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来那度胺作为一种新型治疗药物,用于治疗 von Willebrand 病的胃肠道血管扩张症。

Lenalidomide as a novel therapy for gastrointestinal angiodysplasia in von Willebrand disease.

机构信息

Georgetown University, Washington, DC, USA.

Medstar Washington Hospital Center, Washington, DC, USA.

出版信息

Haemophilia. 2018 Mar;24(2):278-282. doi: 10.1111/hae.13419. Epub 2018 Feb 15.

DOI:10.1111/hae.13419
PMID:29446520
Abstract

INTRODUCTION

Lenalidomide is a thalidomide analog with anti-angiogenic properties. Previous case reports suggest its efficacy in preventing gastrointestinal bleeding (GIB) secondary to angiodysplasia (AD) in hereditary haemorrhagic telangiectasia and potentially in reversing AD. We present the first case series to explore lenalidomide as a treatment for AD-related GIB in patients with von Willebrand disease (VWD).

METHODS

A retrospective chart review was conducted to include patients with VWD, who were evaluated from 2010 to 2013 and who had received lenalidomide to treat recurrent GIB secondary to AD. All patients had failed single-agent use of antifibrinolytic agents. Patients were observed for at least 2 years on therapy.

RESULTS

Five patients (3 males; 68.2 ± 4.9 years) with VWD (3 with type 3 and 1 each with types 1 and 2a) and AD were found. Sites of AD included the stomach, duodenum, jejunum and colon. Lenalidomide was started at 5 mg oral daily. Uptitration to 10 and 15 mg in 1 patient each was necessary due to recurrence of GIB. The mean number of endoscopies performed for control of GIB post lenalidomide was significantly lower compared to pretherapy (0.25 vs 5.50; P = .001). Mean bleed-free duration on lenalidomide was 12.6 ± 4.7 months. Three patients have reported no GIB on lenalidomide.

CONCLUSION

This case series demonstrates significantly reduced number of endoscopies and increased bleed-free duration with lenalidomide treatment in selected patients with VWD and recurrent GIB from AD. Prospective multicenter trials are needed to further define the role of lenalidomide in the management of GIB from angiodysplasia and VWD.

摘要

简介

来那度胺是一种具有抗血管生成特性的沙利度胺类似物。先前的病例报告表明,它在预防遗传性出血性毛细血管扩张症(HHT)中血管发育不良(AD)引起的胃肠道出血(GIB)方面具有疗效,并且可能具有逆转 AD 的作用。我们报告了首例病例系列研究,以探讨来那度胺在血管发育不良相关 GIB 患者中的作用,这些患者患有血管性血友病(VWD)。

方法

对 2010 年至 2013 年接受来那度胺治疗 AD 相关 GIB 反复发作的 VWD 患者进行回顾性图表审查。所有患者均曾单一使用抗纤维蛋白溶解剂治疗失败。在治疗期间至少观察患者 2 年。

结果

发现 5 例 VWD(3 例男性;68.2±4.9 岁)患者合并 AD。AD 的部位包括胃、十二指肠、空肠和结肠。来那度胺起始剂量为 5mg 口服,每日 1 次。由于 GIB 复发,1 例患者增加至 10mg,1 例患者增加至 15mg。与治疗前相比,来那度胺治疗后用于控制 GIB 的内镜检查次数明显减少(0.25 次 vs 5.50 次;P=0.001)。来那度胺无出血时间的平均长度为 12.6±4.7 个月。3 例患者报告来那度胺无 GIB。

结论

本病例系列研究表明,在患有 VWD 和 AD 引起的复发性 GIB 的选定患者中,来那度胺治疗可明显减少内镜检查次数并延长无出血时间。需要进行前瞻性多中心试验,以进一步确定来那度胺在 AD 和 VWD 引起的 GIB 管理中的作用。

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