Avaliação do comportamento vascular do tumor de Ehrlich na forma sólida em camundongos submetidos à eletroquimioterapia com bleomicina / Evaluation of vascular behavior of Ehrlich tumor in solid form in mice submitted to electrochemotherapy with bleomycin

Brunner, Carlos Henrique Maciel

01 October 2015

A eletroquimioterapia (EQT) é uma modalidade de tratamento recente que se baseia na associação de quimioterápicos potencializados pela eletroporação. Possui indicação para neoplasias sólidas de origens histológicas distintas, apresentando baixa morbidade e elevada eficiência. A ação da EQT ocorre em múltiplos sítios, tanto envolvendo a quebra da molécula de DNA, quanto exercendo efeito sobre a vasculatura tumoral. No presente estudo buscou-se maior compreensão dos eventos vasculares, avaliando-se qualitativamente e quantitativamente, com auxílio de marcação imunológica, com fator VIII e VEGF-A, a vascularização do tumor de Ehrlich implantado na forma sólida em camundongos, não tratados e submetidos à EQT com bleomicina, após sete dias de tratamento. No intuito de melhor elucidar os fenômenos vasculares, também foi investigado o efeito do resveratrol associado à EQT. O resveratrol, presente em vegetais como as uvas, possui efeitos de inibição do HIF1-α, reconhecida proteina que estimula a angiogênese em condições de hipoxia tumoral. Os animais submetidos à quimioterapia com bleomicina não apresentaram redução de volume tumoral, ao contrário dos que sofreram EQT com o mesmo fármaco. Evidenciou-se maior densidade microvascular tumoral em animais tratados com quimioterapia, quando comparados aos não tratados e aos submetidos à EQT. O tratamento com resveratrol diminuiu a expressão de VEGF-A e obteve efeito mais pronunciado quando associado à EQT com bleomicina. Através dos fenômenos pesquisados pôde-se evidenciar que a EQT com bleomicina foi efetiva na redução do volume do tumor de Ehrlich e que houve redução da atividade proliferativa assim como da densidade microvascular tumoral. Também observou-se que o resveratrol, ainda mais quando associado à EQT com bleomicina, reduz a proliferação tumoral e a expressão de VEGF-A / The electrochemotherapy (EQT) is a new treatment modality based on the association of chemotherapy potentiated by electroporation. Has indication for solid neoplasms of histological distinct origins, presenting low morbidity and high efficiency. The action of the EQT occurs in multiple sites, both involving the breakage of the DNA molecule, as having an effect on the tumor vasculature. The present study aimed at better understanding of vascular events, evaluating qualitatively and quantitatively, using immune labeling, with factor VIII and VEGF-A, the vascularization of the Ehrlich tumor implanted in solid form in mice, untreated and submitted to EQT with bleomycin, after seven days of treatment. In order to better elucidate the vascular phenomena, was also investigated the effect of resveratrol associated with EQT. The resveratrol present in plants such as grapes, has inhibitory effects of HIF1-α, a protein that is recognized to stimulates angiogenesis in tumor hypoxia. The animals submitted to chemotherapy with bleomycin showed no reduction of tumor volume, unlike those who suffered EQT with the same drug. It was evidenced increased microvessel density tumor in animals treated with chemotherapy, when compared to untreated and those submitted to EQT. The treatment with resveratrol decreased the expression of VEGF-A and obtained effect was more pronounced when associated to the EQT with bleomycin. This research can prove that the EQT with bleomycin was effective in reducing the volume of Ehrlich tumor and that there was a reduction of proliferative activity as well as of microvascular density tumor. Also it was observed that the resveratrol, even more when associated with EQT with bleomycin, reduces the tumor proliferation and the expression of VEGF-A

Bleomicina

Bleomycin

Ehrlich tumor

Electrochemotherapy

Eletroquimioterapia

Resveratrol

Resveratrol

Tumor de Ehrlich

Vascularização

Vascularization

Células NKT, macrófagos M2 e o desenvolvimento da fibrose pulmonar. / NKT cells, M2 macrophages and the development of pulmonary fibrosis.

