Carbohydrate and Lipid Metabolism Research Unit, Faculty of Health Sciences, University of Witwatersrand, Johannesburg, South Africa.
Department of Vascular Medicine, Academisch Medisch Centrum, Amsterdam, Netherlands.
Lancet Diabetes Endocrinol. 2017 Apr;5(4):280-290. doi: 10.1016/S2213-8587(17)30044-X. Epub 2017 Feb 16.
Homozygous familial hypercholesterolaemia is a genetic disorder characterised by substantially raised LDL cholesterol, reduced LDL receptor function, xanthomas, and cardiovascular disease before age 20 years. Conventional therapy is with statins, ezetimibe, and apheresis. We aimed to assess the long-term safety and efficacy of the proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitor evolocumab in a subset of patients with homozygous familial hypercholesterolaemia enrolled in an open-label, non-randomised phase 3 trial.
In this interim subset analysis of the TAUSSIG study, which was undertaken at 35 sites in 17 countries, we included patients aged 12 years or older with homozygous familial hypercholesterolaemia who were on stable LDL cholesterol-lowering therapy for at least 4 weeks; all patients received evolocumab 420 mg subcutaneously monthly, or if on apheresis every 2 weeks. Dosing could be increased to every 2 weeks after 12 weeks in patients not on apheresis. The primary outcome of the TAUSSIG study was treatment-emergent adverse events; secondary outcomes were the effects of evolocumab on LDL cholesterol and other lipids. We analysed patients on an intention-to-treat basis, and all statistical comparisons were done post hoc in this interim analysis. The TAUSSIG study is registered with ClinicalTrials.gov, number NCT01624142, and is ongoing.
106 patients were included in this analysis, 34 receiving apheresis at study entry and 14 younger than 18 years. The first patient was enrolled on June 28, 2012, and the cutoff date for the analysis was Aug 13, 2015; mean follow-up was 1·7 years (SD 0·63). After 12 weeks, mean LDL cholesterol decreased from baseline by 20·6% (SD 24·4; mean absolute decrease 1·50 mmol/L [SD 1·92]); these reductions were maintained at week 48. 47 of 72 patients not on apheresis at study entry increased evolocumab dosing to every 2 weeks, with an additional mean reduction in LDL cholesterol of 8·3% (SD 13·0; mean absolute decrease 0·77 mmol/L [SD 1·38]; p=0·0001). In a post-hoc analysis, mean reductions in LDL cholesterol in patients on apheresis were significant at week 12 (p=0·0012) and week 48 (p=0·0032), and did not differ from reductions achieved in patients not on apheresis (p=0·38 at week 12 and p=0·09 at week 48). We noted a small reduction (median -7·7% [IQR -21·6 to 6·8]) in lipoprotein(a) at week 12 (p=0·0015), with some additional reduction at week 48 (-11·9% [-28·0 to 0·0]; p<0·0001). HDL cholesterol was increased by a mean of 7·6% (SD 18·1) at week 12 (p<0·0001) and 7·6% (SD 20·6) at week 48 (p=0·0007). Evolocumab was well tolerated; 82 (77%) patients reported treatment-emergent adverse events, which were mostly minor. The most common were nasopharyngitis (14 patients [13%]), influenza (13 [12%]), headache (11 [10%]), and upper respiratory tract infection (11 [10%]). Serious adverse events occurred in 18 (17%) patients, with the most common being cardiovascular events (four patients [4%]). There were no deaths and four positively adjudicated cardiovascular events, one (3%) among patients on apheresis and three (4%) among patients who did not receive apheresis.
Our interim results suggest that evolocumab is an effective additional option to reduce LDL cholesterol in patients with homozygous familial hypercholesterolaemia, with or without apheresis.
Amgen.
家族性高胆固醇血症是一种遗传性疾病,其特征是 LDL 胆固醇显著升高, LDL 受体功能降低,黄斑瘤和 20 岁前心血管疾病。常规治疗是他汀类药物、依折麦布和血浆置换。我们旨在评估在一项开放标签、非随机 3 期试验中纳入的杂合子家族性高胆固醇血症患者亚组中,前蛋白转化酶枯草溶菌素/柯萨奇蛋白酶 9(PCSK9)抑制剂依洛尤单抗的长期安全性和疗效。
在这项在 17 个国家的 35 个地点进行的 TAUSSIG 研究的中期亚组分析中,我们纳入了年龄在 12 岁及以上、接受 LDL 胆固醇降低治疗至少 4 周的杂合子家族性高胆固醇血症患者;所有患者每月接受皮下注射 420mg 依洛尤单抗,或每 2 周接受血浆置换。如果患者未接受血浆置换,则在 12 周后可将剂量增加至每 2 周一次。TAUSSIG 研究的主要终点是治疗中出现的不良事件;次要终点是依洛尤单抗对 LDL 胆固醇和其他脂质的影响。我们根据意向治疗原则分析患者,所有统计学比较均在本中期分析中进行事后分析。TAUSSIG 研究在 ClinicalTrials.gov 上注册,编号为 NCT01624142,正在进行中。
本分析纳入了 106 名患者,其中 34 名患者在研究开始时接受了血浆置换,14 名患者年龄小于 18 岁。首例患者于 2012 年 6 月 28 日入组,分析截止日期为 2015 年 8 月 13 日;平均随访时间为 1.7 年(标准差 0.63)。在 12 周后,LDL 胆固醇从基线水平下降了 20.6%(标准差 24.4%;平均绝对下降 1.50mmol/L[标准差 1.92]);这些降低在 48 周时得到维持。在研究开始时未接受血浆置换的 72 名患者中有 47 名将依洛尤单抗剂量增加至每 2 周一次,LDL 胆固醇进一步降低 8.3%(标准差 13.0%;平均绝对下降 0.77mmol/L[标准差 1.38];p=0.0001)。在一项事后分析中,接受血浆置换的患者在第 12 周(p=0.0012)和第 48 周(p=0.0032)的 LDL 胆固醇降低具有显著意义,与未接受血浆置换的患者的降低无差异(第 12 周为 p=0.38,第 48 周为 p=0.09)。我们注意到在第 12 周(p=0.0015)时脂蛋白(a)有一个小幅度的降低(中位数-7.7%[IQR-21.6 至 6.8]),在第 48 周时进一步降低(-11.9%[-28.0 至 0.0];p<0.0001)。HDL 胆固醇平均增加 7.6%(标准差 18.1),第 12 周(p<0.0001)和第 48 周(p=0.0007)均如此。依洛尤单抗耐受性良好;82 名(77%)患者报告了治疗中出现的不良事件,大多数为轻微不良事件。最常见的是鼻咽炎(14 名患者[13%])、流感(13 名[12%])、头痛(11 名[10%])和上呼吸道感染(11 名[10%])。18 名(17%)患者发生严重不良事件,最常见的是心血管事件(四名患者[4%])。无死亡病例,有四起经正向裁定的心血管事件,其中一起(3%)发生在接受血浆置换的患者中,三起(4%)发生在未接受血浆置换的患者中。
我们的中期结果表明,依洛尤单抗是一种有效的额外选择,可降低杂合子家族性高胆固醇血症患者的 LDL 胆固醇,无论是否接受血浆置换。
安进公司。
