Impact of very early introduction of everolimus on liver regeneration after partial liver transplantation in rats / ラット部分肝移植直後からのエベロリムスの導入が肝再生に与える影響

Hirata, Masaaki

23 March 2023

京都大学 / 新制・課程博士 / 博士(医学) / 甲第24530号 / 医博第4972号 / 新制||医||1065(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 小濱 和貴, 教授 小林 恭, 教授 川口 義弥 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

liver transplantation

everolimus

liver regeneration

rejection

490

Análise da viabilidade das células H295R, linhagem de carcinoma adrenocortical tumoral humano, tratadas com diferentes drogas antitumorais. / Antitumor effects of different cytotoxic drugs on the human adrenocortical tumor cells H295R.

Silveira, Elaine

06 November 2014

O carcinoma adrenocortical (ACC) é um tumor maligno raro. O objetivo foi testar a ação de drogas antitumorais na linhagem H295R, em cultura 2D e 3D, analisadas por MTS, ensaios multiparamétricos, e microscopia confocal. Em monocamada (2D), as drogas tiveram maior efeito quando utilizadas com o mitotano 10 mM, sendo: everolimus 10 mM (50±0,02% p &#8804 0.001), imatinib (10 mM 52±0.01% p &#8804 0.001), sunitinib 5 mM (47±0.02% p &#8804 0.001), e nilotinib 5 mM (59±0,03% p &#8804 0.001), com evidência de apoptose. Nos esferoides (3D) foi necessário mitotano 30 M com everolimus 10 mM para se obter diminuição de 32±0.02% p &#8804 0.001 na viabilidade das células, e com nilotinib 10 mM para redução de 57±0.03% p &#8804 0.001, com evidência de necrose e apoptose. Em resumo, os dados sugerem que os esferoides são mais resistentes aos tratamentos, como ocorre com tumores in vivo, e podem representar uma importante abordagem para estudos de ACC. O nilotinib foi o que induziu as melhores respostas, tanto no modelo em 2D quanto 3D, resultados que se apresentam promissores para o tratamento dos carcinomas adrenocorticais. / Adrenocortical carcinoma (ACC) is a rare malignant tumor. The objective was to test the antitumor drugs action in the H295R cell line, in 2D and 3D culture system, by using MTS, multiparameter assay (High Content Screening) and confocal microscopy. In monolayer, all drugs were more effective in combination with mitotane 10 mM: everolimus 10 mM (50±0.02%), 10 mM imatinib (52±0.01%), 5 mM sunitinib (47±0.02%), and 5 mM nilotinib (59±0.03%). The spheroids required mitotano 30 mM with everolimus 10 mM to decrease cell viability (32±0.02% p &#8804 0.001); and with 10 mM nilotinib to inhibit cell viability in 57±0.03% (p &#8804 0.001), with induction of apoptosis and necrosis. In summary, the spheroids were more resistant to treatment and may represent an important approach for studies of ACC. Nilotinib was the tyrosine kinase inhibitor that, either alone or in combination with mitotane, induced higher cytotoxicity, in both 2D and 3D cell cultures, showing promising results for the treatment of adrenocortical carcinoma, as well as for the studies of its mechanism of action.

Adrenocortical carcinoma

Carcinoma adrenocortical

Esferoides

Everolimus

Everolimus

Mitotane

Mitotano

Nilotinib

Nilotinib

Spheroids

Effets pharmacocinétique et pharmacodynamique de l’association d’everolimus et de sorafénib : l'impact des doses et des schémas d'administration sur la combinaison / Pharmacokinetics and Pharmacodynamics effects of Everolimus and Sorafenib combination : impact of doses and sequence of administration on the combination

