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  1. Article ; Online: Molecular Dynamics and Machine Learning reveal distinguishing mechanisms of Competitive Ligands to perturb α,β-Tubulin.

    Basu, Debadrita / Dastidar, Shubhra Ghosh

    Computational biology and chemistry

    2023  Volume 108, Page(s) 108004

    Abstract: The mechanisms of action of ligands competing for the Colchicine Binding Site (CBS) of the α,β-Tubulin are non-standard compared to the commonly witnessed ligand-induced inhibition of proteins. This is because their potencies are not solely judged by the ...

    Abstract The mechanisms of action of ligands competing for the Colchicine Binding Site (CBS) of the α,β-Tubulin are non-standard compared to the commonly witnessed ligand-induced inhibition of proteins. This is because their potencies are not solely judged by the binding affinity itself, but also by their capacity to bias the conformational states of the dimer. Regarding the latter requirement, it is observed that ligands competing for the same pocket that binds colchicine exhibit divergence in potential clinical outcomes. Molecular dynamics-based ∼5.2 µs sampling of α,β-Tubulin complexed with four different ligands has revealed that each ligand has its customized way of influencing the complex. Primarily, it is the proportion of twisting and/or bending characteristic of modes of the intrinsic dynamics which is revealed to be 'fundamental' to tune this variation in the mechanism. The milder influence of 'bending' makes a ligand (TUB092), better classifiable under the group of vascular disrupting agents (VDAs), which are phenotypically effective on cytoskeletons; whereas a stronger impact of 'bending' makes the classical ligand Colchicine (COL) a better Anti-Mitotic agent (AMA). Two other ligands BAL27862 (2RR) and Nocodazole (NZO) fall in the intermediate zone as they fail to explicitly induce bending modes. Random Forest Classification method and K-means Clustering is applied to reveal the efficiency of Machine Learning methods in classifying the Tubulin conformations according to their ligand-specific perturbations and to highlight the significance of specific amino acid residues, mostly positioned in the α-β and β-β interfaces involved in the mechanism. These key residues responsible to yield discriminative actions of the ligands are likely to be highly useful in future endeavours to design more precise inhibitors.
    MeSH term(s) Tubulin/metabolism ; Molecular Dynamics Simulation ; Ligands ; Binding Sites ; Colchicine/pharmacology ; Colchicine/chemistry
    Chemical Substances Tubulin ; Ligands ; Colchicine (SML2Y3J35T)
    Language English
    Publishing date 2023-12-14
    Publishing country England
    Document type Journal Article
    ISSN 1476-928X
    ISSN (online) 1476-928X
    DOI 10.1016/j.compbiolchem.2023.108004
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  2. Article ; Online: Signatures of tRNA

    Dasgupta, Saumya / Dev, Aditya / Chongdar, Nipa / Basak, Premananda / Dastidar, Shubhra Ghosh / Basu, Gautam

    Proteins

    2023  

    Abstract: The canonical function of glutamyl-tRNA synthetase (GluRS) is to glutamylate ... ...

    Abstract The canonical function of glutamyl-tRNA synthetase (GluRS) is to glutamylate tRNA
    Language English
    Publishing date 2023-11-12
    Publishing country United States
    Document type Journal Article
    ZDB-ID 806683-8
    ISSN 1097-0134 ; 0887-3585
    ISSN (online) 1097-0134
    ISSN 0887-3585
    DOI 10.1002/prot.26634
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  3. Article ; Online: Identification and characterization of a flexile G-quadruplex in the distal promoter region of stemness gene REX1.

    Roy, Ananya / Basu, Debadrita / Bose, Debopriya / Dutta, Anindya / Dastidar, Shubhra Ghosh / Chatterjee, Subhrangsu

    International journal of biological macromolecules

    2023  Volume 231, Page(s) 123263

    Abstract: We have identified a parallel G-quadruplex (R1WT) in the distal promoter region (-821 base-pairs upstream of the TSS) of the pluripotent gene REX1. Through biophysical and biochemical approach, we have characterized the G-quadruplex (GQ) as a potential ... ...

