Identification and Validation of Small Molecules Inhibiting Human Adenovirus Replication

Saha, Bratati

01 October 2019

Human adenovirus (HAdV) mainly causes minor illnesses, but can lead to severe disease and death in both immunocompromised and immunocompetent patients. In such cases, the current standards of treatment often do not improve disease outcome and no approved antiviral therapy against HAdV exists. Since HAdV relies on cellular machinery to assist in the progression of the virus lifecycle, we hypothesized that small molecules targeting certain cellular proteins/pathways, without severely affecting cell health, may serve as effective anti-HAdV compounds. Thus, we aimed to identify novel inhibitors of HAdV, and investigate the molecular mechanism to determine new therapeutic targets for intervention in HAdV infection. We first examined the antiviral properties of pan-histone deacetylase (HDAC) inhibitor SAHA and found that the drug affects multiple stages of the HAdV lifecycle, resulting in significant reductions in virus yield. SAHA was effective in decreasing gene expression from clinically relevant HAdV serotypes. Subsequent investigations on the role of HDACs in HAdV infection led us to determine that class I HDAC activity, mainly HDAC2, is necessary for optimal viral gene expression. Using a wildtype-like HAdV reporter construct that allows us to monitor virus replication by fluorescence microscopy, we then designed an efficient system for screening small molecules to identify novel HAdV inhibitors. We screened over 1300 small molecules, and the screen was sensitive enough to detect compounds with both robust and modest antiviral activity. Several positive hits were validated to reduce HAdV gene expression and yield from infected cells. Further investigation on the efficacy of these compounds and the mechanism behind their inhibition of HAdV can lead to the discovery of new pharmacological targets and the development of more effective antivirals.

Adenovirus

Antiviral

Small molecule screen

Viral epigenetics

SAHA

Histone deacetylase

Cardiotonic steroids

Corticosteroids

Corporate Governance : An Empirical Analysis of the Relationship between SAHA’s Corporate Governance Rating Scores and Firm Performance at Istanbul Stock Exchange

Aydemir, Burak

January 2012

This study examines the relationship between SAHA’s corporate governance rating score and firm performance in Turkey for the period between 2008, 2009 and 2010. The purpose of study is to analyze whether there is a relationship between Saha’s corporate governance score which is based on the principles of Capital Market Board of Turkey and firm performance for 16 companies listed in corporate governance index Istanbul Stock Exchange (ISE) by using Saha’s Corporate Governance. It also aims to determine this relationship by attempting to answer the question of whether better governed firms as measured by high corporate governance score have higher firm performance in Turkey. With this purpose three analyses were conducted and random effect model, one type of panel data, is used to analyze whether there is a relationship between corporate governance and firm performance. The conceptual framework for this study is a combinationan of approaches to agency, stakeholder and stewardship theory. Panel data is created as unbalanced data and random effect model is used.Accounting based performance measures of firms: return on asset, return on equity and returnon sales were used to compare with Saha’s Corporate Governance Rating Score based on four sub-indices: 1) shareholder rights, 2) public disclosure and transparency, 3) stakeholders and 4) board of directors. The results based on Saha’s Corporate Governance Score show that corporate governance does matter in Turkey. The study shows that better governed firms measured by high corporate governance score have better performance in Turkey. The result of regressing return on asset, return on equity against Saha’s corporate governance rating score indicates that there is a significantly relationship between corporate governance and firm performace. However, the result of regressing return on sales indicates that there is no statistically significant relation between Saha’s corporate governance score and return on sales.

Corporate Governance

Firm Performance

Saha Corporate Governance Ratings

Istanbul Stock Exchange

Espectroscopia de plasma gerado por laser em regime temporal de nanosegundos e femtosegundos em padrões de aço inoxidável ferrítico

FIGUEIREDO, MARCIO B.

09 October 2014

Made available in DSpace on 2014-10-09T12:53:20Z (GMT). No. of bitstreams: 0 / Made available in DSpace on 2014-10-09T14:09:35Z (GMT). No. of bitstreams: 0 / Dissertacao (Mestrado) / IPEN/D / Instituto de Pesquisas Energeticas e Nucleares - IPEN-CNEN/SP

STAINLESS STEELS

FERRITIC STEELS

PLASMA

SPECTROSCOPY

LASER-PRODUCED PLASMA

SAHA EQUATION

BOLTZMANN EQUATIONS

Espectroscopia de plasma gerado por laser em regime temporal de nanosegundos e femtosegundos em padrões de aço inoxidável ferrítico

FIGUEIREDO, MARCIO B.

