Construction of a system for heterologous production of carbonic anhydrase from Plasmodium falciparum in Pichia pastoris

Gullberg, Erik

January 2008

Malaria is one of the biggest current global health problems, and with the increasing occurance of drug resistant Plasmodium falciparum strains, there is an urgent need for new antimalarial drugs. Given the important role of carbonic anhydrase in Plasmodium falciparum (PfCA), it is a potential novel drug target. Heterologous expression of malaria proteins is problematic due to the unusual codon usage of the Plasmodium genome, so to overcome this problem a synthetic PfCA gene was designed, optimized for expression in Pichia pastoris. This gene was also modified to avoid glycosylation, and cloned into the vector pPICZαA under the control of the methanol inducible promoter AOX1. To facilitate export of the protein into the growth medium, the gene was fused in-frame with the α-factor secretion signal from Saccharomyces cerevisiae. The construct was successfully integrated in the genome of P. pastoris GS115, and attempts were made to express the protein and purify it using immobilized metal ion affinity chromatography.In this work, no expression of the PfCA protein could be detected, so further research should focus on optimization of expression conditions, or redesign of the expression vector.

Carbonic anhydrase

Plasmodium

Pichia pastoris

expression system

Molecular biology

Molekylärbiologi

The interaction of human carbonic anhydrase II to solid surfaces and its applications

Udd, Annika

January 2009

The adsorption of proteins to solid surfaces has been extensively investigated during the past 20-30 years. The knowledge can be applied in biotechnological applications in for example immunoassays and biosensors. Human carbonic anhydrase II is a widely studied protein and the CO2-activity makes it an interesting candidate for biotechnological purposes. To make this possible, the factors affecting the adsorption of proteins have to be mapped. The stability of the protein is under great influence of the adsorption and the protein tends to undergo conformational changes leading to a molten globule like state upon adsorption. The stability of a protein also affects the extent of conformational changes and the nature of the adsorption. A more stable protein, adsorbs with less structural changes as a consequence of adsorption, and desorbs from the surface more rapidly than a less stable one. Also the hydrophobicity, charge and area of the surface are affecting the interaction with the protein. Still, the same adsorption pattern is noticed for the same protein at different surfaces, leading to the conclusion that the properties of the protein affect the interaction, rather than the properties of the surface. Biosensors containing carbonic anhydrase have been developed. These make measurement and detection of zinc ions possible. To be able to use carbonic anhydrase as a potential agent in biotechnology, attached to solid surfaces, the protein has to be biotechnologically engineered to get a more stable structure, or else the denaturation will destroy this possibility.

Human carbonic anhydrase II

solid surfaces

adsorption

applications

Biochemistry

Biokemi

Construction of a system for heterologous production of carbonic anhydrase from Plasmodium falciparum in Pichia pastoris

Gullberg, Erik

January 2008

<p>Malaria is one of the biggest current global health problems, and with the increasing occurance of drug resistant <em>Plasmodium falciparum</em> strains, there is an urgent need for new antimalarial drugs. Given the important role of carbonic anhydrase in <em>Plasmodium falciparum</em> (PfCA), it is a potential novel drug target. Heterologous expression of malaria proteins is problematic due to the unusual codon usage of the <em>Plasmodium </em>genome, so to overcome this problem a synthetic PfCA gene was designed, optimized for expression in <em>Pichia pastoris</em>. This gene was also modified to avoid glycosylation, and cloned into the vector pPICZαA under the control of the methanol inducible promoter AOX1. To facilitate export of the protein into the growth medium, the gene was fused in-frame with the α-factor secretion signal from <em>Saccharomyces cerevisiae</em>. The construct was successfully integrated in the genome of <em>P. pastoris</em> GS115, and attempts were made to express the protein and purify it using immobilized metal ion affinity chromatography.In this work, no expression of the PfCA protein could be detected, so further research should focus on optimization of expression conditions, or redesign of the expression vector.</p>

Carbonic anhydrase

Plasmodium

Pichia pastoris

expression system

Molecular biology

Molekylärbiologi

¹H magnetic resonance spectroscopic imaging of tumour extracellular pH : the role of carbonic anhydrase IX

Lee, Shen-Han

January 2013

No description available.

