Mecanismos de controle da expressão e atividade de metaloproteinases 2 e 9 pela quinase de adesão focal em fibroblastos / Mechanisms of control metalloproteinases 2 and 9 expression and activity by focal adhesion kinase un mouse cardiac fibroblasts

Costa, Ana Paula Dalla

03 May 2009

Orientador: Kleber Gomes Franchini / Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-08-13T09:40:02Z (GMT). No. of bitstreams: 1 Costa_AnaPaulaDalla_M.pdf: 3504258 bytes, checksum: c5455cd7943b5dcb62c07cb63be2f681 (MD5) Previous issue date: 2009 / Resumo: Mudancas dinamicas que ocorrem no intersticio do coracao contribuem diretamente para o remodelamento miocardico decorrente de doencas cardiacas tais como infarto do miocardio, cardiopatia hipertensiva e cardiomiopatias. As metaloproteinases de matriz extracelular (MMPs) sao importantes no remodelamento destas doencas. Estimulos mecanicos e neuro-humoral regulam a expressao e atividade de MMPs atraves de multiplos processos. Em estudos previos verificamos que o silenciamento da FAK no VE de camundongos inibe a fibrose e reduz a atividade de MMP2. Objetivamos avaliar o papel da FAK no controle da ativacao de fibroblastos cardiacos de ratos(FCRNs), induzidos por estiramento mecanico. Os FCRNs foram cultivados em placas Bioflex e submetidos a estiramento ciclico (10%) por ate 8 horas, exceto os controles. A expressao e atividade da FAK foram avaliadas por imunoblottings com anticorpos especificos para FAK ou pFAK Tyr397, respectivamente. A expressao das MMPs 2 e 9 foi avaliada em imunoblottings e a atividade por zimografia ambas no sobrenadante da cultura. O estiramento provocou aumento de 2.4 vezes da quantidade de FAK fosforilada em Tyr397, alem da expressao e a atividade de MMP 2 e 9. Alem disto, modificou os parametros de proliferacao dos FCRNs, mostrando aumento de celulas positivas para Ki67 e BrdU. Do mesmo modo, a diferenciacao em miofibroblastos foi ativada(celulas positivas para a-actina de musculo liso (a-SMA). A inibicao genica da FAK atraves da tecnica de interferencia de RNA (siRNAFAK), nos FCRNs, inibiu a expressao de a-SMA, a atividade e a expressao das MMPs 2 e 9. Alem disso, a deplecao da FAK em FCRNs promoveu a diminuicao da fosforilacao em AKT Ser473, TSC-2 Thr1462, e S6 quinase Thr389 em resposta ao estiramento mecanico. A ativacao dos FCRNs foi impedida pelo pre-tratamento com o inibidor do complexo mTOR, rapamicina. Assim mostramos que a FAK medeia a ativacao de FCRNs invocado pelo estresse mecanico, possivelmente atraves da coordenacao da via de sinalizacao mTOR. Os resultados do presente estudo indicam a ativacao da FAK pode ter um papel critico na proliferacao e diferenciacao, e na ativacao de MMPs em FCRNs quando submetidos a estiramento, e ainda o knockdown da FAK apresenta efeitos contrarios, logo, infere-se o papel da FAK na ativacao de fibroblastos cardiacos. / Abstract: Dynamic changes that occur in the heart interstitium contribute directly to the myocardial remodeling due to heart disease such as myocardial infarction, hypertensive heart disease and cardiomyopathies. The extracellular matrixmetalloproteinases (MMPs) play an important role in remodeling in these diseases. Mechanical and neuro-humoral stimuli regulate the MMPs expression/activity through several processes which include the control of expression, activation by cascades of own MMPs and endogenous inhibitors. In recent studies from our laboratory showed that the FAK silencing in the left ventricle of mice inhibits the fibrosis development, and in parallel reduced the MMP2.activity and expression. The purpose of this study was to evaluate the role of FAK in controlling the MMP 2 and 9 expression and activity in rat cardiac fibroblasts. Cardiac fibroblasts from neonatal rat (FCRNs) were grown on silicon plates and then subjected to cyclic stretch (10%) for up to 8 hours, except the controls. The FAK expression and activity were assessed for imunoblottings through with specific antibodies to FAK or phospho -FAK Tyr397, respectively. The expression of MMP 2 and 9 was evaluated with specific antibodies in imunoblottings and activity through zimography both in the supernatant culture. Furthermore, FCRNs depleted of FAK was defective in AKT Ser473, TSC-2 Thr1462, and S6 kinase Thr389 phosphorylation in response to cyclic stretch. The activation of CF-P3/80 invoked by cyclic stretch was prevented by pre-treatment with the mTOR complex inhibitor rapamycin. These findings demonstrate that FAK signaling plays a critical role in mediating the activation of cardiac fibroblasts invoked by mechanical stress possibly by coordinating the downstream mTOR signaling pathway. The results of this study indicate that the activation of FAK can have a critical role to MMPs activation in cardiac fibroblasts, as well as, the proliferation and differentiation of these cells when subjected to stretching, and the FAK knockdown presents contrary effects, therefore, to corroborate infer the FAK role in differentiation and proliferation cell, and the MMPs balance in cardiac fibroblasts. / Mestrado / Biologia Estrutural, Celular e do Desenvolvimento / Mestre em Fisiopatologia Médica