09 October 2014

Made available in DSpace on 2014-10-09T12:53:20Z (GMT). No. of bitstreams: 0 / Made available in DSpace on 2014-10-09T14:09:35Z (GMT). No. of bitstreams: 0 / No presente trabalho foi realizada uma análise de dois padrões de aço inoxidável ferrítico submetidos à ação de lasers pulsados, um no regime de nanosegundos e outro no regime de femtosegundos. Foram determinadas as temperaturas e densidades do plasma formado a partir da análise espectroscópica da radiação emitida em diferentes faixas espectrais, por diferentes espécies e em diferentes janelas de integração no tempo. As temperaturas foram obtidas de duas formas, pelo método do gráfico de Boltzmann e pela razão entre duas linhas. Os resultados foram comparados com o intuito de verificar se o método da razão conseguia recuperar os resultados obtidos pela abordagem do gráfico de Boltzmann. Foi observada uma grande concordância entre os dois métodos no regime de femtosegundos, ao passo que no regime de nanosegundos a recuperação das temperaturas não foi tão satisfatória. A densidade eletrônica do plasma foi determinada a partir do alargamento Stark e verificou-se que o plasma gerado pelo laser de nanosegundos era mais denso que aquele gerado no regime de femtosegundos. As densidades determinadas sob diferentes janelas de integração do sinal no tempo foram também comparadas sendo que aquelas relativas aos estágios iniciais do plasma eram maiores que aquelas de estágios finais. Com a obtenção das temperaturas e das densidades foi possível caracterizar totalmente o plasma e compará-lo com outros plasmas naturais e artificiais. / Dissertacao (Mestrado) / IPEN/D / Instituto de Pesquisas Energeticas e Nucleares - IPEN-CNEN/SP

stainless steels

ferritic steels

plasma

spectroscopy

laser-produced plasma

saha equation

boltzmann equation

Chemical Biology Approaches for the Molecular Recognition of DNA Double Helix / DNA二重らせんの分子認識に関するケミカルバイオロジー研究

Abhijit, Saha

23 March 2015

京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第18807号 / 理博第4065号 / 新制||理||1585(附属図書館) / 31758 / 京都大学大学院理学研究科化学専攻 / (主査)教授 杉山 弘, 教授 三木 邦夫, 教授 秋山 芳展 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM

Transcription Activation

SAHA-Polyamide

Pluripotency genes

HDAC

Bromouracil DNA

Photo reaction

Electron transfer

400

Action anti-leucémique des inhibiteurs de la méthylation de l’ADN et de la déacétylation des histones

Lemaire, Maryse

04 1900

Les gènes suppresseurs de tumeurs (TSGs) contrôlent la prolifération cellulaire et leur inactivation joue un rôle important dans la leucémogénèse. Deux mécanismes épigénétiques majeurs sont impliqués dans la répression des TSGs: 1- la méthylation de l’ADN et 2- la déacétylation des histones des chromosomes. On les dit épigénétiques car ils n’affectent pas la séquence de l’ADN. Ces phénomènes sont réversibles, faisant donc d’eux des cibles thérapeutiques de choix. Dans le cadre de cette thèse, nous avons évalué le potentiel chimiothérapeutique de différents agents qui visent ces mécanismes épigénétiques et nous les avons administrés seuls et en combinaison dans le but d’améliorer leur efficacité. La 5-aza-2’-désoxycytidine (5-Aza-CdR) est un inhibiteur de la méthylation de l’ADN qui permet la ré-expression des TSGs. Cet agent s’est avéré efficace contre certaines maladies hématologiques et est d’ailleurs approuvé aux États-Unis dans le traitement du syndrome myélodysplasique depuis 2006. Cependant, le protocole d’administration optimal de cet agent, en termes de doses et de durée, n’est toujours pas établi. Nos recherches suggèrent que le celui-ci devrait être plus intensif que ce que rapporte la littérature. Les inhibiteurs des déacétylases des histones (HDACi) ont également montré une activité antinéoplasique intéressante. De récentes recherches ont montré que la combinaison d’agents ciblant à la fois la méthylation de l’ADN et la déacétylation des histones produit une réactivation synergique des TSGs, ce à quoi nous nous sommes intéressé. Nous avons observé que la co-administration d’un HDACi avec la 5-Aza-CdR potentialise son action anti-leucémique. Il est aussi possible d’augmenter l’activité de la 5-Aza-CdR en inhibant sa dégradation par l’enzyme cytidine (CR) désaminase. Nous avons observé que la co-administration du zebularine, un inhibiteur de la CR désaminase, avec la 5-Aza-CdR accroît son efficacité. Le zebularine est aussi un inhibiteur de la méthylation de l’ADN, ce qui pourrait contribuer à la potentialisation de la réponse anti-leucémique observée lors de la co-administration de ces deux agents. En résumé, il est possible d’augmenter l’efficacité anti-leucémique de la 5-Aza-CdR en : 1- intensifiant son protocole d’administration, en termes de doses et de durée, 2- la combinant avec un HDACi, et 3- diminuant sa dégradation par la CR désaminase. L’utilisation de ces résultats précliniques dans l’élaboration de protocoles cliniques pourrait être bénéfique à beaucoup de patients. / The silencing of tumor suppressor genes (TSG) that normally regulate cells proliferation plays an important role in leukemogenesis. Two major mechanisms are involved in TSG’s silencing: DNA methylation and histones deacetylation. Because those phenomenons are reversible, it makes them interesting therapeutic targets for chemotherapeutic agents. We evaluated the antineoplastic potential of different agents that target those events and we administered them alone or in combination with the goal of improving their efficiency. 5-aza-2’-deoxycytidine (5-Aza-CdR) is a DNA methylation inhibitor that can re-express TSGs that are silenced by methylations. This agent demonstrated its efficacy against hematological malignancies. Therefore, 5-Aza-CdR is used since 2006 in United States of America against myelodysplastic syndrome; but its optimal dose-schedule still needs to be established. Our researches suggest that the dose-schedule of 5-Aza-CdR should be more intensive than what is reported from the literature. Inhibitors of histones deacetylation (HDACi) also demonstrated some interesting antineoplastic activity. Recently, observations showed that combination of chemotherapeutic agent that targets both DNA methylation and histones deacetylation lead to a synergic reactivation of silenced TSG. This finding allowed us to observe that the co-administration of an HDACi with 5-Aza-CdR improve its antileukemic potential. Moreover, it is possible to increase the activity of 5-Aza-CdR by preventing its degradation by cytidine (CR) deaminase. We demonstrated that the co-administration of zebularine, an inhibitor of CR deaminase, with 5-Aza-CdR increases its activity. Zebularine is also an inhibitor of DNA methylation, which may contribute to the enhancement of the antileukemic action of this combination. In summary, our preclinical data indicate that the antileukemic activity of 5-Aza-CdR can be enhanced by: 1- increasing his dosage, 2- combining it with HDACi, and 3- preventing its inactivation by CR deaminase. The translation of those preclinical observations into clinical protocols may be effective in patients with advanced leukemia.

