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Neuroprotective effects of novel anorexigenic analogs of prolactin-releasing peptide (PrRP) in models of neurodegeneration in vitro and in vivo
Mengr, Anna ; Maletínská, Lenka (advisor) ; Sumová, Alena (referee) ; Hampl, Aleš (referee)
Alzheimer's disease (AD) is a progressive brain disorder characterized by extracellular beta amyloid (Aβ) plaques, intracellular neurofibrillary tangles formed by hyperphosphorylated Tau protein and neuroinflammation. Since obesity and type 2 diabetes mellitus (T2DM) have been established as risk factors for the development of neurological disorders, anorexigenic and antidiabetic peptides, such as prolactin-releasing peptide (PrRP) seem to be potential neuroprotective agents. In the first part of the study, the molecular mechanisms of action of natural PrRP31 and its lipidized analog palm11 -PrRP31 was studied in the human neuroblastoma cell line SH-SY5Y. Both compounds significantly activated the signaling pathways typical for insulin promoting cell survival and growth. Moreover, PrRP31 and palm11 -PrRP31 increased cell viability and suppressed apoptosis in methylglyoxal-stressed SH-SY5Y cells. The second part of the thesis was focused on the neuroprotective and anti-inflammatory effects of 2-month-long subcutaneous administration of palm11 -PrRP31 in the brains of APP/PS1 mice, model of Aβ pathology. Palm11 -PrRP31 significantly reduced the Aβ plaque load and microgliosis in the hippocampi, cortices, and cerebella. Furthermore, palm11 -PrRP31 increased the synaptogenesis and attenuated...
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Research of epigenetic aspects of hematopoietic and spermatogenesis stem cells.
Hybešová, Michaela ; Pimková, Kristýna (advisor) ; Děd, Lukáš (referee)
Stem cell differentiation is controlled by coordinated regulation of gene transcription. One of the regulatory factors is the loosening of chromatin and the accessibility of DNA to transcription factors. Chromatin remodeling is mediated by remodeling complexes. The ISWI chromatin remodeling ATPase Smarca5 (S5) is an important factor of remodeling complexes. It is a highly conserved chromatin-remodeling factor forming a catalytic subunit that can be found in several oligosubunit complexes. In these complexes, it actively regulates nucleosome structure and remodeling during DNA replication, repair and transcription. S5 has been identified as a key protein in embryonic development. Its deficiency leads to defects in hematopoiesis and male genital development. In the presented study, we focused on the role of S5 in hematopoiesis and spermatogenesis. Using a mouse model with transgenic expression of S5, co-immunoprecipitation and mass spectrometry, we identified S5 complexes in hematopoietic and testicular cells. We also studied the phenotypic consequences of S5 deficiency in mouse testes and found that it leads to impaired sperm development and male sterility. Using transcriptomic and proteomic analysis, we identified several molecular programs that could lead to reproductive disorders. Our work...
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3rd CCP Phenogenomics Conference 2021: Abstract Book
Sedláček, Radislav
The Conference was divided into two blocks. The first day was devoted to the theme “Human diseases and models“. The second day was specifically dedicated to preclinical development, including covid-19, which focused on translation of the basic research into the application. The Conference provided an excellent opportunity to support networking and interactions among the CCP users and experts.
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2nd CCP Phenogenomics Conference 2020: Abstract Book
Sedláček, Radislav
The Conference was divided into two blocks. The first day was devoted to the theme “Human diseases and models“. The second day was specifically dedicated to preclinical development, including covid-19, which focused on translation of the basic research into the application. The Conference provided an excellent opportunity to support networking and interactions among the CCP users and experts.
Plný tet:  PDF
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SWI2/SNF2 ATPases with a focus on the ISWI subfamily: protein complexes and mouse models for their study
Turková, Tereza ; Stopka, Tomáš (advisor) ; Janoštiak, Radoslav (referee)
In the nucleus the DNA is packed along with proteins into a dynamic structure called chromatin. During cell cycle the chromatin structure becomes a subject to various changes. During interphase chromatin structure becomes loose while shortly before cell division it undertakes the form of highly condensed mitotic chromosomes. Structure of chromatin influences significantly mode of gene expression and its pattern. DNA-binding proteins interacting within chromatin are also necessary during this process. To gain the access to the DNA binding factors, the chromatin has to be in a loosened form. As long as the structure of the chromatin is more condensed it creates a barrier for the DNA binding proteins. Therefore it becomes obvious that the remodeling of the chromatin structure is one of the important regulators of gene expression and that the enzymes, which execute remodeling, are of great importance. One of them is ATPase Smarca5, which belongs to the protein subfamily ISWI and which creates the catalytic subunit for several different ATP-dependent chromatin remodeling complexes. Mutations of members of those complexes disturb regulation of transcription and cellular differentiation. In some cases the incorrect function of these complexes can lead to cellular transformation into a tumours state. This...
