Department of Medicine, Endocrinology Section, Pituitary Center Rotterdam, Erasmus University Medical Center, Rotterdam, The Netherlands.
Department of Neurosurgery, Pituitary Center Rotterdam, Erasmus University Medical Center, Rotterdam, The Netherlands.
J Clin Endocrinol Metab. 2018 Feb 1;103(2):586-595. doi: 10.1210/jc.2017-02017.
To assess the efficacy and safety of pasireotide long-acting release (PAS-LAR) alone or in combination with pegvisomant by switching patients with acromegaly who were well controlled with long-acting somatostatin analogues (LA-SSAs) and pegvisomant to PAS-LAR with or without pegvisomant.
Sixty-one patients with acromegaly were enrolled in a prospective open-label study. We included patients with an insulin-like growth factor I (IGF-I) ≤1.2 × upper limit of normal (ULN) during treatment with LA-SSAs and pegvisomant. At baseline, the pegvisomant dose was reduced by 50% up to 12 weeks. When IGF-I remained ≤1.2 × ULN after 12 weeks, patients were switched to PAS-LAR 60 mg monotherapy. When IGF-I was >1.2 × ULN, patients were switched to PAS-LAR 60 mg, and they continued with the 50% reduced pegvisomant dose.
At baseline, mean IGF-I was 0.97 × ULN, and the median pegvisomant dose was 80 mg/wk. At 12 weeks, mean IGF-I increased to 1.59 × ULN, and IGF-I levels ≤1.2 ULN were observed in 24.6% of participants. At 24 weeks, IGF-I levels were reduced into the reference range in 73.8% of patients. Between baseline and 24 weeks, the pegvisomant dose was reduced by 66.1%. PAS-LAR was well tolerated, but hyperglycemia was the most frequent adverse event. The frequency of diabetes increased from 32.8% at baseline to 68.9% at 24 weeks.
Switching to PAS-LAR, either as monotherapy or combination with pegvisomant, can control IGF-I levels in most patients. PAS-LAR demonstrated a pegvisomant-sparing effect of 66% compared with the combination with LA-SSAs. Hyperglycemia was the most important safety issue.
评估单独使用或联合使用培维索孟时帕瑞肽长效释放剂(PAS-LAR)在控制良好的长效生长抑素类似物(LA-SSA)和培维索孟治疗的肢端肥大症患者中的疗效和安全性,将这些患者切换为 PAS-LAR 加或不加培维索孟。
61 例肢端肥大症患者参加了一项前瞻性开放标签研究。我们纳入了在接受 LA-SSA 和培维索孟治疗时胰岛素样生长因子 I(IGF-I)≤1.2×正常值上限(ULN)的患者。基线时,培维索孟剂量在 12 周内减少 50%。12 周后 IGF-I 仍≤1.2×ULN 时,患者转换为 PAS-LAR 60mg 单药治疗。如果 IGF-I>1.2×ULN,则患者转换为 PAS-LAR 60mg,并继续使用 50%减少的培维索孟剂量。
基线时,平均 IGF-I 为 0.97×ULN,中位数培维索孟剂量为 80mg/周。12 周时,平均 IGF-I 增加至 1.59×ULN,24.6%的参与者 IGF-I 水平≤1.2ULN。24 周时,73.8%的患者 IGF-I 水平降至参考范围。与基线相比,24 周时培维索孟剂量减少了 66.1%。PAS-LAR 耐受性良好,但高血糖是最常见的不良事件。糖尿病的发生率从基线时的 32.8%增加到 24 周时的 68.9%。
转换为 PAS-LAR 单药治疗或联合培维索孟治疗,可使大多数患者的 IGF-I 水平得到控制。与联合 LA-SSA 治疗相比,PAS-LAR 表现出 66%的培维索孟节省效应。高血糖是最重要的安全问题。