El Madani, Mévidette

10 July 2017

Mon projet de thèse repose sur l'idée de l'optimisation du rapport bénéfice /risque (fonction d'utilité) des doses de traitements ciblés en oncologie en intégrant la notion de l'efficacité dans les essais de phase précoce plus que la toxicité. Ceci est réalisé par le choix d'un schéma d'administration/dose optimal en se basant sur la modélisation pharmacocinétique-pharmacodynamique (PK-PD). L'application pratique de ce concept fait l'objet de mon projet de thèse, qui se présente par un essai multiparamétrique de phase 1, dont l'objectif principal est d'évaluer la tolérance de l'association de deux agents anticancéreux, évérolimus et sorafenib, à différentes doses et selon différents schémas d'administration, chez des patients ayant un cancer solide métastatique. Dans ce contexte, un modèle mathématique, multi-échelle de translation destiné à quantifier les relations entre différentes doses, pharmacocinétique, pharmacodynamie des effets radiologiques et cliniques est développé pour explorer les intéractions PK-PD ; ce qui permettra ensuite de choisir le protocole d'administration optimal de cette association. Ceci demande une bonne maîtrise de l'approche de population, une méthodologie basée sur un modèle d'effet mixte non linéaire en utilisant le logiciel (NONMEM 7), qui sert à ajuster les modèles aux données ainsi que les analyses pharmacocinétiques des données / The development of everolimus and sorafenib combination was stopped by drug companies, due to the high toxicity index and the lack of a clear benefit/toxicity ratio to guide dose recommendations for a phase II trial.We designed the first multi-parameter phase I study (EVESOR), based on mathematical modeling of data provided from an adequately designed trial. We aimed to identify optimal doses and dosing schedules for the everolimus ands orafenib combination and maximize the simulated benefit/toxicity ratioThere is strong rationale to combine everolimus and sorafenib in treatment of solid tumor patients. Indeed these drugs block 2 important interacting signaling pathways involved in tumor growth: PI3K-AKT-mTor and RAS-RAF-ERK pathways. The determination of the best drug doses and dosing schedules of this combination is a challenge.The combination has been assessed in several phase 1 trials. Preliminary outcomes suggest promising efficacy but potential limiting toxicities such as hand foot syndrome and biological disorders. In these trials, the impact of administration sequences of one drug with respect to other one has not been assessed. Daily monotherapy regimens of both drugs were used. However sorafenib dosing schedule may impact on everolimus tumor delivery and thus on toxicity & efficacy. It should be possible to determine the optimized doses and dosing schedules of both drugs, which are able to maximize the benefit/toxicity ratio using modeling and simulation studies. Adequate data from a phase 1 trial designed with this objective are requiredMathematical modeling may be a promising tool for establishing the links between doses, dosing schedules, pharmacokinetics, pharmacodynamics, pharmacogenomics, radiological and clinical effects and for simulating the benefit/toxicity ratio induced by different doses and dosing schedules of drug combinations

Pharmacocinétique

Schémas d'administration

Dose

Sorafenib

Everolimus

Pharmacokinetics

Sequence of administration

Dose

Sorafenib

Everolimus

615

Etude des altérations moléculaires et évaluation de nouvelles thérapies ciblées dans les cancers du sein triple-négatifs / Molecular alterations analysis and evaluation of new targeted thérapies in triple negative breast cancers

