJ-1 is a conserved, disease-associated protein that protects against oxidative stress and mitochondrial damage in multiple organisms. Human DJ-1 contains a functionally essential cysteine residue (Cys106) whose oxidation is important for regulating protein function by an unknown mechanism. This residue is well-conserved in other DJ-1 homologues, including two (DJ-1α and DJ-1β) in Drosophila melanogaster. Because D. melanogaster is a powerful model system for studying DJ-1 function, we have determined the crystal structure and impact of cysteine oxidation on Drosophila DJ-1β. The structure of D. melanogaster DJ-1β is similar to that of human DJ-1, although two important residues in the human protein, Met26 and His126, are not conserved in DJ-1β. His126 in human DJ-1 is substituted with a tyrosine in DJ-1β, and this residue is not able to compose a putative catalytic dyad with Cys106 that was proposed to be important in the human protein. The reactive cysteine in DJ-1 is oxidized readily to the cysteine-sulfinic acid in both flies and humans, and this may regulate the cytoprotective function of the protein. We show that the oxidation of this conserved cysteine residue to its sulfinate form (Cys-SO(2)(-)) results in considerable thermal stabilization of both Drosophila DJ-1β and human DJ-1. Therefore, protein stabilization is one potential mechanism by which cysteine oxidation may regulate DJ-1 function in vivo. More generally, most close DJ-1 homologues are likely stabilized by cysteine-sulfinic acid formation but destabilized by further oxidation, suggesting that they are biphasically regulated by oxidative modification.

Published

2012

25. A Plant DJ-1 Homolog Is Essential for Arabidopsis thaliana Chloroplast Development

Author

Tara J. Nazarenus, Jiusheng Lin, Mark A. Wilson, Xinwen Liang, Jeanine L. Frey, and Julie M. Stone

Subjects

Angiosperms, Chloroplasts, Arabidopsis, lcsh:Medicine, Plant Science, Plant Genetics, Genes, Plant, 03 medical and health sciences, Chloroplast Proteins, Model Organisms, Genetic Mutation, Plant and Algal Models, Genetics, Arabidopsis thaliana, Animals, Plastid, lcsh:Science, Gene, Biology, Flowering Plants, 030304 developmental biology, Plant Growth and Development, 0303 health sciences, Multidisciplinary, biology, Sequence Homology, Amino Acid, Arabidopsis Proteins, lcsh:R, 030302 biochemistry & molecular biology, fungi, food and beverages, Plants, biology.organism_classification, Chloroplast, Thylakoid, lcsh:Q, Gene Function, Function (biology), Research Article, Developmental Biology

Abstract

Protein superfamilies can exhibit considerable diversification of function among their members in various organisms. The DJ-1 superfamily is composed of proteins that are principally involved in stress response and are widely distributed in all kingdoms of life. The model flowering plant Arabidopsis thaliana contains three close homologs of animal DJ-1, all of which are tandem duplications of the DJ-1 domain. Consequently, the plant DJ-1 homologs are likely pseudo-dimeric proteins composed of a single polypeptide chain. We report that one A. thaliana DJ-1 homolog (AtDJ1C) is the first DJ-1 homolog in any organism that is required for viability. Homozygous disruption of the AtDJ1C gene results in non-viable, albino seedlings that can be complemented by expression of wild-type or epitope-tagged AtDJ1C. The plastids from these dj1c plants lack thylakoid membranes and granal stacks, indicating that AtDJ1C is required for proper chloroplast development. AtDJ1C is expressed early in leaf development when chloroplasts mature, but is downregulated in older tissue, consistent with a proposed role in plastid development. In addition to its plant-specific function, AtDJ1C is an atypical member of the DJ-1 superfamily that lacks a conserved cysteine residue that is required for the functions of most other superfamily members. The essential role for AtDJ1C in chloroplast maturation expands the known functional diversity of the DJ-1 superfamily and provides the first evidence of a role for specialized DJ-1-like proteins in eukaryotic development.

