Entwicklung der Vaskularisierung und des Fasergehaltes im Knochenmark von CML-Patienten während der Behandlung mit Imatinib

Redwitz, Mathias

08 December 2011

Entwicklung der Vaskularisierung und des Fasergehaltes im Knochenmark von CML-Patienten während der Behandlung mit Imatinib Gesteigerte Gefäßneubildung und retikuläre Fibrose sind zwei morphologische Veränderungen im Knochenmark von CML-Patienten, welche mit einem schlechteren Krankheitsverlauf assoziiert sind. Imatinib, ein selektiver Tyrosinkinaseinhibitor, hemmt die angiogenen und fibrogenen Substanzen VEGF und PDGF. Diese Dissertation untersuchte den Einfluss von Imatinib auf die Vaskularisierung und den retikulären Fasergehalt im Knochenmark von Patienten mit chronischer myeloischer Leukämie (CML). Es wurden 67 repräsentative Knochenmarkbiopsien von insgesamt 19 Patienten, behandelt in Multicenter-Studien an der Universitätsklinik Leipzig, eingeschlossen. Davon waren zehn Patienten bereits mit IFN-α + Cytarabin vorbehandelt worden. Neun Patienten mit neudiagnostizierter CML erhielten Imatinib als Ersttherapie. Knochenmarkbiopsien zu den Zeitpunkten t0 (vor Therapiebeginn), t1 (6-15 Monate) und t2 (21-36 Monate) nach Behandlungsstart mit Imatinib wurden untersucht. Weiter wurde eine Kontrollgruppe aus 19 KM-Biopsien gebildet, welche ohne pathologischen Befund waren. Während der Behandlung mit Imatinib kam es bei der Mehrzahl der Patienten zu einer Normalisierung der Gefäßdichte im Knochenmark. Der Fasergehalt im Knochenmark der CML-Patienten sank bei allen Patienten auf Normwerte ab. Dies zeigt den positiven Einfluss von Imatinib auf die morphologischen Veränderungen Vaskularisierung und Faserdichte im Knochenmark von CML-Patienten. Ein Einfluss der Vorbehandlung mit IFN-α + Cytarabin auf die Dynamik der morphologischen Parameter während der Behandlung mit Imatinib war nicht nachweisbar.

info:eu-repo/classification/ddc/610

ddc:610

Enhancing Cardiomyocyte Survival in Drug Induced Cardiac Injury

Maharsy, Wael

11 October 2012

Cardiotoxicity associated with many cancer drugs is a critical issue facing physicians these days and a huge hurdle that must be overcome for a side effects-free cancer therapy. Survival of cardiac myocytes is compromised upon the exposure to certain chemotherapeutic drugs. Unfortunately, the mechanisms implicated in cardiac toxicity and the pathways governing myocyte survival are poorly understood. The following thesis addresses the mechanisms underlying the cardiotoxicity of two anticancer drugs, doxorubicin (DOX) and Imatinib mesylate (Gleevec). Transcription factor GATA-4, has recently emerged as an indispensable factor in the adult heart adaptive response and cardiomyocyte survival. Therefore, the specific aim of this project was to determine the role of GATA-4, its upstream regulators, as well as partners in survival. A combination of cell and molecular techniques done on in vivo, and ex vivo models were utilized to tackle these issues. In this study, we confirmed the cardiotoxicity of the anticancer drug, Imatinib mesylate and found to be age dependent. GATA-4, already known to be implicated in DOX-induced toxicity, was confirmed as an Imatinib target. At the molecular level, we identified IGF-1 and AKT as upstream regulators of GATA-4. Moreover, we confirmed ZFP260 (PEX-1), a key regulator of the cardiac hypertrophic response, as a GATA-4 collaborator in common prosurvival pathways. Collectively, these results provide new insights on the mechanisms underlying drug-induced cardiotoxicity and raise the exciting possibility that cancer drugs are negatively affecting the same prosurvival pathway(s), in which GATA-4 is a critical component. Therapeutic interventions aimed at enhancing GATA-4 activity may be interesting to consider in the context of treatments with anticancer drugs.

Heart

Heart Failure

Cancer

Cardiomyopathy

Cardiotoxicity

Anticancer drugs

Doxorubicin

Imatinib

Haemopoiesis, leukaemia & imatinib: c-fms, a novel target for small molecule inhibitor therapy.