Hatem, Rana

26 November 2015

Parmi les sous-types moléculaires de cancers du sein, le cancer du sein triple-négatif (TNBC) est caractérisé par un très mauvais pronostic et ne bénéficie actuellement d’aucune thérapie ciblée efficace. Dans ce projet, nous avons analysé le profil de certaines altérations oncogéniques dans les tumeurs TNBC et évalué le potentiel thérapeutique de leur ciblage à l’aide des modèles de xénogreffes (PDX).Nous avons d'abord démontré que le récepteur à activité tyrosine kinase RET est surexprimé dans une sous-population de tumeurs du sein TN et HER2+. Le ciblage de RET par son inhibiteur Vandetanib a été testé in vivo dans trois modèles de PDX TNBC et un modèle de PDX HER2+ caractérisés par des niveaux différents d’expression de RET et d’EGFR (les cibles principales du Vandetanib). Le Vandetanib a induit une régression tumorale dans les trois modèles de PDX surexprimant RET ou EGFR. L’effet du Vandetanib a été associé à une inhibition de la voie MAPK, une inhibition de l'angiogenèse et une induction de la nécrose.Nous avons également étudié les altérations de la voie PI3K/AKT/mTOR dans une large série de PDX de cancers du sein incluant des PDX TNBC. La voie PI3K/AKT/mTOR a été trouvée activée dans le cancer du sein triple-négatif. L’altération principalement retrouvée dans cette voie est la perte des deux suppresseurs de la voie, PTEN et/ou INPP4B. Sept des quinze modèles de PDX triple-négatifs testés ont montré une réponse à l’Everolimus. L'analyse des tumeurs traitées a montré que la phosphorylation post-traitement d’AKT est significativement plus fréquente dans les modèles répondeurs par rapport aux non-répondeurs. En conclusion, mon travail de thèse a permis de montrer que le Vandetanib et l'Everolimus pourraient être efficaces pour traiter le cancer du sein triple-négatif. Des études complémentaires sont nécessaires pour valider les biomarqueurs prédictifs de réponse à ces deux thérapies ciblées. / Among breast cancer subtypes, Triple-negative breast cancer (TNBC) has a very poor prognosis. There are currently no known targeted therapies for this subgroup of patients. In this project, we analyzed the profile of certain oncogenic alterations in the TN tumors and evaluated in vivo the therapeutic potential of targeting these alterations in TNBC.We first demonstrated that the tyrosine kinase receptor RET is overexpressed in a subset of TN and HER2+ tumors. Targeting RET by his inhibitor Vandetanib was tested in vivo in three PDX models of TNBC and one model of HER2+ BC with different expression levels of RET and EGFR. Vandetanib induced tumor regression in the three PDX models with high expression of RET or EGFR. Vandetanib effect was associated with inhibition of MAPK pathway, inhibition of angiogenesis and induction of necrosis. PI3K pathway alterations were investigated in an important number of BC PDX including TNBC PDX. PI3K pathway was shown to be activated in TNBC PDX possibly by the loss of the two pathway suppressors, PTEN and/or INPP4B. Treatment by Everolimus induced response in seven among the fifteen TNBC PDX tested. Analysis of treated tumors showed that post-treatment phosphorylation of AKT was more pronounced in responder PDX. The combination of Everolimus with chemotherapy was tested in one PDX and resulted in increased efficacy.In conclusion, in this work we showed that Vandetanib and Everolimus could be effective in treating TNBC. Further investigations are still needed to validate response related biomarkers.

Cancer du sein triple-Négatif

Everolimus

Vandetanib

Pdx

Triple-Negative breast cancer

Everolimus

Vandetanib

Pdx

Untersuchungen zur Aufklärung der adversen Effekte von HES auf Zellen (HK-2) des proximalen Nierentubulus / Studies to elucidate the adverse effects of HES on cells (HK-2) of the proximal renal tubule

