Clinical, genetic, and pathologic characterization of FKRP Mexican founder mutation c.1387A>G

FKRP 墨西哥创始突变 c.1387A>G 的临床、遗传和病理学特征

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作者：Angela J Lee, Karra A Jones, Russell J Butterfield, Mary O Cox, Chamindra G Konersman, Carla Grosmann, Jose E Abdenur, Monica Boyer, Brent Beson, Ching Wang, James J Dowling, Melissa A Gibbons, Alison Ballard, Joanne S Janas, Robert T Leshner, Sandra Donkervoort, Carsten G Bönnemann, Denise M Malick

期刊：

Neurology-Genetics

影响因子：

3.000

时间：

2019

起止号：

2019 Mar 1;5(2):e315.

doi：

10.1212/NXG.0000000000000315

研究方向：

信号转导

Conclusions

The clinical features and muscle pathology in these newly reported patients homozygous for FKRP c.1387A>G confirm that this mutation causes congenital muscular dystrophy. The clinical severity might be explained by the greater reduction in α-DG glycosylation compared with that seen with the c.826C>A mutation. The shared region of homozygosity at 19q13.32 indicates that FKRP c.1387A>G is a founder mutation with an estimated age of 60 generations (∼1,200-1,500 years).

Methods

Standardized clinical data were collected for all patients known to the authors with c.1387A>G mutations in FKRP. Muscle biopsies were reviewed and used for histopathology, immunostaining, Western blotting, and DNA extraction. Genetic analysis was performed on extracted DNA.

Objective

To characterize the clinical phenotype, genetic origin, and muscle pathology of patients with the FKRP c.1387A>G mutation.

Results

We report the clinical phenotypes of 6 patients homozygous for the c.1387A>G mutation in FKRP. Onset of symptoms was <2 years, and 5 of the 6 patients never learned to walk. Brain MRIs were normal. Cognition was normal to mildly impaired. Microarray analysis of 5 homozygous FKRP c.1387A>G patients revealed a 500-kb region of shared homozygosity at 19q13.32, including FKRP. All 4 muscle biopsies available for review showed end-stage dystrophic pathology, near absence of glycosylated α-dystroglycan (α-DG) by immunofluorescence, and reduced molecular weight of α-DG compared with controls and patients with homozygous FKRP c.826C>A limb-girdle muscular dystrophy. Conclusions: The clinical features and muscle pathology in these newly reported patients homozygous for FKRP c.1387A>G confirm that this mutation causes congenital muscular dystrophy. The clinical severity might be explained by the greater reduction in α-DG glycosylation compared with that seen with the c.826C>A mutation. The shared region of homozygosity at 19q13.32 indicates that FKRP c.1387A>G is a founder mutation with an estimated age of 60 generations (∼1,200-1,500 years).