Phase I/II Study of Volasertib (BI 6727), an Intravenous Polo-Like Kinase (Plk) Inhibitor, in Patients with Acute Myeloid Leukemia (AML): Results From the Randomized Phase II Part for Volasertib in Combination with Low-Dose Cytarabine (LDAC) Versus LDAC Monotherapy in Patients with Previously Untreated AML Ineligible for Intensive Treatment

Maertens, Johan; Lübbert, Michael; Fiedler, Walter; Fouillard, L; Haaland, Alf Kristian; Brandwein, Joseph; Leprêtre, Stéphane; Turlure, Pascal; Bug, Gesine; Müller‐Tidow, Carsten; Krämer, Alwin; Voß, Florian; Taube, Tillmann; Fritsch, Holger; Döhner, Hartmut

doi:10.1182/blood.v120.21.411.411

Cited by 13 publications

(9 citation statements)

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“…Blocking of Plk1 activity with small molecule inhibitors such as Bl 2536 and volasertib produced regressions in multiple preclinical adult cancer models . Volasertib has entered clinical evaluation and has advanced to phase 2 testing .…”

Section: Introductionmentioning

confidence: 99%

Initial testing (stage 1) of the polo‐like kinase inhibitor volasertib (BI 6727), by the Pediatric Preclinical Testing Program

Görlick

Kolb

Keir

et al. 2013

Pediatric Blood & Cancer

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Background Volasertib (BI 6727) is a potent inhibitor of Polo-like kinase 1 (Plk1), that is overexpressed in several childhood cancers and cell lines. Because of its novel mechanism of action, volasertib was evaluated through the PPTP. Procedures Volasertib was tested against the PPTP in vitro cell line panel at concentrations from 0.1 nM to 1.0 μM and against the PPTP in vivo xenograft panels administered I.V at a dose of 30 mg/kg (solid tumors) or 15 mg/kg (ALL models) using a q7dx3 schedule. Results In vitro volasertib demonstrated cytotoxic activity, with a median relative IC50 value of 14.1 nM, (range 6.0 nM to 135 nM). Volasertib induced significant differences in EFS in 19 of 32 (59%) of the evaluable solid tumor xenografts and in 2 of 4 (50%) of the evaluable ALL xenografts. Volasertib induced tumor growth inhibition meeting criteria for intermediate EFS T/C (>2) activity in 11 of 30 (37%) evaluable solid tumor xenografts, including neuroblastoma (4 of 6) and glioblastoma (2 of 3) panels, and 2 of 4 ALL models. Objective responses (CR’s) were observed for 4 of 32 solid tumor (2 neuroblastoma, 1 glioblastoma, and 1 rhabdomyosarcoma) and 1 of 4 ALL xenografts. Conclusions Volasertib shows potent in vitro activity against the PPTP cell lines with no histotype selectivity. In vivo, volasertib induced regressions in several xenograft models. However, pharmacokinetic data suggest that mice tolerate higher systemic exposure to volasertib than humans, suggesting that the current results may over-estimate potential clinical efficacy against the childhood cancers studied.

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Section: Introductionmentioning

confidence: 99%

Initial testing (stage 1) of the polo‐like kinase inhibitor volasertib (BI 6727), by the Pediatric Preclinical Testing Program

Görlick

Kolb

Keir

et al. 2013

Pediatric Blood & Cancer

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“…Response was seen in 31% of patients (13 of 42) treated with the combination versus 13% of patients (6 of 45) treated with LDAC alone (p ϭ 0.0523), and overall survival was 8.0 months with the combination versus 5.2 months with LDAC alone (p ϭ 0.0996). 71 These results led to Breakthrough Therapy designation by the FDA and initiation of POLO-AML-2, a phase III randomized trial of the same regimens in patients with AML who are aged 65 or older and ineligible for intensive therapy.…”

Section: Kinase Inhibitorsmentioning

confidence: 99%

Novel Therapies in AML: Reason for Hope or Just Hype?

Larkin

Blum

2014

American Society of Clinical Oncology Educational Book

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We have entered the genomic sequencing era in the treatment of acute myeloid leukemia (AML); our patients increasingly and justifiably demand personalized treatment based on aberrations of their own leukemia. Except in rare cases we are not yet able to provide truly personalized therapy, so the question of "hope or hype?" posed by the American Society for Clinical Oncology (ASCO) for this educational topic is quite timely. The answer based solely on advances in genomic sequencing is "both". There is an element of expectation among the public that we are "almost there" in solving the genetic cancer puzzle, an expectation indeed based on hype. However, there is no question that ultimate success lies in understanding the genetic underpinnings of disease. When decades of research in molecular biology and immunology are combined with transformative advances in cancer genetics, the answer is undeniably that our patients finally have reason for hope. Here, we review selected novel therapies for AML in areas such as immunotherapeutics, epigenetics, kinase inhibition/pathway inhibition, and the marrow microenvironment.

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“…Currently, at least six unique PLK1 inhibitors have reached phase I or II clinical trails for various cancers, and BI-6727 (volasertib) was recently designated a "breakthrough therapy" by the FDA in the treatment of acute myeloid leukemia after raising complete remission rates 3-fold for patients enrolled in a phase II trial. (64)(65)(66)(67) However, without detailed mechanistic studies, it is difficult to know if the clinical success of these targets is attributable, even in part, to mitotic disruption. As these therapies demonstrate clinical success, it will be important to expand them into cancers with documented KT-MT attachment defects.…”

Section: Repurposing Current Therapies To Target Kt-mt Attachmentsmentioning

confidence: 99%

Pediatric Glioblastoma Therapies Based on Patient-Derived Stem Cell Resources

Paddison¹

2014

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Cited by 13 publications

References 0 publications

Initial testing (stage 1) of the polo‐like kinase inhibitor volasertib (BI 6727), by the Pediatric Preclinical Testing Program

Initial testing (stage 1) of the polo‐like kinase inhibitor volasertib (BI 6727), by the Pediatric Preclinical Testing Program

Novel Therapies in AML: Reason for Hope or Just Hype?

Pediatric Glioblastoma Therapies Based on Patient-Derived Stem Cell Resources

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