Your search keyword '"MAZURKIEWICZ-PISAREK, A."' showing total 26 results

1. In vitro immune evaluation of adenoviral vector-based platform for infectious diseases

Author

Joanna Baran, Łukasz Kuryk, Teresa Szczepińska, Michał Łaźniewski, Mariangela Garofalo, Anna Mazurkiewicz-Pisarek, Diana Mikiewicz, Alina Mazurkiewicz, Maciej Trzaskowski, Magdalena Wieczorek, Katarzyna Pancer, Ewelina Hallmann, Lidia Brydak, Dariusz Plewczynski, Tomasz Ciach, Jolanta Mierzejewska, and Monika Staniszewska

Subjects

adenoviral vectors, vaccine platform, innate and adaptive immunity, Biotechnology, TP248.13-248.65

Abstract

New prophylactic vaccine platforms are imperative to combat respiratory infections. The efficacy of T and B memory cell-mediated protection, generated through the adenoviral vector, was tested to assess the effectiveness of the new adenoviral-based platforms for infectious diseases. A combination of adenovirus AdV1 (adjuvant), armed with costimulatory ligands (ICOSL and CD40L), and rRBD (antigen: recombinant nonglycosylated spike protein rRBD) was used to promote the differentiation of T and B lymphocytes. Adenovirus AdV2 (adjuvant), without ligands, in combination with rRBD, served as a control. In vitro T-cell responses to the AdV1+rRBD combination revealed that CD8+ platform-specific T-cells increased (37.2±0.7% vs. 23.1±2.1%), and T-cells acted against SARS-CoV-2 via CD8+TEMRA (50.0±1.3% vs. 36.0±3.2%). Memory B cells were induced after treatment with either AdV1+rRBD (84.1±0.8% vs. 82.3±0.4%) or rRBD (94.6±0.3% vs. 82.3±0.4%). Class-switching from IgM and IgD to isotype IgG following induction with rRBD+Ab was observed. RNA-seq profiling identified gene expression patterns related to T helper cell differentiation that protect against pathogens. The analysis determined signaling pathways controlling the induction of protective immunity, including the MAPK cascade, adipocytokine, cAMP, TNF, and Toll-like receptor signaling pathway. The AdV1+rRBD formulation induced IL-6, IL-8, and TNF. RNA-seq of the VERO E6 cell line showed differences in the apoptosis gene expression stimulated with the platforms vs. mock. In conclusion, AdV1+rRBD effectively generates T and B memory cell-mediated protection, presenting promising results in producing CD8+ platform-specific T cells and isotype-switched IgG memory B cells. The platform induces protective immunity by controlling the Th1, Th2, and Th17 cell differentiation gene expression patterns. Further studies are required to confirm its effectiveness.

Published

2023

2. Expression of the gene encoding blood coagulation factor VIII without domain B in E. coli bacterial expression system

Author

Anna Mazurkiewicz-Pisarek, Alina Mazurkiewicz, Diana Mikiewicz, Piotr Baran, and Tomasz Ciach

Subjects

factor viii, hemophilia type a, recombinant coagulation factor viii, prokaryotic expression system, e. coli, recombinant protein production system, Biotechnology, TP248.13-248.65

Abstract

In this article, we have demonstrated the feasibility of generating an active form of recombinant blood coagulation factor VIII using an E. coli bacterial expression system as a potential treatment for hemophilia type A. Factor VIII (FVIII), an essential blood coagulation protein, is a key component of the fluid phase blood coagulation system. So far, all available recombinant FVIII formulations have been produced using eukaryotic expression systems. Mammalian cells can produce catalytically active proteins with all the necessary posttranslational modifications. However, cultivating such cells is time-consuming and highly expensive, and the amount of the obtained product is usually low. In contrast to eukaryotic cells, bacterial culture is inexpensive and allows the acquisition of large quantities of recombinant proteins in a short time. With this study, we aimed to obtain recombinant blood coagulation factor VIII using the E. coli bacterial expression system, a method not previously explored for this purpose. Our research encompasses the synthesis of blood coagulation factor VIII and its expression in a prokaryotic system. To achieve this, we constructed a prokaryotic expression vector containing a synthetic factor VIII gene, which was then used for the transformation of an E. coli bacterial strain. The protein expression was confirmed by mass spectrometry, and we assessed the stability of the gene construct while determining the optimal growth conditions. The production of blood coagulation factor VIII by the E. coli bacterial strain was carried out on a quarter-technical scale. We established the conditions for isolation, denaturation, and renaturation of the protein, and subsequently confirmed the activity of FVIII.