Dewar, Andrea L.

January 2004

Understanding the factors that regulate the growth and differentiation of haemopoietic stem cells (HSC) remains a major challenge. In this study, the proliferation and differentiation of CD34+ cells from normal donors and chronic myeloid leukaemia (CML) patients was compared. The proliferation and entry of CML cells into the cell cycle was decreased relative to cells from normal donors, and greater heterogeneity in the phenotype of CML cells at the initiation of culture was observed. Analysis of phenotype concomitant with cell division also demonstrated that the differentiation of normal CD34+ cells was consistent between donors, while marked variability was observed in the differentiation of CD34+ cells from CML patients. This included expression of CD13, CD33, CD38 and HLA-DR, which were linked to cell division in normal but not CML cells. The tyrosine kinase inhibitor, imatinib, is a novel drug displaying promising results in the treatment of CML by specifically inhibiting the growth of leukaemic cells. To examine whether myelosuppression observed in patients treated with imatinib may arise from inhibition of normal haemopoiesis, imatinib was added to colony assays established using cells from normal bone marrow. Suppression of monocyte/macrophage growth, but not that of eosinophils or neutrophils, was observed at therapeutic concentrations of imatinib. Inhibition of monocytic differentiation to macrophages was also observed and was associated with decreased functional capacity such as altered antigen uptake, production of proinflammatory cytokines and stimulation of responder cells. The specific suppression of monocyte/macrophage differentiation and function was not due to blockade of tyrosine kinases known to be inhibited by imatinib and was consistent with an inhibition of the M-CSF/c-fms signalling pathway. This hypothesis was tested using a cell line that was dependent on M-CSF for growth and survival. Cell proliferation and phosphorylation of c-fms were inhibited at an IC50 of 1.9μM and 1.4μM imatinib respectively and this was not attributable to decreased c-fms expression. These important findings therefore identify c-fms as a further target of imatinib, and suggest that imatinib should be considered for treatment of diseases where c-fms is implicated. This includes breast and ovarian cancer and inflammatory conditions such as rheumatoid arthritis. Potential side effects resulting from imatinib treatment must also be considered. / Thesis (Ph.D.)--School of Medicine, 2004.

Enhancing Cardiomyocyte Survival in Drug Induced Cardiac Injury

Maharsy, Wael

11 October 2012

Cardiotoxicity associated with many cancer drugs is a critical issue facing physicians these days and a huge hurdle that must be overcome for a side effects-free cancer therapy. Survival of cardiac myocytes is compromised upon the exposure to certain chemotherapeutic drugs. Unfortunately, the mechanisms implicated in cardiac toxicity and the pathways governing myocyte survival are poorly understood. The following thesis addresses the mechanisms underlying the cardiotoxicity of two anticancer drugs, doxorubicin (DOX) and Imatinib mesylate (Gleevec). Transcription factor GATA-4, has recently emerged as an indispensable factor in the adult heart adaptive response and cardiomyocyte survival. Therefore, the specific aim of this project was to determine the role of GATA-4, its upstream regulators, as well as partners in survival. A combination of cell and molecular techniques done on in vivo, and ex vivo models were utilized to tackle these issues. In this study, we confirmed the cardiotoxicity of the anticancer drug, Imatinib mesylate and found to be age dependent. GATA-4, already known to be implicated in DOX-induced toxicity, was confirmed as an Imatinib target. At the molecular level, we identified IGF-1 and AKT as upstream regulators of GATA-4. Moreover, we confirmed ZFP260 (PEX-1), a key regulator of the cardiac hypertrophic response, as a GATA-4 collaborator in common prosurvival pathways. Collectively, these results provide new insights on the mechanisms underlying drug-induced cardiotoxicity and raise the exciting possibility that cancer drugs are negatively affecting the same prosurvival pathway(s), in which GATA-4 is a critical component. Therapeutic interventions aimed at enhancing GATA-4 activity may be interesting to consider in the context of treatments with anticancer drugs.