Metaloproteinase 2 da matriz

Metaloproteinase 9 da matriz

Fibroblasto

Focal adhesion kinase

Matrix metalloproteinase 2

Matrix metalloproteinase 9

Fibroblasts

Análise da expressão das metaloproteinases 2 e 9 e seus reguladores no câncer de bexiga / Expression of metalloproteinases 2 and 9 and their regulator genes in bladder cancer

Luís Felipe Piovesan

20 January 2012

Introdução: O Carcinoma Urotelial de Bexiga (CUB) é o segundo tumor urológico mais prevalente no Brasil. Devido ao elevado custo médico no processo que envolve seu diagnóstico, tratamento e seguimento, o CUB é um dos tipos de tumores mais caros para os sistemas de saúde. Embora existam fatores prognósticos definidos, como o estadiamento patológico, a diferenciação histológica e a presença de invasão angiolinfática (IAL), os mesmos demonstram-se insuficientes para uma acurada definição de comportamento da doença. Com a evolução da pesquisa molecular um grande número de potenciais novos marcadores de agressividade tem surgido. As Metaloproteinases da matriz (MMP) sao proteínas teciduais, pertencentes à família das endoproteinases, que degradam vários componentes da matriz extracelular. A expressão de diversas MMPs, especialmente MMP-2 e MMP-9 (gelatinases), bem como seus ativadores e inibidores, tem sido estudada como potencial marcador de comportamento tumoral em várias neoplasias. Objetivos: Avaliarmos os níveis de expressão dos genes das gelatinases MMP-2 e MMP-9 no CUB, assim como proteínas envolvidas em suas vias de ativação e inibição (MMP-14, IL-8, TIMP-1, TIMP-2, RECK e TGF-! ). Material e Método: Estudamos pela técnica de qRT-PCR a expressão dos 8 genes em amostras de CUB de 40 pacientes submetidos a RTUb, tendo como grupo controle amostras de urotélio sem câncer de 6 pacientes submetidos a prostatectomia aberta por HPB, bem como sua relação com marcadores prognósticos clássicos (estádio, grau e IAL). Resultados: Houve uma superexpressão de MMP-9 na maioria das amostras de CUB, bem como subexpressão de MMP-2, TIMP-1, TIMP-2, MMP-14, IL-8, TGF-! e RECK. Comparando os níveis de expressão dos genes com o estádio patológico, houve uma superexpressão de MMP-9 nos tumores pT1-2, quando comparados com pTa (p=0,026), bem como maior expressão de IL-8 nos tumores pT1 e pT2 (p=0,015 e p=0,048, respectivamente). Embora estatisticamente nao significativa, houve uma superexpressão de MMP-14 nos tumores pT2, quando comparados aos demais (p=0,087). Com relação ao grau histológico, também identificamos superexpressão de MMP-9 nos tumores de alto grau, quando comparados aos de baixo grau (p=0,012), assim como maior expressão de IL-8 nos tumores de alto grau (p=0,003). Conclusão: Houve uma superexpressão de MMP-9 e uma subexpressão de MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, IL-8 e TGF-! no CUB, quando comparado com o grupo controle. Também identificamos uma superexpressão de MMP-9 e IL-8 em tumores pT1-2 quando comparados com pTa e de alto grau quando comparados com baixo grau. A subexpressão dos principais inibidores da MMP-9 (TIMP-1 e RECK) pode explicar sua superexpressão no CUB, assim como a superexpressão de IL-8 nos tumores invasivos e de alto grau pode agir como fator ativador da MMP-9 nestes mesmos tumores / Introduction: Bladder cancer (BC) is the second most common urological tumor in Brazil. Because its high cost on diagnosis, treatment and follow-up, BC is one of the most expensive malignancies for health care providers. Although we have well-known prognostic factors, like pathological stage, histologic grade and lymphovascular invasion, they are insufficient to figure more accurate tumor aggressiveness. Recent molecular biology helped us to discover a huge amount of potential markers. Matrix metalloproteinases (MMP) are tissue endopeptidases that degrade components of extracellular matrix. Expression of several MMP, specially MMP-2 and MMP-9 (gelatinases), and their activators and inhibitors, are investigated as potential behavior markers in many neoplasms. Objectives: The aim of this study was to evaluate expression levels of gelatinases MMP-2 and MMP-9 genes by quantitative real-time polymerase chain reaction (qRT-PCR) in BC, as well as other proteins evolved in the activation and inhibition pathways (MMP-14, IL-8, TIMP-1, TIMP-2, RECK e TGF-b). Material and Method: Present study analyzed tissue expression of 8 genes in BC samples of transutethral resection of 40 patients by qRT-PCR, as well as their relation with current prognostic factors (stage, grade and LVI). The control group was composed of utothelial tissue from 6 patients with benign prostatic hyperplasia (BPH) treated surgically with retropubic prostatectomy. Results: In the tumor samples, MMP-9 presented an overexpression and MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, IL-8, and TGF-b were underexpressed in BC tissue compared to control. Comparing gene level expression to pathologic stage, there was MMP-9 overexpression in pT1-2 tumors compared to pTa (p=0.026), as wall as IL-8 overexpression in pT1 and pT2 tumors (p=0.015 e p=0.048, respectively). Although not statiscally significant, there was MMP-14 overexpression in pT2 tumors in comparison to pTa-1 (p=0.087). About grade, there was MMP-9 overexpression in high-grade tumors compared to low-grade (p=0.012), as well as IL-8 overexpression in high-grade tumors (p=0.003). There was not relation of any gene expression to LVI. Conclusions: We found overexpression of MMP-9 and underexpression of MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, TGF-b and IL-8 in BC compared with the control group. According to the prognostic factors we found increased levels of MMP-9 and IL-8 gene expression in pT1-2 compared to pTa tumors and high-grade compared to low-grade tumors. Underexpression of major MMP-9 inhibitors (TIMP-1 and RECK) could explain MMP-9 overexpression in BC, as well as IL-8 overexpression in high-grade and stage tumors could act as activation factor of MMP-9 in these tumors

