Lumacaftor/ Ivacaftor 可提高伴有严重气流阻塞的囊性纤维化患者的运动耐量。
Lumacaftor/ Ivacaftor improves exercise tolerance in patients with Cystic Fibrosis and severe airflow obstruction.
机构信息
Centre for Healthy Lungs, Hunter Medical Research Institute, University of Newcastle, Lookout Rd New, Lambton, NSW, 2305, Australia.
Adult Cystic Fibrosis Centre, Department of Respiratory and Sleep Medicine, John Hunter Hospital, Newcastle, Australia.
出版信息
BMC Pulm Med. 2019 Jun 17;19(1):106. doi: 10.1186/s12890-019-0866-y.
BACKGROUND
Treatment of patients with Cystic Fibrosis homozygous for the Phe508del gene, with Lumacaftor /Ivacaftor (LUM/IVA) improves outcomes in patients with FEV1 > 40% predicted. We set out to observe the most sensitive clinical measure that would change with treatment in terms of exercise capacity or lung function in adults with severe lung disease as defined by an FEV1 < 40% predicted when clinically stable.
METHODS
10 adults homozygous for the Phe508del received LUM/IVA. We assessed; six minute walk test (6MWT), spirometry, gas transfer (DLCO), plethysmography, and nitrogen multiple breath washout (MBW) at baseline, 4, 12, 24 and 52 weeks. Comparison was made with 10 matched historical controls that had been observed over 12 months.
RESULTS
There was a significant improvement in 6MWT by 4 weeks of treatment; with a mean increase of 78 m (SD 62.3) and this increased to 118.1 m (SD 80.9) (ANOVA p = 0.006) by 52 weeks. Significant improvements were also seen in the resting heart rate and the oxygen saturation (SaO2) after 6 min walking. A significant improvement was not seen in FEV1 though until 24 weeks, though this was maintained at 52 weeks (ANOVA, p = 0.0004). There were no significant differences seen in the MBW or DLCO. After 12 months treatment with LUM/IVA, in comparison to historical controls; the 6MWT increased by 118 m (SD 80.9), but fell in the controls - 61.3 m (SD 31.1). FEV1; LUM/IVA led to an increase of 0.398 L/min, compared to a fall in the controls - 0.18 (SD 0.2).
CONCLUSION
In adults homozygous for Phe508del with severe disease, treatment with LUM/IVA results in a clinically significant improvement in 6MWT that was evident at 4 weeks and maintained at 52 weeks. Improvement in exercise tolerance is an important outcome to consider in those with more severe airways disease.
TRIAL REGISTRATION
This was an observational trial conducted on individuals who became eligible to receive LUM/IVA. All investigations were carried out as part of routine clinical care. The trial was registered in retrospect on the 13/5/2019 on the Australian New Zealand Clinical Trials registry; ACTRN12619000708156 .
背景
对于携带纯合子 Phe508del 基因突变的囊性纤维化患者,使用 Lumacaftor/Ivacaftor(LUM/IVA)治疗可改善 FEV1>40%预测值的患者的结局。我们旨在观察在临床稳定时 FEV1<40%预测值的情况下,最敏感的临床指标,该指标在运动能力或肺功能方面会因治疗而发生变化,用于定义患有严重肺部疾病的成年人。
方法
10 名纯合子 Phe508del 患者接受了 LUM/IVA 治疗。我们在基线、4 周、12 周、24 周和 52 周时评估了 6 分钟步行测试(6MWT)、肺活量测定、气体转移(DLCO)、体积描记法和氮多次呼吸冲洗(MBW)。与 10 名经过 12 个月观察的匹配历史对照进行了比较。
结果
治疗 4 周后 6MWT 显著改善,平均增加 78m(SD 62.3),52 周时增加至 118.1m(SD 80.9)(ANOVA p=0.006)。静息心率和 6 分钟步行后血氧饱和度(SaO2)也有显著改善。尽管在 24 周时才观察到 FEV1 的显著改善,但这种改善一直持续到 52 周(ANOVA,p=0.0004)。MBW 或 DLCO 未见显著差异。在接受 LUM/IVA 治疗 12 个月后,与历史对照组相比,6MWT 增加了 118m(SD 80.9),但对照组则下降了-61.3m(SD 31.1)。FEV1;LUM/IVA 导致每分通气量增加 0.398L/min,而对照组下降-0.18(SD 0.2)。
结论
在携带纯合子 Phe508del 基因突变且疾病严重的成年人中,使用 LUM/IVA 治疗可显著改善 6MWT,这在 4 周时就已经显现,并在 52 周时得以维持。运动耐量的改善是对更严重气道疾病患者的一个重要考虑因素。
试验注册
这是一项对符合接受 LUM/IVA 治疗条件的个体进行的观察性试验。所有研究均作为常规临床护理的一部分进行。该试验于 2019 年 5 月 13 日在澳大利亚和新西兰临床试验注册处进行了回顾性注册;ACTRN12619000708156。
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