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从剂量强度角度看甲状腺癌患者接受仑伐替尼治疗时早期血压控制的重要性。

The importance of early-stage blood pressure control in thyroid cancer patients treated with lenvatinib from the perspective of dose intensity.

机构信息

Department of Surgery, Ito Hospital, 4-3-6 Jingumae, Shibuya-ku, Tokyo, 150-8308, Japan.

Pharmaceutical Division, Department of Medical Technique, Ito Hospital, 4-3-6 Jingumae, Shibuya-ku, Tokyo, 150-8308, Japan.

出版信息

Support Care Cancer. 2023 Nov 29;31(12):729. doi: 10.1007/s00520-023-08163-x.

Abstract

PURPOSE

Lenvatinib (LEN) is a multikinase inhibitor that strongly inhibits tyrosine kinase receptors, especially VEGFR-2, which can cause hypertension, as well as strong tumor shrinkage. Though control of any side effects (SEs) is important for maintaining dose intensity (DI), hypertension is particularly important, because blood pressure (BP) can change quickly and respond to LEN administration and withdrawal, and it can be controlled with antihypertensive medications. Focusing on the early phase of treatment, the effect of BP 8 weeks after LEN initiation (BP) on DI at 8 weeks (DI) was investigated.

METHODS

The subjects were 85 thyroid cancer patients who started LEN at 24 mg/day and continued for ≥8 weeks. The BP at the start of LEN (BP), BP grade, and DI were examined.

RESULTS

Median (range) systolic BP changed significantly from BP of 117 (84-167) mmHg to BP of 134 (103-168) mmHg (p<0.001). Antihypertensive treatment at baseline, systolic BP, and male sex were related to higher DI on multivariate analysis. The median DI of the 23 patients who required dose modification due to hypertension was 20.2 mg/day (n=6) in grade 1, 15.8 mg/day (n=13) in grade 2, and 14.5 mg/day (n=4) in grade 3, showing a trend toward lower DI as the grade level increased.

CONCLUSION

LEN can increase BP by 20 mmHg at 8 weeks even with intensive antihypertensive management. Baseline antihypertensive treatment and BP can affect DI. A higher DI may be achieved by aiming for a low 8-week BP with more intensive antihypertensive therapy after LEN initiation.

摘要

目的

仑伐替尼(LEN)是一种多激酶抑制剂,强烈抑制酪氨酸激酶受体,特别是 VEGFR-2,这可能导致高血压,以及强烈的肿瘤缩小。尽管控制任何副作用(SEs)对于维持剂量强度(DI)很重要,但高血压尤其重要,因为血压(BP)会迅速变化,并对 LEN 给药和停药作出反应,并且可以用降压药物来控制。关注治疗的早期阶段,研究了 LEN 起始后 8 周(BP)的 BP 对 8 周时 DI(DI)的影响。

方法

该研究对象为 85 名甲状腺癌患者,他们开始服用 24mg/天的 LEN,并持续服用至少 8 周。检查了 LEN 起始时的 BP(BP)、BP 等级和 DI。

结果

中位(范围)收缩压从 117(84-167)mmHg 显著变化至 134(103-168)mmHg(p<0.001)。基线时的降压治疗、收缩压和男性是多变量分析中与更高 DI 相关的因素。由于高血压需要剂量调整的 23 名患者的中位 DI 为 1 级时 20.2mg/天(n=6),2 级时 15.8mg/天(n=13),3 级时 14.5mg/天(n=4),随着等级水平的升高,DI 呈下降趋势。

结论

即使进行强化降压治疗,LEN 也可能在 8 周时使 BP 升高 20mmHg。基线降压治疗和 BP 会影响 DI。通过在 LEN 起始后进行更强化的降压治疗,以实现较低的 8 周 BP,可能会获得更高的 DI。

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