Heart

Heart Failure

Cancer

Cardiomyopathy

Cardiotoxicity

Anticancer drugs

Doxorubicin

Imatinib

Long-term Changes in Alveolarization in the Postnatal Rat Following Transient Inhibition of Early "Classical" Alveologenesis

Lau, Mandy

06 April 2010

Rationale: Activation of the platelet-derived growth factor receptors-α and -β (PDGF-Rα and -Rβ) is critical in the formation of secondary crests/septa during alveologenesis, and its regulation has been found to be disrupted in rat lung injury models. Objective: To determine whether the process of secondary septation can occur after transient pharmacologic inhibition of PDGF-R action during postnatal days (P)1 – 7 in rats. Hypothesis: The initial process of secondary crest formation is time-limited and, if missed, will result in a permanent loss of alveoli. Methods: Imatinib mesylate, a PDGF-R inhibitor, was injected intraperitoneally from P1 – 7. Pups were sacrificed on P2, 4, 8, 14, 28 and 65 for studies of alveolar development. Main results: The injection of imatinib inhibited PDGF-R action, resulting in a permanent decrease in alveolar number in treated rats. Conclusions: Inhibition of secondary septation during the first 7 days of life resulted in a decrease in alveolar number lasting into early adult life. This is consistent with a critical time window for secondary septation, which, if disrupted, results in long-term adverse effects on lung development.

alveolarization

lung development

alveologenesis

secondary crests

septation

imatinib

0719

0433

Long-term Changes in Alveolarization in the Postnatal Rat Following Transient Inhibition of Early "Classical" Alveologenesis

Lau, Mandy

06 April 2010

Rationale: Activation of the platelet-derived growth factor receptors-α and -β (PDGF-Rα and -Rβ) is critical in the formation of secondary crests/septa during alveologenesis, and its regulation has been found to be disrupted in rat lung injury models. Objective: To determine whether the process of secondary septation can occur after transient pharmacologic inhibition of PDGF-R action during postnatal days (P)1 – 7 in rats. Hypothesis: The initial process of secondary crest formation is time-limited and, if missed, will result in a permanent loss of alveoli. Methods: Imatinib mesylate, a PDGF-R inhibitor, was injected intraperitoneally from P1 – 7. Pups were sacrificed on P2, 4, 8, 14, 28 and 65 for studies of alveolar development. Main results: The injection of imatinib inhibited PDGF-R action, resulting in a permanent decrease in alveolar number in treated rats. Conclusions: Inhibition of secondary septation during the first 7 days of life resulted in a decrease in alveolar number lasting into early adult life. This is consistent with a critical time window for secondary septation, which, if disrupted, results in long-term adverse effects on lung development.

alveolarization

lung development

alveologenesis

secondary crests

septation

imatinib

0719

0433

Imatinib as a Dominant Therapeutic Strategy in the Treatment of Chronic Myelogenous Leukemia: A Decision-Analytic Approach

Ballard, Erin Elissa

January 2004

Class of 2004 Abstract / Objective: To develop and populate a decision-analytic model comparing the cost and efficacy of imatinib versus allogenic bone marrow transplantation (BMT) with a matched unrelated donor in the treatment of newly-diagnosed, Philadelphia positive (Ph (+)), chronic phase, chronic myelogenous leukemia (CML). Design: Markov cohort analysis and Monte Carlo microsimulation. Measurements and Main Results: Direct medical costs were measured from the perspective of a third-party payer. Efficacy data and probabilities were obtained from survivability findings emanating primarily from randomized controlled trials (RCTs). A two-year time horizon was employed with three month treatment cycles. BMT was established as the baseline comparator and the base case was defined as a 35 year old, Ph(+) male patient with newly-diagnosed CML. Results from the Monte Carlo trial found that the incremental cost-efficacy ratio was −$5,000 for imatinib (95th % Confidence Interval: −$70,000, $84,000). Analysis of the cost-efficacy plane indicated that imatinib dominated BMT in 84.69 percent of cases, while BMT was dominant in 0.76 percent of cases. Sensitivity analyses of costs and discount rates found results to be robust. Conclusion: Imatinib was observed in a majority of cases to be both less costly and more efficacious relative to BMT in the treatment of CML, suggesting that this pharmaceutical agent is a dominant therapeutic strategy. When available, the incorporation of long-term clinical data are required to assess cost-efficacy beyond the two-year time horizon of this study.