Published

2011

26. Escherichia coli Thioredoxin-like Protein YbbN Contains an Atypical Tetratricopeptide Repeat Motif and Is a Negative Regulator of GroEL*

Author

Jiusheng Lin and Mark A. Wilson

Subjects

Amino Acid Motifs, Crystallography, X-Ray, Biochemistry, Chaperonin, Protein structure, Ribosomal protein, Escherichia coli, HSP70 Heat-Shock Proteins, Oxidoreductases Acting on Sulfur Group Donors, Enzyme Inhibitors, Molecular Biology, Heat-Shock Proteins, biology, Escherichia coli Proteins, Cell Biology, Chaperonin 60, HSP40 Heat-Shock Proteins, GroEL, Protein Structure, Tertiary, Tetratricopeptide, Chaperone (protein), Protein Structure and Folding, biology.protein, Protein folding, Thioredoxin, Molecular Chaperones

Abstract

Many proteins contain a thioredoxin (Trx)-like domain fused with one or more partner domains that diversify protein function by the modular construction of new molecules. The Escherichia coli protein YbbN is a Trx-like protein that contains a C-terminal domain with low homology to tetratricopeptide repeat motifs. YbbN has been proposed to act as a chaperone or co-chaperone that aids in heat stress response and DNA synthesis. We report the crystal structure of YbbN, which is an elongated molecule with a mobile Trx domain and four atypical tetratricopeptide repeat motifs. The Trx domain lacks a canonical CXXC active site architecture and is not a functional oxidoreductase. A variety of proteins in E. coli interact with YbbN, including multiple ribosomal protein subunits and a strong interaction with GroEL. YbbN acts as a mild inhibitor of GroESL chaperonin function and ATPase activity, suggesting that it is a negative regulator of the GroESL system. Combined with previous observations that YbbN enhances the DnaK-DnaJ-GrpE chaperone system, we propose that YbbN coordinately regulates the activities of these two prokaryotic chaperones, thereby helping to direct client protein traffic initially to DnaK. Therefore, YbbN may play a role in integrating the activities of different chaperone pathways in E. coli and related bacteria.

Published

2011

27. Characterization of abiotic stress-responsive Arabidopsis thaliana RD29A and RD29B genes and evaluation of transgenes

Author

Jiusheng Lin, Joseph Msanne, Tala Awada, and Julie M. Stone

Subjects

Abiotic component, Dehydration, Abiotic stress, Transgene, Cold-Shock Response, Mutant, Arabidopsis, Promoter, Plant Science, Chimeric gene, Salt Tolerance, Biology, biology.organism_classification, Genes, Plant, Plants, Genetically Modified, Plant Roots, Cell biology, Gene Expression Regulation, Plant, Stress, Physiological, Botany, Genetics, Arabidopsis thaliana, Transgenes, Photosynthesis, Gene

Abstract

Abiotic stresses have adverse effects on plant growth and productivity. The homologous RD29A and RD29B genes are exquisitely sensitive to various abiotic stressors. Therefore, RD29A and RD29B gene sequences have potential to confer abiotic stress resistance in crop species grown in arid and semi-arid regions. To our knowledge, no information on the physiological roles of the proteins encoded by RD29A and RD29B are available in the literature. To understand how these proteins function, we used reverse genetic approaches, including identifying rd29a and rd29b T-DNA knockout mutants, and examining the effects of complementing transgenes with the genes under control of their native promoters and chimeric genes with the native promoters swapped. Four binary vectors with the RD29A and RD29B promoters upstream of the cognate RD29A and RD29B cDNAs and as chimeric genes with noncognate promoters were used to transform rd29a and rd29b plants. Cold, drought, and salt induced both genes; the promoter of RD29A was found to be more responsive to drought and cold stresses, whereas the promoter of RD29B was highly responsive to salt stress. Morphological and physiological responses of rd29a and rd29b plants to salt stress were further investigated. Root growth, and photosynthetic properties declined significantly, while solute concentration (Ψπ), water use efficiency (WUE) and δ(13)C ratio increased under salt stress. Unexpectedly, the rd29a and rd29b knockout mutant lines maintained greater root growth, photosynthesis, and WUE under salt stress relative to control. We conclude that the RD29A and RD29B proteins are unlikely to serve directly as protective molecules.

Published

2010