Grabarz, Felipe

14 November 2014

A fibrose pulmonar é uma via comum de várias doenças agudas e crônicas do interstício pulmonar que pode resultar na cicatrização anormal do pulmão. Há acúmulo excessivo das proteínas da matriz extracelular levando a desestruturação das paredes alveolares, e consequente perda das trocas gasosas pelos pulmões. As células NKT são grande fonte de citocinas e podem ser cruciais na polarização de macrófagos para o fenótipo M2. O projeto tem a hipótese de que as células NKT podem influenciar o desenvolvimento da fibrose pulmonar via modulação de macrófagos. Para isso, animais selvagens e knockout para células NKT invariante (Ja18-/-) foram submetidos ao protocolo de indução de fibrose pulmonar pela bleomicina. Os resultados indicam que o grupo Ja18-/- assim como os grupos experimentais que receberam agonistas para células NKT apresentaram uma proteção contra a fibrose pulmonar uma vez que houve menor síntese de hidroxiprolina, deposição de colágeno, citocinas pró-fibróticas e a manutenção de macrófagos M1 no tecido pulmonar. / Pulmonary fibrosis is a common pathway of various acute and chronic interstitial lung diseases that may result in abnormal healing of the lung. There is excessive accumulation of extracellular matrix proteins, leading to disruption of the alveolar walls and the consequent loss of gas exchange through the lungs. NKT cells are a big source of cytokines and may be crucial in the polarization of macrophages to the M2 phenotype. This project has hypothesized that NKT cells can influence the development of pulmonary fibrosis through modulation of macrophages. For this, wild and knockout invariant NKT cells (Ja18-/-) mice were subjected to the protocol of bleomycin induced pulmonary fibrosis. The results indicate that the group Ja18-/- as well as the experimental groups receiving agonists for NKT cells showed protection against lung fibrosis since there was less synthesis of hydroxyproline, collagen deposition, pro-fibrotic cytokines and maintenance of macrophages M1 in lung tissue.

Bleomicina

Bleomycin

Células NKT

Fibrose pulmonar

Lung fibrosis

M2 macrophages

Macrófagos M2

NKT cells

Bleomicino pernaša į navikines ląsteles in vivo ir navikų gydymas taikant elektroporaciją ir sonoporaciją / Bleomycin transfer into tumor cells in vivo and tumor treatment using electroporation and sonoporation methods

Juknevičiūtė, Eglė

20 June 2012

Apie vėžį yra žinoma jau daug ir įvairios informacijos, taip pat netrūksta žinių ir kokiais būdais bei vaistais galima kovoti su šia liga. Farmacijoje yra atrasta ir sukurta nemažai aktyvių antivėžinių chemoterapinių preparatų vėžiui gydyti ar skirtų bent šios ligos slopinimui ir gyvenimo trukmės prailginimui. Todėl kita svarbi ir aktuali problema yra vaistų patekimas į reikiamą vietą – taikinį, kaip padėti vaistui patektį būtent į vėžines ląsteles ar audinį ir sumažinti riziką, kad vaistas pažeis normalius, sveikus audinius ir organus ir nepakenks jų funkcionavimui. Šiame tiriamajame darbe ir stengiamasi atsakyti į šią problemą, pasitelkus du metodus, kurie palengvina medžiagų patekimą į ląsteles – elektroporaciją ir sonoporaciją. Šių metodų funkcija yra panaši, tiek elektroporacijos, tiek sonoporacijos metu ląstelių plazminėse membranose susiformuoja poros, pro kurias gali patekti įvairios medžiagos (vaistai, dažai, baltymai, genai), kurios natūraliu būdu į ląstelę nepatenka arba patenka labai maži jų kiekiai, jei pernašoje dalyvauja ląstelės membranoje esantys baltymai nešikliai. Šiame darbe naudojami šie du, jau minėti metodai siekiant palengvinti chemoterapijoje naudojamo vaisto bleomicino patekimą į vėžines ląsteles in vivo. Tyrimams in vivo objektu buvo pasirinktos CBA – klono linijos pelės, kurioms į viršutinę nugaros dalį buvo įskiepyta MH22A hepatoma. Eksperimento duomenys rodo, kad tiek elektroporacija, tiek sonoporacija ir suminis abiejų metodų poveikis yra... [toliau žr. visą tekstą] / There is a lot of various information about cancer as well as plenty of knowledge and types of drugs to treat this disease. Pharmacy has discovered and developed a number of active anti-cancer chemotherapeutic agents for cancer treatment, or at least useful for reducing the spread of cancer. Therefore, another important and urgent problem is development of new method that would help to deliver directly into cancer cells or tissue. This in turn would allow to reduce side effects of the drug and preserve healthy tissues and organs. In this experimental work we attempted to answer this problem, using two methods that facilitate the transfer of materials into the cells - electroporation and sonoporation. These methods are based on similar principle: both electroporation and sonoporation affects the cell membranes to form pores that allow for various products (medicines, dyes, proteins, genes) to get access into the cell. The cell naturally is not accessible for those materials or the permeability is very small, in case special or nonspecific transport systems exist for this specific molecule. In this study we used the following two methods in order to facilitate the anticancer drug bleomycin delivery into cancer cells in vivo. The subject of these experiments in vivo is CBA – line clone mice bearing MH22A hepatoma tumors, transplanted on upper part of the flank. Experimental data showed that both electroporation and sonoporation and combination of both methods are effective in... [to full text]