Chronic Myelogenous Leukemia

Imatinib

Bone Marrow Transplants (BMT)

Cost Effectiveness

Enhancing Cardiomyocyte Survival in Drug Induced Cardiac Injury

Maharsy, Wael

January 2012

Cardiotoxicity associated with many cancer drugs is a critical issue facing physicians these days and a huge hurdle that must be overcome for a side effects-free cancer therapy. Survival of cardiac myocytes is compromised upon the exposure to certain chemotherapeutic drugs. Unfortunately, the mechanisms implicated in cardiac toxicity and the pathways governing myocyte survival are poorly understood. The following thesis addresses the mechanisms underlying the cardiotoxicity of two anticancer drugs, doxorubicin (DOX) and Imatinib mesylate (Gleevec). Transcription factor GATA-4, has recently emerged as an indispensable factor in the adult heart adaptive response and cardiomyocyte survival. Therefore, the specific aim of this project was to determine the role of GATA-4, its upstream regulators, as well as partners in survival. A combination of cell and molecular techniques done on in vivo, and ex vivo models were utilized to tackle these issues. In this study, we confirmed the cardiotoxicity of the anticancer drug, Imatinib mesylate and found to be age dependent. GATA-4, already known to be implicated in DOX-induced toxicity, was confirmed as an Imatinib target. At the molecular level, we identified IGF-1 and AKT as upstream regulators of GATA-4. Moreover, we confirmed ZFP260 (PEX-1), a key regulator of the cardiac hypertrophic response, as a GATA-4 collaborator in common prosurvival pathways. Collectively, these results provide new insights on the mechanisms underlying drug-induced cardiotoxicity and raise the exciting possibility that cancer drugs are negatively affecting the same prosurvival pathway(s), in which GATA-4 is a critical component. Therapeutic interventions aimed at enhancing GATA-4 activity may be interesting to consider in the context of treatments with anticancer drugs.

Heart

Heart Failure

Cancer

Cardiomyopathy

Cardiotoxicity

Anticancer drugs

Doxorubicin

Imatinib

STAT3 Contributes to Resistance Towards BCR-ABL Inhibitors in a Bone Marrow Microenvironment Model of Drug Resistance in Chronic Myeloid Leukemia Cells

Bewry, Nadine N

02 December 2009

Imatinib mesylate (imatinib) represents a potent molecularly targeted therapy against the oncogenic tyrosine kinase, BCR-ABL. Although imatinib has shown considerable efficacy against chronic myeloid leukemia (CML), displaying high rates of complete hematological and complete cytogenetic responses, treatment with imatinib is not curative and overtime advanced-stage CML patients often become refractory to further treatment. Acquired resistance to imatinib has been associated with mutations within the kinase domain of BCR-ABL, BCR-ABL gene amplification, leukemic stem cell quiescence as well as over-expression of the multidrug resistance (MDR1) gene. However, in vitro resistance models often fail to consider the role of the tumor microenvironment in the emergence of the imatinib-resistant phenotype. The bone marrow is the predominant microenvironment of CML and is a rich source of both soluble factors and extracellular matrixes, which may influence drug response. To address the influence of the bone marrow microenvironment on imatinib sensitivity, we utilized an in vitro co-culture bone marrow stroma model. Using a transwell system, we demonstrated that soluble factors secreted by the human bone marrow stroma cell line, HS-5, were sufficient to cause resistance to apoptosis induced by imatinib in CML cell lines. We subsequently determined that culturing CML cells in HS-5-derived conditioned media (CM) inhibits apoptosis induced by imatinib and other second generation BCR-ABL inhibitors. These data suggest that more potent BCR-ABL inhibitors will not overcome resistance associated with the bone marrow microenvironment. Additionally, we determined that CM increases the clonogenic survival of CML cells following treatment with imatinib. HS-5 cells are reported to express several cytokines and growth factors known to activate signal transducer and activator of transcription 3 (STAT3). Given its crucial role in the survival of hematopoietic cells, we asked whether, 1) CM derived from HS-5 cells can activate STAT3 in CML cells and 2) does activation of STAT3 confer resistance to BCR-ABL inhibitors. We demonstrated that exposure of the CML cell lines, K562 and KU812, to CM caused an increase in phospho-Tyr STAT3, while no increases in phospho-Tyr STAT5 were noted. Moreover, resistance was associated with increased levels of the STAT3 target genes, Bcl-xl, Mcl-1 and survivin. Furthermore, reducing STAT3 levels with siRNA sensitized K562 cells cultured in CM to imatinib-induced cell death (p<0.05, Student’s t-test). Importantly, STAT3 dependency was specific for cells grown in CM, as reducing STAT3 levels in regular growth conditions had no effect on imatinib sensitivity. Together, these data support a novel mechanism of BCR-ABL-independent imatinib resistance and provide preclinical rationale for using STAT3 inhibitors to increase the efficacy of imatinib within the context of the bone marrow microenvironment.