Expressão gênica

Metaloproteinase 2 da matriz

Metaloproteinase 9 da matriz

Neoplasias da bexiga urinária

Prognóstico

Gene expression

Matrix metalloproteinase 2

Matrix metalloproteinase 9

Prognosis

Urinary bladder neoplasms

Efeitos de polimorfismos genéticos sobre as concentrações circulantes de metaloproteinases da matriz extracelular em mulheres com migrânea = Effects of genetic polymorphisms on the circulating concentrations of extracellular matrix metalloproteinases in women with migraine / Effects of genetic polymorphisms on the circulating concentrations of extracellular matrix metalloproteinases in women with migraine

Gonçalves, Flávia Magazoni, 1983-

21 August 2018

Orientador: José Eduardo Tanus dos Santos / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas / Made available in DSpace on 2018-08-21T14:39:20Z (GMT). No. of bitstreams: 1 Goncalves_FlaviaMagazoni_D.pdf: 13094273 bytes, checksum: b37b538d1e8c37ba2a2ec5c8c99a5a30 (MD5) Previous issue date: 2012 / Resumo: A migrânea é uma cefaleia primária comum e altamente incapacitante que atinge cerca de 10% da população mundial, especialmente as mulheres. Apesar dos esforços, a fisiopatologia da migrânea não está completamente elucidada. No entanto, acredita-se que as metaloproteinases da matriz (MMPs) estejam envolvidas no rompimento da barreira-hematoencefálica durante uma crise de migrânea. O objetivo do presente trabalho é avaliar se polimorfismos funcionais nos genes da MMP-2 (C-1306T e C-735T) e da MMP-9 (C-1562T, -90(CA)n e R(279)Q) e haplótipos estão associados com a migrânea e se eles podem modificar os níveis circulantes de MMPs na migrânea. Para avaliar o efeito de polimorfismos da MMP-9, foram estudadas 102 mulheres sem migrânea (grupo controle) e 187 mulheres com migrânea (141 com migrânea sem aura; MSA e 46 com migrânea com aura; MA). As genotipagens para os polimorfismos C-1562T, -90(CA)n e R(279)Q da MMP-9 foram realizadas por PCR-RFLP, PCR convencional seguida de eletroforese em gel de poliacrilamida e PCR em Tempo Real, utilizando-se o sistema Taqman® para discriminação de alelo, respectivamente. As concentrações plasmáticas de MMP-9 e TIMP-1 foram determinadas por ELISA. Os genótipos para os polimorfismos da MMP-2 foram determinados por PCR em Tempo Real, utilizando-se o sistema Taqman® para discriminação de alelo em 148 mulheres sem migrânea e em 204 mulheres com migrânea (153 MSA e 51 MA). As concentrações plasmáticas da MMP-2 e do TIMP-2 foram avaliadas, respectivamente, por zimografia e por ELISA. Os haplótipos foram inferidos utilizando o programa PHASE. Este estudo é o primeiro a mostrar que polimorfismos funcionais e haplótipos nos genes da MMP-2 e da MMP-9 podem afetar os níveis circulantes das MMPs em pacientes com migrânea. Enquanto o haplótipo H6 (CLQ) da MMP-9 foi associado aos maiores níveis plasmáticos de MMP-9 nas pacientes com migrânea (359,8±69,53ng/ml versus 195,8±9,70ng/ml para o CLR; 201,5±18,67ng/ml para o CHR e 200,2±17,02ng/ml para o CHQ), as maiores concentrações de MMP-2 foram encontradas nas pacientes com migrânea com aura com o genótipo CC para o polimorfismo C-735T (1,29±0,07U.A. versus 