Biology

Elektroporacija

Sonoporacija

Bleomicinas

Navikas

Hepatoma

Electroporation

Sonoporation

Bleomycin

Tumor

Hepatoma

An Investigation of the Interaction of DNA With Selected Peptides and Proteins

January 2014

abstract: The communication of genetic material with biomolecules has been a major interest in cancer biology research for decades. Among its different levels of involvement, DNA is known to be a target of several antitumor agents. Additionally, tissue specific interaction between macromolecules such as proteins and structurally important regions of DNA has been reported to define the onset of certain types of cancers. Illustrated in Chapter 1 is the general history of research on the interaction of DNA and anticancer drugs, most importantly different congener of bleomycin (BLM). Additionally, several synthetic analogues of bleomycin, including the structural components and functionalities, are discussed. Chapter 2 describes a new approach to study the double-strand DNA lesion caused by antitumor drug bleomycin. The hairpin DNA library used in this study displays numerous cleavage sites demonstrating the versatility of bleomycin interaction with DNA. Interestingly, some of those cleavage sites suggest a novel mechanism of bleomycin interaction, which has not been reported before. Cytidine methylation has generally been found to decrease site-specific cleavage of DNA by BLM, possibly due to structural change and subsequent reduced bleomycin-mediated recognition of DNA. As illustrated in Chapter 3, three hairpin DNAs known to be strongly bound by bleomycin, and their methylated counterparts, were used to study the dynamics of bleomycin-induced degradation of DNAs in cancer cells. Interestingly, cytidine methylation on one of the DNAs has also shown a major shift in the intensity of bleomycin induced double-strand DNA cleavage pattern, which is known to be a more potent form of bleomycin induced cleavages. DNA secondary structures are known to play important roles in gene regulation. Chapter 4 demonstrates a structural change of the BCL2 promoter element as a result of its dynamic interaction with the individual domains of hnRNP LL, which is essential to facilitate the transcription of BCL2. Furthermore, an in vitro protein synthesis technique has been employed to study the dynamic interaction between protein domains and the i-motif DNA within the promoter element. Several constructs were made involving replacement of a single amino acid with a fluorescent analogue, and these were used to study FRET between domain 1 and the i-motif, the later of which harbored a fluorescent acceptor nucleotide analogue. / Dissertation/Thesis / Doctoral Dissertation Chemistry 2014

Biochemistry

Molecular biology

Chemistry

BCL2 i-Motif

Bleomycin

Cancer

Cytidine Methylation

hnRNP LL

Marcacao da bleomicina com tecnecio-99m para diagnostico em medicina nuclear

NASSUTE, JOSE C.

