lenvatinib对小鼠急性血管和心脏的影响。

IF 3.2 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS

Cardio-oncology Pub Date : 2025-02-11 DOI:10.1186/s40959-025-00307-8

Dustin N Krüger, Patrizia Pannucci, Callan D Wesley, Cedric H G Neutel, Wim Martinet, Guido R Y De Meyer, Stephen J Hill, Jeanette Woolard, Constantijn Franssen, Pieter-Jan Guns

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引用次数: 0

摘要

背景：靶向血管内皮生长因子（VEGF）受体信号的酪氨酸激酶抑制剂（TKIs）被用于癌症治疗以抑制血管生成。不幸的是，已知VEGF抑制剂会诱发患者严重的高血压。本研究旨在阐明TKI lenvatinib在短期小鼠模型中对血压、动脉硬度、血管反应性以及心功能的影响，以揭示与VEGF抑制相关的心血管（CV）毒性的潜在因素。方法：雄性C57BL/6J小鼠随机分为2组，分别给予lenvatinib 4 mg/kg/d和40%羟丙基β-环糊精治疗4 d。在另一项研究中，小鼠接受为期4天的治疗，然后进行为期4天的冲洗，在第2天和第7天进行超声心动图和血压测量。随后测定了胸主动脉段的离体血管反应性。结果：Lenvatinib从治疗第2天开始诱导高血压和动脉僵硬（即脉波速度增加）。此外，治疗后左心室射血分数降低，心室扩张。Lenvatinib既没有诱导内皮功能障碍，也没有损害血管平滑肌细胞对一氧化氮（NO）的反应性。有趣的是，lenvatinib显示了atp介导的松弛的浓度依赖性增加。此外，在4天的洗脱期后，lenvatinib治疗小鼠的高血压没有完全缓解。然而，动脉僵硬，atp介导的松弛和心脏适应恢复。结论：这项全面的研究为VEGF抑制、血管功能和心脏结局之间的相互作用提供了有价值的见解，强调需要细致的理解和进一步探索lenvatinib对心血管系统的不同影响。此外，该研究提出了VEGF和ATP之间的协同形成，表明通过P2Yx受体信号传导增强了反应。

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Acute vascular and cardiac effects of lenvatinib in mice.

Background: Tyrosine kinase inhibitors (TKIs) targeting vascular endothelial growth factor (VEGF) receptor signalling are used in cancer therapy to inhibit angiogenesis. Unfortunately, VEGF inhibitors are known to induce severe hypertension in patients. This study aimed to elucidate the impact of the TKI lenvatinib on blood pressure, arterial stiffness, vascular reactivity, as well as cardiac function in a short-term murine model to shed light on potential contributors to cardiovascular (CV) toxicities associated with VEGF inhibition.

Methods: Male C57BL/6J mice were randomly divided into 2 cohorts, either treated for 4 days with lenvatinib 4 mg/kg/day or 40% hydroxypropyl β-cyclodextrin as control. In an additional study, mice were subjected to a 4-day treatment followed by a 4-day wash-out, with echocardiography and blood pressure measurements performed on day 2 and 7. Subsequently, ex vivo vascular reactivity of thoracic aortic segments was determined.

Results: Lenvatinib induced hypertension and arterial stiffness (i.e., increased pulse wave velocity), starting from day 2 of treatment. Further, left ventricular ejection fraction was reduced and the ventricle dilated upon treatment. Lenvatinib induced neither endothelial dysfunction nor impaired vascular smooth muscle cell reactivity to nitric oxide (NO). Interestingly, lenvatinib demonstrated a concentration-dependent increase in ATP-mediated relaxation. In addition, after the 4-day wash-out period, lenvatinib-treated mice did not show complete remission of hypertension. However, arterial stiffness, ATP-mediated relaxation and cardiac adaptation were recovered.

Conclusion: This comprehensive investigation provides valuable insights into the interplay between VEGF inhibition, vascular function and cardiac outcomes, emphasising the need for nuanced understanding and further exploration of the differential effects of lenvatinib on the CV system. Additionally, the study proposes a synergistic formation between VEGF and ATP, indicating an enhanced response via P2Yx receptor signalling.

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来源期刊

Cardio-oncology Medicine-Cardiology and Cardiovascular Medicine

CiteScore

5.00

自引率

3.00%

发文量

审稿时长

7 weeks