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对于标准剂量治疗下进展的分化良好的神经内分泌癌患者,缩短长效奥曲肽给药间隔是有效的。

Shortened interval of long-acting octreotide administration is effective in patients with well-differentiated neuroendocrine carcinomas in progression on standard doses.

机构信息

Multidisciplinary Group for Diagnosis and Treatment of Neuroendocrine Tumors, Umbria Regional Cancer Network, Perugia, Italy.

出版信息

J Endocrinol Invest. 2012 Mar;35(3):326-31. doi: 10.3275/7869. Epub 2011 Jul 13.

DOI:10.3275/7869
PMID:21757992
Abstract

BACKGROUND

In patients with well-differentiated (WD) neuroendocrine tumors (NET), long-acting octreotide (LAR), conventionally administered at a dose of 30 mg every 28 days, has well-documented anti-secretive but limited antiproliferative effects.

AIM

The objective of this study was to evaluate a different schedule of LAR treatment consistent with a shorter interval between administrations (21 days) in WDNET patients with progressive disease at standard-dose interval.

SUBJECTS AND METHODS

Twenty-eight patients followed for diagnosis and therapy of WDNET who had tumor progression during therapy with LAR 30 mg every 28 days were enrolled. Clinical, biological, and objective tumor response was evaluated after LAR 30 mg every 21 days. Time to progression was also evaluated after LAR 30 mg every 21 days and compared to LAR 30 mg every 28 days.

RESULTS

The treatment with LAR 30 mg every 21 days resulted in complete and partial control of clinical symptoms in 40% and 60% of cases, respectively. Circulating neuroendocrine markers were significantly decreased in 30% of cases. A stabilization of disease was obtained in 93% and objective response in 7%. The median time to progression was significantly longer by using the shortened interval of LAR administration as compared to the standard one (30 vs 9 months, p<0.0001). The treatment was safe and well tolerated.

CONCLUSIONS

The shortened schedule of LAR administration was able to re-institute control of clinical symptoms, to decrease level of circulating neuroendocrine markers and to increase time to progression in patients previously escaping from a standard schedule treatment.

摘要

背景

在分化良好(WD)的神经内分泌肿瘤(NET)患者中,长效奥曲肽(LAR)的常规给药剂量为每 28 天 30mg,其具有充分的抗分泌作用,但对增殖的抑制作用有限。

目的

本研究旨在评估一种不同的 LAR 治疗方案,该方案与每 21 天给药的较短间隔时间一致,适用于在标准剂量间隔时间内疾病进展的 WD NET 患者。

受试者和方法

本研究纳入了 28 例因 LAR 30mg 每 28 天治疗而出现肿瘤进展的 WD NET 患者,这些患者在诊断和治疗过程中接受了 LAR 30mg 每 28 天的治疗。在接受 LAR 30mg 每 21 天治疗后,评估了临床、生物学和客观肿瘤反应。在接受 LAR 30mg 每 21 天治疗后,也评估了无进展生存期,并与 LAR 30mg 每 28 天治疗进行了比较。

结果

LAR 30mg 每 21 天治疗后,40%和 60%的病例分别完全和部分控制了临床症状,30%的病例循环神经内分泌标志物显著下降。93%的病例疾病稳定,7%的病例客观缓解。与标准间隔相比,缩短 LAR 给药间隔可显著延长无进展生存期(30 个月 vs 9 个月,p<0.0001)。该治疗方案安全且耐受良好。

结论

缩短 LAR 给药方案可重新控制临床症状,降低循环神经内分泌标志物水平,并延长先前逃避标准方案治疗的患者的无进展生存期。

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