    Abstract We have identified a parallel G-quadruplex (R1WT) in the distal promoter region (-821 base-pairs upstream of the TSS) of the pluripotent gene REX1. Through biophysical and biochemical approach, we have characterized the G-quadruplex (GQ) as a potential molecular switch that may control REX1 promoter activity to determine the transcriptional fate. Small- molecule interactive study of the monomeric form of R1WT (characterized as R1mut2) with TMPyP4 and BRACO-19 revealed GQ destabilization upon interaction with TMPyP4 and stabilization upon interaction with BRACO-19. This distinctive drug interactivity suggests the in cellulo R1WT to be a promising drug target. The endogenous existence of R1WT was confirmed by BG4 antibody derived chromatin immunoprecipitation experiment. Here in, we also report the endogenous interaction of GQ specific transcription factors (TFs) with R1WT region in the human chromatin of cancer cell. The wild-type G-quadruplex was found to interact with four important transcription factors, (i) specificity protein (Sp1) (ii) non-metastatic cell 2 (NM23-H2): a diphosphatase (iii) cellular nucleic acid binding protein (CNBP) and (iv) heterogenous nuclear ribonucleoprotein K (hnRNPK) in the REX1 promoter. In contrast, nucleolin protein (NCL) binding was found to be low to the said G-quadruplex. The flexibility of R1WT between folded and unfolded states, obtained from experimental and computational analysis strongly suggests R1WT to be an important gene regulatory element in the genome. It controls promoter DNA relaxation with the coordinated interaction of transcription factors, the deregulation of which seeds stemness characteristic in cancer cells for further metastatic progression.
    MeSH term(s) Humans ; G-Quadruplexes ; Transcription Factors/genetics ; DNA/chemistry ; Promoter Regions, Genetic
    Chemical Substances Transcription Factors ; DNA (9007-49-2)
    Language English
    Publishing date 2023-01-14
    Publishing country Netherlands
    Document type Journal Article
    ZDB-ID 282732-3
    ISSN 1879-0003 ; 0141-8130
    ISSN (online) 1879-0003
    ISSN 0141-8130
    DOI 10.1016/j.ijbiomac.2023.123263
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  4. Article ; Online: Mechanisms of influence of the microtubule over-stabilizing ligands on the structure and intrinsic dynamics of α,β-Tubulin.

    Basu, Debadrita / Majumdar, Sarmistha / Mandal, Nishita / Dastidar, Shubhra Ghosh

    Computational biology and chemistry

    2021  Volume 96, Page(s) 107617

    Abstract: The intervention into the cell cycle progression by administering microtubule over-stabilizing ligands that arrest the mitotic cell division by preventing spindle dissociation, is a promising strategy to fight against cancers. The building blocks of the ... ...

