Your search keyword '"Arun Dhillon"' showing total 17 results

1. Cryo-EM structures of Trypanosoma brucei gambiense ISG65 with human complement C3 and C3b and their roles in alternative pathway restriction

Author

Hagen Sülzen, Jakub Began, Arun Dhillon, Sami Kereïche, Petr Pompach, Jitka Votrubova, Farnaz Zahedifard, Adriana Šubrtova, Marie Šafner, Martin Hubalek, Maaike Thompson, Martin Zoltner, and Sebastian Zoll

Subjects

Science

Abstract

Abstract African Trypanosomes have developed elaborate mechanisms to escape the adaptive immune response, but little is known about complement evasion particularly at the early stage of infection. Here we show that ISG65 of the human-infective parasite Trypanosoma brucei gambiense is a receptor for human complement factor C3 and its activation fragments and that it takes over a role in selective inhibition of the alternative pathway C5 convertase and thus abrogation of the terminal pathway. No deposition of C4b, as part of the classical and lectin pathway convertases, was detected on trypanosomes. We present the cryo-electron microscopy (EM) structures of native C3 and C3b in complex with ISG65 which reveal a set of modes of complement interaction. Based on these findings, we propose a model for receptor-ligand interactions as they occur at the plasma membrane of blood-stage trypanosomes and may facilitate innate immune escape of the parasite.

Published

2023

2. A multifaceted strategy to improve recombinant expression and structural characterisation of a Trypanosoma invariant surface protein

Author

Hagen Sülzen, Jitka Votrubova, Arun Dhillon, and Sebastian Zoll

Subjects

Medicine, Science

Abstract

Abstract Identification of a protein minimal fragment amenable to crystallisation can be time- and labour intensive especially if large amounts are required and the protein has a complex fold and functionally important post-translational modifications. In addition, a lack of homologues and structural information can further complicate the design of a minimal expression construct. Recombinant expression in E. coli promises high yields, low costs and fast turnover times, but falls short for many extracellular, eukaryotic proteins. Eukaryotic expression systems provide an alternative but are costly, slow and require special handling and equipment. Using a member of a structurally uncharacterized, eukaryotic receptor family as an example we employ hydrogen–deuterium exchange mass spectrometry (HDX-MS) guided construct design in conjunction with truncation scanning and targeted expression host switching to identify a minimal expression construct that can be produced with high yields and moderate costs.

Published

2022

3. Molecular Basis for Bordetella pertussis Interference with Complement, Coagulation, Fibrinolytic, and Contact Activation Systems: the Cryo-EM Structure of the Vag8-C1 Inhibitor Complex

Author

Arun Dhillon, Justin C. Deme, Emily Furlong, Dorina Roem, Ilse Jongerius, Steven Johnson, and Susan M. Lea

Subjects

Bordetella pertussis, immune evasion, complement system, serpin, autotransporters, C1-INH, Microbiology, QR1-502

Abstract

ABSTRACT Complement, contact activation, coagulation, and fibrinolysis are serum protein cascades that need strict regulation to maintain human health. Serum glycoprotein, a C1 inhibitor (C1-INH), is a key regulator (inhibitor) of serine proteases of all the above-mentioned pathways. Recently, an autotransporter protein, virulence-associated gene 8 (Vag8), produced by the whooping cough pathogen, Bordetella pertussis, was shown to bind to C1-INH and interfere with its function. Here, we present the structure of the Vag8–C1-INH complex determined using cryo-electron microscopy at a 3.6-Å resolution. The structure shows a unique mechanism of C1-INH inhibition not employed by other pathogens, where Vag8 sequesters the reactive center loop of C1-INH, preventing its interaction with the target proteases. IMPORTANCE The structure of a 10-kDa protein complex is one of the smallest to be determined using cryo-electron microscopy at high resolution. The structure reveals that C1-INH is sequestered in an inactivated state by burial of the reactive center loop in Vag8. By so doing, the bacterium is able to simultaneously perturb the many pathways regulated by C1-INH. Virulence mechanisms such as the one described here assume more importance given the emerging evidence about dysregulation of contact activation, coagulation, and fibrinolysis leading to COVID-19 pneumonia.