Published

2023

3. Mast Cells as a Target—A Comprehensive Review of Recent Therapeutic Approaches

Author

Joanna Baran, Anna Sobiepanek, Anna Mazurkiewicz-Pisarek, Marta Rogalska, Aleksander Gryciuk, Lukasz Kuryk, Soman N. Abraham, and Monika Staniszewska

Subjects

mast cells, cytokines, degranulation, anaphylaxis, cancer, therapy, Cytology, QH573-671

Abstract

Mast cells (MCs) are the immune cells distributed throughout nearly all tissues, mainly in the skin, near blood vessels and lymph vessels, nerves, lungs, and the intestines. Although MCs are essential to the healthy immune response, their overactivity and pathological states can lead to numerous health hazards. The side effect of mast cell activity is usually caused by degranulation. It can be triggered by immunological factors, such as immunoglobulins, lymphocytes, or antigen–antibody complexes, and non-immune factors, such as radiation and pathogens. An intensive reaction of mast cells can even lead to anaphylaxis, one of the most life-threatening allergic reactions. What is more, mast cells play a role in the tumor microenvironment by modulating various events of tumor biology, such as cell proliferation and survival, angiogenesis, invasiveness, and metastasis. The mechanisms of the mast cell actions are still poorly understood, making it difficult to develop therapies for their pathological condition. This review focuses on the possible therapies targeting mast cell degranulation, anaphylaxis, and MC-derived tumors.

Published

2023

4. Portable Surface Plasmon Resonance Detector for COVID-19 Infection

Author

Maciej Trzaskowski, Anna Mazurkiewicz-Pisarek, Jakub Waldemar Trzciński, Marcin Drozd, Rafał Podgórski, Anna Zabost, and Ewa Augustynowicz-Kopeć

Subjects

surface plasmon resonance, COVID-19, point-of-care detection, portable devices, Chemical technology, TP1-1185

Abstract

Methods based on nucleic acid detection are currently the most commonly used technique in COVID-19 diagnostics. Although generally considered adequate, these methods are characterised by quite a long time-to-result and the necessity to prepare the material taken from the examined person—RNA isolation. For this reason, new detection methods are being sought, especially those characterised by the high speed of the analysis process from the moment of sampling to the result. Currently, serological methods of detecting antibodies against the virus in the patient’s blood plasma have attracted much attention. Although they are less precise in determining the current infection, such methods shorten the analysis time to several minutes, making it possible to consider them a promising method for screening tests in people with suspected infection. The described study investigated the feasibility of a surface plasmon resonance (SPR)-based detection system for on-site COVID-19 diagnostics. A simple-to-use portable device was proposed for the fast detection of anti-SARS-CoV-2 antibodies in human plasma. SARS-CoV-2-positive and -negative patient blood plasma samples were investigated and compared with the ELISA test. The receptor-binding domain (RBD) of spike protein from SARS-CoV-2 was selected as a binding molecule for the study. Then, the process of antibody detection using this peptide was examined under laboratory conditions on a commercially available SPR device. The portable device was prepared and tested on plasma samples from humans. The results were compared with those obtained in the same patients using the reference diagnostic method. The detection system is effective in the detection of anti-SARS-CoV-2 with the detection limit of 40 ng/mL. It was shown that it is a portable device that can correctly examine human plasma samples within a 10 min timeframe.

