Estudo da resposta do caramujo Biomphalaria glabrata (Say, 1818) frente a estímulos ambientais estressores, com enfoque na proteína HSP70 / Study of the response from the snail Biomphalaria glabrata (say, 1818) facing stressor environmental stimuli, with focus on the protein HSP70

Cantinha, Rebeca da Silva

11 December 2012

Moluscos têm sido empregados como bioindicadores em estudos de contaminação ambiental. Nesse contexto, o caramujo de água doce Biomphalaria glabrata tem sido avaliado como um bom modelo laboratorial, e estudos prévios apontaram sua aplicação na pesquisa ambiental. A proteína HSP70 é uma molécula de 70 kDa, pertencente a uma família de proteínas com papel na manutenção da homeostase dos seres vivos: as proteínas de choque térmico (HSPs); e vem sendo estudada como potencial biomarcador de dano ambiental, indicando estresse e protegendo os organismos dos danos às proteínas. Neste trabalho, foi caracterizada a proteína HSP70 de B. glabrata pelo Western blot, com o objetivo de seu emprego em aplicações ambientais futuras. Para isso, caramujos de 5-6 meses de idade, com diâmetro de concha de 14,4 (±1,7) mm, foram expostos ao calor e ao cloreto de cádmio (CdCl2) a fim de se verificar a resposta desta proteína frente a esses estresses. Os animais foram dissecados para investigação da indução da HSP70. As proteínas foram extraídas dos tecidos com tampão RIPA, separadas em eletroforese desnaturante em gel de poliacrilamida, transferidas para uma membrana de nitrocelulose e detectadas com anticorpo específico para HSP70. A CL50/96h foi determinada como sendo 0,34 (0,30-0,37) ppm para o CdCl2 e serviu de referência para os experimentos de indução da proteína. Foi observado que a exposição a temperaturas subletais aumentou a resistência dos caramujos à temperatura letal de 42 °C. Exposições prévias ao calor de 33 °C e ao CdCl2 a 0,22 ppm aumentou a sobrevivência dos caramujos B. glabrata à concentração letal de CdCl2 (0,7 ppm) e à temperatura letal (42 °C), respectivamente. Os achados do Western blot apontaram para um possível papel da HSP70 nesse processo. Os resultados mostraram relação entre a proteína HSP70 e o aumento na sobrevivência aos estímulos letais após prévia exposição a estresses moderados. O Western blot mostrou uma indução da HSP70 nos grupos pré-expostos, se comparados aos grupos controles. A glândula digestiva foi o tecido mais responsivo, no que concerne à indução da proteína HSP70, comparando com tecidos de cabeça/pé e ovoteste. Foi encontrado o pico de indução da HSP70 nos caramujos B. glabrata após 48 horas de exposição ao calor de 33 °C, e após 96 horas de exposição ao CdCl2 a 0,22 ppm. Apesar do bem conhecido papel da HSP70 na termotolerância e tolerância a outros agentes estressores nos organismos vivos, esta foi a primeira vez que isto foi demonstrado no B. glabrata, oferecendo subsídios para a sua aplicação em estudos de monitoramento ambiental. Os resultados apresentados aqui abrem o caminho para estudos futuros dessa proteína no molusco, e fornecem mais bases para o conhecimento do B. glabrata. / Molluscs have been employed as bioindicators in studies of environmental stress. In this way the freshwater snail Biomphalaria glabrata has been evaluated as a good laboratory model, and previous studies have pointed for its application in environmental research. The HSP70 protein is a molecule of 70 kDa from a family of proteins with role in maintaining homeostasis: the Heat Shock Proteins (HSPs), and it has been studied as a potential biomarker for environmental injury indicating stress and providing protection against the protein damage. In this work, the protein HSP70 was characterized in B. glabrata by Western blotting aiming its employment in future environmental applications. To this purpose, 5-6 months old snails, with shell diameter of 14,4 (±1,7) mm, were exposed to heat and to cadmium chloride (CdCl2) in order to verify the response of this protein to the stresses. Animals were dissected to investigate induction of HSP70. Proteins were extracted from tissues with RIPA buffer, fractionated in denaturing polyacrilamide gel electrophoresis, transferred to nitrocellulose membrane, and detected with a HSP70-specific antibody. The CL50/96h was determined as 0,34 (0,30-0,37) ppm for CdCl2 and served as reference in the experiments for protein induction. It was observed that exposure to sublethal temperatures improved the resistance of snails B. glabrata to the lethal temperature of 42 ºC. Previous sublethal exposure to heat at 33 °C and to CdCl2 at 0,22 ppm improved the survival of snails B. glabrata to a lethal concentration of CdCl2 (0,7 ppm) and to a lethal temperature (42 ºC), respectively. The findings of Western blot pointed to a possible role of HSP70 protein in this process. Results showed a correlation between HSP70 and the improvement of survival to lethal stimuli after a previous exposure to mild stresses. The Western blot showed an induction of HSP70 protein in the preexposed groups as compared to the control ones. The digestive gland was the most responsive tissue to stress regarding the HSP70 protein induction compared with heat/foot and ovotestis. An induction peak of HSP70 was found after 48 hours of exposure to heat at 33 °C, and after 96 hours of exposure to CdCl2 at 0,22 ppm. Despite of the well known role of HSP70 in thermotolerance and tolerance to other stress agents in living organisms, it was the first time it was shown in B. glabrata, supporting its application in environmental monitoring studies. The results presented here open a way to future studies of this protein in the mollusc, and provide more basements to knowledge of B. glabrata.