Stein, Florian

January 2022

In der Volumentherapie galt das Kolloid Hydroxyethylstärke (HES) lange Zeit als ideale Infusionslösung und war der in Deutschland am häufigsten eingesetzte Plasmaexpander. In den letzten Jahren mehrten sich jedoch die Hinweise, dass HES insbesondere bei kritisch Kranken zu einer akuten Nierenfunktionsverschlechterung beitragen könnte, welche das klinische Ergebnis wesentlich beeinflusst. Der genaue Pathomechanismus ist bis heute nicht geklärt. Bekannt ist, dass sich HES nach intravenöser Applikation in vielen verschiedenen Geweben ablagert, wobei eine renale Anreicherung bevorzugt in proximalen Tubuluszellen stattfindet. Histopathologisch finden sich große Mengen intrazellulärer Vesikel im Zytoplasma, welche zu einer Zellschwellung führen, die auch als osmotische Nephrose bezeichnet und als prinzipiell reversibel erachtet wird. Der zelluläre Abbau soll dabei im Allgemeinen über das lysosomale System stattfinden. Dieses ist fester Bestandteil der Autophagie, welche ein evolutionär in allen Eukaryonten konservierter stress-induzierter kataboler Prozess ist, der der zellulären Homöostase und energieeffizienten Selbstreinigung dient. Hierbei werden defekte Makromoleküle durch Lysosomen in ihre Grundbestandteile zerlegt und der Zelle als Bausteine wieder zur Verfügung gestellt. In dieser Arbeit wurde in einem ersten Schritt der Einfluss von HES der 3. Generation auf die Viabilität von HK-2-Zellen mit zwei unabhängigen in vitro Assays überprüft. Diese beruhen auf einem Substratumsatz durch zytosolische bzw. mitochondriale Dehydrogenasen. Für beide Assays konnte zu verschiedenen Inkubationszeitpunkten bis 21 Stunden jeweils eine konzentrationsabhängige Viabilitätsreduktion durch HES festgestellt werden, welche auch nach einer „Regenerationsphase“ noch verringert nachweisbar und somit partiell reversibel war. Im nächsten Schritt wurde die Hypothese überprüft, ob eine medikamentöse Induktion der Autophagie die beobachtete Viabilitätsreduktion abschwächen oder sogar aufheben kann. Hierbei wurde analog zu einer Arbeit von Liu et al. (2014) eine Inkubationszeit von insgesamt acht Stunden gewählt, da nach diesem Zeitraum eine perinukleäre Cluster-Bildung der Lysosomen beobachtet werden konnte, welche für eine erhöhte Autophagierate spricht. Es kamen im Folgenden HES-Lösungen von 0,75% zum Einsatz, da diese aufgrund einer Viabilitätsreduktion um zirka ein Drittel als am besten geeignet betrachtet wurden. Der Autophagieinduktor Everolimus zeigte hierbei in dem auf mitochondrialen Dehydrogenasen basierenden EZ4U-Assay eine fast vollständige Aufhebung der HES-vermittelten Viabilitätsreduktion. Dieser Effekt konnte durch den MAP-Kinase-Kinase-Blocker U0126 aufgehoben werden. Andere Autophagiemodulatoren hingegen bewirkten zumeist nur geringe Änderungen der Zellviabilität. Zuletzt wurde auf Proteinebene untersucht, ob zentrale Moleküle bzw. Komplexe der Autophagie unter HES zum einen im zeitlichen Verlauf und zum anderen unter zusätzlichem Einfluss der Modulatoren eine Expressionsänderung aufwiesen. HES alleine bewirkte im zeitlichen Verlauf weitestgehend keine signifikante Expressionsänderung. Auch im Vergleich zu einer 0%-HES-Kontrolllösung konnten keine relevanten Unterschiede festgestellt werden. Die Koinkubation mit Everolimus führte zu einer erhöhten Expression der Quotienten ppERK/pERK und LC3BII/LC3BI, U0126 konnte dies jeweils weitestgehend wieder aufheben. Perifosin bewirkte ebenso wie 3-Methyladenin eine verringerte Expression von Akt, Chloroquin führte zu keiner signifikanten Expressionsänderung aller bestimmter Proteine. Darüber hinaus verursachten alle Modulatoren keine signifikante Expressionsänderung des zentralen Autophagiekomplexes Beclin1 sowie von LAMP2 und SQSTM1. Insgesamt sprechen die Ergebnisse dieser Arbeit gegen eine allgemeine, direkte Beeinflussung von klassischer Autophagie durch HES. Der Autophagieinduktor Everolimus zeigte jedoch einen protektiven Effekt auf die Zellviabilität, welcher vermutlich über einen Autophagie-vermittelten Weg verursacht wird. Unsere Arbeitsgruppe konnte darüber hinaus eine HES-vermittelte Reduktion von ROS beobachten. Das Autophagienetzwerk ist eng mit der zellulären Redox-Homöostase verknüpft. Eine verminderte ROS-Bildung könnte zu einer verminderten Autophagierate und somit auch verringerten Zellviabilität führen, welche durch Everolimus kompensiert wird. Bisher ungeklärt ist auch, auf welchem Weg HES in die Zelle aufgenommen wird. Denkbar wäre, dass größere HES-Moleküle via Endozytose in die Zelle gelangen. Hierbei ist der mTORC1-Komplex ein wichtiger Regulator, der durch Everolimus gehemmt