Published

2023

5. Molecular dissection of the replication system of plasmid pIGRK encoding two in-frame Rep proteins with antagonistic functions

Author

Paweł Wawrzyniak, Agnieszka Sobolewska-Ruta, Piotr Zaleski, Natalia Łukasiewicz, Paulina Kabaj, Piotr Kierył, Agata Gościk, Anna Bierczyńska-Krzysik, Piotr Baran, Anna Mazurkiewicz-Pisarek, Andrzej Płucienniczak, and Dariusz Bartosik

Subjects

Overlapping genes, Plasmid replication, Replication system, Rep protein, In-frame proteins, Transcription regulation, Microbiology, QR1-502

Abstract

Abstract Background Gene overlapping is a frequent phenomenon in microbial genomes. Excluding so-called “trivial overlapping”, there are significant implications of such genetic arrangements, including regulation of gene expression and modification of protein activity. It is also postulated that, besides gene duplication, the appearance of overlapping genes (OGs) is one of the most important factors promoting a genome’s novelty and evolution. OGs coding for in-frame proteins with different functions are a particularly interesting case. In this study we identified and characterized two in-frame proteins encoded by OGs on plasmid pIGRK from Klebsiella pneumoniae, a representative of the newly distinguished pHW126 plasmid family. Results A single repR locus located within the replication system of plasmid pIGRK encodes, in the same frame, two functional polypeptides: a full-length RepR protein and a RepR’ protein (with N-terminal truncation) translated from an internal START codon. Both proteins form homodimers, and interact with diverse DNA regions within the plasmid replication origin and repR promoter operator. Interestingly, RepR and RepR’ have opposing functions – RepR is crucial for initiation of pIGRK replication, while RepR’ is a negative regulator of this process. Nevertheless, both proteins act cooperatively as negative transcriptional regulators of their own expression. Conclusions Regulation of the initiation of pIGRK replication is a complex process in which a major role is played by two in-frame proteins with antagonistic functions. In-frame encoded Rep proteins are uncommon, having been described in only a few plasmids. This is the first description of such proteins in a plasmid of the pHW126 family.

Published

2019

6. Antimicrobial Peptides: Challenging Journey to the Pharmaceutical, Biomedical, and Cosmeceutical Use

Author

Mazurkiewicz-Pisarek, Anna, primary, Baran, Joanna, additional, and Ciach, Tomasz, additional

Published

2023

7. Mast Cells as a Target—A Comprehensive Review of Recent Therapeutic Approaches

Author

Baran, Joanna, primary, Sobiepanek, Anna, additional, Mazurkiewicz-Pisarek, Anna, additional, Rogalska, Marta, additional, Gryciuk, Aleksander, additional, Kuryk, Lukasz, additional, Abraham, Soman N., additional, and Staniszewska, Monika, additional

Published

2023

8. Portable Surface Plasmon Resonance Detector for COVID-19 Infection

Author

Trzaskowski, Maciej, primary, Mazurkiewicz-Pisarek, Anna, additional, Trzciński, Jakub Waldemar, additional, Drozd, Marcin, additional, Podgórski, Rafał, additional, Zabost, Anna, additional, and Augustynowicz-Kopeć, Ewa, additional

Published

2023

9. Molecular dissection of the replication system of plasmid pIGRK encoding two in-frame Rep proteins with antagonistic functions

Author

Wawrzyniak, Paweł, Sobolewska-Ruta, Agnieszka, Zaleski, Piotr, Łukasiewicz, Natalia, Kabaj, Paulina, Kierył, Piotr, Gościk, Agata, Bierczyńska-Krzysik, Anna, Baran, Piotr, Mazurkiewicz-Pisarek, Anna, Płucienniczak, Andrzej, and Bartosik, Dariusz