Biomphalaria glabrata

Biomphalaria glabrata

cádmio

cadmium

choque térmico

environmental stress

estresse ambiental

heat shock

HSP70

HSP70

Morfogênese do bacterioma e multiplicação de simbiontes ao longo do desenvolvimento de Diaphorina citri (Hemiptera: Liviidae) e sua resposta ao estresse térmico / Bacteriome morphogenesis and symbiont growth during development of Diaphorina citri (Hemiptera: Liviidae), and its response to heat stress

Dossi, Fábio Cleisto Alda

12 August 2013

Diaphorina citri depende dos endossimbiontes presentes em seu bacterioma, as bactérias Carsonella e Profftella, para o fornecimento de nutrientes essenciais ao seu desenvolvimento. D. citri também está associada à bactéria Wolbachia, que infecta inúmeros tecidos desse inseto, incluindo seu bacterioma. Esses simbiontes são transmitidos verticalmente, sendo incorporados ao bacterioma. Neste estudo, são abordados os eventos relacionados à formação do bacterioma, à dinâmica da densidade dos simbiontes durante o ciclo biológico do hospedeiro e à sensibilidade dos simbiontes ao estresse térmico. A morfogênese do bacterioma durante a embriogênese de D. citri foi descrita por meio de histologia e marcação com sondas oligonucleotídicas fluorescentes (FISH) específicas para os simbiontes do bacterioma. No início da embriogênese, as bactérias permanecem agrupadas em uma massa no polo posterior do ovo. Vitelófagos se aderem à massa de simbiontes no início da blastulação, precedendo à formação dos bacteriócitos. O bacterioma transitório resultante possui bacteriócitos que contém o simbionte do sincício (Profftella), localizado externamente aos que contém o simbionte do bacteriócito (Carsonella). Na sequência do desenvolvimento, ocorre a reorganização dos bacteriócitos, evento seguido pela formação da região sincicial. O bacterioma é movido para a região abdominal do embrião durante a catatrepsis, passando ao formato trilobado típico ao final da embriogênese. A densidade dos simbiontes associados ao psílideo dos citros durante o seu desenvolvimento foi determinada por PCR quantitativo em tempo real (qPCR). A densidade dos diferentes simbiontes, dada pela análise do número de cópias dos genes 16S rRNA (Carsonella e Profftella) e ftsZ (Wolbachia), revelaram o crescimento contínuo dos simbiontes ao longo do desenvolvimento do hospedeiro. As curvas e taxas de crescimento dos simbiontes, estimadas por meio da equação de Gompertz, indicaram relação inversamente proporcional à especificidade das relações simbiontehospedeiro e o tempo para atingir a taxa máxima de crescimento. A densidade de Carsonella foi significativamente menor daquela de Profftella em todos os estágios analisados, apesar da tendência de aumento paralelo. As taxas de crescimento de Wolbachia foram similares às de Carsonella, mas a densidade foi inferior. Nos adultos, a densidade dos três simbiontes foi maior nos machos. Entretanto, esses simbiontes continuaram a apresentar crescimento em fêmeas em atividade de oviposição, mesmo com a sua incorporação aos oócitos, o que diverge da diminuição normalmente observada em outros sistemas. Os simbiontes de D. citri responderam de forma variável ao estresse térmico. Os diferentes simbiontes apresentaram resposta própria aos diversos períodos de exposição às diferentes condições térmicas de estresse. Ainda, foi detectada a influência de um simbionte na capacidade de resposta do outro, demonstrando a existência de mecanismos de comunicação e regulação entre os simbiontes de D. citri. O estudo demonstra a influência do estresse térmico sobre a densidade dos simbiontes e a necessidade de se compreender melhor a biologia das interações insetosimbiontes e a dinâmica das relações com o ambiente. / Diaphorina citri feeds on phloem-sap and depends on bacterial symbionts harbored in the bacteriome as a supplementary source of nutrients lacking in the diet. These bacteria are vertically transmitted, being incorporated into the developing bacteriome. Here, we focus on the events related to bacteriome morphogenesis, symbiont density during host development and the effects of exposure to high temperatures on the establishment of endosymbionts during immature development. The bacteriome morphogenesis during D. citri embryogenesis was investigated by means of histology and fluorescence in situ hybridization analysis (FISH) using symbiont-specific oligonucleotide probes. During early embryogenesis, the bacteria remain aggregated in a symbiont-ball at the posterior pole of the egg. Vitellophages adhere to the symbiont mass during early blastulation, preceding bacteriocyte formation. As a result, the transient bacteriome has the bacteriocytes that harbors the syncytium symbiont (Profftella) arranged externally to those harboring Carsonella. The bacteriome is moved to the embryo abdominal region as a result of katatrepsis, becoming trilobated during the later embryonic development. The infection density of the endosymbionts associated to the Asian citrus psyllid was determined using real-time quantitative PCR (qPCR), throughout the host life cycle. Copy number of genes 16S rRNA (Carsonella and Profftella) and ftsZ (Wolbachia), revealed the continuous growth of symbionts during host development. Growth curves and rates of symbionts estimated using the Gompertz equation indicated an inversely proportional correlation between the degree of symbiont cospeciation with the host and the time to achieve the maximum growth rate. Carsonella density was significantly lower than that of Profftella at all stages analyzed, despite their joint growth trend. The growth rates of Wolbachia were similar to those of Carsonella, but Wolbachia had a lower density. In adults, the density of the three symbionts was higher in males. However, density in reproductive females remained high, despite the incorporation of symbionts in the oocytes. The increased density of symbionts in postreproductive adults contrasts with the decrease observed in other symbiotic systems. The infection density is mutually related to biological effects, but the symbiont may vary the response to heat stress. Density of Profftella and Carsonella was higher than that of Wolbachia, although there were different response patterns related to temperatures and treatment times. Symbionts associated with D. citri have their growth affected by the symbionts. This study demonstrates the effects of the heat shock on symbiont density during nymphal development and illustrates the need of further work the biology of insect-symbiont interactions and the dynamics of its relationships with the environment for a better understading of such associations.