wird und somit über eine verringerte HES-Aufnahme zu einer Viabilitätssteigerung führen könnte. Kleinere HES-Moleküle dagegen könnten über Glukose-Transporter aufgenommen werden, die möglicherweise über AMPK reguliert werden. / In volume therapy, the colloid hydroxyethyl starch (HES) was long considered the ideal infusion solution and was the most commonly used plasma expander in Germany. In recent years, however, there has been increasing evidence that HES may contribute to acute renal function deterioration, particularly in critically ill patients, which significantly affects clinical outcome. The exact pathomechanism has not been elucidated to date. What is known is that HES is deposited in many different tissues after intravenous administration, with renal accumulation occurring preferentially in proximal tubule cells. Histopathologically, large amounts of intracellular vesicles are found in the cytoplasm, leading to cell swelling, also known as osmotic nephrosis, which is considered reversible in principle. Cellular degradation is generally thought to occur via the lysosomal system. This is an integral part of autophagy, which is an evolutionarily conserved stress-induced catabolic process in all eukaryotes that serves cellular homeostasis and energy-efficient self-purification. In this process, defective macromolecules are broken down into their basic components by lysosomes and made available again to the cell as building blocks. In this work, as a first step, the influence of 3rd generation HES on the viability of HK-2 cells was tested using two independent in vitro assays. These are based on substrate turnover by cytosolic and mitochondrial dehydrogenases, respectively. For both assays, a concentration-dependent viability reduction by HES was detected at different incubation times up to 21 hours, which was still detectable in a reduced manner after a "regeneration phase" and thus partially reversible. In the next step, the hypothesis was tested whether a drug induction of autophagy could attenuate or even reverse the observed viability reduction. Here, analogous to a work by Liu et al. (2014), an incubation period of eight hours in total was chosen, since after this period a perinuclear cluster formation of the lysosomes could be observed, which speaks for an increased autophagy rate. In the following, HES solutions of 0.75% were used, as these were considered most suitable due to a viability reduction of about one third. The autophagy inducer everolimus showed an almost complete abolition of the HES-mediated viability reduction in the mitochondrial dehydrogenase-based EZ4U assay. This effect could be abolished by the MAP kinase kinase blocker U0126. In contrast, other autophagy modulators mostly caused only minor changes in cell viability. Finally, we investigated at the protein level whether central molecules or complexes of autophagy showed a change in expression under HES on the one hand in the time course and on the other hand under the additional influence of the modulators. HES alone largely did not cause a significant change in expression over time. Also in comparison to a 0%-HES control solution no relevant differences could be detected. Coincubation with everolimus increased the expression of ppERK/pERK and LC3BII/LC3BI ratios, and U0126 largely reversed this in each case. Perifosine caused decreased expression of Akt, as did 3-methyladenine, and chloroquine caused no significant change in expression of all specific proteins. In addition, all modulators did not cause a significant change in expression of the central autophagy complex Beclin1, as well as LAMP2 and SQSTM1. Overall, the results of this work argue against a general direct effect of HES on classical autophagy. However, the autophagy inducer everolimus showed a protective effect on cell viability, which is presumably caused by an autophagy-mediated pathway. Furthermore, our research group was able to observe a HES-mediated reduction of ROS. The autophagy network is closely linked to cellular redox homeostasis. Decreased ROS formation could lead to decreased autophagy rate and thus decreased cell viability, which is compensated by everolimus. The pathway by which HES is taken up into the cell has also not yet been clarified. It is conceivable that larger HES molecules enter the cell via endocytosis. Here, the mTORC1 complex is an important regulator that is inhibited by everolimus and could thus lead to an increase in viability via reduced HES uptake. Smaller HES molecules, on the other hand, could be taken up via glucose transporters, which are possibly regulated via AMPK.