Published

2019

10. In vitro immune evaluation of adenoviral vector-based platform for infectious diseases.

Author

KURYK, JOANNA BARAN1,ŁUKASZ, SZCZEPIŃSKA, TERESA, ŁAŹNIEWSKI, MICHAŁ, GAROFALO, MARIANGELA, MAZURKIEWICZ-PISAREK, ANNA, MIKIEWICZ, DIANA, MAZURKIEWICZ, ALINA, TRZASKOWSKI, MACIEJ, WIECZOREK, MAGDALENA, PANCER, KATARZYNA, HALLMANN, EWELINA, BRYDAK, LIDIA, PLEWCZYNSKI, DARIUSZ, CIACH, TOMASZ, MIERZEJEWSKA, JOLANTA, and STANISZEWSKA, MONIKA

Subjects

T helper cells, T cell differentiation, B cell differentiation, GENETIC vectors, IMMUNOLOGIC memory, COMMUNICABLE diseases, PLANT protection

Abstract

New prophylactic vaccine platforms are imperative to combat respiratory infections. The efficacy of T and B memory cell-mediated protection, generated through the adenoviral vector, was tested to assess the effectiveness of the new adenoviral-based platforms for infectious diseases. A combination of adenovirus AdV1 (adjuvant), armed with costimulatory ligands (ICOSL and CD40L), and rRBD (antigen: recombinant nonglycosylated spike protein rRBD) was used to promote the differentiation of T and B lymphocytes. Adenovirus AdV2 (adjuvant), without ligands, in combination with rRBD, served as a control. In vitro T-cell responses to the AdV1+rRBD combination revealed that CD8+ platform-specific T-cells increased (37.2 ± 0.7% vs. 23.1 ± 2.1%), and T-cells acted against SARS-CoV-2 via CD8+TEMRA (50.0 ± 1.3% vs. 36.0 ± 3.2%). Memory B cells were induced after treatment with either AdV1+rRBD (84.1 ± 0.8% vs. 82.3 ± 0.4%) or rRBD (94.6 ± 0.3% vs. 82.3 ± 0.4%). Class-switching from IgM and IgD to isotype IgG following induction with rRBD+Ab was observed. RNA-seq profiling identified gene expression patterns related to T helper cell differentiation that protect against pathogens. The analysis determined signaling pathways controlling the induction of protective immunity, including the MAPK cascade, adipocytokine, cAMP, TNF, and Toll-like receptor signaling pathway. The AdV1+rRBD formulation induced IL-6, IL-8, and TNF. RNA-seq of the VERO E6 cell line showed differences in the apoptosis gene expression stimulated with the platforms vs. mock. In conclusion, AdV1+rRBD effectively generates T and B memory cell-mediated protection, presenting promising results in producing CD8+ platform-specific T cells and isotype-switched IgG memory B cells. The platform induces protective immunity by controlling the Th1, Th2, and Th17 cell differentiation gene expression patterns. Further studies are required to confirm its effectiveness. [ABSTRACT FROM AUTHOR]

Published

2023

11. In vitro immune evaluation of adenoviral vector-based platform for infectious diseases

Author

Baran, Joanna, primary, Kuryk, Łukasz, additional, Szczepińska, Teresa, additional, Łaźniewski, Michał, additional, Garofalo, Mariangela, additional, Mazurkiewicz-Pisarek, Anna, additional, Mikiewicz, Diana, additional, Mazurkiewicz, Alina, additional, Trzaskowski, Maciej, additional, Wieczorek, Magdalena, additional, Pancer, Katarzyna, additional, Hallmann, Ewelina, additional, Brydak, Lidia, additional, Plewczynski, Dariusz, additional, Ciach, Tomasz, additional, Mierzejewska, Jolanta, additional, and Staniszewska, Monika, additional

Published

2023

12. Expression of the gene encoding blood coagulation factor VIII without domain B in E. coli bacterial expression system

Author

Mazurkiewicz-Pisarek, Anna, primary, Mazurkiewicz, Alina, additional, Mikiewicz, Diana, additional, Baran, Piotr, additional, and Ciach, Tomasz, additional