Bacterioma

Bacteriome

Choque térmico

Densidade de simbiontes

Embriogênese

Embryogenesis

Heat shock

Symbiont density

Influence of hyperthermia and antioxidant supplementation on redox balance and heat shock protein response to exercise

Mohd Sukri, Nursyuhada

January 2018

Physical activity of moderate intensity and duration leads to healthy biological adaptations in humans. However, very intense and prolonged exercise may induce disruption in redox balance, potentially increasing oxidative stress. In addition, exposure to environmental heat stress and associated hyperthermia further increases oxidative stress and may induce the expression of heat shock proteins. However, antioxidant supplementation is believed to minimise the effect of oxidative stress and may therefore help reduce or limit the heat shock response to exercise heat stress. The first study (Chapter 4) examined whether exertional heat illness (EHI) casualties among military recruits may exhibit greater disturbances in redox balance following exercise compared to non-EHI controls. Nine (n=9) recruits were identified as having suspected EHI during the Loaded March (LM) on day 1, with a peak mean (SD) body core temperature of 40.1 (0.5) °C. Fifteen (n=15) recruits were identified as having suspected EHI during the Log Race (LR) on day 2, with a peak mean (SD) body core temperature of 39.7 (0.5) °C. A further twenty-one (n=21) recruits, which successfully finished both LM and LR events, were treated as controls (CON). Interestingly, the plasma antioxidant concentration was significantly elevated from pre to post-exercise (p < 0.001) for EHI and CON groups, during both LM and LR events, with no changes on lipid peroxide protein carbonyl concentrations. These data suggest there is no increase in lipid peroxide or protein carbonyl level damage in response to intense hyperthermic military exercise, regardless of acute heat illness. It is possible that military training augments the body's defence capabilities, thus reducing oxidative stress and damage induced by free radical production. To date there is a scarcity of data examining the effects of acute intake of antioxidant supplements on oxidative stress and heat shock response during continuous exercise in a hot environment. Hence, the aims of the second study (Chapter 5) were to examine the effects of acute ingestion of Quercetin (Q), Quercetin + vitamin C (QC) or placebo (P) 14 hours before, 2 hours before and every 20 minutes during trials on oxidative stress and heat shock response. In this randomised, crossover study 10 recreationally active males (age 21±2 y, V̇ O2max 54.9±8.4 ml.kg.min-1) completed three running trials at 70% V̇ O2max for 60 minutes in the heat (33.0±0.3°C; 28.5±1.8% relative humidity). Exercise heat stress significantly elevated plasma quercetin (p=0.02), antioxidant power (FRAP) (p < 0.001),plasma heat shock protein 70 (HSP70) (p=0.009) and plasma heat shock protein 90α(HSP90α) (p < 0.001) over time, but no differences were detected between trials. Also, no changes were observed in protein carbonyl concentration. Acute intake of quercetin significantly increased the level of plasma quercetin however, this did not affect the plasma antioxidant capacity or heat shock response to exercise heat stress. The increases in plasma HSP70 and HSP90α concentrations might act as supplementary antioxidants, reducing the oxidative damage reflected in the absence of changes in protein carbonyl. Exercise heat stress is effective in inducing both intracellular HSP70 (muscle and peripheral blood mononuclear cell (PBMC)) and extracellular HSP70 (plasma) concentrations. Thus, the third study (Chapter 6) tested the hypothesis that this acute quercetin supplementation would induce similar trends in plasma HSP70 and intracellular HSP70 concentrations 2 days following exercise heat stress. In this randomised, crossover study, 9 recreationally active males (age 22±2y, V̇ O2max 50.3±3.3ml.kg.min-1) completed three running trials at 