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ADH-1 治疗转移性肾上腺皮质癌——病例报告。

ADH-1 in the treatment of metastatic adrenocortical carcinoma--case report.

机构信息

The Ottawa Hospital Cancer Centre, Ottawa, ON, Canada.

出版信息

Anticancer Res. 2011 Nov;31(11):3921-5.

PMID:22110220
Abstract

Adrenocortical Carcinoma (ACC) is rare with an annual incidence of 0.5-2 cases per million worldwide. Some ACC tumors over express N-cadherin, which correlates with metastatic potential. ADH-1 (Exherin™) is a competitive inhibitor of N-cadherin, resulting in rapid onset of tumor vascular angiolysis and apoptosis in preclinical models. Targeting N-cadherin may cause direct anti-tumor and anti-vascular effects. We report a case of ACC with benefit from ADH-1 therapy. A 24 year old woman with an N-cadherin expressing metastatic ACC was treated on a phase I trial and treated with ADH-1 subsequently received additional doses through a special access program. The patient presented with cushingoid features from cortisol over-secretion and was diagnosed with metastatic ACC in January 2003. Tumor progression followed treatment with a combination of doxorubicin, cisplatin and mitotane. In October 2003, as a part of a phase I clinical trial she was treated with as a single dose of ADH-1 at 150 mg/m(2). This resulted in transient normalization of cortisol, tumor necrosis on CT imaging, and reduction in tumor perfusion on DCE-MRI. Following progression on several additional lines of chemotherapy, she was again treated with ADH-1 under a Special Access Program (SAP). After 33 weekly doses (22 with 150 mg/m(2) and 11 with 300 mg/m(2)) radiographic tumor progression was demonstrated and treatment discontinued. She survived 40 months with metastatic disease, dying 12 months after her last dose of ADH-1. This observation merits consideration for prospectively evaluating the efficacy of ADH-1 in patients with cortisol secreting ACC that over express N-cadherin.

摘要

肾上腺皮质癌 (ACC) 发病率较低,全球范围内每年每百万人中有 0.5-2 例。一些 ACC 肿瘤过度表达 N-钙黏蛋白,这与转移潜能相关。ADH-1(Exherin™)是 N-钙黏蛋白的竞争性抑制剂,可导致临床前模型中肿瘤血管迅速发生血管溶解和凋亡。靶向 N-钙黏蛋白可能会产生直接的抗肿瘤和抗血管作用。我们报告了一例接受 ADH-1 治疗获益的 ACC 病例。一名 24 岁的女性患有表达 N-钙黏蛋白的转移性 ACC,她在 I 期临床试验中接受了 ADH-1 治疗,随后通过特殊准入计划接受了额外剂量的 ADH-1 治疗。该患者因皮质醇过度分泌而出现库欣综合征特征,并于 2003 年 1 月被诊断为转移性 ACC。肿瘤进展后,接受多柔比星、顺铂和米托坦联合治疗。2003 年 10 月,作为 I 期临床试验的一部分,她接受了 150mg/m2 的 ADH-1 单次剂量治疗。这导致皮质醇短暂正常化,CT 成像上肿瘤坏死,并减少 DCE-MRI 上的肿瘤灌注。在接受了几轮化疗后,她再次接受了特殊准入计划 (SAP) 下的 ADH-1 治疗。接受 33 周剂量治疗(22 次剂量为 150mg/m2,11 次剂量为 300mg/m2)后,显示出放射性肿瘤进展,并停止了治疗。她在转移性疾病中存活了 40 个月,在最后一次 ADH-1 剂量后 12 个月死亡。这一观察结果值得考虑,以便前瞻性评估 ADH-1 在表达 N-钙黏蛋白的分泌皮质醇的 ACC 患者中的疗效。

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