Leucémie

Cancer

5-Aza-2'-désoxycytidine

Zebularine

Phénylbutyrate

SAHA

LAQ824

Cytidine désaminase

Leukemia

Cancer

5-Aza-2'-deoxycytidine

Zebularine

Phenylbutyrate

SAHA

LAQ824

Cytidine deaminase

Novel proapoptotic p63 isoforms are driven by an endogenous retrovirus in the male germ line of humans and great apes, likely increasing genome stability / Neue proapoptotische p63-Isoformen werden von einem endogenen Retrovirus in den männlichen Keimbahnen von Mensch und Menschenaffen gesteuert und erhöhen wahrscheinlich die genomische Stabilität

Beyer, Ulrike

29 October 2010

No description available.

570 Biowissenschaften, Biologie

Biology (incl. Psychology)

TP63

ERV9 LTR

Spermatogonien

genomische Integrität

Primatenevolution

Apoptose

Hodenkrebs

HDAC-Inhibitoren

SAHA

TP63

ERV9 LTR

spermatogonia

genomic surveillance

primate evolution

apoptosis

testicular cancer

HDAC inhibitors

SAHA

42.13

WF 200: Molekularbiologie

Action anti-leucémique des inhibiteurs de la méthylation de l’ADN et de la déacétylation des histones