0,96±0,06U.A. para os genótipos CT ou TT) e com o haplótipo H1 (CC) (1,24±0,05U.A. versus 0,94±0,05U.A. para o haplótipo CT) no gene da MMP-2. Apesar de não investigarmos os mecanismos moleculares que explicam esses resultados, podemos sugerir que o aumento dos níveis das MMPs associados a genótipos e haplótipos específicos podem predispor essas pacientes a um aumento da permeabilidade vascular da barreira hematoencefálica, promovendo assim o desenvolvimento de um ambiente neuroinflamatório no sistema nervoso central, contribuindo para uma crise de migrânea / Abstract: Migraine is a common primary headache and highly disabling, affecting approximately 10% of the population worldwide, especially women. Despite the efforts, the pathophysiology of migraine is not completely understood. However, it is believed that the matrix metalloproteinases (MMPs) are involved in the disruption of blood-brain barrier (BBB) during migraine attacks. The aim of this study was to evaluate whether functional polymorphisms in MMP-2 (C-1306T and C-735T) and MMP-9 (C-1562T, -90(CA)n and R(279)Q) genes and haplotypes are associated with migraine and whether they modify circulating MMPs levels in migraine. To evaluate the effect of MMP-9 polymorphisms, we studied 102 healthy women (controls) and 187 women with migraine (141 migraine without aura; MWA, and 46 migraine with aura; MA). Genotypes for C-1562T, -90(CA)n e R(279)Q MMP-9 polymorphisms were determined by PCR-RFLP, by conventional PCR followed by electrophoresis in polyacrylamide gels and by real time-PCR using Taqman® allele discrimination assays, respectively. The plasma MMP-9 and TIMP-1 concentrations were measured by ELISA. Genotypes for MMP-2 polymorphisms were determined by real time-PCR using Taqman® allele discrimination assays in 148 healthy women without history of migraine and in 204 women with migraine (153 MWA and 51 MA). The plasma concentrations of MMP-2 and TIMP-2 were evaluated by gelatin zymography and ELISA, respectively. Haplotypes were inferred using the PHASE program. This is the first study to show that functional MMP-2 and MMP-9 polymorphisms and haplotypes can affect the circulating MMPs levels in patients with migraine. While the MMP-9 H6 (CLQ) haplotyple is associated with high MMP-9 concentrations in patients with migraine (359,8±69,53ng/ml versus 195,8±9,70ng/ml for CLR; 201,5±18,67ng/ml for CHR and 200,2±17,02ng/ml for CHQ) , the highest concentrations of MMP-2 were found in patients with migraine with aura carrying the CC genotype for C-735T polymorphism (1,29±0,07A.U. versus 0,96±0,06A.U. for CT or TT genotypes) and the H1 (CC) haplotype (1,24±0,05A.U. versus 0,94±0,05A.U. for CT haplotype) in the MMP-2 gene. Although we have not investigated the molecular mechanisms explaining these results, we can suggest that an increase of the MMPs levels associated with these genotypes and haplotypes may predispose these patients to increased vascular BBB permeability, thus promoting the development of an inflammatory environment in their central nervous systems, which contributes to migraine attacks / Doutorado / Farmacologia / Doutora em Farmacologia