Published

2023

13. Antimicrobial Peptides: Challenging Journey to the Pharmaceutical, Biomedical, and Cosmeceutical Use

Author

Anna Mazurkiewicz-Pisarek, Joanna Baran, and Tomasz Ciach

Subjects

Inorganic Chemistry, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Antimicrobial peptides (AMPs), or host defence peptides, are short proteins in various life forms. Here we discuss AMPs, which may become a promising substitute or adjuvant in pharmaceutical, biomedical, and cosmeceutical uses. Their pharmacological potential has been investigated intensively, especially as antibacterial and antifungal drugs and as promising antiviral and anticancer agents. AMPs exhibit many properties, and some of these have attracted the attention of the cosmetic industry. AMPs are being developed as novel antibiotics to combat multidrug-resistant pathogens and as potential treatments for various diseases, including cancer, inflammatory disorders, and viral infections. In biomedicine, AMPs are being developed as wound-healing agents because they promote cell growth and tissue repair. The immunomodulatory effects of AMPs could be helpful in the treatment of autoimmune diseases. In the cosmeceutical industry, AMPs are being investigated as potential ingredients in skincare products due to their antioxidant properties (anti-ageing effects) and antibacterial activity, which allows the killing of bacteria that contribute to acne and other skin conditions. The promising benefits of AMPs make them a thrilling area of research, and studies are underway to overcome obstacles and fully harness their therapeutic potential. This review presents the structure, mechanisms of action, possible applications, production methods, and market for AMPs.

Published

2023

14. Molecular dissection of the replication system of plasmid pIGRK encoding two in-frame Rep proteins with antagonistic functions

Author

Anna Bierczyńska-Krzysik, Anna Mazurkiewicz-Pisarek, Andrzej Plucienniczak, Dariusz Bartosik, Paweł Wawrzyniak, Paulina Kabaj, Piotr Kierył, Natalia Łukasiewicz, Piotr Baran, Piotr Zaleski, Agata Gościk, and Agnieszka Sobolewska-Ruta

Subjects

Microbiology (medical), lcsh:QR1-502, Replication Origin, Locus (genetics), Biology, Replication system, Microbiology, Genome, lcsh:Microbiology, In-frame proteins, 03 medical and health sciences, chemistry.chemical_compound, Overlapping genes, Plasmid, Bacterial Proteins, Start codon, Gene Duplication, Gene duplication, Cloning, Molecular, Promoter Regions, Genetic, Gene, 030304 developmental biology, Genetics, Regulation of gene expression, 0303 health sciences, 030306 microbiology, Transcription regulation, Gene Expression Regulation, Bacterial, Rep protein, DNA-Binding Proteins, Klebsiella pneumoniae, chemistry, Protein Multimerization, Plasmid replication, DNA, Research Article, Plasmids

Abstract

BackgroundGene overlapping is a frequent phenomenon in microbial genomes. Excluding so-called “trivial overlapping”, there are significant implications of such genetic arrangements, including regulation of gene expression and modification of protein activity. It is also postulated that, besides gene duplication, the appearance of overlapping genes (OGs) is one of the most important factors promoting a genome’s novelty and evolution. OGs coding for in-frame proteins with different functions are a particularly interesting case. In this study we identified and characterized two in-frame proteins encoded by OGs on plasmid pIGRK fromKlebsiella pneumoniae, a representative of the newly distinguished pHW126 plasmid family.ResultsA singlerepRlocus located within the replication system of plasmid pIGRK encodes, in the same frame, two functional polypeptides: a full-length RepR protein and a RepR’ protein (withN-terminal truncation) translated from an internal START codon. Both proteins form homodimers, and interact with diverse DNA regions within the plasmid replication origin andrepRpromoter operator. Interestingly, RepR and RepR’ have opposing functions – RepR is crucial for initiation of pIGRK replication, while RepR’ is a negative regulator of this process. Nevertheless, both proteins act cooperatively as negative transcriptional regulators of their own expression.ConclusionsRegulation of the initiation of pIGRK replication is a complex process in which a major role is played by two in-frame proteins with antagonistic functions. In-frame encoded Rep proteins are uncommon, having been described in only a few plasmids. This is the first description of such proteins in a plasmid of the pHW126 family.