imatinib

nilotinib

dasatinib

STAT5

hematopoiesis

cytokines

American Studies

Arts and Humanities

Auswirkungen einer Langzeitexposition mit den Tyrosinkinase-Inhibitoren Imatinib, Dasatinib und Bosutinib auf das Skelett und weitere Organsysteme im neu etablierten Tiermodell der juvenilen Ratte

Tauer, Josephine Tabea

24 July 2013

Hintergrund und Fragestellung: Seit der Zulassung des Tyrosinkinase-Inhibitors (TKI) Imatinib im Jahre 2001 hat sich die Therapie der chronisch myeloischen Leukämie (CML) grundlegend verändert. Imatinib inhibiert die konstitutiv aktive Tyrosinkinase BCR-ABL, welche die verstärkte Proliferation der leukämischen Zellen und die Entwicklung der CML bedingt. Das sehr gute klinische Ansprechen auf eine Imatinib-Behandlung resultierte in einer beschleunigten Zulassung dieses TKI auch bei pädiatrischen Patienten im Jahre 2003. Aufgrund von Punktmutationen und/oder strukturellen Änderungen innerhalb des BCR-ABL Fusionsproteins können sich Resistenzen gegenüber Imatinib entwickeln. Deshalb wurden Zweit- und Drittgenerations TKI wie Dasatinib und Bosutinib entwickelt. Imatinib wirkt nicht hoch spezifisch und hemmt neben BCR-ABL auch weitere Tyrosinkinasen, wie z.B. c-KIT, PDGF-R und c-FMS, welche am Knochenstoffwechsel beteiligt sind. Die Stimulation des Rezeptors c-FMS bewirkt die Differenzierung monozytärer Vorläuferzellen in knochenabbauende Osteoklasten. Zusätzlich unterliegt die Entwicklung der knochenaufbauenden Osteoblasten spezifischen Signalkaskaden an denen PDGF-R und c-Abl beteiligt sind. Als Nebenwirkung einer TKI-Therapie beeinträchtigt die Inhibition dieser Signaltransduktionswege somit das Knochen-“Remodelling“, indem die Entwicklung und funktionelle Aktivität von Osteoklasten reduziert wird. Gleichzeitig wird die Aktivität von Osteoblasten gestärkt, aber deren Proliferation inhibiert. Diese Dysbalance von Knochenaufbau und -abbau mit gestörter Kalziumhomöostase bedingt bei erwachsenen CML-Patienten veränderte endokrinologische Parameter des Kalziumhaushaltes, eine vermehrte Knochenmineralisation und eine erhöhte trabekuläre Knochendichte. Dagegen wurden bei pädiatrischen CML-Patienten unter Imatinib-Therapie Längenwachstumsstörungen beobachtet, welche bezüglich des Wirkmechanismuses von Imatinib auf den wachsenden Knochen bis heute noch nicht im Detail geklärt sind. Spekulativ ist auch, ob Zweit- und Drittgenerations-TKI ebenso wie Imatinib den Knochenstoffwechsel bei pädiatrischen Patienten stören. Angelehnt an ein erfolgreiches Applikationsschema bei erwachsenen CML-Patienten steht zusätzlich die Frage im Raum, ob eine intermittierende Gabe von TKIs (einen Monat Therapie, einen Monat Pause) eine Minderung der Nebenwirkung auf den Knochen bewirken könnte, ohne die Wirkung auf die CML-Behandlung zu beeinträchtigen. Vor diesem Hintergrund wurde ein Nagermodel etabliert, um Nebenwirkungen auf den Knochenstoffwechsel unter TKI-Exposition zu analysieren. Junge, wachsende Ratten wurden hierzu vom präpubertären Alter bis zur Adoleszenz kontinuierlich oder intermittierend mit den TKIs Imatinib, Dasatinib und Bosutinib exponiert und die Wirkung auf das wachsende Skelettsystem untersucht. Methoden: 4 Wochen alte männliche Wistar Ratten wurden über einen Zeitraum von 10 Wochen chronisch mit jeweils einem der drei im Trinkwasser gelösten TKIs exponiert. Neben einer unbehandelten Kontrollkohorte erhielt eine Gruppe jeweils eine Standarddosis und eine hohe Dosis (entsprechend der doppelten Standarddosis) des entsprechenden TKIs kontinuierlich. Eine weitere Gruppe erhielt die hohe Dosis intermittierend (an drei aufeinanderfolgenden Tagen TKI, danach vier Tage nur Wasser). Die Konzentrationen im Trinkwasser betrugen für Imatinib 1 mM und 2 mM und für Dasatinib und Bosutinib jeweils 50 µM und 100 µM. Nach zweiwöchiger (präpubertär), vierwöchiger (pubertäres Stadium) und zehnwöchiger Exposition (postpubertär) wurden die Tiere aller Gruppen nekropsiert und Röhrenknochen, Lendenwirbel und