Published

2021

4. A multifaceted strategy to improve recombinant expression and structure determination of complex proteins: A Trypanosoma surface protein as an example

Author

Hagen Sülzen, Jitka Votrubova, Arun Dhillon, and Sebastian Zoll

Abstract

Identification of a protein minimal fragment amenable to crystallisation can be time- and labour intensive especially if large amounts are required and the protein has a complex fold and functionally important post-translational modifications. In addition, a lack of homologues and structural information can further complicate the design of a minimal expression construct. Recombinant expression in E. coli promises high yields, low costs and fast turnover times, but falls short for many extracellular, eukaryotic proteins. Eukaryotic expression systems provide an alternative but are costly, slow and require special handling and equipment. Using a member of a structurally uncharacterized, eukaryotic receptor family as an example we employ hydrogen-deuterium exchange mass spectrometry (HDX-MS) guided construct design in conjunction with truncation scanning and targeted expression host switching to identify a minimal expression construct that can be produced with high yields and low costs.

Published

2022

5. Green bioprocess of degumming of jute fibers and bioscouring of cotton fabric by recombinant pectin methylesterase and pectate lyases from Clostridium thermocellum

Author

Kiran Kumar Gali, Arun Dhillon, Vikky Rajulapati, Vimal Katiyar, and Arun Goyal

Subjects

0106 biological sciences, 0303 health sciences, food.ingredient, Pectin, biology, Chemistry, Bioengineering, biology.organism_classification, 01 natural sciences, Applied Microbiology and Biotechnology, Biochemistry, law.invention, Biotechnological process, 03 medical and health sciences, food, law, 010608 biotechnology, Pectate lyase, Ultimate tensile strength, Recombinant DNA, Clostridium thermocellum, Food science, Fiber, Bioprocess, 030304 developmental biology

Abstract

Enzymatic processes are emerging as important green biotechnological processes in textile industry. The application of recombinant pectin methylesterase (CtPME) and pectate lyase (CtPL1B) from Clostridium thermocellum for enzymatic degumming of jute or bioscouring of cotton was evaluated. The effectiveness of processes by combination of two enzymes were evaluated that effective degumming of jute and bioscouring of cotton as compared with individual enzyme. The optimum concentrations of two enzymes mixture for both processes, degumming of jute and bio scouring of cotton were 5 mg/mL (2.1 U/mL) of CtPME and 5 mg/mL (3.0 U/mL) of CtPL1B under optimized conditions of 60 min, 100 rpm and 50 °C. FESEM images showed more effective removal of pectin from jute fiber and cotton fabric by enzyme mixture, nevertheless similar to NaOH treatment. Wettability analysis showed mixture of enzymes and NaOH treated cotton fabric absorbed a water drop in 10 s and 8 s, respectively. UTM analysis showed higher tensile strength and Young’s modulus for jute fiber and cotton fabric treated with enzyme mixture than untreated and were similar to those of NaOH treated. These results showed that the CtPME and CtPL1B mixture can be used for replacing the chemical process by green bioprocess in textile industry.