616.99

Bone Phenotype of Carbonic Anhydrase II Deficient and Calbindin-D28k Knockout Mice and Development of a Method to Measure In Vivo Bone Strains in Mice

Margolis, David Stephen

January 2008

Since the development of knockout and transgenic mouse models, mice have become the most widely used mammalian animal model to study bone. Despite the advances in knowledge of bone biology and function that have occurred from use of mouse models, many studies use primarily qualitative techniques, which may result in overlooking important subtle pathophysiologic changes. The hypothesis of this dissertation is that quantitative techniques to measure bone structure and function could identify the physiologic role of carbonic anhydrase II and calbindin-D28k in mouse bone, despite earlier qualitative studies indicating mice without these proteins have normal bone structure and function. Furthermore, a method to quantify bone function in vivo will be tested in a mouse model.Although carbonic anhydrase II deficient mice are less severely affected than patients, the mice demonstrate features of osteopetrosis including metaphyseal widening and a 50% increase in trabecular bone volume. The mice partially compensate for inhibited osteoclast function by increasing osteoclast number.Calbindin-D28k knockout mice demonstrated an increase in bone volume that results from additional bone at the endosteal surfaces. The higher bone volume results in increased stiffness and failure loads, highlighting the potential use of drugs that inhibit calbindin-D28k to treat diseases such as osteoporosis.Finally, calcium phosphate ceramic and hydroxyapatite particles used as strain gauge coatings demonstrated bone bonding to mouse femora after two months in vivo. The use of hydroxyapatite particles to coat strain gauges is the first time this method has been used with all commercially available materials, and will allow other research groups to use this technique. The major limitation to in vivo bone strain measurement in mice is the relatively large size of the sensors, which resulted in increased second moments of inertia in the implanted bones.Overall, this dissertation demonstrates that the use of quantitative techniques, including histology, histomorphometry, µCT imaging, and mechanical testing can measure subtle changes in bone properties that have been previously overlooked. Development of additional quantitative methods to study bone biomechanics in mouse models may encourage other research groups to quantify bone properties if no changes are noted using primarily qualitative methods.

Carbonic Anhydrase II

Calbindin-D28k

In Vivo Bone Strain Measurement

Pirimidino junginių - potencialių karboanhidrazių slopuklių - sintezė ir savybės / Synthesis And Properties Of Pyrimidine Derivatives – Potent Carbonic Anhydrase Inhibitors