    Abstract The intervention into the cell cycle progression by administering microtubule over-stabilizing ligands that arrest the mitotic cell division by preventing spindle dissociation, is a promising strategy to fight against cancers. The building blocks of the microtubules and the spindles, i.e. the α,β-tubulin dimer, upon binding of such ligands, stay more comfortably in the microtubular multimeric form; the phenomenon of which is the key to the said over-stabilization. Using two such over-stabilizing ligands, Taxol and Taxotere, the present work reports the collective changes that these ligands induce on the structure and dynamics of the α,β-tubulin dimer which could be reconciled as the molecular basis of the over-stabilization of the microtubules; the trends have been found to be statistically significant across all independent calculations on them. The ligand binding increases the coherence between the residue communities of the two opposite faces of the β-subunit, which in a periodic arrangement in microtubule are knwon to form intermolecular contact with each other. This is likely to create an indirect cooperativity between those structural regions and this is a consequence of the reshuffling of the internal network of interactions upon ligand binding. Such reorganizations are also complemented by the increased contributions of the softer modes of the intrinsic dynamics more, which is likely to increase the plasticity of the system favourable for making structural adjustments in a multimer. Further, the ligands are able to compensate the drawback of lacking one phosphate group in protein-GDP interactions compared to the same for protein-GTP and this is in agreement with the hints form the earlier reports. The findings form a mechanistic basis of the enhanced capacity of the α,β-tubulin dimer to get more favourably accommodated into the microtubule superstructure upon binding either of Taxol and Taxotere.
    MeSH term(s) Docetaxel/chemistry ; Docetaxel/pharmacology ; Guanosine Diphosphate/chemistry ; Guanosine Diphosphate/metabolism ; Guanosine Triphosphate/chemistry ; Guanosine Triphosphate/metabolism ; Ligands ; Microtubules/drug effects ; Microtubules/metabolism ; Models, Molecular ; Molecular Conformation ; Paclitaxel/chemistry ; Paclitaxel/pharmacology ; Protein Conformation ; Tubulin/metabolism
    Chemical Substances Ligands ; Tubulin ; Guanosine Diphosphate (146-91-8) ; Docetaxel (15H5577CQD) ; Guanosine Triphosphate (86-01-1) ; Paclitaxel (P88XT4IS4D)
    Language English
    Publishing date 2021-12-08
    Publishing country England
    Document type Journal Article
    ISSN 1476-928X
    ISSN (online) 1476-928X
    DOI 10.1016/j.compbiolchem.2021.107617
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  5. Article ; Online: In silico analyses of Wnt1 nsSNPs reveal structurally destabilizing variants, altered interactions with Frizzled receptors and its deregulation in tumorigenesis.

    Mondal, Amalesh / Paul, Debarati / Dastidar, Shubhra Ghosh / Saha, Tanima / Goswami, Achintya Mohan

    Scientific reports

    2022  Volume 12, Issue 1, Page(s) 14934

    Abstract: Wnt1 is the first mammalian Wnt gene, which is discovered as proto-oncogene and in human the gene is located on the chromosome 12q13. Mutations in Wnt1 are reported to be associated with various cancers and other human diseases. The structural and ... ...

    Abstract Wnt1 is the first mammalian Wnt gene, which is discovered as proto-oncogene and in human the gene is located on the chromosome 12q13. Mutations in Wnt1 are reported to be associated with various cancers and other human diseases. The structural and functional consequences of most of the non-synonymous SNPs (nsSNPs), present in the human Wnt1 gene, are not known. In the present work, extensive bioinformatics analyses are used to screen 292 nsSNPs of Wnt1 for predicting pathogenic and harmless polymorphisms. We have identified 10 highly deleterious nsSNPs among which 7 are located within the highly conserved areas. These 10 nsSNPs are also predicted to affect the post-translational modifications of Wnt1. Further, structure based stability analyses of these 10 highly deleterious nsSNPs revealed 8 variants as highly destabilizing. These 8 highly destabilizing variants were shown to have high BC score and high RMSIP score from normal mode analyses. Based on the deformation energies, obtained from the normal mode analyses, variants like G169A, G169S, G331R and G331S were found to be unstable. Molecular Dynamics (MD) simulations revealed structural stability and fluctuation of WT Wnt1 and its prioritized variants. RMSD remained fluctuating mostly between 4 and 5 Å and occasionally between 3.5 and 5.5 Å ranges. RMSF in the CTD region (residues 330-360) of the binding pocket were lower compared to that of WT. Studying the impacts of nsSNPs on the binding interface of Wnt1 and seven Frizzled receptors have predicted substitutions which can stabilize or destabilize the binding interface. We have found that Wnt1 and FZD8-CRD is the best docked complex in our study. MD simulation based analyses of wild type Wnt1-FZD8-CRD complex and the 8 prioritized variants revealed that RMSF was higher in the unstructured regions and RMSD remained fluctuating in the region of 5 Å ± 1 Å. We have also observed differential Wnt1 gene expression pattern in normal, tumor and metastatic conditions across different tissues. Wnt1 gene expression was significantly higher in metastatic tissues of lungs, colon and skin; and was significantly lower in metastatic tissues of breast, esophagus and kidney. We have also found that Wnt1 deregulation is associated with survival outcome in patients with gastric and breast cancer. Furthermore, these computationally screened highly deleterious nsSNPs of Wnt1 can be analyzed in population based genetic studies and may help understand the Wnt1 associated diseases.
    MeSH term(s) Carcinogenesis ; Computational Biology ; Frizzled Receptors/genetics ; Humans ; Molecular Dynamics Simulation ; Polymorphism, Single Nucleotide ; Wnt1 Protein/chemistry ; Wnt1 Protein/genetics ; Wnt1 Protein/metabolism
    Chemical Substances Frizzled Receptors ; WNT1 protein, human ; Wnt1 Protein
    Language English
    Publishing date 2022-09-02
    Publishing country England
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 2615211-3
    ISSN 2045-2322 ; 2045-2322
    ISSN (online) 2045-2322
    ISSN 2045-2322
    DOI 10.1038/s41598-022-19299-x
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  6. Article ; Online: Sequence driven interaction of amino acids in de-novo designed peptides determines c-Myc G-quadruplex unfolding inducing apoptosis in cancer cells.