09 October 2014

Made available in DSpace on 2014-10-09T12:29:39Z (GMT). No. of bitstreams: 0 / Made available in DSpace on 2014-10-09T14:00:09Z (GMT). No. of bitstreams: 1 00415.pdf: 688647 bytes, checksum: dc9c99e0bc59ebf00ca91a85600c5cf6 (MD5) / Dissertacao (Mestrado) / IEA/D / Instituto de Energia Atomica - IEA

antibiotics

bleomycin

diagnosis

labelled compounds

transition metals

distribution

antimitotic drugs

technetium 99

Probing Receptors and Enzymes with Synthetic Small Molecules

January 2013

abstract: ABSTRACT Manipulation of biological targets using synthetic or naturally occurring organic compounds has been the focal point of medicinal chemistry. The work described herein centers on the synthesis of organic small molecules that are targeted either to cell surface receptors, to the ribosomal catalytic center or to human immunodeficiency virus reverse transcriptase. Bleomycins (BLMs) are a family of naturally occurring glycopeptidic antitumor agents with an inherent selectivity towards cancer cells. DeglycoBLM, which lacks the sugar moiety of bleomycin, has much lower cytotoxicity in cellular assays. A recent study using microbbuble conjugates of BLM and deglycoBLM showed that BLM was able to selectively bind to breast cancer cells, whereas the deglyco analogue was unable to target either the cancer or normal cells. This prompted us to further investigate the role of the carbohydrate moiety in bleomycin. Fluorescent conjugates of BLM, deglycoBLM and the BLM carbohydrate were studied for their ability to target cancer cells. Work presented here describes the synthesis of the fluorescent carbohydrate conjugate. Cell culture assays showed that the sugar moiety was able to selectively target various cancer cells. A second conjugate was prepared to study the importance of the C-3 carbamoyl group present on the mannose residue of the carbohydrate. Three additional fluorescent probes were prepared to improve the uptake of this carbohydrate moiety into cancer cells. Encouraged by the results from the fluorescence experiments, the sugar moiety was conjugated to a cytotoxic molecule to selectively deliver this drug into cancer cells. The nonsense codon suppression technique has enabled researchers to site specifically incorporate noncanonical amino acids into proteins. The amino acids successfully incorporated this way are mostly α-L-amino acids. The non-α-L-amino acids are not utilized as substrates by ribosome catalytic center. Hoping that mutations near the ribosome peptidyltransferase site might alleviate its bias towards α-L-amino acids, a library of modified ribosomes was generated. Analogues of the naturally occurring antibiotic puromycin were used to select promising candidates that would allow incorporation of non-α-L-amino acids into proteins. Syntheses of three different puromycin analogues are described here. The reverse transcriptase enzyme from HIV-1 (HIV-1 RT) has been a popular target of HIV therapeutic agents due to its crucial role in viral replication. The 4-chlorophenyl hydrazone of mesoxalic acid (CPHM) was identified in a screen designed to find inhibitors of strand transfer reactions catalyzed by HIV-1 RT. Our collaborators designed several analogues of CPHM with different substituents on the aromatic ring using molecular docking simulations. Work presented here describes the synthesis of eight different analogues of CPHM. / Dissertation/Thesis / Ph.D. Chemistry 2013

Chemistry

Organic chemistry

Bleomycin

HIV

Mesoxalic Acid Hydrazone

Multivalency

Puromycin

Sugars

Carbohydrates

Bleomycin, From Start to Finish; Total Synthesis of Novel Analogues to in vitro Fluorescence Microscopy Imaging