70% V̇ O2max for 60 minutes in the heat (32.9±0.3°C; 28.3±1.2% relative humidity). This study demonstrated that there is no positive relationship between both intracellular of HSP70 (muscle and PBMC) and plasma HSP70 (eHSP70) 2 days following exercise heat stress. These data suggest that the release of eHSP70 could originate from others tissue or cells. Additionally, the absence of differences between trials in the expression of muscle HSP70, PBMC HSP70 and plasma HSP70 might indicate it is implausible that quercetin might inhibit the expression of HSP70 in plasma, muscle and PBMC 2 days following the exercise heat stress stimulus. Overall, the results from this thesis emphasise that the hyperthermia experienced in response to exercise and environmental heat stress could potentially influence the human redox response and heat shock response. Besides, there is reasonable evidence that acute quercetin co-ingestion with vitamin C has the potential to improve the bioavailability and bioactive effects of quercetin, however, the effects of quercetin supplementation in reducing oxidative stress in response to exercise heat stress remains to be elucidated. In addition, the anti-oxidative ability of acute ingestion of quercetin to suppress the intracellular and extracellular heat shock response remains uncertain and worthy for further investigation.

Expressão da Heat Shock Protein 70 em usuários do tabaco

Santos, Thyego Mychell Moreira

January 2018

Orientador: Ilda de Godoy / Resumo: O tabagismo é responsável pelo maior número de mortes evitáveis ​​no mundo e está relacionado ao desenvolvimento de várias doenças, principalmente a doença pulmonar obstrutiva crônica (DPOC). Assim, a busca por biomarcadores precoces torna-se relevante para sua identificação e para o sucesso terapêutico. Os objetivos do nosso estudo foram avaliar a concentração da proteína de choque térmico 70 (HSP70), expressão do gene HSP70, anticorpos anti-HSP70 auto, marcador inflamatório sistêmico através da citocina interleucina-8 (IL-8) e proteína C reativa (PCR), alterações imunológicas e danos no DNA no sangue periférico de fumantes crônicos assintomáticos e não fumantes. Nossos resultados mostraram concentrações séricas aumentadas de HSP70, anti-HSP70, IL-8, PCR e neutrófilos, e danos no DNA de células sanguíneas de fumantes em comparação ao não-fumantes. Portanto, o tabagismo foi responsável por levar a alteração nos parâmetros fisiológicos e moleculares associados ao risco de desenvolver DPOC e outras doenças pulmonares. Com base nos dados, sugerimos que a HSP70 pode ser responsável pelo aumento dos níveis de citocinas inflamatórias e, consequentemente, o aumento do influxo de neutrófilos para os pulmões e aumento dos danos ao DNA e auto-anticorpos anti-HSP70. / Abstract: Smoking is responsible for the largest number of preventable deaths in the world, and is related to the development of several diseases, mainly chronic obstructive pulmonary disease (COPD). Thus, the search for early biomarkers of such diseases becomes relevant for their identification and for successful therapy. The objectives of our study were to evaluate the concentration of heat shock protein 70 (HSP70), expression of the HSP70 gene, anti-HSP70 auto antibodies, the systemic inflammatory marker through cytokine interleukin-8 (IL-8) and CPR, immunological changes and DNA damage in peripheral blood of chronic asymptomatic smokers and non-smokers. Our results showed increased serum concentrations of HSP70, anti-HSP70, IL-8, CPR and neutrophils, and DNA damage in blood cells of smokers than in non-smokers. Therefore, cigarette smoking was confirmed as a noxious agent on physiological and molecular parameters associated with the risk for developing COPD and other lung diseases. Based on the data we suggest that HSP70 can be responsible for the increased levels of inflammatory cytokines, and consequently, the increased influx of neutrophils into the lungs and increased DNA damages e anti-HSP70 auto antibodies. / Doutor