Published

2020

6. Enhanced catalytic efficiency of Bacillus amyloliquefaciens SS35 endoglucanase by ultraviolet directed evolution and mutation analysis

Author

Shweta Singh, Arun Goyal, and Arun Dhillon

Subjects

060102 archaeology, Bacillus amyloliquefaciens, biology, Renewable Energy, Sustainability and the Environment, Chemistry, 020209 energy, Lignocellulosic biomass, 06 humanities and the arts, 02 engineering and technology, Cellobiose, Cellulase, Directed evolution, biology.organism_classification, Hydrolysis, chemistry.chemical_compound, Biochemistry, Enzymatic hydrolysis, 0202 electrical engineering, electronic engineering, information engineering, biology.protein, 0601 history and archaeology, Glycoside hydrolase

Abstract

Bacillus amyloliquefaciens SS35 was subjected to ultraviolet irradiation to improve the enzymatic hydrolysis of lignocellulosic biomass. The resulting mutant, UV2, produced endoglucanase, carboxymethyl cellulase, CMCase-UV2 with 1.6–4.1-fold higher activity against cellulosic substrates than the wild type, CMCase-WT. CMCase-UV2 exhibited wider pH stability in the acidic range than CMCase-WT. The TLC analysis showed that the hydrolysis of CMC-Na and β-glucan by CMCase-UV2 produced glucose along with cello-oligosaccharides and cellobiose in 45 min, whereas, CMCase-WT produced, only cello-oligosaccharides and cellobiose in 120 min by endolytic mode of action. The hydrolysis of pretreated Pennisetum purpureum by CMCase-UV2 gave total reducing sugar yield 154.2 mg/g pretreated biomass in 48 h, which was 1.8-fold higher than CMCase-WT. CMCase-UV2 was the promising endoglucanase which improves the saccharification of lignocellulosic biomass therefore, it will improve the efficiency of the process, lignocellulose-based biorefineries for bioethanol production. The gene encoding cellulase was amplified from wild-type and UV2 strains using degenerate primers designed from phylogenetically related spp. Bacillus amyloliquefaciens KHG19 for family 5 glycoside hydrolase. Sequences analysis of genes from wild-type and UV2 strains showed the mutation, D233G. These results will provide information for protein engineering in designing mutant of endoglucanase for improved catalytic efficiency and pH stability.

Published

2020

7. Human RAD51 paralogue RAD51C fosters repair of alkylated DNA by interacting with the ALKBH3 demethylase

Author

Arun Goyal, Arun Dhillon, Monisha Mohan, Roy Anindya, and Deepa Akula

Subjects

Alkylation, DNA Repair, RAD51, Plasma protein binding, Genome Integrity, Repair and Replication, 03 medical and health sciences, chemistry.chemical_compound, DNA Adducts, 0302 clinical medicine, Transferases, Genetics, Humans, Cells, Cultured, 030304 developmental biology, 0303 health sciences, biology, Mutagenesis, HEK 293 cells, Cell biology, DNA-Binding Proteins, DNA Alkylation, HEK293 Cells, chemistry, 030220 oncology & carcinogenesis, PC-3 Cells, biology.protein, Demethylase, AlkB Homolog 3, Alpha-Ketoglutarate-Dependent Dioxygenase, Rad51 Recombinase, Function (biology), DNA, DNA Damage, Protein Binding

Abstract

The integrity of our DNA is challenged daily by a variety of chemicals that cause DNA base alkylation. DNA alkylation repair is an essential cellular defence mechanism to prevent the cytotoxicity or mutagenesis from DNA alkylating chemicals. Human oxidative demethylase ALKBH3 is a central component of alkylation repair, especially from single-stranded DNA. However, the molecular mechanism of ALKBH3-mediated damage recognition and repair is less understood. We report that ALKBH3 has a direct protein-protein interaction with human RAD51 paralogue RAD51C. We also provide evidence that RAD51C–ALKBH3 interaction stimulates ALKBH3-mediated repair of methyl-adduct located within 3′-tailed DNA, which serves as a substrate for the RAD51 recombinase. We further show that the lack of RAD51C–ALKBH3 interaction affects ALKBH3 function in vitro and in vivo. Our data provide a molecular mechanism underlying upstream events of alkyl adduct recognition and repair by ALKBH3.