Lemaire, Maryse

04 1900

Les gènes suppresseurs de tumeurs (TSGs) contrôlent la prolifération cellulaire et leur inactivation joue un rôle important dans la leucémogénèse. Deux mécanismes épigénétiques majeurs sont impliqués dans la répression des TSGs: 1- la méthylation de l’ADN et 2- la déacétylation des histones des chromosomes. On les dit épigénétiques car ils n’affectent pas la séquence de l’ADN. Ces phénomènes sont réversibles, faisant donc d’eux des cibles thérapeutiques de choix. Dans le cadre de cette thèse, nous avons évalué le potentiel chimiothérapeutique de différents agents qui visent ces mécanismes épigénétiques et nous les avons administrés seuls et en combinaison dans le but d’améliorer leur efficacité. La 5-aza-2’-désoxycytidine (5-Aza-CdR) est un inhibiteur de la méthylation de l’ADN qui permet la ré-expression des TSGs. Cet agent s’est avéré efficace contre certaines maladies hématologiques et est d’ailleurs approuvé aux États-Unis dans le traitement du syndrome myélodysplasique depuis 2006. Cependant, le protocole d’administration optimal de cet agent, en termes de doses et de durée, n’est toujours pas établi. Nos recherches suggèrent que le celui-ci devrait être plus intensif que ce que rapporte la littérature. Les inhibiteurs des déacétylases des histones (HDACi) ont également montré une activité antinéoplasique intéressante. De récentes recherches ont montré que la combinaison d’agents ciblant à la fois la méthylation de l’ADN et la déacétylation des histones produit une réactivation synergique des TSGs, ce à quoi nous nous sommes intéressé. Nous avons observé que la co-administration d’un HDACi avec la 5-Aza-CdR potentialise son action anti-leucémique. Il est aussi possible d’augmenter l’activité de la 5-Aza-CdR en inhibant sa dégradation par l’enzyme cytidine (CR) désaminase. Nous avons observé que la co-administration du zebularine, un inhibiteur de la CR désaminase, avec la 5-Aza-CdR accroît son efficacité. Le zebularine est aussi un inhibiteur de la méthylation de l’ADN, ce qui pourrait contribuer à la potentialisation de la réponse anti-leucémique observée lors de la co-administration de ces deux agents. En résumé, il est possible d’augmenter l’efficacité anti-leucémique de la 5-Aza-CdR en : 1- intensifiant son protocole d’administration, en termes de doses et de durée, 2- la combinant avec un HDACi, et 3- diminuant sa dégradation par la CR désaminase. L’utilisation de ces résultats précliniques dans l’élaboration de protocoles cliniques pourrait être bénéfique à beaucoup de patients. / The silencing of tumor suppressor genes (TSG) that normally regulate cells proliferation plays an important role in leukemogenesis. Two major mechanisms are involved in TSG’s silencing: DNA methylation and histones deacetylation. Because those phenomenons are reversible, it makes them interesting therapeutic targets for chemotherapeutic agents. We evaluated the antineoplastic potential of different agents that target those events and we administered them alone or in combination with the goal of improving their efficiency. 5-aza-2’-deoxycytidine (5-Aza-CdR) is a DNA methylation inhibitor that can re-express TSGs that are silenced by methylations. This agent demonstrated its efficacy against hematological malignancies. Therefore, 5-Aza-CdR is used since 2006 in United States of America against myelodysplastic syndrome; but its optimal dose-schedule still needs to be established. Our researches suggest that the dose-schedule of 5-Aza-CdR should be more intensive than what is reported from the literature. Inhibitors of histones deacetylation (HDACi) also demonstrated some interesting antineoplastic activity. Recently, observations showed that combination of chemotherapeutic agent that targets both DNA methylation and histones deacetylation lead to a synergic reactivation of silenced TSG. This finding allowed us to observe that the co-administration of an HDACi with 5-Aza-CdR improve its antileukemic potential. Moreover, it is possible to increase the activity of 5-Aza-CdR by preventing its degradation by cytidine (CR) deaminase. We demonstrated that the co-administration of zebularine, an inhibitor of CR deaminase, with 5-Aza-CdR increases its activity. Zebularine is also an inhibitor of DNA methylation, which may contribute to the enhancement of the antileukemic action of this combination. In summary, our preclinical data indicate that the antileukemic activity of 5-Aza-CdR can be enhanced by: 1- increasing his dosage, 2- combining it with HDACi, and 3- preventing its inactivation by CR deaminase. The translation of those preclinical observations into clinical protocols may be effective in patients with advanced leukemia.

Leucémie

Cancer

5-Aza-2'-désoxycytidine

Zebularine

Phénylbutyrate

SAHA

LAQ824

Cytidine désaminase

Leukemia

Cancer

5-Aza-2'-deoxycytidine

Zebularine

Phenylbutyrate

SAHA

LAQ824

Cytidine deaminase

Advancing Synthetic Gene Regulators Development with High-Throughput Sequencing Technologies / ハイスループットシークエンシング技術を用いた革新的遺伝子制御法の開発に関する研究

Anandhakumar, Chandran

24 September 2015

京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第19260号 / 理博第4115号 / 新制||理||1592(附属図書館) / 32262 / 京都大学大学院理学研究科化学専攻 / (主査)教授 杉山 弘, 教授 三木 邦夫, 教授 藤井 紀子 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM

Chemical Biology

Bind-n-Seq

SAHA-PIP

Alkylating PIP

Synthetic Gene regulators

High-throughput sequencing

ERBB2

400

Chemical Biology Approaches for Regulating Eukaryotic Gene Expression / ケミカルバイオロジー的アプローチによる真核細胞の遺伝子発現制御法の検討

Junetha, Syed Jabarulla

24 September 2015

京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第19261号 / 理博第4116号 / 新制||理||1592(附属図書館) / 32263 / 京都大学大学院理学研究科化学専攻 / (主査)教授 杉山 弘, 教授 三木 邦夫, 教授 藤井 紀子 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM

EVI1 oncogene

Gene Silencing

SAHA-PIP

Retinal Gene Circuit

Synthetic Gene Activator

Long Noncoding RNA

Triple Helix

400