Metaloproteinase 2 da matriz

Metaloproteinase 9 da matriz

Haplótipos

Transtornos de enxaqueca

Matrix metalloproteinase 2

Matrix metalloproteinase 9

Tissue inhibitor of metalloproteinases

Haplotypes

Migraine disorders

Análise da expressão das metaloproteinases 2 e 9 e seus reguladores no câncer de bexiga / Expression of metalloproteinases 2 and 9 and their regulator genes in bladder cancer

Piovesan, Luís Felipe

20 January 2012

Introdução: O Carcinoma Urotelial de Bexiga (CUB) é o segundo tumor urológico mais prevalente no Brasil. Devido ao elevado custo médico no processo que envolve seu diagnóstico, tratamento e seguimento, o CUB é um dos tipos de tumores mais caros para os sistemas de saúde. Embora existam fatores prognósticos definidos, como o estadiamento patológico, a diferenciação histológica e a presença de invasão angiolinfática (IAL), os mesmos demonstram-se insuficientes para uma acurada definição de comportamento da doença. Com a evolução da pesquisa molecular um grande número de potenciais novos marcadores de agressividade tem surgido. As Metaloproteinases da matriz (MMP) sao proteínas teciduais, pertencentes à família das endoproteinases, que degradam vários componentes da matriz extracelular. A expressão de diversas MMPs, especialmente MMP-2 e MMP-9 (gelatinases), bem como seus ativadores e inibidores, tem sido estudada como potencial marcador de comportamento tumoral em várias neoplasias. Objetivos: Avaliarmos os níveis de expressão dos genes das gelatinases MMP-2 e MMP-9 no CUB, assim como proteínas envolvidas em suas vias de ativação e inibição (MMP-14, IL-8, TIMP-1, TIMP-2, RECK e TGF-! ). Material e Método: Estudamos pela técnica de qRT-PCR a expressão dos 8 genes em amostras de CUB de 40 pacientes submetidos a RTUb, tendo como grupo controle amostras de urotélio sem câncer de 6 pacientes submetidos a prostatectomia aberta por HPB, bem como sua relação com marcadores prognósticos clássicos (estádio, grau e IAL). Resultados: Houve uma superexpressão de MMP-9 na maioria das amostras de CUB, bem como subexpressão de MMP-2, TIMP-1, TIMP-2, MMP-14, IL-8, TGF-! e RECK. Comparando os níveis de expressão dos genes com o estádio patológico, houve uma superexpressão de MMP-9 nos tumores pT1-2, quando comparados com pTa (p=0,026), bem como maior expressão de IL-8 nos tumores pT1 e pT2 (p=0,015 e p=0,048, respectivamente). Embora estatisticamente nao significativa, houve uma superexpressão de MMP-14 nos tumores pT2, quando comparados aos demais (p=0,087). Com relação ao grau histológico, também identificamos superexpressão de MMP-9 nos tumores de alto grau, quando comparados aos de baixo grau (p=0,012), assim como maior expressão de IL-8 nos tumores de alto grau (p=0,003). Conclusão: Houve uma superexpressão de MMP-9 e uma subexpressão de MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, IL-8 e TGF-! no CUB, quando comparado com o grupo controle. Também identificamos uma superexpressão de MMP-9 e IL-8 em tumores pT1-2 quando comparados com pTa e de alto grau quando comparados com baixo grau. A subexpressão dos principais inibidores da MMP-9 (TIMP-1 e RECK) pode explicar sua superexpressão no CUB, assim como a superexpressão de IL-8 nos tumores invasivos e de alto grau pode agir como fator ativador da MMP-9 nestes mesmos tumores / Introduction: Bladder cancer (BC) is the second most common urological tumor in Brazil. Because its high cost on diagnosis, treatment and follow-up, BC is one of the most expensive malignancies for health care providers. Although we have well-known prognostic factors, like pathological stage, histologic grade and lymphovascular invasion, they are insufficient to figure more accurate tumor aggressiveness. Recent molecular biology helped us to discover a huge amount of potential markers. Matrix metalloproteinases (MMP) are tissue endopeptidases that degrade components of extracellular matrix. Expression of several MMP, specially MMP-2 and MMP-9 (gelatinases), and their activators and inhibitors, are investigated as potential behavior markers in many neoplasms. Objectives: The aim of this study was to evaluate expression levels of gelatinases MMP-2 and MMP-9 genes by quantitative real-time polymerase chain reaction (qRT-PCR) in BC, as well as other proteins evolved in the activation and inhibition pathways (MMP-14, IL-8, TIMP-1, TIMP-2, RECK e TGF-b). Material and Method: Present study analyzed tissue expression of 8 genes in BC samples of transutethral resection of 40 patients by qRT-PCR, as well as their relation with current prognostic factors (stage, grade and LVI). The control group was composed of utothelial tissue from 6 patients with benign prostatic hyperplasia (BPH) treated surgically with retropubic prostatectomy. Results: In the tumor samples, MMP-9 presented an overexpression and MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, IL-8, and TGF-b were underexpressed in BC tissue compared to control. Comparing gene level expression to pathologic stage, there was MMP-9 overexpression in pT1-2 tumors compared to pTa (p=0.026), as wall as IL-8 overexpression in pT1 and pT2 tumors (p=0.015 e p=0.048, respectively). Although not statiscally significant, there was MMP-14 overexpression in pT2 tumors in comparison to pTa-1 (p=0.087). About grade, there was MMP-9 overexpression in high-grade tumors compared to low-grade (p=0.012), as well as IL-8 overexpression in high-grade tumors (p=0.003). There was not relation of any gene expression to LVI. Conclusions: We found overexpression of MMP-9 and underexpression of MMP-2, TIMP-1, TIMP-2, MMP-14, RECK, TGF-b and IL-8 in BC compared with the control group. According to the prognostic factors we found increased levels of MMP-9 and IL-8 gene expression in pT1-2 compared to pTa tumors and high-grade compared to low-grade tumors. Underexpression of major MMP-9 inhibitors (TIMP-1 and RECK) could explain MMP-9 overexpression in BC, as well as IL-8 overexpression in high-grade and stage tumors could act as activation factor of MMP-9 in these tumors