Published

2019

8. Development of bi-functional chimeric enzyme (CtGH1-L1-CtGH5-F194A) from endoglucanase (CtGH5) mutant F194A and β-1,4-glucosidase (CtGH1) from Clostridium thermocellum with enhanced activity and structural integrity

Author

Kedar Sharma, Priyanka Nath, Sumitha Banu Jamaldheen, Vijayanand S. Moholkar, Arun Dhillon, Arun Goyal, and Krishan Kumar

Subjects

0106 biological sciences, Cellobiose, Environmental Engineering, Recombinant Fusion Proteins, Mutant, Bioengineering, Cellulase, 010501 environmental sciences, 01 natural sciences, Clostridium thermocellum, chemistry.chemical_compound, 010608 biotechnology, Escherichia coli, Glycoside hydrolase, Biomass, Site-directed mutagenesis, Waste Management and Disposal, 0105 earth and related environmental sciences, Thermostability, chemistry.chemical_classification, biology, Renewable Energy, Sustainability and the Environment, Hydrolysis, beta-Glucosidase, Temperature, General Medicine, biology.organism_classification, Enzyme, Biochemistry, chemistry, Mutagenesis, Site-Directed, biology.protein

Abstract

Site-directed mutagenesis of β-1,4-endoglucanase from family 5 glycoside hydrolase (CtGH5) from Clostridium thermocellum was performed to develop a mutant CtGH5-F194A that gave 40 U/mg specific activity against carboxymethyl cellulose, resulting 2-fold higher activity than wild-type CtGH5. CtGH5-F194A was fused with a β-1,4-glucosidase, CtGH1 from Clostridium thermocellum to develop a chimeric enzyme. The chimera (CtGH1-L1-CtGH5-F194A) expressed as a soluble protein using E. coli BL-21cells displaying 3- to 5-fold higher catalytic efficiency for endoglucanase and β-glucosidase activities. TLC analysis of hydrolysed product of CMC by chimera 1 revealed glucose as final product confirming both β-1,4-endoglucanase and β-1,4-glucosidase activities, while the products of CtGH5-F194A were cellobiose and cello-oligosaccharides. Protein melting studies of CtGH5-F194A showed melting temperature (Tm), 68 °C and of CtGH1, 79 °C, whereas, chimera showed 78 °C. The improved structural integrity, thermostability and enhanced bi-functional enzyme activities of chimera makes it potentially useful for industrial application in converting biomass to glucose and thus bioethanol.

Published

2019

9. Bio‐scouring of cotton fabric and enzymatic degumming of jute fibres by a thermo‐alkaline recombinant rhamnogalacturonan lyase, ctrglf fromClostridium thermocellum

Author

Vikky Rajulapati, Arun Dhillon, and Arun Goyal

Subjects

0106 biological sciences, 0301 basic medicine, chemistry.chemical_classification, biology, General Chemical Engineering, Lyase, biology.organism_classification, 01 natural sciences, law.invention, 03 medical and health sciences, 030104 developmental biology, Enzyme, chemistry, Biochemistry, law, 010608 biotechnology, Recombinant DNA, Clostridium thermocellum

Published

2018

10. Molecular basis forB. pertussisinterference with complement, coagulation, fibrinolytic and contact activation systems: The cryo-EM structure of the Vag8-C1 inhibitor complex

Author

Dorina Roem, Steven Johnson, Arun Dhillon, Emily Furlong, Susan M. Lea, Ilse Jongerius, and Justin C. Deme

Subjects

chemistry.chemical_classification, Bordetella pertussis, Proteases, biology, Virulence, biology.organism_classification, C1-inhibitor, Cell biology, Serine, chemistry, Coagulation, biology.protein, Autotransporter domain, Glycoprotein

