TY - JOUR
T1 - Severe classical congenital muscular dystrophy and merosin expression
AU - Vajsar, Jiri
AU - Chitayat, David
AU - Becker, Laurence E.
AU - Ho, Michael
AU - Ben-Zeev, Bruria
AU - Jay, Venita
PY - 1998/9
Y1 - 1998/9
N2 - It has been suggested that patients with autosomal recessive merosin deficient congenital muscular dystrophy (CMD), as opposed to the merosin positive cases form a homogeneous subgroup of a clinically more severe form of CMD. We examined merosin expression in muscle biopsies from five children with the severe classical form of CMD. Merosin deficiency was found only in 1 patient, a 6-year-old female, with abnormal brain myelination. However, her initial biopsy did not reveal the classical picture of dystrophy. The four merosin positive cases exhibited severe muscle weakness but their brain imagings were normal. There were no familial cases, except for the mother of 1 patient who had a milder form of the disease, suggesting an autosomal dominant mode of inheritance. In contrast to previous reports, the merosin deficient CMD cases were rare in our group. Furthermore, merosin positive cases were also associated with severe phenotype suggesting that a severe phenotype is not exclusive to merosin deficient cases. Finally, the absence of merosin in a neonate with hypotonia and weakness can be helpful in making a definitive diagnosis of CMD, even though the dystrophic process may not be evident yet and histology may be non-specific.
AB - It has been suggested that patients with autosomal recessive merosin deficient congenital muscular dystrophy (CMD), as opposed to the merosin positive cases form a homogeneous subgroup of a clinically more severe form of CMD. We examined merosin expression in muscle biopsies from five children with the severe classical form of CMD. Merosin deficiency was found only in 1 patient, a 6-year-old female, with abnormal brain myelination. However, her initial biopsy did not reveal the classical picture of dystrophy. The four merosin positive cases exhibited severe muscle weakness but their brain imagings were normal. There were no familial cases, except for the mother of 1 patient who had a milder form of the disease, suggesting an autosomal dominant mode of inheritance. In contrast to previous reports, the merosin deficient CMD cases were rare in our group. Furthermore, merosin positive cases were also associated with severe phenotype suggesting that a severe phenotype is not exclusive to merosin deficient cases. Finally, the absence of merosin in a neonate with hypotonia and weakness can be helpful in making a definitive diagnosis of CMD, even though the dystrophic process may not be evident yet and histology may be non-specific.
KW - Congenital muscular dystrophy
KW - Hypotonia
KW - Merosin
UR - http://www.scopus.com/inward/record.url?scp=0031694752&partnerID=8YFLogxK
U2 - 10.1111/j.1399-0004.1998.tb04283.x
DO - 10.1111/j.1399-0004.1998.tb04283.x
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C2 - 9788720
AN - SCOPUS:0031694752
SN - 0009-9163
VL - 54
SP - 193
EP - 198
JO - Clinical Genetics
JF - Clinical Genetics
IS - 3
ER -