脊髓性肌萎缩症(SMA)是最常见的遗传性疾病之一,直到最近,婴儿死亡的主要遗传原因。三种疾病修饰治疗方法极大地改变了受严重影响的婴儿(SMA1型)的疾病轨迹和结果。特别是在症状前阶段开始。这些治疗方法之一是基于腺相关病毒载体9(AAV9)的基因疗法,它是全身性递送的,并已被欧洲医学机构批准用于具有多达三个SMN2基因拷贝或具有SMA1型临床表现的SMA患者。虽然这种广泛的适应症为患者选择提供了灵活性,对于支持治疗的证据有限或没有证据的患者,这也引起了人们对风险-获益比的担忧.2020年,我们召集了一个欧洲神经肌肉专家工作组,以支持合理使用onasemnogeneabeparvovec,采用改进的德尔菲法。三年后,我们已经召集了一个类似但更大的欧洲专家小组,他们评估了新出现的证据,即asemnogeneabeparvovec在治疗老年和体重较重的SMA患者中的作用,整合来自最近临床试验和现实世界证据的见解。这项努力导致了12项协商一致声明,在9个方面达成了强烈共识,在其余3个方面达成了共识,反映了onasemnogeneabeparvovec在治疗SMA中不断发展的作用。
Spinal muscular atrophy (SMA) is one of the most common genetic diseases and was, until recently, a leading genetic cause of infant mortality. Three disease-modifying treatments have dramatically changed the disease trajectories and outcome for severely affected infants (SMA type 1), especially when initiated in the presymptomatic phase. One of these treatments is the adeno-associated viral vector 9 (AAV9) based gene therapy onasemnogene abeparvovec (Zolgensma®), which is delivered systemically and has been approved by the European Medicine Agency for SMA patients with up to three copies of the SMN2 gene or with the clinical presentation of SMA type 1. While this broad indication provides flexibility in patient selection, it also raises concerns about the risk-benefit ratio for patients with limited or no evidence supporting treatment. In 2020, we convened a European neuromuscular expert working group to support the rational use of onasemnogene abeparvovec, employing a modified Delphi methodology. After three years, we have assembled a similar yet larger group of European experts who assessed the emerging evidence of onasemnogene abeparvovec\'s role in treating older and heavier SMA patients, integrating insights from recent clinical trials and real-world evidence. This effort resulted in 12 consensus statements, with strong consensus achieved on 9 and consensus on the remaining 3, reflecting the evolving role of onasemnogene abeparvovec in treating SMA.