Blut asserviert. Zur Beurteilung des Knochenmetabolismus wurden folgende Parameter erhoben: Knochenlängen, Knochendichten mittels pQCT, trabekuläre Strukturen mittels µCT, Knochenfestigkeit mittels des 3-Punkt-Biege-Test und endokrinologische Parameter im Serum mittels ELISA. Zusätzlich wurde der jeweilige TKI Serum-Spiegel bestimmt. Ergebnisse: Die Gewichtsentwicklung, körperliche Entwicklung und das Sozialverhalten zeigten keine Unterschiede beim Vergleich von Kontrollkohorten mit exponierten Tieren. Die kontinuierliche Exposition mit Imatinib und Dasatinib bewirkte dosisabhängig eine Reduktion der Knochenlängen der Femura und der Tibiae. Bosutinib zeigte diesen Effekt nicht. Die intermittierende Exposition mit hoher Dosis resultierte in einer Knochenlängenreduktion, welche exakt dem Effekt der Standarddosis entsprach. Weiterhin resultierte aus der Exposition mit Imatinib oder Dasatinib eine Verminderung der trabekulären Knochendichten der Femura und Tibiae im präpubertären Stadium. Ratten, welche hoch dosiert Imatinib erhielten, zeigten diese Reduktion ebenfalls im pubertären Stadium, nicht jedoch unter Dasatinib- und Bosutinib-Exposition. Postpubertär unterschieden sich die trabekulären Dichten von Femura und Tibiae der exponierten Gruppen nicht von den Kontrollkohorten. Auf die kortikale Knochendichte und die kortikale Dicke dieser Röhrenknochen zeigte sich kein messbarer Effekt der TKI. Dennoch trat - nur nach Exposition der hohen Imatinibdosis - eine signifikant verminderte femorale Bruchfestigkeit postpubertär auf. Am Lendenwirbelkörper war pubertär und postpubertär die Höhe unter Imatinib-Exposition vermindert, während die Gesamt- und kortikale Knochendichte präpubertär erhöht war bei tendenziell erniedrigter trabekulärer Knochendichte. Die kortikale Dicke wurde durch alle TKI nicht beeinflusst. Dasatinib und Bosutinib bewirkten keinen Effekt auf die Wirbelhöhe, aber eine tendenzielle Minderung der trabekulären Knochendichte. Der serologisch erfassbare Knochenresorptionsmarker „tatrate resistant acidic phosphatase“ (TRAP) war unter kontinuierlicher Exposition mit hoher Dosis von Imatinib zu allen Zeitpunkten erniedrigt. Postpubertär zeigte sich dieser Effekt auch unter Standard- und Hochdosis von Bosutinib. Der Knochenformationsmarker Osteocalcin war unter Imatinib bei allen Kohorten zu allen Analysezeitpunkten erniedrigt, während Dasatinib und Bosutinib keinen Effekt auf diesen Parameter zeigten. Die erfassten Serum-Hormonparameter (Wachstumshormon, Parathormon) lagen unter der Exposition mit Imatinib als erhöhte Wachstumshormonspiegel pubertär und als verminderte Parathormonspiegel prä- und pubertär vor. Unter der Exposition mit Dasatinib kam es ebenfalls pubertär zu einer Erhöhung der Wachstumshormonspiegel und präpubertär zu einer tendenziellen Erhöhung der Parathormonspiegel. Postpubertär normalisierten sich beide Parameter unter der Exposition mit Imatinib und Dasatinib wieder. Unter Bosutinib konnte nur postpubertär erniedrigte Parathormonspiegel ermittelt werden. Eine intermittierende TKI-Exposition resultierte in einem Aufholwachstum und einer teilweise Normalisierung der knochenspezifischen Serumparameter. Als wichtige unerwartete Nebenwirkung zeigte sich unter Langzeitexposition mit Imatinib und Dasatinib eine Zunahme des Herzgewichtes. Unter Imatinib resultierten daraus keine klinischen Auffälligkeiten, während unter Dasatinib eine Herzinsuffizienz zum Tod eines Tieres führte. Bosutinib zeigte keine weiteren makropathologisch erfassbaren Nebenwirkungen. Bis heute sind keine kardialen Nebenwirkungen bei pädiatrischen Patienten nach mehrjähriger TKI-Therapie publiziert. Schlussfolgerung: Das etablierte juvenile Nagertiermodell ist gut geeignet, um die Nebenwirkungen einer Langzeitexposition von TKI auf den wachsenden Knochen zu erfassen. Bei Kindern und Adoleszenten klinisch beschriebene Wachstumsretardierungen unter Imatinib ließen sich zweifelsfrei bei Ratten verifizieren. Bei fehlenden