January 2013

abstract: The bleomycins are a family of glycopeptide-derived antibiotics isolated from various Streptomyces species and have been the subject of much attention from the scientific community as a consequence of their antitumor activity. Bleomycin clinically and is an integral part of a number of combination chemotherapy regimens. It has previously been shown that bleomycin has the ability to selectively target tumor cells over their non-malignant counterparts. Pyrimidoblamic acid, the N-terminal metal ion binding domain of bleomycin is known to be the moiety that is responsible for O2 activation and the subsequent chemistry leading to DNA strand scission and overall antitumor activity. Chapter 1 describes bleomycin and related DNA targeting antitumor agents as well as the specific structural domains of bleomycin. Various structural analogues of pyrimidoblamic acid were synthesized and subsequently incorporated into their corresponding full deglycoBLM A6 derivatives by utilizing a solid support. Their activity was measured using a pSP64 DNA plasmid relaxation assay and is summarized in Chapter 2. The specifics of bleomycin—DNA interaction and kinetics were studied via surface plasmon resonance and are presented in Chapter 3. By utilizing carefully selected 64-nucleotide DNA hairpins with variable 16-mer regions whose sequences showed strong binding in past selection studies, a kinetic profile was obtained for several BLMs for the first time since bleomycin was discovered in 1966. The disaccharide moiety of bleomycin has been previously shown to be a specific tumor cell targeting element comprised of L-gulose-D-mannose, especially between MCF-7 (breast cancer cells) and MCF-10A ("normal" breast cells). This phenomenon was further investigated via fluorescence microscopy using multiple cancerous cell lines with matched "normal" counterparts and is fully described in Chapter 4. / Dissertation/Thesis / Ph.D. Chemistry 2013

Chemistry

Biochemistry

Pharmaceutical sciences

Bleomycin

Bozeman

cancer

Fluorescence Microscopy

Pyrimidoblamic acid

Surface Plasmon Resonance

Marcacao da bleomicina com tecnecio-99m para diagnostico em medicina nuclear

NASSUTE, JOSE C.

09 October 2014

Made available in DSpace on 2014-10-09T12:29:39Z (GMT). No. of bitstreams: 0 / Made available in DSpace on 2014-10-09T14:00:09Z (GMT). No. of bitstreams: 1 00415.pdf: 688647 bytes, checksum: dc9c99e0bc59ebf00ca91a85600c5cf6 (MD5) / Dissertacao (Mestrado) / IEA/D / Instituto de Energia Atomica - IEA

antibiotics

bleomycin

diagnosis

labelled compounds

transition metals

distribution

antimitotic drugs

technetium 99

Avaliação do comportamento vascular do tumor de Ehrlich na forma sólida em camundongos submetidos à eletroquimioterapia com bleomicina / Evaluation of vascular behavior of Ehrlich tumor in solid form in mice submitted to electrochemotherapy with bleomycin

Carlos Henrique Maciel Brunner

01 October 2015

A eletroquimioterapia (EQT) é uma modalidade de tratamento recente que se baseia na associação de quimioterápicos potencializados pela eletroporação. Possui indicação para neoplasias sólidas de origens histológicas distintas, apresentando baixa morbidade e elevada eficiência. A ação da EQT ocorre em múltiplos sítios, tanto envolvendo a quebra da molécula de DNA, quanto exercendo efeito sobre a vasculatura tumoral. No presente estudo buscou-se maior compreensão dos eventos vasculares, avaliando-se qualitativamente e quantitativamente, com auxílio de marcação imunológica, com fator VIII e VEGF-A, a vascularização do tumor de Ehrlich implantado na forma sólida em camundongos, não tratados e submetidos à EQT com bleomicina, após sete dias de tratamento. No intuito de melhor elucidar os fenômenos vasculares, também foi investigado o efeito do resveratrol associado à EQT. O resveratrol, presente em vegetais como as uvas, possui efeitos de inibição do HIF1-α, reconhecida proteina que estimula a angiogênese em condições de hipoxia tumoral. Os animais submetidos à quimioterapia com bleomicina não apresentaram redução de volume tumoral, ao contrário dos que sofreram EQT com o mesmo fármaco. Evidenciou-se maior densidade microvascular tumoral em animais tratados com quimioterapia, quando comparados aos não tratados e aos submetidos à EQT. O tratamento com resveratrol diminuiu a expressão de VEGF-A e obteve efeito mais pronunciado quando associado à EQT com bleomicina. Através dos fenômenos pesquisados pôde-se evidenciar que a EQT com bleomicina foi efetiva na redução do volume do tumor de Ehrlich e que houve redução da atividade proliferativa assim como da densidade microvascular tumoral. Também observou-se que o resveratrol, ainda mais quando associado à EQT com bleomicina, reduz a proliferação tumoral e a expressão de VEGF-A / The electrochemotherapy (EQT) is a new treatment modality based on the association of chemotherapy potentiated by electroporation. Has indication for solid neoplasms of histological distinct origins, presenting low morbidity and high efficiency. The action of the EQT occurs in multiple sites, both involving the breakage of the DNA molecule, as having an effect on the tumor vasculature. The present study aimed at better understanding of vascular events, evaluating qualitatively and quantitatively, using immune labeling, with factor VIII and VEGF-A, the vascularization of the Ehrlich tumor implanted in solid form in mice, untreated and submitted to EQT with bleomycin, after seven days of treatment. In order to better elucidate the vascular phenomena, was also investigated the effect of resveratrol associated with EQT. The resveratrol present in plants such as grapes, has inhibitory effects of HIF1-α, a protein that is recognized to stimulates angiogenesis in tumor hypoxia. The animals submitted to chemotherapy with bleomycin showed no reduction of tumor volume, unlike those who suffered EQT with the same drug. It was evidenced increased microvessel density tumor in animals treated with chemotherapy, when compared to untreated and those submitted to EQT. The treatment with resveratrol decreased the expression of VEGF-A and obtained effect was more pronounced when associated to the EQT with bleomycin. This research can prove that the EQT with bleomycin was effective in reducing the volume of Ehrlich tumor and that there was a reduction of proliferative activity as well as of microvascular density tumor. Also it was observed that the resveratrol, even more when associated with EQT with bleomycin, reduces the tumor proliferation and the expression of VEGF-A