Tabagismo.

Danos no DNA

Inflamação sistêmica

Heat shock Protein 70

Smoking

DNA damage

Systemic inflammation

The effects of targeted therapy on cell viability and apoptosis on CML and AML cell lines

Marsico, Paolo

January 2019

Tyrosine kinase inhibitors (TKIs) are currently the first therapy option for chronic myeloid leukaemia (CML) and acute myeloid leukaemia (AML) patients. However, many patients affected by CML and AML may develop resistance to TKIs or may not recover under this treatment regime. New potential and more effective treatments are recently emerging. Heat shock protein inhibitors (HSPIs) and the proteasome inhibitor Bortezomib are drugs which have been yet to be successfully tested on leukemic patients, despite being successful on other malignancies such as multiple myeloma (MM). The combination between HSPIs and Bortezomib could potentially be successful in killing leukemic cells, by enhancing their respective molecular mechanisms. Indeed, HSPIs would bind to HSP72 avoiding the protein to exert its ligase function to the proteasome, whilst Bortezomib could stop the ubiquitinated proteins to enter the proteasome and ultimately inducing apoptosis. To test the effects of such combination, cell viability was measured via MTS assay, apoptosis levels were tested through Annexin V\PI assays. Involvement of HSP72 and pro-survival protein Bcl-2 were measured via flow-cytometry. The cells were administered with HSPIs and Bortezomib first as single agents for 24 hours, to establish working minimal concentration. Also, the drugs were tested for a shorter time, to understand when the drugs start to be effective. It emerged that one hour is sufficient for the drugs to give an initial effect in terms of cell viability and apoptosis. Following, combination experiments of HSPIs and Bortezomib were performed; the first drug was administered for one hour, the second following one hour and the cells were incubated for 24 hours. This was repeated alternatively for both type of drugs on the different cell lines. MTS and Annexin V\PI showed that there is not a synergistic effect between drugs, but instead there is antagonism. No necrosis was found at any level of the study. The cells were then probed for HSP72 and Bcl-2, to investigate their involvement in apoptosis mechanisms. Following 6 hours of combined and single agent treatment, both type of drugs inhibit HSP72 but failed to reduce the expression of Bcl-2, particularly on AML cells. It is thus proposed that CML and AML cells may die by apoptosis following a short time of treatment with HSPIs and Bortezomib by an extrinsic pathway of apoptosis, independent from Bcl-2 involvement and from mitochondrial pathway of apoptosis. This study may be the first to indicate a potential use of HSPIs and Bortezomib on CML and AML patients for a short time of treatment, although not in combination. Future studies are needed to further investigate the mechanisms of action of these drugs, aiming to potentially give CML and AML patients another successful therapy option to overcome resistance to canonic chemotherapy.