klinischen Daten von Kindern zu Dasatinib präjudiziert das Modell, dass Dasatinib so wie Imatinib den gleichen, Bosutinib hingegen kaum einen Effekt auf den Knochen ausübt. Eine intermittierende Gabe der TKI scheint die Nebenwirkungen auf den Knochen abzumildern und könnte eine neue Möglichkeit der TKI-Therapie für pädiatrische Patienten darstellen. Aus dem Tiermodell der Langzeit-exponierten juvenilen Ratte lässt sich ableiten, dass beim wachsenden Kind unter jahrelanger TKI-Therapie klinisch sorgfältig der Knochenstoffwechsel und das Längenwachstum überwacht und unter Dasatinib zusätzlich kardiale Nebenwirkungen beachten werden sollten. / Background: Since its approval in 2001 the tyrosine kinase inhibitor (TKI) imatinib has revolutionized the therapy of chronic myeloid leukaemia (CML). Imatinib inhibits the constitutively active tyrosine kinase (TK) BCR-ABL causing the increased proliferation of the leukemic cells and the progress of CML. According to improved survival rates imatinib has been licensed as frontline therapy also for paediatric CML in 2003. However, due to point mutations or structural changes within the BCR-ABL fusion protein resistance to imatinib occurs. Therefore 2nd and 3rd generation TKI like dasatinib and bosutinib have been developed. Beside BCR-ABL, Imatinib exerts also off-target effects on further TKs like c-KIT, PDGF-R, c-FMS which are involved in bone metabolism. Stimulation of the receptor c-FMS leads to the differentiation of monocytic progenitors to bone resorbing osteoclasts. In addition, the development of bone forming osteoblasts underlies specific signalling cascades involving PDGF-R and c-Abl. As a side effect of TKI therapy these specific signalling cascades are inhibited impairing bone remodelling by reducing the development and functional activity of osteoclasts. Simultaneously osteoblasts’ differentiation is promoted while their proliferation is inhibited. This dysbalance of bone formation and resorption results in altered endocrinological serum markers of the calcium homeostasis, increased bone mineralization, and increased trabecular bone density in adult CML patients. In contrast paediatric CML patients show longitudinal growth retardations under imatinib therapy, however, the detailed action of imatinib on the growing bone is not clarified yet. Additionally, it is unclear if 2nd and 3rd generation TKI will also disturb bone metabolism in paediatric CML patients. Based on an effective treatment strategy in adult CML patients, it is also questioned if intermittent TKI treatment (one month “on”, one month “off”) could minimise side effects on the bone without impairing CML therapy. On this background a rodent model was established to study side effects of TKI treatment on bone metabolism. Juvenile growing rats where exposed from prepubertal age till adolescence continuously or intermittently to imatinib, dasatinib, and bosutinib and the effects on the growing skeleton were analysed. Methods: Four weeks old male Wistar rats were chronically exposed to varying concentrations of one of the three TKIs via the drinking water for 10 weeks. Besides untreated controls a standard dosage group and a high dosage group (equalling the twofold standard dose) received every TKI continuously, while an additional group received the high dosage TKI in an intermittent fashion (3 days per week: “on” TKI; 4 days water without TKI). The concentrations applied were 1 mM and 2 mM for imatinib and 50 µM and 100 µM each for dasatinib and bosutinib, respectively. After 2 weeks (prepubertal), 4 weeks (pubertal stage), and 10 weeks (postpubertal) of exposure, respectively, animals were sacrificed and long bones, lumbar vertebra and blood were isolated. To evaluate bone metabolism the following parameters were analysed: bone length, bone mineral density (BMD) by pQCT, trabecular structure by µCT, bone strength by 3-point bending test, and endocrinological parameters by ELISA. Additionally, serum