| Title : Gene-specific long-term course, neurodevelopmental outcome and quality of life in patients with LIS1\/PAFAH1B1-, DCX-, DYNC1H1-, TUBA1A- and TUBG1-related lissencephaly - Proepper_2026_Orphanet.J.Rare.Dis_21_ |
| Author(s) : Proepper CR , Schwarz LM , Schuetz SM , von Au K , Bast T , Beaud N , Borggraefe I , Bosch F , Busse M , Chung J , Debus O , Diepold K , Fries T , von Gersdorff G , Haeussler M , Hahn A , Hartlieb T , Heiming R , Herkenrath P , Kluger G , Kreth JH , Kurlemann G , Moeller P , Morris-Rosendahl DJ , Panzer A , Philippi H , Ruegner S , Toepfer C , Vieker S , Wiemer-Kruel A , Winter A , Schuierer G , Hehr U , Geis T |
| Ref : Orphanet J Rare Dis , 21 : , 2026 |
|
Abstract :
BACKGROUND: Classic lissencephaly is a malformation of cortical development that includes agyria and pachygyria. The major clinical symptoms are developmental impairment, muscular hypotonia, and drug-resistant epilepsy. The severity of the clinical phenotype depends on the associated gene and mutation. This study aimed to systematically investigate the genotype-specific course of the disease including neurodevelopmental outcome, medical complications, use of non-pharmacological supportive therapies, and its impact on the quality of life of the affected families. METHODS: 47 patients with genetically and radiologically confirmed lissencephaly were included with mutation in LIS1/PAFAH1B1 (n = 38), DCX (n = 5 males), DYNC1H1 (n = 2), TUBA1A (n = 1) and TUBG1 (n = 1) genes. Standardized questionnaires were completed by families and treating pediatricians. Quality of life was assessed with the PedsQL Family Impact Module. RESULTS: Prenatal abnormalities, most commonly microcephaly, were observed in 14/37 (38%) of LIS1/PAFAH1B1 patients and 2/5 (40%) of DCX patients. Early symptoms included microcephaly, developmental delay, muscular hypotonia, and epileptic seizures. The median age at suspected diagnosis was 5 months for LIS1/PAFAH1B1 patients and 9 months for DCX patients. Compared to LIS1/PAFAH1B1, DCX-related lissencephaly patients showed significantly better neurodevelopmental outcome in reaching more advanced milestones such as walking unassisted (z=-2.23, p = 0.026) and speaking sentences (z=-2.53, p = 0.011). Frequent medical complications included recurrent respiratory infections (14/38 (37%) of LIS1/PAFAH1B1 patients; 1/4 (25%) of DCX patients) and dysphagia/ vomiting (23/37 (62%); 2/4 (50%)), which may require tube feeding (15/38 (40%); 1/5 (20%)). A median of eight different supportive therapies was used per patient (range 1-17), with physiotherapy and respiratory therapy considered the most effective. The scores obtained for health-related quality of life (HRQL) were low (parental HRQL mean 61.23; SD 16.79). CONCLUSIONS: Our study confirms the severely impaired developmental potential and frequent neurological and medical complications in lissencephaly patients from an early age. The psychomotor prognosis in LIS1/PAFAH1B1-related lissencephaly is significantly worse compared to DCX-related lissencephaly. Supportive therapies are used intensively and are considered to be very effective. The disease puts a high burden on caregivers and the entire family. This emphasizes the need for appropriate epilepsy treatment, personalized care for patients and professional support for their families. |
| PubMedSearch : Proepper_2026_Orphanet.J.Rare.Dis_21_ |
| PubMedID: 42177523 |
Proepper CR, Schwarz LM, Schuetz SM, von Au K, Bast T, Beaud N, Borggraefe I, Bosch F, Busse M, Chung J, Debus O, Diepold K, Fries T, von Gersdorff G, Haeussler M, Hahn A, Hartlieb T, Heiming R, Herkenrath P, Kluger G, Kreth JH, Kurlemann G, Moeller P, Morris-Rosendahl DJ, Panzer A, Philippi H, Ruegner S, Toepfer C, Vieker S, Wiemer-Kruel A, Winter A, Schuierer G, Hehr U, Geis T (2026)
Gene-specific long-term course, neurodevelopmental outcome and quality of life in patients with LIS1\/PAFAH1B1-, DCX-, DYNC1H1-, TUBA1A- and TUBG1-related lissencephaly
Orphanet J Rare Dis
21 :
Proepper CR, Schwarz LM, Schuetz SM, von Au K, Bast T, Beaud N, Borggraefe I, Bosch F, Busse M, Chung J, Debus O, Diepold K, Fries T, von Gersdorff G, Haeussler M, Hahn A, Hartlieb T, Heiming R, Herkenrath P, Kluger G, Kreth JH, Kurlemann G, Moeller P, Morris-Rosendahl DJ, Panzer A, Philippi H, Ruegner S, Toepfer C, Vieker S, Wiemer-Kruel A, Winter A, Schuierer G, Hehr U, Geis T (2026)
Orphanet J Rare Dis
21 :