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舒尼替尼治疗恶性副神经节瘤/嗜铬细胞瘤的理论依据和证据

Rationale and evidence for sunitinib in the treatment of malignant paraganglioma/pheochromocytoma.

作者信息

Joshua Anthony M, Ezzat Shereen, Asa Sylvia L, Evans Andrew, Broom Reuben, Freeman Marc, Knox Jennifer J

机构信息

Department of Medical Oncology, Princess Margaret Hospital, University Health Network, 610 University Avenue, M5G 2M9 Toronto, Ontario, Canada.

出版信息

J Clin Endocrinol Metab. 2009 Jan;94(1):5-9. doi: 10.1210/jc.2008-1836. Epub 2008 Nov 11.

Abstract

CONTEXT

Paragangliomas are tumors that develop from extraadrenal chromaffin cells. Approximately 20% of paragangliomas are malignant, and surgical resection is considered the primary treatment when possible. The optimal systemic treatment for advanced disease is undefined, due in part to lack of effective agents. Here we report our experience suggesting that sunitinib is an effective agent in this malignancy.

SETTING AND PATIENTS

Three patients with metastatic paraganglioma were treated with sunitinib at the Princess Margaret Hospital. Limited analyses of tumor tissue and germline DNA were available.

INTERVENTION

Sunitinib at a standard dose (50 mg daily, 4 wk on, 2 wk off) was titrated to patient tolerance.

RESULTS

One patient has achieved a near complete response, and two patients demonstrated partial responses. Two patients demonstrated germline defects suggesting a pseudo-hypoxic drive to the tumor whereas the third demonstrated immunohistochemical evidence of this phenomenon.

CONCLUSIONS

Sunitinib appears to be an active agent in this malignancy based on this limited cohort, with an understandable mechanism of action similar to that described in other hypoxia-driven tumors. A single arm phase 2 trial is underway.

摘要

背景

副神经节瘤是起源于肾上腺外嗜铬细胞的肿瘤。约20%的副神经节瘤为恶性,可能的情况下手术切除被视为主要治疗方法。由于缺乏有效药物,晚期疾病的最佳全身治疗方法尚不明确。在此我们报告我们的经验,提示舒尼替尼在这种恶性肿瘤中是一种有效药物。

研究背景与患者

三名转移性副神经节瘤患者在玛嘉烈公主医院接受舒尼替尼治疗。可获得对肿瘤组织和种系DNA的有限分析结果。

干预措施

将舒尼替尼的标准剂量(每日50毫克,服用4周,停药2周)根据患者耐受性进行调整。

结果

一名患者实现了近乎完全缓解,两名患者表现出部分缓解。两名患者表现出种系缺陷,提示肿瘤存在假低氧驱动,而第三名患者表现出该现象的免疫组化证据。

结论

基于这一有限队列,舒尼替尼在这种恶性肿瘤中似乎是一种有效药物,其作用机制与其他低氧驱动肿瘤中所描述的机制相似,易于理解。一项单臂2期试验正在进行中。

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