Abstract

Complement, contact activation, coagulation, and fibrinolysis are serum protein cascades that need strict regulation to maintain human health. Serum glycoprotein, C1-inhibitor (C1-INH) is a key regulator (inhibitor) of serine proteases of all the above-mentioned pathways. Recently, an autotransporter protein, Virulence Associated Gene 8 (Vag8) produced by the whopping cough causing pathogen,Bordetella pertussishas been shown to bind and interfere with C1-INH function. Here we present the structure of Vag8: C1-INH complex determined using cryo-electron microscopy at 3.6 Å resolution. The structure shows a unique mechanism of C1-INH inhibition not employed by other pathogens where Vag8 sequesters the Reactive Centre Loop of the C1-INH preventing its interaction with the target proteases.ImportanceThe structure 105 kDa protein complex is one of the smallest to be determined using cryo-electron microscopy at high resolution. The mechanism of disrupting C1-INH revealed by the structure is crucial to understand how pathogens by producing a single virulence factor can disturb several homeostasis pathways. Virulence mechanisms such as the one described here assume more importance given the emerging evidence about dysregulation of contact activation, coagulation and fibrinolysis leading to COVID-19 pneumonia.

Published

2020

11. Estrogen suppresses HOXB2 expression via ERα in breast cancer cells

Author

Sachin Kumar, Dixcy Jaba Sheeba John Mary, Ajay Kumar, Mohan C. Manjegowda, Deepak Modi, Neha Singh, Anil M. Limaye, and Arun Dhillon

Subjects

0301 basic medicine, medicine.drug_class, Down-Regulation, Breast Neoplasms, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Breast cancer, Phenols, Cell Line, Tumor, Gene expression, Genetics, medicine, Animals, Humans, Estrogen binding, skin and connective tissue diseases, Promoter Regions, Genetic, Transcription factor, Homeodomain Proteins, Gene knockdown, Estrogen Receptor alpha, Promoter, General Medicine, medicine.disease, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Estrogen, 030220 oncology & carcinogenesis, Cancer research, MCF-7 Cells, Pyrazoles, Female, Chromatin immunoprecipitation, hormones, hormone substitutes, and hormone antagonists, Neoplasm Transplantation, Transcription Factors

Abstract

The expression of HOXB2, a homeobox transcription factor, is altered in a variety of solid tumors. Using an in vivo screen to identify regulators of breast tumor growth in murine mammary fat pads, Boimel and co-workers recently identified HOXB2 as a tumor suppressor. However, the mechanistic underpinnings of its role in breast cancer is not understood. Given the emerging interaction of estrogen-regulated gene expression and altered HOX gene expression network in the pathophysiology of breast cancer, this study addressed the relationship between estrogen signaling and HOXB2 expression. Using a mouse model and human breast cancer cell lines, we show that estrogen suppresses HOXB2 expression. Suppression of HOXB2 by PPT, a known ERα agonist, in MCF-7 and T47D cells indicated the involvement of ERα, which was confirmed by siRNA-mediated ERα knockdown experiments. In-silico analysis of the upstream promoter region revealed the presence of three putative EREs. Chromatin immunoprecipitation experiments showed that upon estrogen binding, ERα engaged with EREs in the 5' upstream region of HOXB2 in MCF-7 and T47D cells. Future investigations should address the implications of estrogen-mediated suppression on the proposed tumor suppressor function of HOXB2.

Published

2020

12. Novel insights into the degradation of β-1,3-glucans by the cellulosome of Clostridium thermocellum revealed by structure and function studies of a family 81 glycoside hydrolase

Author

Márcia A. S. Correia, Arun Goyal, Krishan Kumar, Vikky Rajulapati, Kedar Sharma, Carlos M. G. A. Fontes, Virgínia M. R. Pires, Arun Dhillon, and Ana Luísa Carvalho

Subjects

Models, Molecular, 0301 basic medicine, beta-Glucans, Glycoside Hydrolases, Stereochemistry, 030106 microbiology, Mutant, Curdlan, Biochemistry, Substrate Specificity, Clostridium thermocellum, Cellulosome, 03 medical and health sciences, chemistry.chemical_compound, Hydrolysis, Laminarin, Protein Domains, Structural Biology, Glycoside hydrolase, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Molecular mass, biology, General Medicine, biology.organism_classification, Cellulosomes, Kinetics, 030104 developmental biology, chemistry, Mutagenesis, Site-Directed