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Molecular mechanism of carcinogenicity of aristolochic acid
Levová, Kateřina ; Stiborová, Marie (advisor) ; Ryšlavá, Helena (referee) ; Souček, Pavel (referee)
Aristolochic acids (AA) are carcinogenic and nephrotoxic alkaloids from Aristolochia species. Aristolochic acid I (AAI), the major component of AA, causes the development of Aristolochic acid nephropathy (AAN) and Balkan endemic nephropathy (BEN). These two diseases cause total renal failure and urothelial malignancies. The fact that these diseases have not been developed in all persons, who have been exposed to their action, might be causd by different activities and protein levels of the enzymes metabolizing AAI. Thus, the identification of enzymes involved in the metabolism, and detailed knowledge of their expression and catalytic specifities is a major importance. Aristolochic acid I (AAI) can be metabolized by several types of reactions. Like most nitroaromatics, the main activation pathway of AAI is reduction of its nitro group to form a cyclic acylnitrenium ion, which can bind to the purine bases, thereby forming AAI-DNA adducts. The detoxication pathway of AAI is its oxidative demethylation by cytochromes P450 forming detoxication metabolite 8-hydroxyaristolochic acid Ia (AAIa). In the present thesis, using rat and human enzymes and as well as several mice models, the metabolism of AAI in vitro and in vivo was investigated. The first model has deleted gene for NADPH:cytochrome P450...
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SWI2/SNF2 ATPases with a focus on the ISWI subfamily: protein complexes and mouse models for their study
Turková, Tereza ; Stopka, Tomáš (advisor) ; Janoštiak, Radoslav (referee)
In the nucleus the DNA is packed along with proteins into a dynamic structure called chromatin. During cell cycle the chromatin structure becomes a subject to various changes. During interphase chromatin structure becomes loose while shortly before cell division it undertakes the form of highly condensed mitotic chromosomes. Structure of chromatin influences significantly mode of gene expression and its pattern. DNA-binding proteins interacting within chromatin are also necessary during this process. To gain the access to the DNA binding factors, the chromatin has to be in a loosened form. As long as the structure of the chromatin is more condensed it creates a barrier for the DNA binding proteins. Therefore it becomes obvious that the remodeling of the chromatin structure is one of the important regulators of gene expression and that the enzymes, which execute remodeling, are of great importance. One of them is ATPase Smarca5, which belongs to the protein subfamily ISWI and which creates the catalytic subunit for several different ATP-dependent chromatin remodeling complexes. Mutations of members of those complexes disturb regulation of transcription and cellular differentiation. In some cases the incorrect function of these complexes can lead to cellular transformation into a tumours state. This...
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Intestinal cancer and mouse models of the disease
Baloghová, Nikol ; Janečková, Lucie (advisor) ; Gemperle, Jakub (referee)
Intestinal cancer is a serious and common disease. To understand the mechanisms of its development, it is important to know the structure of the intestinal epithelium, as well as the signalling pathways that maintain the homeostasis and regulate cell proliferation and differentiation. Development of the intestinal cancer is a multistep process in which many molecular events underlie initiation and progression of the disease. Transgenic mice produced by genetic engineering are essential tools in both research of the intestinal cancer initiation and progression and possible treatment strategies. The aim of this work is to describe the intestinal anatomy and the renewal of the intestinal epithelium including the role of multiple signalling pathways, to summarize the most common mutations conditioning human colorectal carcinoma development and to define the existing mouse models of the disease.
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Molecular mechanism of carcinogenicity of aristolochic acid
Levová, Kateřina ; Stiborová, Marie (advisor) ; Ryšlavá, Helena (referee) ; Souček, Pavel (referee)
Aristolochic acids (AA) are carcinogenic and nephrotoxic alkaloids from Aristolochia species. Aristolochic acid I (AAI), the major component of AA, causes the development of Aristolochic acid nephropathy (AAN) and Balkan endemic nephropathy (BEN). These two diseases cause total renal failure and urothelial malignancies. The fact that these diseases have not been developed in all persons, who have been exposed to their action, might be causd by different activities and protein levels of the enzymes metabolizing AAI. Thus, the identification of enzymes involved in the metabolism, and detailed knowledge of their expression and catalytic specifities is a major importance. Aristolochic acid I (AAI) can be metabolized by several types of reactions. Like most nitroaromatics, the main activation pathway of AAI is reduction of its nitro group to form a cyclic acylnitrenium ion, which can bind to the purine bases, thereby forming AAI-DNA adducts. The detoxication pathway of AAI is its oxidative demethylation by cytochromes P450 forming detoxication metabolite 8-hydroxyaristolochic acid Ia (AAIa). In the present thesis, using rat and human enzymes and as well as several mice models, the metabolism of AAI in vitro and in vivo was investigated. The first model has deleted gene for NADPH:cytochrome P450...
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