Hydroxyethylstärke

Autophagie <Physiologie>

Everolimus

Nierenversagen

ddc:610

Clinical Pharmacokinetics of the Novel Combination of BEZ235, PI3K/mTOR Inhibitor, and Everolimus, mTOR Inhibitor: Phase I Clinical Studies and Non-clinical Mechanistic Assessment

Moorthy, Ganesh

11 September 2015

No description available.

Pharmaceuticals

pharmacokinetics

Phase I

PBPK

DDI

BEZ235

Everolimus

Nouvelles molécules thérapeutiques en développement pour les tumeurs neuroendocrines d'origine gastroentéropencréatiques et hypophysaires : preuves de concept in vitro / New therapy in gastroenteropancreatic neuroendocrine cells and pituitary adenomas : Proof of concept in vitro

Mohamed, Amerh Amira

05 November 2013

Les GEPNETs (tumeurs neuroendocrines gastroentéropancréatiques), représentent le deuxième cancer digestif. L’octréotide (agoniste Sst2) contrôle efficacement leurs sécrétions et plus modérément la croissance cellulaire. Au cours de ma première partie de thèse, j’ai développé la culture primaire de GEPNETs humaines. Ceci m’a permis d’étudier l’effet antiprolifératif et antisécretoire du pasireotide (pan agoniste Sst) et de l’évérolimus (inhibiteur de la voie pi3 kinase Akt) en comparaison avec l’octréotide. J’ai mis en évidence un effet inhibiteur significatif et similaire de l’octréotide et du pasiréotide sur la viabilité cellulaire et la sécrétion de chromogranine A. Cependant, le trafic intracellulaire du Sst2 est diffèrent en présence de pasireotide. L’évérolimus inhibe la viabilité et la secretion cellulaire des GEPNETs de manière similaire aux SSA. Nous n’avons pas retrouvé d’additivité entre l’évérolimus et les SSA. Dans la deuxième partie de mon travail j'ai étudié l’effet de la surexpression du Sst2 dans les cellules de prolactinomes et NFPA humains. Apres surexpression de Sst2, l’octréotide est capable d’inhiber la sécrétion de PRL et la prolifération cellulaire des NFPAs. Cette surexpression n’améliore pas la sensibilité aux dopastatines (agonistes chimériques Sst2-D2DR) des prolactinomes alors qu’une amélioration est bien observée dans les NFPAs. En conclusion, la culture primaire des GEPNETs représente un bon modèle d’étude pharmacologique. La coopération Sst2–D2DR dans les NFPA est effective dans ce modèle et permettra l’étude des mécanismes mises en jeu par les dopastatines. / GEPNETs represent, in terms of prevalence, the second digestive cancer. Octreotide (Sst2 agonists) effectively control their secretion and partially cell growth. we developed a primary cell culture of human GEPNETs. Cell culture allowed the study of antisecretory and antiproliferative effect of pasireotide and everolimus, alone or in combination, as compared to octreotide, in 20 tumors. We highlighted a significant and similar maximal inhibitory effect of octreotide and Pasireotide either on cell viability or on chromogranin A secretion in all analyzed tumors. However, the intracellular trafficking of Sst2 was strikely different in the presence of pasireotide and octreotide. In all analyzed tumors, everolimus inhibits cell viability and secretion of GEPNETs similarly to SSA. We couldn’t reveal any additivity between everolimus and SSA in cell viability suppression.My second goal was to study the effect of overexpression of Sst2 by adenoviral transfer in cells of human prolactinomas and NFPA. In both cell types. Nevertheless, octreotide efficiently suppressed PRL secretion and cell proliferation (NFPA). Overexpression of Sst2 did not improve the efficcacy of dopastatines (chimeric Sst2 - D2DR agonists) on prolactin secretion in prolactinomas, but clealy improved suppression of cell proliferation in NFPA. These results suggest that dopostatin promotes a Sst2 D2DR cooperation in NFPA, but not in prolactinomas, where DRDR activation remains dominant. In conclusion, GEPNETs primary cell culture represents a good model for pharmacological In pituitary adenomas, Sst2 overexpression opens an interesting perspective for gene therapy in recurrent NFPA after surgery.

Endocrinologie

Tumeurs neuroendocrine

Adenomes hypophysaires

Recepteur à la somatostatine

Pasireotide

Everolimus,

Endocrinology

Pituitary adenomas

Neuroendocrine tumors

Somatostatin receptor

Pasireotide

Everolimus

Estudo piloto do impacto da terapia antiproliferativa com everolimus administrado por via oral na diminuição de reestenose após implante de stent auto-expansível de nitinol para tratamento de lesões oclusivas da artéria femoral superficial / Pilot study of the impact of antiproliferative therapy with everolimus administered orally in the reduction of restenosis after implantation of selfexpandable nitinol stent for treatment of occlusive lesions of the superficial femoral artery