levels of TKIs were investigated. Results: In comparison to controls no alterations of exposed animals’ bodyweight, overall development and social behaviour were observed. Continuous exposure of imatinib and dasatinib led dose dependently to reduced femoral and tibial length. No such effect was observed under bosutinib. Intermitted exposure of high-dose TKIs resulted in reduced effects on femoral and tibial length identical to the effect observed in groups receiving just standard dose. Furthermore, exposure of imatinib and dasatinib lowered femoral and tibial trabecular BMD prepubertally. Rats receiving high dose imatinib showed reduced femoral and tibial trabecular BMD at pubertal stage, while this effect was not observed under dasatinib and bosutinib exposure. Postpubertally, femoral and tibial trabecular BMD of all exposed groups did not differ from controls. Femoral and tibial cortical BMD and cortical thickness were not affected by TKI exposure. However, under high dose imatinib exposure femoral mechanical breaking strength was reduced postpubertally. In vertebra the height was reduced under imatinib exposure pubertally and postpubertally, while the total and cortical BMD were increased prepubertally and trabecular BMD tended to be reduced. Cortical thickness was not affected by any TKI tested. Dasatinib and bosutinib exhibited no effect on the height of the vertebra but trabecular BMD tended to be reduced. The serum bone resorption marker ‘tartrate resistant acidic phosphatase’ (TRAP) was found reduced under continuous exposure of high dose of imatinib at all time points tested. Postpubertally, the same effect was detected after standard and high dosage of bosutinib. The bone formation marker osteocalcin was reduced in all groups and at all time points tested under imatinib exposure, whereas no such effect was observed for dasatinib and bosutinib. Serum bone related hormone markers (growth hormone (GH) and parathyroid hormone (PTH)) revealed under imatinib exposure increased GH levels pubertally whereas PTH was reduced pre- und pubertally. During dasatinib exposure GH levels were elevated pubertally and PTH levels were increased prepubertally. Postpubertally, both parameters normalised again under imatinib and dasatinib exposure. During bosutinib exposure reduced PTH levels were detected postpubertally only. Intermitted TKI exposure resulted in catch-up growth and partial normalisation of bone specific serum parameters. As major unexpected side effect during exposure increasing heart weights could be observed under long-time imatinib and dasatinib exposure. No clinical changes were observed under imatinib, whereas dasatinib led to cardiac insufficiency leading to death of one animal. Bosutinib showed no additional macrospathologic assessable side effects. To date no cardiac side effects were published in paediatric patients under prolonged TKI therapy. Conclusion: The established juvenile rat model is appropriate to examine side effects of long-term TKI exposure on the growing bone. Published longitudinal growth retardation in children and adolescents under imatinib treatment could be unequivocally mimicked in this rat model. Due to not yet available clinical experience with dasatinib in paediatric patients, this model predicts that dasatinib alters bone metabolism like imatinib whereas bosutinib shows less detectable effects. Intermitted TKI treatment may reduce side effects on the growing bone and therefore could represent a new opportunity of TKI therapy for paediatric patients. Summing up, TKI long-term exposure in this juvenile rat model challenges physicians to diligently monitor bone metabolism in not outgrown paediatric patients during long-term TKI treatment and additionally assess cardiac side effects under dasatinib exposure.

Tyrosinkinase Inhibitor

Knochen

Imatinib

Dasatinib

Bosutinib

wachsend

tyrosine kinase inhibitor

bone

imatinib

dasatinib

bosutinib

growing

ddc:610

rvk:YC 2504