Published

2019

15. Expression of yeast deubiquitination enzyme UBP1 analogues in E. coli

Author

Chojnacka Luiza, Mikiewicz-Sygula Diana, Plucienniczak Grazyna, Mazurkiewicz-Pisarek Anna, Wojtowicz Anna, Lukasiewicz Natalia, and Plucienniczak Andrzej

Subjects

Microbiology, QR1-502

Abstract

Abstract Background It has been shown that proteins fused to ubiquitin undergo greater expression in E. coli and are easier to purify and renaturate than nonhybrid foreign proteins. However, there is no commercial source of large quantities of specific deubiquitinating proteases. This is the reason why hybrid proteins containing ubiquitin at their N-end cannot be used in large scale biotechnological processes. Results and Conclusion We have described the synthesis of the yeast deubiquination enzyme UBP1 muteins in E. coli. We have shown that an efficient overproduction of the enzyme in E. coli may be achieved after the introduction of several changes in the nucleotide sequence encoding UBP1. One of the conditions of an effective synthesis of the UBP1 muteins is the removal of the 5'-end sequence encoding the transmembrane region of the enzyme. The obtained variants of the enzyme may be successfully used for processing large amounts of hybrid proteins comprising ubiquitin or tagged ubiquitin at their N-ends.

Published

2005

16. The factor VIII protein and its function

Author

Anna Mazurkiewicz-Pisarek, Grazyna Plucienniczak, Tomasz Ciach, and Andrzej Plucienniczak

Subjects

Models, Molecular, 0301 basic medicine, Severe bleeding, Coagulation protein, Heavy chain, Factor VIII, Chemistry, Single chain, Hemophilia A, Immunoglobulin light chain, General Biochemistry, Genetics and Molecular Biology, Factor IXa, 03 medical and health sciences, 030104 developmental biology, Biochemistry, Humans, Secretion, Function (biology)

Abstract

Factor VIII (FVIII), an essential blood coagulation protein, is a key component of the fluid phase blood coagulation system. Human factor VIII is a single chain of about 300 kDa consisting of domains described as A1-A2-B-A3-C1-C2. The protein undergoes processing prior to secretion into blood resulting in a heavy chain of 200 kDa (A1-A2-B) and a light chain of 80 kDa (A3-C1-C2) linked by metal ions. The role of factor VIII is to increase the catalytic efficiency of factor IXa in the activation of factor X. Variants of these factors lead frequently also to severe bleeding disorders.

Published

2016

17. The factor VIII protein and its function.

Author

Mazurkiewicz-Pisarek, Anna, primary, Płucienniczak, Grażyna, primary, Ciach, Tomasz, primary, and Płucienniczak, Andrzej, primary

Published

2016

18. Expression of yeast deubiquitination enzyme UBP1 analogues in E. coli

Author

Grazyna Plucienniczak, Diana Mikiewicz-Sygula, Natalia Lukasiewicz, Anna Mazurkiewicz-Pisarek, Luiza Chojnacka, Andrzej Plucienniczak, and Anna Wojtowicz

Subjects

chemistry.chemical_classification, Proteases, biology, Research, lcsh:QR1-502, Bioengineering, Applied Microbiology and Biotechnology, lcsh:Microbiology, Yeast, Deubiquitinating enzyme, Biotechnological process, Enzyme, Biochemistry, chemistry, Ubiquitin, biology.protein, Biotechnology, Deubiquitination

Abstract

Background It has been shown that proteins fused to ubiquitin undergo greater expression in E. coli and are easier to purify and renaturate than nonhybrid foreign proteins. However, there is no commercial source of large quantities of specific deubiquitinating proteases. This is the reason why hybrid proteins containing ubiquitin at their N-end cannot be used in large scale biotechnological processes. Results and Conclusion We have described the synthesis of the yeast deubiquination enzyme UBP1 muteins in E. coli. We have shown that an efficient overproduction of the enzyme in E. coli may be achieved after the introduction of several changes in the nucleotide sequence encoding UBP1. One of the conditions of an effective synthesis of the UBP1 muteins is the removal of the 5'-end sequence encoding the transmembrane region of the enzyme. The obtained variants of the enzyme may be successfully used for processing large amounts of hybrid proteins comprising ubiquitin or tagged ubiquitin at their N-ends.