    Banerjee, Nilanjan / Chatterjee, Oishika / Roychowdhury, Tanaya / Basu, Debadrita / Dutta, Anindya / Chowdhury, Madhurima / Dastidar, Shubhra Ghosh / Chatterjee, Subhrangsu

    Biochimica et biophysica acta. General subjects

    2022  Volume 1867, Issue 2, Page(s) 130267

    Abstract: c-MYC proto-oncogene harbors a putative G-quadruplex structure (Pu27) at the ... ...

    Abstract c-MYC proto-oncogene harbors a putative G-quadruplex structure (Pu27) at the NHEIII
    MeSH term(s) G-Quadruplexes ; Proto-Oncogene Proteins c-myc/genetics ; Amino Acids ; Promoter Regions, Genetic ; Peptides/pharmacology ; Apoptosis ; Neoplasms
    Chemical Substances Proto-Oncogene Proteins c-myc ; Amino Acids ; Peptides
    Language English
    Publishing date 2022-11-02
    Publishing country Netherlands
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 60-7
    ISSN 1872-8006 ; 1879-2596 ; 1879-260X ; 1879-2642 ; 1879-2618 ; 1879-2650 ; 0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
    ISSN (online) 1872-8006 ; 1879-2596 ; 1879-260X ; 1879-2642 ; 1879-2618 ; 1879-2650
    ISSN 0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
    DOI 10.1016/j.bbagen.2022.130267
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  7. Article ; Online: Physical interaction between nuclear accumulated CC-NB-ARC-LRR protein and WRKY64 promotes EDS1 dependent Fusarium wilt resistance in chickpea.

    Chakraborty, Joydeep / Priya, Prerna / Dastidar, Shubhra Ghosh / Das, Sampa

    Plant science : an international journal of experimental plant biology

    2018  Volume 276, Page(s) 111–133

    Abstract: Fusarium wilt is one of the most serious diseases affecting chickpea (Cicer arietinum L.). Here, we identified a putative Resistance Gene Analog (CaRGA) from chickpea, encoding a coiled-coil (CC) nucleotide-binding oligomerization domain (NB-ARC) ... ...