Rôle des protéines de choc thermique dans les néoplasies myéloprolifératives : implication de HSP27 dans la myélofibrose / Role of heat shock protein in myeloproliferative neoplasms : involvement of HSP27 in myelofibrosis

Sevin, Margaux

19 December 2017

La myélofibrose (MF) est la plus agressive des néoplasies myéloprolifératives (NMP). Elle porte à elle seule le plus mauvais pronostic pour les patients puisqu’elle s’accompagne d’une fibrose de la moelle osseuse évoluant vers une insuffisance médullaire. Les inhibiteurs de la kinase JAK2 ont apporté de nouveaux espoirs pour le traitement des NPM mais leurs effets ont été essentiellement bénéfiques sur les symptômes et non sur la fibrose elle-même ni sur le cours de la maladie. Plus récemment, la protéine de choc thermique 90 (HSP90) - connue pour stabiliser JAK2 - est apparue comme une cible thérapeutique prometteuse pour les NMP. Cependant, les inhibiteurs de la HSP90 ont montré une toxicité importante accompagnée d’une expression compensatoire des HSPs inductibles (i.e HSP70, HSP27), connues pour favoriser l’émergence de phénomène de résistance. Par ailleurs, des études ont montré que HSP27 était fortement exprimée chez les patients présentant une fibrose pulmonaire idiopathique ou rénale montrant l’importance de HSP27 dans les processus fibrotiques. Sur la base de l’ensemble de ces données, nous avons évalué d’une part l'efficacité chez l’animal d'un oligonucléotide inhibiteur spécifique de HSP27 appelé OGX-427 (en essai clinique dans plusieurs cancers). D’autre part, nous avons déterminé le niveau d’expression intra- et extracellulaire de HSP27 chez des patients atteints de MF. L'effet de l'OGX-427 a été évalué dans deux modèles murins de myélofibrose, laquelle est induite soit par la sécrétion excessive de thrombopoïétine (TPOhigh) soit par la mutation JAKV617F. Nous avons mis en évidence dans les souris traitées par l’OGX-427, une réduction de la taille de la rate, de la prolifération mégacaryocytaire et de l’hématopoïèse extramédullaire par rapport aux souris contrôles, révélant ainsi un effet bénéfique de l’inhibition de HSP27 sur la progression de la maladie. De toutes récentes observations complémentaires à ce travail ont également montré une diminution de la fibrose réticulinique dans la moelle osseuse de souris JAKV617F. Au niveau moléculaire, nous démontrons que l'effet prolifératif induit par la voie de signalisation exacerbée - JAK2/STAT5 - est régulé par HSP27 via des interactions directes. Pour finir, nous avons détecté une augmentation de l'expression de HSP27 aussi bien dans les progéniteurs circulants CD34+ que dans le sérum des patients atteints de NMP avec MF. Ce travail révèle pour la première fois le rôle intra et extracellulaire de HSP27 dans la physiopathologie de la MF et le bénéfice thérapeutique potentiel de l’utilisation des inhibiteurs de HSP27 dans cette maladie. / Myelofibrosis (MF) is the most aggressive myeloproliferative neoplasms (MPN) with the highest degree of morbidity and mortality, including progressive bone marrow fibrosis resulting into bone marrow failure. JAK2 kinase inhibitors have been successfully used for a few years in MPN and more particularly for MF treatment. Nevertheless, their beneficial effects are mainly restricted on symptoms and not on the course of the disease. Recently, heat shock protein 90 (HSP90) - known to stabilize JAK2 - has been reported as a promising therapeutic target in MPN. However HSP90 inhibitors show toxicity and induce the expression of stress-inducible proteins such as HSP70 and, most likely HSP27 as previously shown in other cancers. In addition, we and others have shown that HSP27, was strongly expressed in patients with idiopathic pulmonary or kidney tubulointerstitial fibrosis, underlying a relevant role of HSP27 in fibrotic processes. Taking into account both the beneficial effects of HSP inhibitors in leukemia and in MPN, and the possible implication of HSP27 in fibrosis, we have evaluated here the status of HSP27 in MF patient’s samples and assess the effectiveness of an HSP27 oligonucleotide inhibitor called OGX-427 in murine models. We report here the effect of OGX-427 in two murine models of thrombopoietin- and JAKV617F-induced myelofibrosis. OGX-427 limited the progression of the disease associated with a reduction of spleen weight and of megakaryocytic expansion. And more recently, our additional results show a decrease of reticulin fibrosis in JAK2V617F’s bone marrow. We show that HSP27 regulates JAK2/STAT5 proliferative effect through direct interactions, and we report an increase expression of HSP27 both in CD34+ circulating progenitors and in the serum of patients with NMP with fibrosis. Taking altogether, this work supports that extra and intracellular HSP27 plays a key role of in the pathophysiology in MF and highlight the potential therapeutic benefit of HSP27 inhibitors in this disorder.