Sūdžius, Jurgis

19 May 2011

Šio darbo tikslas – pirimidino junginių – potencialių karboanhidrazių (CA) slopiklių –kūrimas. Teoriniai 4-[N-(pirimidin-4-il)]aminobenzensulfonamidų, turinčių pakaitus 2-, 5- ir 6-oje pirimidino žiedo padėtyje, sąveikos su aktyviuoju hCA centru tyrimai parodė, kad šie junginiai gali įsiterpti į aktyvųjį baltymo centrą ir su hCA turėtų sąveikauti kaip tipiški klasikiniai CA slopikliai. Tiksliniai 4-[N-(2,5,6-pakeisti pirimidin-4-il)amino]benzensulfonamidai sintetinti 4,6-dichlorpirimidinuose, 5-oje padėtyje turinčiuose cian-, formil- arba nitrogrupes, chloro atomą keičiant 4-aminobenzensulfonamidu. Bendradarbiaujant su Biotechnologijos instituto mokslininkais, kurie atliko hCA slopinimo susintetintais junginiais tyrimus, tobulintos šių junginių hCA slopinimo savybės. Slopiklių struktūros modifikuotos keičiant jungtuko tarp benzensulfonamido ir pirimidino fragmentų ilgį ir įvedant naujus pakaitus pirimidino žiede, kai kuriais atvejais taip sudarant naujas heterociklines sistemas. Šiuo tikslu ištirta pirimidin-5-karbaldehidų kondensacija su indolin-2-tionais. Nustatyta, kad 4-[N-(pirimidin-4-il)amino](metil-,etil-)benzensulfonamidai, 5-oje pirimidino žiedo padėtyje turintys cian-, formil- arba nitrogrupes, o 6-oje pirimidino žiedo padėtyje turintys benzilamino-, chlor-, metoksi- arba oksogrupes, yra nano- – mikromolinės eilės hCA slopikliai, galintys atrankiai slopinti hCAI, II ar XIII. Jų hCA slopinimo aktyvumą lemia sulfonamido grupės sąveika su katalitiniu cinko jonu ir... [toliau žr. visą tekstą] / The aim of the work was design of pyrimidine derivatives – potent carbonic anhydrase (CA) inhibitors. Theoretical investigation of interaction of 4-[N-(pyrimidin-4-yl)]aminobenzenesulfonamides containing substituents at 2-, 5- and 6- positions of pyrimidine ring with an active site of hCAs suggested that these compounds can fit into an active site of the enzymes and should interact with them as typical hCA inhibitors. Synthesis of target compounds was carried out by substitution of chloro group at 4,6-dichloropyrimidines containing cyano-, formyl- or nitro groups at position 5 of the pyrimidine ring with 4-aminobenzenesulfonamide. Regarding inhibition of hCAs with the synthesized compounds data acquired by the scientists of Institute of Biotechnology, structures of inhibitors were modified in order to improve their binding properties to hCA. It was performed by variation of a linker length between benzenesulfonamide and pyrimidine fragments and by introduction of new substituents at position 6 of the pyrimidine ring. In some cases these modifications led to the formation of new heterocyclic systems. For this purpose condensation of indoline-2-thiones with pyrimidine-5-carbaldehydes was investigated. It was determined that 4-[N-(pyrimidin-4-yl)amino](methyl-,ethyl-)benzenesulfonamides containing cyano-, formyl- or nitro groups at position 5 of the pyrimidine ring and benzylamino-, chloro-, methoxy- or oxo groups at position 6 of the pyrimidine ring inhibit hCA in... [to full text]

Chemistry

Pirimidinas

Karboanhidrazių slopikliai

Dokinimas

Pyrimidine

Carbonic anhydrase inhibitors

Docking

Synthesis And Properties Of Pyrimidine Derivatives – Potent Carbonic Anhydrase Inhibitors / Pirimidino junginių - potencialių karboanhidrazių slopiklių - sintezė ir savybės