    Abstract Fusarium wilt is one of the most serious diseases affecting chickpea (Cicer arietinum L.). Here, we identified a putative Resistance Gene Analog (CaRGA) from chickpea, encoding a coiled-coil (CC) nucleotide-binding oligomerization domain (NB-ARC) containing leucine-rich repeat (LRR) protein (CC-NLR protein) that confers resistance against Fusarium oxysporum f. sp. ciceri race1 (Foc1). Over-expression and silencing of CaRGA in chickpea resulted in enhanced resistance and hyper-susceptibility, respectively against Foc1. Furthermore, defense response to Foc1 depends on CC-NLR interaction with WRKY64 transcription factor. CaRGA mediated wilt resistance largely compromised when WRKY64 was silenced. We also determined in planta intramolecular interactions and self-association of chickpea CC-NLR protein. The study shows CC domain suppressing auto-activation of the full-length CC-NLR protein in the absence of pathogen through self-inhibitory intramolecular interaction with NB-ARC domain, which is attenuated by self-interactions to LRR domain. Chickpea CC-NLR protein forms homocomplexes and then interacts with WRKY64. CC-NLR protein further phosphorylates WRKY64 thereby, ubiquitination and proteasome mediated degradation are protected. Phosphorylated WRKY64 with increased stability binds to EDS1 promoter and stimulates its transcription that induces in planta ectopic cell-death. The detailed analysis of CC-NLR and WRKY interactions provide a better understanding of the immune regulation by NLR proteins under biotic stresses.
    MeSH term(s) Cicer/genetics ; Cicer/immunology ; Cicer/physiology ; Disease Resistance ; Fusarium/growth & development ; Fusarium/physiology ; Gene Expression Regulation, Plant ; Glucans/metabolism ; Host-Pathogen Interactions ; NLR Proteins/genetics ; NLR Proteins/metabolism ; Phylogeny ; Plant Diseases/immunology ; Plant Diseases/microbiology ; Plant Proteins/genetics ; Plant Proteins/metabolism ; Protein Domains ; Signal Transduction
    Chemical Substances Glucans ; NLR Proteins ; Plant Proteins ; callose (9064-51-1)
    Language English
    Publishing date 2018-08-22
    Publishing country Ireland
    Document type Journal Article
    ZDB-ID 742010-9
    ISSN 1873-2259 ; 0168-9452
    ISSN (online) 1873-2259
    ISSN 0168-9452
    DOI 10.1016/j.plantsci.2018.08.008
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  8. Article: HKT1;5 Transporter Gene Expression and Association of Amino Acid Substitutions With Salt Tolerance Across Rice Genotypes.

    Shohan, Mohammad Umer Sharif / Sinha, Souvik / Nabila, Fahmida Habib / Dastidar, Shubhra Ghosh / Seraj, Zeba I

    Frontiers in plant science

    2019  Volume 10, Page(s) 1420

    Abstract: Plants need to maintain a low ... ...

    Abstract Plants need to maintain a low Na
    Language English
    Publishing date 2019-11-04
    Publishing country Switzerland
    Document type Journal Article
    ZDB-ID 2613694-6
    ISSN 1664-462X
    ISSN 1664-462X
    DOI 10.3389/fpls.2019.01420
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  9. Article: Overexpression of LYK4, a lysin motif receptor with non-functional kinase domain, enhances tolerance to Alternaria brassicicola and increases trichome density in Brassica juncea

    De, Aishee / Maity, Atanu / Mazumder, Mrinmoy / Mondal, Banani / Mukherjee, Amrita / Ghosh, Swagata / Ray, Pranita / Polley, Smarajit / Dastidar, Shubhra Ghosh / Basu, Debabrata

    Plant science. 2021 Aug., v. 309

    2021  

    Abstract: Lysin motif receptor-like kinases (LYKs) are involved in the recognition of chitin and activation of plant immune response. In this study, we found LYK4 to be strongly induced in resistant Sinapis alba compared with susceptible Brassica juncea on ... ...