Myélofibrose

Protéines de choc thermique

HSP27

Thérapie

Myelofibrosis

Heat shock protein

HSP27

Therapy

571.6

Roles of prolactin in salinity adaptation, Hsp70 expression and apoptosis in sparus sarba. / CUHK electronic theses & dissertations collection

January 2007

Also, the branchial hsp70 levels in fish following chronic salinity acclimation and abrupt hypo-osmotic exposure to 6 ppt were assessed by Western blotting. Upon chronic salinity acclimation, the lowest branchial hsp70 level was found in fish cultured in an iso-osmotic salinity of 12 ppt and the highest was in 50 ppt and 6 ppt environments. Freshwater acclimation resulted in return to lower hsp70 level. The results indicated that iso-osmotic salinity would bring about the least stress level while 50 ppt and 6 ppt were the most stressful salinities to Sparus sarba as indicated by using hsp70 expression as a biomarker of stress. Compared to 50 ppt and 6 ppt, the stress level of fish in fresh water was lower. On the other hand, Sparus sarba exhibited a significant increase in branchial hsp70 level immediately after abrupt hypo-osmotic exposure to 6 ppt when compared with seawater fish sampled at the same time point and increased hsp70 level was sustained throughout the sampling period, indicating the exposure was stressful to the fish. / In the present study, pituitary and serum levels of prolactin in a marine teleost, Sparus sarba, chronically acclimated to various salinities: fresh water (0 ppt), hypo-osmotic (6 ppt), iso-osmotic (12 ppt), normal seawater (33 ppt) and hypersaline (50 ppt) or abruptly exposed to a hypo-osmotic environment of 6 ppt were quantified by the developed peptide-based indirect ELISAs. Progressive increases in pituitary and serum prolactin were found as chronic salinity acclimation progressed from seawater to fresh water. Also, prolactin secretion was immediately induced by abrupt hypo-osmotic exposure to 6 ppt and remained significantly elevated up to 5 days post-exposure to 6 ppt. The results underline the importance of prolactin in marine teleosts kept in fresh water or waters of low salinity. However, there was no significant difference in pituitary prolactin during the course of the abrupt hypo-osmotic exposure experiment. The results may indicate that prolactin might be secreted rapidly from pituitary in large quantities to cope with abrupt exposure to a low-salinity environment. / In the present study, the effects of pharmacological drugs on prolactin levels in pituitary and serum of Sparus sarba were investigated. An increase in prolactin synthesis and release but a decrease in branchial hsp70 expression were found after treatment with sulpiride, a DA-D2 receptor antagonist. In contrast, a reduction in prolactin levels in pituitary and serum but an elevation in hsp70 level in gill were observed following administration of bromocriptine, a DA-D2 receptor agonist. Since hsp70 expression indicates the stress levels, the results of these studies supported the notion that increased prolactin synthesis and release might be related to a reduced stress state and prolactin might have a protective effect on stress tolerance in fish. / Lastly, the role of prolactin in regulating apoptosis in Sparus sarba branchial cells was examined. Successful induction of apoptosis was indicated by an increase in the apoptotic parameter caspase-3 activity in primary cultures of Sparus sarba branchial cells treated with camptothecin, a specific inducer of apoptosis. In this study, prolactin was shown to be anti-apoptotic in Sparus sarba branchial cells as co-treatment with ovine prolactin (oPRL) and camptothecin has been observed to attenuate the elevated caspase-3 activity in gill cell primary cultures. Also, prolactin was found to protect the branchial cells from apoptosis by maintaining the hsp70 level in the cells treated with camptothecin. / The objectives of the present study were to investigate the roles of prolactin in salinity adaptation, hsp70 expression and apoptosis in silver sea bream (Spaurs sarba). Firstly, specific peptide-based indirect ELISAs were developed for pituitary and serum prolactin of Sparus sarba. These assays had been validated by parallelism between the dilution response curves using serially diluted pituitary homogenate and serum sample with the standard curves of the synthetic peptide derived from the amino acid sequence of black sea bream (Acanthopagrus schlegelii ) prolactin. / Ng, Ho Yuen Andus. / "September 2007." / Adviser: N. Y. S. Woo. / Source: Dissertation Abstracts International, Volume: 69-08, Section: B, page: 4567. / Thesis (Ph.D.)--Chinese University of Hong Kong, 2007. / Includes bibliographical references (p. 143-189). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Electronic reproduction. [Ann Arbor, MI] : ProQuest Information and Learning, [200-] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts in English and Chinese. / School code: 1307.