Abstract

The family 81 glycoside hydrolase (GH81) from Clostridium thermocellum is a β-1,3-glucanase belonging to cellulosomal complex. The gene encoding GH81 from Clostridium thermocellum (CtLam81A) was cloned and expressed displaying a molecular mass of ~82 kDa. CtLam81A showed maximum activity against laminarin (100 U/mg), followed by curdlan (65 U/mg), at pH 7.0 and 75 °C. CtLam81A displayed Km, 2.1 ± 0.12 mg/ml and Vmax, 109 ± 1.8 U/mg, against laminarin under optimized conditions. CtLam81A activity was significantly enhanced by Ca2+ or Mg2+ ions. Melting curve analysis of CtLam81A showed an increase in melting temperature from 91 °C to 96 °C by Ca2+ or Mg2+ ions and decreased to 82 °C by EDTA, indicating that Ca2+ and Mg2+ ions may be involved in catalysis and in maintaining structural integrity. TLC and MALDI-TOF analysis of β-1,3-glucan hydrolysed products released initially, showed β-1,3-glucan-oligosaccharides degree of polymerization (DP) from DP2 to DP7, confirming an endo-mode of action. The catalytically inactive mutant CtLam81A-E515A generated by site-directed mutagenesis was co-crystallized and tetragonal crystals diffracting up to 1.4 A resolution were obtained. CtLam81A-E515A contained 15 α-helices and 38 β-strands forming a four-domain structure viz. a β-sandwich domain I at N-terminal, an α/β-domain II, an (α/α)6 barrel domain III, and a small 5-stranded β-sandwich domain IV.

Published

2018

13. Insights into the structural characteristics and substrate binding analysis of chondroitin AC lyase (PsPL8A) from Pedobacter saltans

Author

Arun Goyal, Kedar Sharma, Aruna Rani, and Arun Dhillon

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, Mutant, Molecular Conformation, Ab initio, Biochemistry, Substrate Specificity, Catalysis, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Structural Biology, Amino Acid Sequence, Molecular Biology, Protein secondary structure, Binding Sites, Chondroitin Lyases, 030102 biochemistry & molecular biology, Small-angle X-ray scattering, Circular Dichroism, Isothermal titration calorimetry, Sequence Analysis, DNA, General Medicine, Recombinant Proteins, Enzyme Activation, 030104 developmental biology, chemistry, Docking (molecular), Mutation, Mutagenesis, Site-Directed, Spectrophotometry, Ultraviolet, Pedobacter, Protein Binding, Chondroitin AC lyase

Abstract

The structure of chondroitin AC lyase (PsPL8A) of family 8 polysaccharide lyase was characterized. Modeled PsPL8A structure showed, it contains N-terminal (α/α)6 incomplete toroidal fold and a layered β sandwich structure at C-terminal. Ramchandran plot displayed 98.5% residues in favoured and 1.2% in generously allowed region. Secondary structure of PsPL8A by CD revealed 27.31% α helices 22.7% β sheets and 49.9% random coils. Protein melting study showed, PsPL8A completely unfolds at 60°C. SAXS analysis showed, PsPL8A is fully folded in solution form. The ab initio derived dummy model of PsPL8A superposed well with its modeled structure excluding some α-helices and loop region. Structural superposition and docking analysis showed, N153, W105, H203, Y208, Y212, R266 and E349 were involved in catalysis. Mutants N153A, H203A, Y212F, R266A and E349A created by SDM revealed no residual activity. Isothermal titration calorimetry analysis of Y212F and H203A with C4S polysaccharide, showed moderate binding by Y212F (Ka=9.56±3.81×105) and no binding with H203A, showing active contribution of Y212 in substrate binding. Residues Y212 and H203 or R266 might act as general base and general acid respectively. Residues N153 and E349 are likely contributing in charge neutralization and stabilizing enolate anion intermediate during β-elimination.