    Abstract Lysin motif receptor-like kinases (LYKs) are involved in the recognition of chitin and activation of plant immune response. In this study, we found LYK4 to be strongly induced in resistant Sinapis alba compared with susceptible Brassica juncea on challenge with Alternaria brassicicola. In silico analysis and in vitro kinase assay revealed that despite the presence of canonical protein kinase fold, B.juncea LYK4 (BjLYK4) lacks several key residues of a prototype protein kinase which renders it catalytically inactive. Transient expression analysis confirmed that fluorescently tagged BjLYK4 localizes specifically to the plasma membrane. Overexpression (OE) of BjLYK4 in B. juncea enhanced tolerance against A. brassicicola. Interestingly, the OE lines also exhibited a novel trichome dense phenotype and increased jasmonic acid (JA) responsiveness. We further showed that many chitin responsive WRKY transcription factors and JA biosynthetic genes were strongly induced in the OE lines on challenge with the pathogen. Moreover, several JA inducible trichome developmental genes constituting the WD-repeat/bHLH/MYB activator complex were also upregulated in the OE lines compared with vector control and RNA interference line. These results suggest that BjLYK4 plays an essential role in chitin-dependent activation of defense response and chitin independent trichome development likely by influencing the JA signaling pathway.
    Keywords Alternaria brassicicola ; Brassica juncea ; RNA interference ; Sinapis alba ; biosynthesis ; chitin ; computer simulation ; immune response ; jasmonic acid ; pathogens ; phenotype ; plasma membrane ; protein kinases ; prototypes ; trichomes ; vector control
    Language English
    Dates of publication 2021-08
    Publishing place Elsevier B.V.
    Document type Article
    ZDB-ID 742010-9
    ISSN 1873-2259 ; 0168-9452
    ISSN (online) 1873-2259
    ISSN 0168-9452
    DOI 10.1016/j.plantsci.2021.110953
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  10. Article ; Online: Overexpression of LYK4, a lysin motif receptor with non-functional kinase domain, enhances tolerance to Alternaria brassicicola and increases trichome density in Brassica juncea.

    De, Aishee / Maity, Atanu / Mazumder, Mrinmoy / Mondal, Banani / Mukherjee, Amrita / Ghosh, Swagata / Ray, Pranita / Polley, Smarajit / Dastidar, Shubhra Ghosh / Basu, Debabrata

    Plant science : an international journal of experimental plant biology

    2021  Volume 309, Page(s) 110953

    Abstract: Lysin motif receptor-like kinases (LYKs) are involved in the recognition of chitin and activation of plant immune response. In this study, we found LYK4 to be strongly induced in resistant Sinapis alba compared with susceptible Brassica juncea on ... ...

    Abstract Lysin motif receptor-like kinases (LYKs) are involved in the recognition of chitin and activation of plant immune response. In this study, we found LYK4 to be strongly induced in resistant Sinapis alba compared with susceptible Brassica juncea on challenge with Alternaria brassicicola. In silico analysis and in vitro kinase assay revealed that despite the presence of canonical protein kinase fold, B.juncea LYK4 (BjLYK4) lacks several key residues of a prototype protein kinase which renders it catalytically inactive. Transient expression analysis confirmed that fluorescently tagged BjLYK4 localizes specifically to the plasma membrane. Overexpression (OE) of BjLYK4 in B. juncea enhanced tolerance against A. brassicicola. Interestingly, the OE lines also exhibited a novel trichome dense phenotype and increased jasmonic acid (JA) responsiveness. We further showed that many chitin responsive WRKY transcription factors and JA biosynthetic genes were strongly induced in the OE lines on challenge with the pathogen. Moreover, several JA inducible trichome developmental genes constituting the WD-repeat/bHLH/MYB activator complex were also upregulated in the OE lines compared with vector control and RNA interference line. These results suggest that BjLYK4 plays an essential role in chitin-dependent activation of defense response and chitin independent trichome development likely by influencing the JA signaling pathway.
    MeSH term(s) Alternaria/physiology ; Arabidopsis Proteins/genetics ; Arabidopsis Proteins/metabolism ; Cyclopentanes/metabolism ; Gene Expression ; Mustard Plant/enzymology ; Mustard Plant/genetics ; Oxylipins/metabolism ; Plant Diseases/immunology ; Plant Diseases/microbiology ; Plant Growth Regulators ; Signal Transduction ; Transcription Factors/genetics ; Transcription Factors/metabolism ; Trichomes/genetics ; Trichomes/metabolism
    Chemical Substances Arabidopsis Proteins ; Cyclopentanes ; Oxylipins ; Plant Growth Regulators ; Transcription Factors ; jasmonic acid (6RI5N05OWW)
    Language English
    Publishing date 2021-05-25
    Publishing country Ireland
    Document type Journal Article
    ZDB-ID 742010-9
    ISSN 1873-2259 ; 0168-9452
    ISSN (online) 1873-2259
    ISSN 0168-9452
    DOI 10.1016/j.plantsci.2021.110953
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