Sūdžius, Jurgis

19 May 2011

The aim of the work was design of pyrimidine derivatives – potent carbonic anhydrase (CA) inhibitors. Theoretical investigation of interaction of 4-[N-(pyrimidin-4-yl)]aminobenzenesulfonamides containing substituents at 2-, 5- and 6- positions of pyrimidine ring with an active site of hCAs suggested that these compounds can fit into an active site of the enzymes and should interact with them as typical hCA inhibitors. Synthesis of target compounds was carried out by substitution of chloro group at 4,6-dichloropyrimidines containing cyano-, formyl- or nitro groups at position 5 of the pyrimidine ring with 4-aminobenzenesulfonamide. Regarding inhibition of hCAs with the synthesized compounds data acquired by the scientists of Institute of Biotechnology, structures of inhibitors were modified in order to improve their binding properties to hCA. It was performed by variation of a linker length between benzenesulfonamide and pyrimidine fragments and by introduction of new substituents at position 6 of the pyrimidine ring. In some cases these modifications led to the formation of new heterocyclic systems. For this purpose condensation of indoline-2-thiones with pyrimidine-5-carbaldehydes was investigated. It was determined that 4-[N-(pyrimidin-4-yl)amino](methyl-,ethyl-)benzenesulfonamides containing cyano-, formyl- or nitro groups at position 5 of the pyrimidine ring and benzylamino-, chloro-, methoxy- or oxo groups at position 6 of the pyrimidine ring inhibit hCA in... [to full text] / Šio darbo tikslas – pirimidino junginių – potencialių karboanhidrazių (CA) slopiklių –kūrimas. Teoriniai 4-[N-(pirimidin-4-il)]aminobenzensulfonamidų, turinčių pakaitus 2-, 5- ir 6-oje pirimidino žiedo padėtyje, sąveikos su aktyviuoju hCA centru tyrimai parodė, kad šie junginiai gali įsiterpti į aktyvųjį baltymo centrą ir su hCA turėtų sąveikauti kaip tipiški klasikiniai CA slopikliai. Tiksliniai 4-[N-(2,5,6-pakeisti pirimidin-4-il)amino]benzensulfonamidai sintetinti 4,6-dichlorpirimidinuose, 5-oje padėtyje turinčiuose cian-, formil- arba nitrogrupes, chloro atomą keičiant 4-aminobenzensulfonamidu. Bendradarbiaujant su Biotechnologijos instituto mokslininkais, kurie atliko hCA slopinimo susintetintais junginiais tyrimus, tobulintos šių junginių hCA slopinimo savybės. Slopiklių struktūros modifikuotos keičiant jungtuko tarp benzensulfonamido ir pirimidino fragmentų ilgį ir įvedant naujus pakaitus pirimidino žiede, kai kuriais atvejais taip sudarant naujas heterociklines sistemas. Šiuo tikslu ištirta pirimidin-5-karbaldehidų kondensacija su indolin-2-tionais. Nustatyta, kad 4-[N-(pirimidin-4-il)amino](metil-,etil-)benzensulfonamidai, 5-oje pirimidino žiedo padėtyje turintys cian-, formil- arba nitrogrupes, o 6-oje pirimidino žiedo padėtyje turintys benzilamino-, chlor-, metoksi- arba oksogrupes, yra nano- – mikromolinės eilės hCA slopikliai, galintys atrankiai slopinti hCAI, II ar XIII. Jų hCA slopinimo aktyvumą lemia sulfonamido grupės sąveika su katalitiniu cinko jonu ir... [toliau žr. visą tekstą]

Chemistry

Pyrimidine

Carbonic anhydrase inhibitors

Docking

Pirimidinas

Karboanhidrazių slopikliai

Dokinimas

Rekombinantinių žmogaus karboanhidrazių I, II, VII, IX, XIII sąveikos su ligandais tyrimas / Analysis of ligand binding to recombinant human carbonic anhydrases I, II, VII, IX and XIII

Baranauskienė, Lina

27 March 2013

Karboanhidrazės (CA) yra metalofermentai, katalizuojantys virsmus tarp anglies dioksido ir bikarbonato. Jų slopinimas gali būti taikomas gydyti tokias skirtingas ligas kaip glaukoma, vėžys, nutukimas, epilepsija, osteoporozė ir kt. Šiuo metu yra beveik 30 mažamolekulinių junginių, kurie naudojami kaip vaistai, su padidėjusiu karboanhidrazių aktyvumu susijusioms ligoms gydyti. Darbe tirta rekombinantinių žmogaus karboanhidrazių I, II, VII, IX ir XIII sąveika su sulfonamidiniais ligandais. Įvertintas tirtų baltymų stabilumas skirtingomis eksperimentinėmis sąlygomis, nustatyta priešvėžinio taikinio CA IX oligomerinė būsena. Modeliniais baltymais naudojant karboanhidrazes, praplėstos terminio poslinkio metodo taikymo ribos. Išmatuoti 40 naujų susintetintų junginių sąveikos su karboanhidrazėmis termodinaminiai parametrai, išanalizuota CA XIII sąveikos su sulfonamidiniais slopikliais termodinamika, atskiriant tikruosius, nuo eksperimento sąlygų ir susijusių reakcijų nepriklausančius jungimosi parametrus. / Carbonic anhydrases (CAs) are metalloenzymes that catalyze the conversion between carbon dioxide and bicarbonate. Their inhibition can be applied for treatment of different diseases, such as glaucoma, cancer, obesity, epilepsy, osteoporosis, etc. There are nearly 30 small molecule ligands that are used as drugs for carbonic anhydrase related diseases. In this work interaction between recombinant human carbonic anhydrases I, II, VII, IX, XIII and sulfonamide ligands was analysed. Stability of selected carbonic anhydrases was evaluated in different experimental conditions. Oligomeric structure of anticancer target CA IX was determined. Using carbonic anhydrases as model proteins, the application range of thermal shift assay was extended. Binding parameters of 40 new compounds to human carbonic anhydrases were measured. The binding thermodynamics of sulfonamide ligands to CA XIII was analyzed and intrinsic binding parameters, independent of the experimental conditions and linked protonation reactions, were determined.