Published

2018

14. SAXS and homology modelling based structure characterization of pectin methylesterase a family 8 carbohydrate esterase from Clostridium thermocellum ATCC 27405

Author

Arun Goyal, Kedar Sharma, Arun Dhillon, and Vikky Rajulapati

Subjects

0301 basic medicine, Circular dichroism, Biophysics, Molecular Dynamics Simulation, Biochemistry, Esterase, Protein Structure, Secondary, Clostridium thermocellum, 03 medical and health sciences, X-Ray Diffraction, Catalytic Domain, Scattering, Small Angle, Amino Acid Sequence, Molecular Biology, Protein secondary structure, Multiple sequence alignment, Sequence Homology, Amino Acid, biology, Small-angle X-ray scattering, Chemistry, Circular Dichroism, biology.organism_classification, Molecular Docking Simulation, Crystallography, 030104 developmental biology, Radius of gyration, Carboxylic Ester Hydrolases, Ramachandran plot

Abstract

Pectin methylesterase (CtPME) from Clostridium thermocellum of family 8 carbohydrate esterase (CE8) belongs to pectin methylesterase super family (E.C.3.1.1.11). BLAST analysis of CtPME showed 38% sequence identity with PME from Erwinia chrysanthemi. Multiple sequence alignment of CtPME with other known structures of pectin methylesterase revealed the conserved and semi-conserved amino acid residues. Homology modelling of CtPME structure revealed a characteristic right handed parallel β-helices. The energy of modelled structure was minimized by using YASARA software. The Ramachandran plot of CtPME shows 83.7% residues in non-glycine and non-proline residues in most-favorable region, 13.8% in additional allowed region and 1.4% in generously allowed region, indicating that CtPME has a stable conformation. The secondary structure of CtPME predicted using PSI-Pred software and confirmed by the circular dichroism (CD) showed α-helices (3.1%), β-sheets (40.1%) and random coils (56.9%). Small Angle X-ray Scattering (SAXS) analysis demonstrated the overall shape and structural characterization of CtPME in solution form. Guinier analysis gave the radius of gyration (Rg) 2.28 nm for globular shape and 0.74 nm for rod shape. Kratky plot gave the indication that protein is fully folded in solution. The ab initio derived dummy atom model of CtPME superposed well on modelled CtPME structure.

Published

2018

15. STRUCTURE MODELING AND CHARACTERIZATION OF A RHAMNOGALACTURONAN LYASE (CtRGL) FROM Clostridium thermocellum

Author

Arun Dhillon and Arun Goyal

Subjects

Rhamnogalacturonan I, Clostridium thermocellum, lcsh:Biochemistry, Polysaccharide lyase, Circular Dichroism, Rhamnogalacturonan lyase, Homology modeling, lcsh:QD415-436, Pectin, Docking

Abstract

The truncated N-terminal catalytic module (CtRGL) of molecular size ~ 64 kDa of cellulosomal rhamnogalacturonan lyase, (CtRGLf) from Clostridium thermocellum belonging to family 11 polysaccharide lyase(PL11) was structurally characterized. Multiple sequence alignment revealed that CtRGL has conserved active site as well as Ca2+ binding sites. The secondary structure prediction by PsiPred and Circular Dichroism analysis showed the presence of approximately, 2% α-helix, 30% β-sheet and 65% loops. The structure of CtRGL based on homology modeling showed a β-propeller fold. Structure validation by Ramachandran plot revealed 99.6% residues in allowed region. Comparison of CtRGL structure with that of YesW and YesX proteins from Bacillus subtilis showed conserved catalytic cleft and endo-lytic mode of action. Docking analysis of CtRGL established Arg398, Thr475, Lys476 and Tyr536 as key residues of the active site. Lys476 was predicted to act as a catalytic base and Thr475 as a catalytic acid during â-elimination. This study provides an insight into the structural determinants for mode of action and substrate recognition.