Bleomicina

Eletroquimioterapia

Resveratrol

Tumor de Ehrlich

Vascularização

Bleomycin

Ehrlich tumor

Electrochemotherapy

Resveratrol

Vascularization

Células NKT, macrófagos M2 e o desenvolvimento da fibrose pulmonar. / NKT cells, M2 macrophages and the development of pulmonary fibrosis.

Felipe Grabarz

14 November 2014

A fibrose pulmonar é uma via comum de várias doenças agudas e crônicas do interstício pulmonar que pode resultar na cicatrização anormal do pulmão. Há acúmulo excessivo das proteínas da matriz extracelular levando a desestruturação das paredes alveolares, e consequente perda das trocas gasosas pelos pulmões. As células NKT são grande fonte de citocinas e podem ser cruciais na polarização de macrófagos para o fenótipo M2. O projeto tem a hipótese de que as células NKT podem influenciar o desenvolvimento da fibrose pulmonar via modulação de macrófagos. Para isso, animais selvagens e knockout para células NKT invariante (Ja18-/-) foram submetidos ao protocolo de indução de fibrose pulmonar pela bleomicina. Os resultados indicam que o grupo Ja18-/- assim como os grupos experimentais que receberam agonistas para células NKT apresentaram uma proteção contra a fibrose pulmonar uma vez que houve menor síntese de hidroxiprolina, deposição de colágeno, citocinas pró-fibróticas e a manutenção de macrófagos M1 no tecido pulmonar. / Pulmonary fibrosis is a common pathway of various acute and chronic interstitial lung diseases that may result in abnormal healing of the lung. There is excessive accumulation of extracellular matrix proteins, leading to disruption of the alveolar walls and the consequent loss of gas exchange through the lungs. NKT cells are a big source of cytokines and may be crucial in the polarization of macrophages to the M2 phenotype. This project has hypothesized that NKT cells can influence the development of pulmonary fibrosis through modulation of macrophages. For this, wild and knockout invariant NKT cells (Ja18-/-) mice were subjected to the protocol of bleomycin induced pulmonary fibrosis. The results indicate that the group Ja18-/- as well as the experimental groups receiving agonists for NKT cells showed protection against lung fibrosis since there was less synthesis of hydroxyproline, collagen deposition, pro-fibrotic cytokines and maintenance of macrophages M1 in lung tissue.

Bleomicina

Células NKT

Fibrose pulmonar

Macrófagos M2

Bleomycin

Lung fibrosis

M2 macrophages

NKT cells