Published

2005

19. Cloning, expression in CHO-dhfr cells and purification of the 6-histag blood coagulation factor

Author

Mazurkiewicz-Pisarek, A., primary, Zielinski, M., additional, Mikiewicz, D., additional, Jagiello, A., additional, Wojtowicz-Krawiec, A., additional, Płucienniczak, G., additional, and Płucienniczak, A., additional

Published

2012

20. Cloning, expression in CHO-dhfr cells and purification of the 6-histag blood coagulation factor

Author

Grazyna Plucienniczak, Diana Mikiewicz, A. Mazurkiewicz-Pisarek, Marcin Zielinski, Agata Jagiełło, Andrzej Plucienniczak, and Anna Wojtowicz-Krawiec

Subjects

Cloning, Coagulation, Chemistry, Bioengineering, General Medicine, Molecular Biology, Molecular biology, Biotechnology

Published

2012

21. Expression of yeast deubiquitination enzyme UBP1 analogues in E. coli

Author

Wojtowicz, Anna, primary, Mazurkiewicz-Pisarek, Anna, additional, Plucienniczak, Grazyna, additional, Mikiewicz-Sygula, Diana, additional, Chojnacka, Luiza, additional, Lukasiewicz, Natalia, additional, and Plucienniczak, Andrzej, additional

Published

2005

22. Synthetic construction of FVIII gene and expression in CHO-dhfr cells

Author

Anna Mazurkiewicz-Pisarek, Zielinski, M., Plucienniczak, G., Mikiewicz, D., Jagiello, A., Romanik, A., and Plucienniczak, A.

23. The RepRS, RepRS2 and RepMSS proteins in the specyfic DNA binding activity

Author

Wojtowicz-Krawiec, A., Lukasiewicz, N., Mikiewicz, D., Anna Mazurkiewicz-Pisarek, Chojnacka-Puchta, L., Jagiello, A., Wawrzyniak, P., Sokolowska, I., Plucienniczak, G., and Plucienniczak, A.

24. CONSTRUCTION, CLONING AND EXPRESSION OF THE ANTI-CD22 MONOCLONAL ANTIBODY IN THE E. COLI BACTERIAL EXPRESSION SYSTEM.

Author

MIKIEWICZ, D., ŁUKASIEWICZ, N., SOBOLEWSKA-RUTA, A., BIERCZYŃSKA-KRZYSIK, A., WÓJTOWICZ-KRAWIEC, A., SOKOŁOWSKA, I., ZIELIŃSKI, M., MAZURKIEWICZ-PISAREK, A., and PŁUCIENNICZAK, A.

Published

2018

25. CONSTRUCTION, CLONING AND EXPRESSION OF THE FVIII GENE WITHOUT B DOMAIN IN CHO-DHFR CELLS.

Author

MAZURKIEWICZ-PISAREK, A., CIACH, T., ZIELIŃSKI, M., MAZURKIEWICZ, A., MIKIEWICZ, D., and PŁUCIENNICZAK, A.

Published

2018

26. EXPRESSION OF THE FVIII GENE WITHOUT B DOMAIN IN E. COLI BACTERIAL EXPRESSION SYSTEM.

Author

MAZURKIEWICZ-PISAREK, A., CIACH, T., MAZURKIEWICZ, A., BIERCZYŃSKA-KRZYSIK, A., MIKIEWICZ, D., SOBOLEWSKA-RUTA, A., and PŁUCIENNICZAK, A.

Published

2018