Biochemistry

Karboanhidrazė

Sulfonamidas

Termodinamika

Carbonic anhydrase

Sulfonamide

Thermodynamics

Analysis of ligand binding to recombinant human carbonic anhydrases I, II, VII, IX and XIII / Rekombinantinių žmogaus karboanhidrazių I, II, VII, IX, XIII sąveikos su ligandais tyrimas

Baranauskienė, Lina

27 March 2013

Carbonic anhydrases (CAs) are metalloenzymes that catalyze the conversion between carbon dioxide and bicarbonate. Their inhibition can be applied for treatment of different diseases, such as glaucoma, cancer, obesity, epilepsy, osteoporosis, etc. There are nearly 30 small molecule ligands that are used as drugs for carbonic anhydrase related diseases. In this work interaction between recombinant human carbonic anhydrases I, II, VII, IX, XIII and sulfonamide ligands was analysed. Stability of selected carbonic anhydrases was evaluated in different experimental conditions. Oligomeric structure of anticancer target CA IX was determined. Using carbonic anhydrases as model proteins, the application range of thermal shift assay was extended. Binding parameters of 40 new compounds to human carbonic anhydrases were measured. The binding thermodynamics of sulfonamide ligands to CA XIII was analyzed and intrinsic binding parameters, independent of the experimental conditions and linked protonation reactions, were determined. / Karboanhidrazės (CA) yra metalofermentai, katalizuojantys virsmus tarp anglies dioksido ir bikarbonato. Jų slopinimas gali būti taikomas gydyti tokias skirtingas ligas kaip glaukoma, vėžys, nutukimas, epilepsija, osteoporozė ir kt. Šiuo metu yra beveik 30 mažamolekulinių junginių, kurie naudojami kaip vaistai, su padidėjusiu karboanhidrazių aktyvumu susijusioms ligoms gydyti. Darbe tirta rekombinantinių žmogaus karboanhidrazių I, II, VII, IX ir XIII sąveika su sulfonamidiniais ligandais. Įvertintas tirtų baltymų stabilumas skirtingomis eksperimentinėmis sąlygomis, nustatyta priešvėžinio taikinio CA IX oligomerinė būsena. Modeliniais baltymais naudojant karboanhidrazes, praplėstos terminio poslinkio metodo taikymo ribos. Išmatuoti 40 naujų susintetintų junginių sąveikos su karboanhidrazėmis termodinaminiai parametrai, išanalizuota CA XIII sąveikos su sulfonamidiniais slopikliais termodinamika, atskiriant tikruosius, nuo eksperimento sąlygų ir susijusių reakcijų nepriklausančius jungimosi parametrus.

Biochemistry

Carbonic anhydrase

Sulfonamide

Thermodynamics

Karboanhidrazė

Sulfonamidas

Termodinamika

Carbonic anhydrase II promotes cardiomyocyte hypertrophy

Brown, Brittany Fielding

Unknown Date

No description available.

transport metabolon

heart failure

carbonic anhydrase

AE3

bicarbonate transport

hypertrophy