Department of Neurology, Friedrich-Baur-Institute, LMU Klinikum, University Hospital of the Ludwig-Maximilians-Universität München, Munich, Germany.
Department of Medical Genetics, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Canada.
Orphanet J Rare Dis. 2023 Aug 31;18(1):257. doi: 10.1186/s13023-023-02869-1.
Pantothenate kinase-associated neurodegeneration (PKAN) is a rare autosomal recessive genetic disorder of PANK2, which enables mitochondrial synthesis of coenzyme A. Its loss causes neurodegeneration with iron accumulation primarily in motor-related brain areas. Symptoms include dystonia, parkinsonism, and other disabilities. PKAN has been categorized as classic PKAN, with an age of onset ≤ 10 years, rapid progression, and early disability or death; and atypical PKAN, with later onset, slower progression, generally milder, and more diverse symptom manifestations. Available treatments are mostly palliative. Information on the lived experience of patients with PKAN and their caregivers or on community-level disease burden is limited. It is necessary to engage patients as partners to expand our understanding and improve clinical outcomes. This patient-oriented research study used multiple-choice and free-form question surveys distributed by patient organizations to collect information on the manifestations and disease burden of PKAN. It also assessed respondents' experiences and preferences with clinical research to inform future clinical trials.
The analysis included 166 surveys. Most respondents (87%) were parents of a patient with PKAN and 7% were patients, with 80% from Europe and North America. The study cohort included 85 patients with classic PKAN (mean ± SD age of onset 4.4 ± 2.79 years), 65 with atypical PKAN (13.8 ± 4.79 years), and 16 identified as "not sure". Respondents reported gait disturbances and dystonia most often in both groups, with 44% unable to walk. The classic PKAN group reported more speech, swallowing, and visual difficulties and more severe motor problems than the atypical PKAN group. Dystonia and speech/swallowing difficulties were reported as the most challenging symptoms. Most respondents reported using multiple medications, primarily anticonvulsants and antiparkinsonian drugs, and about half had participated in a clinical research study. Study participants reported the most difficulties with the physical exertion associated with imaging assessments and travel to assessment sites.
The survey results support the dichotomy between classic and atypical PKAN that extends beyond the age of onset. Inclusion of patients as clinical research partners shows promise as a pathway to improving clinical trials and providing more efficacious PKAN therapies.
泛酸激酶相关神经退行性变(PKAN)是一种罕见的常染色体隐性遗传疾病,由 PANK2 引起,可使辅酶 A 在线粒体中合成。其缺失导致铁在主要与运动相关的脑区中积累,从而引起神经退行性变。症状包括肌张力障碍、帕金森病和其他残疾。PKAN 分为经典 PKAN,发病年龄≤10 岁,进展迅速,早期残疾或死亡;以及非典型 PKAN,发病较晚,进展较慢,通常较轻,症状表现更为多样。现有的治疗方法大多是姑息性的。关于 PKAN 患者及其照顾者的生活体验或社区层面疾病负担的信息有限。有必要让患者作为合作伙伴参与进来,以扩大我们的认识并改善临床结果。这项以患者为中心的研究使用了患者组织分发的多项选择题和自由格式问题调查,收集了 PKAN 的临床表现和疾病负担信息。它还评估了受访者对临床研究的经验和偏好,以为未来的临床试验提供信息。
分析包括 166 份调查。大多数受访者(87%)是 PKAN 患者的父母,7%是患者,80%来自欧洲和北美。研究队列包括 85 名经典 PKAN 患者(平均发病年龄 4.4±2.79 岁)、65 名非典型 PKAN 患者(13.8±4.79 岁)和 16 名不确定患者。受访者报告说,两组患者最常出现步态障碍和肌张力障碍,44%的患者无法行走。经典 PKAN 组报告的言语、吞咽和视觉困难以及更严重的运动问题比非典型 PKAN 组多。肌张力障碍和言语/吞咽困难被报告为最具挑战性的症状。大多数受访者报告使用多种药物,主要是抗惊厥药和抗帕金森病药物,约一半的人参加过临床研究。研究参与者报告说,在进行影像学评估和前往评估地点时,最困难的是体力消耗。
调查结果支持经典和非典型 PKAN 之间的二分法,这种二分法不仅限于发病年龄。将患者纳入临床研究合作伙伴,有望改善临床试验并提供更有效的 PKAN 治疗方法。