Expressão gênica

Gene expression

Matrix metalloproteinase 2

Matrix metalloproteinase 9

Metaloproteinase 2 da matriz

Metaloproteinase 9 da matriz

Neoplasias da bexiga urinária

Prognosis

Prognóstico

Urinary bladder neoplasms

Osteoblast Production by Reserved Progenitor Cells in Zebrafish Bone Regeneration and Maintenance

Brand, Michael, Hans, Stefan, Ando, Kazunori, Shibata, Eri, Kawakami, Atsushi

06 May 2019

Mammals cannot re-form heavily damaged bones as in large fracture gaps, whereas zebrafish efficiently regenerate bones even after amputation of appendages. However, the source of osteoblasts that mediate appendage regeneration is controversial. Several studies in zebrafish have shown that osteoblasts are generated by dedifferentiation of existing osteoblasts at injured sites, but other observations suggest that de novo production of osteoblasts also occurs. In this study, we found from cell-lineage tracing and ablation experiments that a group of cells reserved in niches serves as osteoblast progenitor cells (OPCs) and has a significant role in fin ray regeneration. Besides regeneration, OPCs also supply osteoblasts for normal bone maintenance. We further showed that OPCs are derived from embryonic somites, as is the case with embryonic osteoblasts, and are replenished from mesenchymal precursors in adult zebrafish. Our findings reveal that reserved progenitors are a significant and complementary source of osteoblasts for zebrafish bone regeneration.