Published

2017

16. A New Member of Family 11 Polysaccharide Lyase, Rhamnogalacturonan Lyase (CtRGLf) from Clostridium thermocellum

Author

Carlos M. G. A. Fontes, Arun Goyal, José A. M. Prates, Fernando M. V. Dias, Vania O. Fernandes, Arun Dhillon, Maria S.J. Centeno, and Luís M. A. Ferreira

Subjects

0301 basic medicine, food.ingredient, Pectin, Polysaccharide-Lyases, chemistry.chemical_element, Bioengineering, Calcium, Applied Microbiology and Biotechnology, Biochemistry, Catalysis, Substrate Specificity, Clostridium thermocellum, 03 medical and health sciences, food, Bacterial Proteins, Cloning, Molecular, Molecular Biology, chemistry.chemical_classification, biology, Chemistry, Lyase, biology.organism_classification, Enzyme assay, 030104 developmental biology, Enzyme, Rhamnogalacturonan I, biology.protein, Pectins, Biotechnology

Abstract

A thermostable, alkaline rhamnogalacturonan lyase (RG lyase) CtRGLf, of family 11 polysaccharide lyase from Clostridium thermocellum was cloned, expressed, purified and biochemically characterised. Both, the full-length CtRGLf (80 kDa) protein and its truncated derivative CtRGL (63.9 kDa) were expressed as soluble proteins and displayed maximum activity against rhamnogalacturonan I (RG I). CtRGLf showed maximum activity at 70 °C, while CtRGL at 60 °C. Both enzymes showed maximum activity at pH 8.5. CtRGLf and CtRGL do not show higher activity on substrates with high β-D-galactopyranose (D-Galp) substitution, this catalytic property deviates from that of some earlier characterised RG lyases which prefer substrates with high D-Galp substitution. The enzyme activity of CtRGLf and CtRGL was enhanced by 1.5 and 1.3 fold, respectively, in the presence of 3 mM of Ca(2+) ions. The TLC analysis of the degraded products of RG I, released by the action of CtRGLf and CtRGL revealed the production of RG oligosaccharides as major products confirming their endolytic activity.

Published

2016

17. Insights into Structure and Reaction Mechanism of β-Mannanases

Author

Kedar Sharma, Arun Dhillon, and Arun Goyal

Subjects

0301 basic medicine, 030103 biophysics, Reaction mechanism, Sequence (biology), Cell Biology, General Medicine, Biology, Into-structure, Biochemistry, Structure and function, Cell wall, 03 medical and health sciences, TIM barrel, Glycoside hydrolase, Molecular Biology, Function (biology)

Abstract

β-mannanases have been shown to play an important role in various biological processes such as the cell wall component degradation, defence signalling in plants, the mobilization of storage reserves and in various industrial processes. To date, glycoside hydrolases (GHs) have been divided into 135 families and 14 clans from A to N based upon their sequence, overall structural fold and function. β-mannanases belong glycoside hydrolases and exist under four different glycoside hydrolase families, GH5, GH26, GH113 and GH134. GH5 and GH26 are combined in clan GH-A. GH5 and GH26 contain hydrolases which follow the retaining type reaction mechanism. Structural survey of β-mannanases of GH5 and GH26, suggests that both families contain similar TIM barrel fold. In addition, they also share common catalytic residues and their location in the structure. Despite these structural similarities, a distinct difference lies between the substrate binding sub-sites which define substrate specificity. This review summarizes the recent reports on the structure and function perspectives of β-mannanases of GH5 and GH26 and highlights the similarities and differences between them.

Published

2017