Fishes--Adaptation

Prolactin--Physiological effect

Rhabdosargus sarba--Physiology

In vitro study of hormonal regulation of heat shock protein 70 expression in sea bream. / CUHK electronic theses & dissertations collection

January 2003

Zhou Liran. / "June 2003." / Thesis (Ph.D.)--Chinese University of Hong Kong, 2003. / Includes bibliographical references (p. 182-216). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Mode of access: World Wide Web. / Abstracts in English and Chinese.

Sebastes marinus--Physiology

Stress (Physiology)

Hormones--Physiological effect

Fishes--Physiology

Investigation of the role of essential proteins in gene silencing at the centromere of Schizosaccharomyces pombe

Dobbs, Edward

January 2012

The centromeres of eukaryotes have a region on which the kinetochore is assembled, flanked by heterochromatin which provides cohesion between the sister chromatids during cell division. When centromeric heterochromatin is lost chromosomes no longer segregate evenly into the daughter cells during cell division. In the fission yeast Schizosaccharomyces pombe (S. pombe) RNA interference (RNAi) is responsible for maintaining this heterochromatin. The pathway is part of a feedback loop whereby siRNAs generated from non-coding centromere transcripts are loaded into an Argonaute complex. The siRNAs guide the complex to the homologous centromere repeats in order to recruit Clr4 which modifies histone H3 with the heterochromatin mark H3K9me. A previous screen to find factors affecting centromere silencing isolated 13 loci termed centromere: suppressor of position-effect (csp) 1-13. Several csp mutants have been identified to be RNAi components. In this investigation the csp6 locus has been identified to be the Hsp70 gene ssa2+. It has been demonstrated that Argonaute proteins from plants and flies require Hsp70/90 chaperone activity for loading of siRNA. It therefore seems likely that Hsp70 may play a similar role in fission yeast. Genetic and biochemical techniques have been used in this study to investigate if the csp6 alleles are affecting siRNA loading in S. pombe. RNA Polymerase II (RNAPII) transcribes the pre-siRNA transcripts from the centromere repeats. csp3 was identified to be an allele of the RNAPII subunit rpb7+. rpb7-G150D was found to cause a silencing defect in the centromeric heterochromatin through a defect in transcription. Another RNAPII mutation, rpb2-m203, was found to have strong silencing defects caused by an unidentified non-transcriptional role in RNAi-mediated heterochromatin formation at the centromere. In order to gain more insight into the role of RNAPII in heterochromatin assembly I performed a screen in which the subunits rpb3 and rpb11 were subjected to random mutagenesis. Several mutants were isolated and characterisation of phenotypes regarding heterochromatin at the centromere has been carried out for nine of the mutants. As a result a novel phenomenon of RNAi-independent silencing at the centromere has been discovered.

572.8

Small heat shock protein interactions with in vivo partners

Collier, Miranda

January 2018

Small heat-shock proteins (sHsps) are part of a broad cellular sys- tem that functions to maintain a stable proteome under stress. They also perform a variety of regulatory roles at physiological conditions. Despite the multitude of sHsp targets, their interactions with partners are not well understood due to highly dynamical structures. In this thesis, I apply a variety of biophysical and structural approaches to examine distinct interactions made by the abundant human sHsps αβ-crystallin and Hsp27. First, I find that αβ-crystallin binds a cardiac-specific domain of the muscle sarcomere protein titin. A cardiomyopathy-causative variant of αβ-crystallin is shown to disrupt this interaction, with demonstrated implications for tissue biomechanics. Next, I investigate the conformation and unfolding behaviour of another sarcomere-associated protein, filamin C, finding support for the hypothesis that it is mechanosensitive. This leads into an interrogation of the interaction between filamin C and Hsp27, which we find is modulated by phosphorylation of Hsp27. This modulation only manifests during filamin C unfolding, pointing toward a protective chaperoning mode against over-extension during mechanical stress. This finding is bolstered by up-regulation and interaction of both proteins in a mouse model of heart failure. I establish a system for similar studies of a third sHsp, cvHsp, which is muscle-specific and implicated in various myopathies but scantly understood at the molecular level compared to αβ-crystallin and Hsp27. Finally, I probe the stoichiometries and kinetics of complexes formed between αβ-crystallin and Hsp27 themselves, which co-assemble into a highly polydisperse ensemble. This involved the development of a high-resolution native mass spectrometry method for disentangling heterogeneous systems. Together these findings add to our understanding of the roles and mechanisms of ATP-independent molecular chaperones.