Eribulin induces irreversible mitotic blockade: implications of cell-based pharmacodynamics for in vivo efficacy under intermittent dosing conditions.

Towle MJ; Salvato KA; Wels BF; Aalfs KK; Zheng W; Seletsky BM; Zhu X; Lewis BM; Kishi Y; Yu MJ; Littlefield BA

首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >Eribulin induces irreversible mitotic blockade: implications of cell-based pharmacodynamics for in vivo efficacy under intermittent dosing conditions.

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Eribulin induces irreversible mitotic blockade: implications of cell-based pharmacodynamics for in vivo efficacy under intermittent dosing conditions.

机译：依瑞布林诱导不可逆的有丝分裂阻滞：在间歇给药条件下，基于细胞的药效学对体内功效的影响。

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Eribulin (E7389), a mechanistically unique microtubule inhibitor in phase III clinical trials for cancer, exhibits superior efficacy in vivo relative to the more potent compound ER-076349, a fact not explained by different pharmacokinetic properties. A cell-based pharmacodynamic explanation was suggested by observations that mitotic blockade induced by eribulin, but not ER-076349, is irreversible as measured by a flow cytometric mitotic block reversibility assay employing full dose/response treatment. Cell viability 5 days after drug washout established relationships between mitotic block reversibility and long-term cell survival. Similar results occurred in U937, Jurkat, HL-60, and HeLa cells, ruling out cell type-specific effects. Studies with other tubulin agents suggest that mitotic block reversibility is a quantifiable, compound-specific characteristic of antimitotic agents in general. Bcl-2 phosphorylation patterns parallel eribulin and ER-076349 mitotic block reversibility patterns, suggesting persistent Bcl-2 phosphorylation contributes to long-term cell-viability loss after eribulin's irreversible blockade. Drug uptake and washout/retention studies show that [3H]eribulin accumulates to lower intracellular levels than [3H]ER-076349, yet is retained longer and at higher levels. Similar findings occurred with irreversible vincristine and reversible vinblastine, pointing to persistent cellular retention as a component of irreversibility. Our results suggest that eribulin's in vivo superiority derives from its ability to induce irreversible mitotic blockade, which appears related to persistent drug retention and sustained Bcl-2 phosphorylation. More broadly, our results suggest that compound-specific reversibility characteristics of antimitotic agents contribute to interactions between cell-based pharmacodynamics and in vivo pharmacokinetics that define antitumor efficacy under intermittent dosing conditions.

机译：Eribulin（E7389）是一项在癌症的III期临床试验中机制独特的微管抑制剂，相对于更有效的化合物ER-076349，其在体内具有优越的疗效，这一事实并未用不同的药代动力学特性加以解释。观察结果提示，以细胞为基础的药效学解释表明，如采用全剂量/反应治疗的流式细胞术有丝分裂阻滞可逆性试验所测量，由埃布林而非ER-076349诱导的有丝分裂阻滞是不可逆的。药物冲洗后5天的细胞生存能力建立了有丝分裂阻滞可逆性与长期细胞存活之间的关系。在U937，Jurkat，HL-60和HeLa细胞中也发生了类似的结果，排除了细胞类型特异性作用。对其他微管蛋白药物的研究表明，有丝分裂阻滞可逆性通常是抗有丝分裂药物的可量化的，化合物特异性的特征。 Bcl-2磷酸化模式与eribulin和ER-076349有丝分裂阻滞可逆性模式平行，表明持久性Bcl-2磷酸化有助于在eribulin不可逆转的阻断后长期丧失细胞生存力。药物吸收和清除/保留研究表明，[3H] eribulin的累积细胞内水平低于[3H] ER-076349，但保留时间更长，水平更高。不可逆的长春新碱和可逆的长春碱也有类似的发现，表明持续的细胞滞留是不可逆性的组成部分。我们的结果表明，eribulin在体内的优越性源于其诱导不可逆的有丝分裂阻滞的能力，这似乎与持久的药物保留和持续的Bcl-2磷酸化有关。更广泛地说，我们的结果表明抗有丝分裂剂的化合物特异性可逆性特征有助于确定间歇给药条件下基于细胞的药效学和体内药代动力学之间的相互作用，从而定义抗肿瘤功效。

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《Cancer research: The official organ of the American Association for Cancer Research, Inc》 |2011年第2期|共10页
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Towle MJ; Salvato KA; Wels BF; Aalfs KK; Zheng W; Seletsky BM; Zhu X; Lewis BM; Kishi Y; Yu MJ; Littlefield BA;
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1. Eribulin induces irreversible mitotic blockade: implications of cell-based pharmacodynamics for in vivo efficacy under intermittent dosing conditions. [J] . Towle MJ, Salvato KA, Wels BF, Cancer research: The official organ of the American Association for Cancer Research, Inc . 2011,第2期

机译：依瑞布林诱导不可逆的有丝分裂阻滞：在间歇给药条件下，基于细胞的药效学对体内功效的影响。
2. Pharmacodynamics of omalizumab: implications for optimised dosing strategies and clinical efficacy in the treatment of allergic asthma. [J] . Hochhaus G, Brookman L, Fox H, Current medical research and opinion . 2003,第6期

机译：omalizumab的药效学：对优化剂量策略和治疗过敏性哮喘的临床疗效的意义。
3. In Vivo Efficacy of Continuous Infusion versus Intermittent Dosing of Linezolid Compared to Vancomycin in a Methicillin-Resistant Staphylococcus aureus Rabbit Endocarditis Model. [J] . Jacqueline C, Batard E, Perez L, Antimicrobial agents and chemotherapy. . 2002,第12期

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4. Pharmacodynamic Modelling of Drug-Induced Ventilatory Depression and Automatic Drug Dosing in Conscious Sedation [C] . Zanderigo, Eleonora, Caruso, Engineering in Medicine and Biology Society, 2006 Annual International Conference of the IEEE . 2006

机译：药物引起的通气抑制和自觉镇静的自动给药的药效学模型
5. Exposure to fluorescent excitation light induces dose-dependent, irreversible force relaxation in living fibroblast cells [D] . Knoll, Samantha Grace. 2016

机译：暴露于荧光激发光引起活性成纤维细胞中的剂量依赖性，不可逆的力松弛
6. In Vivo Efficacy of Continuous Infusion versus Intermittent Dosing of Linezolid Compared to Vancomycin in a Methicillin-Resistant Staphylococcus aureus Rabbit Endocarditis Model [O] . Cédric Jacqueline, Eric Batard, Lucia Perez, 2002

机译：在耐甲氧西林的金黄色葡萄球菌兔心内膜炎模型中连续输注与间断给药利奈唑胺与万古霉素相比的体内疗效
7. Eribulin Induces Irreversible Mitotic Blockade: Implications of Cell-Based Pharmacodynamics for In vivo Efficacy under Intermittent Dosing Conditions [O] . Murray J. Towle, Kathleen A. Salvato, Bruce F. Wels, 2010

机译：Eribulin诱导不可逆的有丝分裂性封锁：在间歇给药条件下，细胞基药效学的影响在体内疗效

Eribulin induces irreversible mitotic blockade: implications of cell-based pharmacodynamics for in vivo efficacy under intermittent dosing conditions.

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