Your search keyword '"Spinal muscular atrophy with lower extremity predominance"' showing total 4 results

1. Expanding the phenotype of DYNC1H1-associated diseases with a rare variant resulting in spinal muscular atrophy with lower extremity predominance (SMA-LED) and upper motor neuron signs.

Author

Lee, Jessica, Millington, Philip, Dayasiri, Kavinda, Ramdas, Sithara, Jayawant, Sandeep, and Anand, Geetha

Abstract

Background. Spinal muscular atrophy with lower extremity predominance (SMA-LED) is an autosomal dominant disorder. Since SMA-LED affects lower motor neurons, the disease is characterized by weakness and atrophy of lower limb muscles. We present a familial case series of SMA-LED with upper motor neuron signs associated with a rare variant in DYNC1H1. Case. The index case was referred to Pediatric Neurology at the age of two and half years, due to delayed mobility. The child was diagnosed with congenital vertical talus at birth, which was managed with serial bilateral casting and surgery. The delayed mobility was initially attributed to lower limb weakness secondary to prolonged periods of immobilization from casting of his lower limbs. He had a striking waddling gait and proximal muscle weakness on neurological assessment. He had lower motor neuron signs predominantly in his lower limbs that were in keeping with SMA-LED. Surprisingly, he also demonstrated a brisk crossed adductor response that was not in keeping with an isolated primary neuro-muscular disorder and suggested a mixed upper and lower motor neuron pathology. The inherited neuropathy gene panel revealed a heterozygous sequence change in the DYNC1H1 gene which was present in all affected family members. Conclusions. We present the first report of a familial case series of SMA-LED with upper motor neuron signs associated with an extremely rare variant in DYNC1H1: c.1808A>T (p.Glu603Val). As per the American College of Medical Genetics and Genomics (ACMG) guidelines for variant classification, we would recommend that this variant be reclassified as "Likely Pathogenic" due to matching 1 moderate (PM1--PM6) and ≥4 supporting (PP1--PP5) criteria in the reported case series. [ABSTRACT FROM AUTHOR]

Published

2023

2. Exome Sequencing Identifies De Novo DYNC1H1 Mutations Associated With Distal Spinal Muscular Atrophy and Malformations of Cortical Development.

Author

Chen, Yulin, Xu, Yufei, Li, Guoqiang, Li, Niu, Yu, Tingting, Yao, Ru-en, Wang, Xiumin, Shen, Yiping, and Wang, Jian

Subjects

*SPINAL muscular atrophy, *GENETIC mutation, *MOLECULAR motor proteins, *EXOMES, *DYNEIN, *PATIENTS

Abstract

Exome sequencing has become a formidable tool for identifying potential de novo variants in causative genes of human diseases, such as neurodegenerative disorders. This article describes a 16-month-old girl with spinal muscular atrophy with lower extremity predominance and a 13-month-old girl with malformations of cortical development. Exome sequencing identified a novel de novo heterozygous missense mutation c.3395G>A (p.Gly1132Glu) and a previously reported de novo heterozygous missense mutation c.10151G>A (p.Arg3384Gln) in the DYNC1H1 gene. Bioinformatics predictions for c.3395G>A and c.10151G>A indicated pathogenicity of the mutations. DYNC1H1 is a pivotal component of cytoplasmic dynein complex, which is a microtubule-related motor involved in retrograde transport. Previous studies indicated that mutant dynein showed decreased run-length of the motor proteins and diminished retrograde transport, which were clearly associated with neuronal death and neurologic diseases. The present findings expand the mutational spectrum of the DYNC1H1 gene, reemphasizing the significance of the DYNC1H1 protein in the functioning of neurons. [ABSTRACT FROM AUTHOR]

Published

2017

3. Exome Sequencing Identifies DYNC1H1 Variant Associated With Vertebral Abnormality and Spinal Muscular Atrophy With Lower Extremity Predominance.

Author

Punetha, Jaya, Monges, Soledad, Franchi, Maria Emilia, Hoffman, Eric P., Cirak, Sebahattin, and Tesi-Rocha, Carolina

Subjects

*EXONS (Genetics), *NUCLEOTIDE sequence, *SPINE abnormality diagnosis, *SPINAL muscular atrophy, *LEG physiology, *NEUROPATHY, *HETEROGENEITY, *DIAGNOSIS, *PATIENTS

Abstract

Background Molecular diagnosis of the distal spinal muscular atrophies or distal hereditary motor neuropathies remains challenging because of clinical and genetic heterogeneity. Next generation sequencing offers potential for identifying de novo mutations of causative genes in isolated cases. Patient Description We present a 3.6-year-old girl with congenital scoliosis, equinovarus, and L5/S1 left hemivertebra who demonstrated delayed walking and lower extremities atrophy. She was negative for SMN1 deletion testing, and parents show no sign of disease. Results Whole exome sequencing of the affected girl showed a novel de novo heterozygous missense mutation c.1792C>T (p.Arg598Cys) in the tail domain of the DYNC1H1 gene encoding for cytoplasmic dynein heavy chain 1. The mutation changed a highly conserved amino acid and was absent from both parents. Conclusion De novo mutations of DYNC1H1 have been found in individuals with autosomal dominant mental retardation with neuronal migration defects. Dominantly inherited mutations of DYNC1H1 have been reported to cause spinal muscular atrophy with predominance of lower extremity involvement and Charcot-Marie-Tooth type 2O. This is the first report of a de novo DYNC1H1 mutation associated with the spinal muscular atrophy with predominance of lower extremity phenotype with a spinal deformity (lumbar hemivertebrae). This case also demonstrates the power of next generation sequencing to discover de novo mutations on a genome-wide scale. [ABSTRACT FROM AUTHOR]

Published

2015

4. A DYNC1H1 mutation causes a dominant spinal muscular atrophy with lower extremity predominance.

Author

Tsurusaki, Yoshinori, Saitoh, Shinji, Tomizawa, Kazuhiro, Sudo, Akira, Asahina, Naoko, Shiraishi, Hideaki, Ito, Jun-ichi, Tanaka, Hajime, Doi, Hiroshi, Saitsu, Hirotomo, Miyake, Noriko, and Matsumoto, Naomichi

Abstract

Whole-exome sequencing of two affected sibs and their mother who showed a unique quadriceps-dominant form of neurogenic muscular atrophy disclosed a heterozygous DYNC1H1 mutation [p.H306R (c.917A>G)]. The identical mutation was recently reported in a pedigree with the axonal form of Charcot-Marie-Tooth disease. Three other missense mutations in DYNC1H1 were also identified in families with dominant spinal muscular atrophy with lower extremity predominance. Their clinical features were consistent with those of our family. Our study has demonstrated that the same DYNC1H1 mutation could cause spinal muscular atrophy as well as distal neuropathy, indicating pleotropic effects of the mutation. [ABSTRACT FROM AUTHOR]

Published

2012