info:eu-repo/classification/ddc/610

ddc:610

ROLE OF ALTERNATIVE MACROPHAGE ACTIVATION IN MEDIATING FIBROSIS IN <i>PSEUDOMONAS AERUGINOSA</i> PNEUMONIA

Birket, Susan Elizabeth

01 January 2012

Patients with cystic fibrosis who are infected with the pathogen Pseudomonas aeruginosa have shown favorable responses to the drug azithromycin (AZM). This drug works in an anti-inflammatory capacity, improving clinical outcomes and improving quality of life in this population. The drug has also been shown to affect macrophage polarization by shifting these cells away from an inflammatory phenotype toward an alternatively activated anti-inflammatory phenotype. The full impact of this phenotypic change is not well understood in the context of the response to P. aeruginosa infection, or the overall immune response in cystic fibrosis. To understand how the AZM-polarized macrophage affects other types of cells, we utilized a co-culture in vitro system, with macrophages and fibroblasts incubating together. In this system, we determined that AZM causes upregulation of the pro-fibrotic mediator transforming growth factor-β as well as the extracellular matrix (ECM) protein fibronectin. The mediator of ECM turnover, matrix metalloproteinase (MMP)-9 was upregulated in this system as well. In an in vivo model of P. aeruginosa infection, MMP- 9 and fibronectin were increased in the bronchoalveolar lavage 7 days post-infection in mice that were treated with AZM. This was accompanied by a decrease in damage to the lung tissue, determine by histological examination. To determine if these changes would continue in human subjects with cystic fibrosis, a clinical study was done in this population. Subjects with AZM treatment had decreased TGF-β levels, but no differences in MMP-9 or fibronectin. Interestingly, correlations between certain fibrotic mediators and inflammatory cytokines, specifically interleukin -1β, were different in subjects with AZM treatment compared to subjects without AZM therapy. Together, these data indicate that AZM alters the fibrotic response from the macrophages, as well as the interaction of the inflammatory response and fibrosis development.

Azithromycin

alternative macrophage

transforming growth factor-β

matrix metalloproteinase-9

Pseudomonas aeruginosa

Pharmacy and Pharmaceutical Sciences

The Enzymology of Fetuin: A Potential Link Between Periodontal Diseases and Calcifying Atheromas

Schure, Ryan Samuel

27 November 2013

Periodontal diseases may increase risk of vascular calcification in cardiovascular diseases but the potential mechanisms are not defined. Fetuin, a naturally-occurring serum glycoprotein in humans, protects against ectopic arterial calcification. We considered that patients with periodontitis could be at increased risk of developing calcifying atheromas because periodontal-disease associated enzymes may enter the circulation and subsequently degrade fetuin, thereby disrupting its ability to inhibit calcification. By in silico investigation, MMP -3 and -7 were predicted to cleave fetuin but only MMP-7 actually degraded human fetuin in vitro. MMP-7 degradation of fetuin was time- and concentration- dependent and was inhibited by an MMP Inhibitor. By mass spectrometry the presence of novel, MMP-7-mediated cleavage sites in fetuin were found. Fetuin bound tightly to MMP-7 (kd =2.96 x 10-9 M). The degradation of fetuin by MMP-7 could explain, at least in part, the apparent association between periodontal diseases and calcifying atheromas.

fetuin

periodontitis

cardiovascular disease

calcifying atheroma

biochemistry

matrix metalloproteinase

0567

0487

The Enzymology of Fetuin: A Potential Link Between Periodontal Diseases and Calcifying Atheromas

Schure, Ryan Samuel

27 November 2013

Periodontal diseases may increase risk of vascular calcification in cardiovascular diseases but the potential mechanisms are not defined. Fetuin, a naturally-occurring serum glycoprotein in humans, protects against ectopic arterial calcification. We considered that patients with periodontitis could be at increased risk of developing calcifying atheromas because periodontal-disease associated enzymes may enter the circulation and subsequently degrade fetuin, thereby disrupting its ability to inhibit calcification. By in silico investigation, MMP -3 and -7 were predicted to cleave fetuin but only MMP-7 actually degraded human fetuin in vitro. MMP-7 degradation of fetuin was time- and concentration- dependent and was inhibited by an MMP Inhibitor. By mass spectrometry the presence of novel, MMP-7-mediated cleavage sites in fetuin were found. Fetuin bound tightly to MMP-7 (kd =2.96 x 10-9 M). The degradation of fetuin by MMP-7 could explain, at least in part, the apparent association between periodontal diseases and calcifying atheromas.