Carrillo, Luis Ramon Virgen

15 June 2009

INTRODUÇÃO: A implantação de stent auto-expansível de nitinol para o tratamento das lesões oclusivas femoro-poplíteas tem sido associado com maus resultados a longo prazo. O everolimus administrado via oral para inibir reestenoses do stent foi investigado recentemente em animais com bons resultados, porém sua segurança e eficácia não têm sido estudada em seres humanos. O propósito deste estudo piloto foi avaliar o impacto da terapia antiproliferativa com everolimus administrado via oral por 28 dias na diminuição de reestenose após implante de stent auto-expansível de nitinol para tratamento de lesões oclusivas da artéria femoral superficial. MÉTODOS E RESULTADOS: Trinta e quatro pacientes foram recrutados para este estudo randomizado, prospectivo. O grupo que recebeu everolimus via oral foi constituído por 15 pacientes e o grupo que não recebeu medicação composto por 19 pacientes. As características basais e do procedimento foram similares entre os dois grupos. Todos os pacientes tinham isquemia crônica do membro inferior e oclusão da artéria femoral superficial (média da lesão de 83,14 mm no grupo sem medicação e 105 mm no grupo everolimus). O objetivo primário do estudo foi a redução da porcentagem média do diâmetro da reestenose intra-stent após seis meses da angioplastia avaliada por angiografia quantitativa. A porcentagem média do diâmetro das reestenoses foi 46,9% no grupo tratado com everolimus e 44,5% no grupo que não recebeu a medicação (p=0,81). Não foram observados efeitos colaterais graves nos grupos. No acompanhamento clínico aos 24 meses não houve diferenças significativas entre os grupos em relação a eventos clínicos. A patência primária, primária assistida e secundária em 24 meses, foi 42%, 74% e 79% no grupo sem medicação e 27%, 73% e 73% no grupo tratado com everolimus. CONCLUSÃO: O everolimus via oral por 28 dias em doses altas é seguro e bem tolerado, com baixo índice de efeitos colaterais, porém não é eficaz na redução da porcentagem média do diâmetro da reestenose intra-stent em pacientes com implante de stents auto-expansíveis de nitinol nas lesões oclusivas complexas da artéria femoral superficial. / INTRODUCTION: The implantation of a self-expanding of nitinol stent in the treatment of femoropopliteal occlusive lesions has been associated with a poor outcome in a long term setting. Everolimus administered orally to inhibit restenosis of the stent was investigated recently in animals with good results, but its safety and efficacy has not been studied in humans. The purpose of this pilot study was to evaluate the impact of antiproliferative therapy with everolimus administered orally for 28 days in the reduction of restenosis after implantation of self-expandable nitinol stent for treatment of occlusive lesions of the superficial femoral artery. METHODS AND RESULTS: Thirty-four patients were recruited for this randomized, prospective study. The group that received oral Everolimus was consisted of 15 patients and the group that received no medication was 19 patients. The baseline characteristics and procedure were similar in both groups. All the patients had chronic lower limb ischemia and occlusion of the superficial femoral artery (mean of the lesion of 83.14 mm in the group without medication and 105 mm in the everolimus group). The primary objective of the study was to evaluate the reduction of the average percentage of the diameter of in-stent restenosis six months after angioplasty assessed by quantitative angiography. The in-stent mean percent diameter stenosis was 46.9% in the group treated with everolimus and 44.5% in the group that received no medication (p = 0.81). There were no serious side effects seen in either group in the clinical follow up at 24 months. There was no significant difference between groups in relation to clinical events. The primary patency, assisted primary and secondary in 24 months was 42%, 74% and 79% in the group without medication and 27%, 73% and 73% in the group treated with Everolimus. CONCLUSION: Everolimus administered orally for 28 consecutive days to stent implantation in high doses proves to be safe and well tolerated, with low rate of side effects, but it is not effective in reducing the average percentage of diameter of in-stent restenosis in patients with implantation of self-expandable nitinol stent in complex occlusive lesions of the superficial femoral artery.

Angiografia

Angiography

Artéria femoral/patologia

Everolimus/therapeutic use

Everolimus/uso terapêutico

Extremidade inferior

Femoral artery/pathology

Implante de prótese vascular/métodos

Ischemia

Isquemia

Lower extremity

Einfluss von unterschiedlichen immunsuppressiven Strategien auf Proliferation, Stoffwechsel und Differenzierung humaner fetaler neuraler Progenitorzellen in vitro

Glien, Anja

26 February 2015

The influence of immunosuppressive drugs on neural stem/progenitor cell fate in vitro.

neurale Progenitorzellen

Transplantation

Immunsupressiva

Mycophenolat

Cyclosporin A

Everolimus

Prednisolon

Neural progenitor cells

Human

Immunosuppressive drugs

Transplantation

Mycophenolate

Cyclosporine A

Everolimus

Prednisolone

ddc:610

Therapeutisches Drug Monitoring von Immunsuppressiva: Vergleich intrazellulärer Konzentrationsmessungen mit Messungen in Vollblut / Therapeutic drug monitoring of immunosuppressants: Comparison of intracellular concentration with concentration in whole blood

Bräuer, Marie-Luise

12 November 2018

No description available.

610

Therapeutisches Drug Monitoring

Immunsuppression

Ciclosporin

Tacrolimus

Everolimus

intrazellulär

Vollblut

Transplantation

Leber

therapeutic drug monitoring

immunosuppression

cyclosporine

tacrolimus

everolimus

intracellular

whole blood

transplantation

liver

Medizin (PPN619874732)