fetuin

periodontitis

cardiovascular disease

calcifying atheroma

biochemistry

matrix metalloproteinase

0567

0487

The Role of Vascular Matrix Metalloproteinase-2 and Heme Oxygenase-2 in Mediating the Response to Hypoxia

He, Jeff ZiJian

24 September 2009

Systemic hypoxia frequently occurs in patients with cardiopulmonary diseases. Maintenance of vascular reactivity and endothelial viability is essential to preserving oxygen delivery in these patients. The role of matrix metalloproteinase-2 (MMP-2) and heme oxygenase-2 (HO-2) in the vascular response to hypoxia were investigated. In the first part of the thesis, the role of MMP-2 in regulating systemic arterial contraction after prolonged hypoxia was investigated. MMP-2 inhibition with cyclic peptide CTTHWGFTLC (CTT) reduced phenylephrine (PE)-induced contraction in aortae and mesenteric arteries harvested from rats exposed to hypoxia for 7 d. Responses to PE were reduced in MMP-2-/- mice exposed to hypoxia for 7 d compared to wild-type controls. CTT reduced contraction induced by big endothelin-1 (big ET-1) in aortae harvested from rats exposed to hypoxia. Increased contraction to big ET-1 after hypoxia was observed in wild-type controls, but not MMP-2-/- mice. Rat aortic MMP-2 and MT1-MMP protein levels and MMP activity were increased after 7 d of hypoxia. Rat aortic MMP-2 and MT1-MMP mRNA levels were increased in the deep medial vascular smooth muscle. These results suggest that hypoxic induction of MMP-2 activity potentiates contraction in systemic conduit and resistance arteries through proteolytic activation of big ET-1. The second part of the thesis investigated oxygen regulation of HO-2 protein and whether it plays a role in preserving endothelial cell viability during hypoxia. HO-2, but not HO-1, protein level was maintained during hypoxia in human endothelial cells through enhanced translation of HO-2 transcripts. Inhibition of HO-2 expression increased the production of reactive oxygen species, decreased mitochondrial membrane potential, and enhanced apoptotic cell death and activated caspases during hypoxia, but not during normoxia. These data indicate that HO-2 is translationally regulated and important in maintaining endothelial viability and function during hypoxia. In summary, the thesis demonstrates the importance of MMP-2 and HO-2 in preserving vascular function during prolonged systemic hypoxia. These enzymatic pathways may, therefore, represent novel therapeutic targets that may be exploited to ameliorate the effects of hypoxia in patients with cardiopulmonary disease.

hypoxia

endothelium

matrix metalloproteinase-2

heme oxygenase-2

apoptosis

protein translation

vascular reactivity

0307

Fragment Based Drug Discovery with Surface Plasmon Resonance Technology

Nordström, Helena

January 2013

Fragment based drug discovery (FBDD) has been applied to two protease drug targets, MMP-12 and HIV-1 protease. The primary screening and characterization of hit fragments were performed with surface plasmon resonance -technology. Further evaluation of the interaction was done by inhibition studies and in one case with X-ray crystallography. The focus of the two projects was different. Many MMP inhibitors contain a strong zinc chelating group, hydroxamate, interacting with the catalytic zinc atom. This strategy may be the cause for the low specificity of MMP inhibitors. Using FBDD we found a fragment with an unusual strong affinity for MMP-12. An inhibition assay confirmed that it was an inhibitor but indicated a stoichiometry of 2:1. Crystallography data revealed that an adduct of the fragment was bound in the active site, with interactions both with the catalytic zinc and the S1’ pocket. This may present a new scaffold for MMP-12 inhibitors. For HIV-1 protease the focus was on identifying inhibitors not sensitive to current resistance mutations. A fragment library for screening with SPR-technology was designed and used for screening against wild type enzyme and three variants with resistance mutations. Many of the hits were promiscuous but a number of fragments with possible allosteric inhibition mechanism were identified. The temperature dependency of the dissociation rate and reported resistance mutations was studied with thermodynamics. A good, but not perfect correlation was found between resistance and both the dissociation data and the free energy for dissociation compared to data from wild type enzyme. However, the type of mutation also influenced the results. The flap mutation G48V displayed thermodynamic profiles not completely correlating with resistance. It was found that dissociation rate and thermodynamics may complement each other when studying resistance, but only one of them may not be enough.

Fragment based drug discovery

SPR biosensor

matrix metalloproteinase-12

HIV-1 protease

resistance