A novel autosomal recessive myopathy with external ophthalmoplegia linked to chromosome 17p13.1-p12

doi:10.1093/brain/awh338

Brain Advance Access originally published online on November 17, 2004
Brain 2005 128(1):42-51; doi:10.1093/brain/awh338

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A novel autosomal recessive myopathy with external ophthalmoplegia linked to chromosome 17p13.1-p12

Alexander Lossos¹^,*, Lekbir Baala⁸^,9^,*, Dov Soffer², Lea Averbuch-Heller⁵^,#, Shlomo Dotan³, Arnold Munnich⁸, Stanislas Lyonnet⁸, J. Moshe Gomori⁴, Adnan Genem⁶, Meir Neufeld³, Oded Abramsky¹, Joel Zlotogora⁷ and Zohar Argov¹

¹ Department of Neurology, the Agnes Ginges Center for Human Neurogenetics, and Departments of ² Pathology ³ Ophthalmology and ⁴ Radiology, Hadassah-Hebrew University Hospital, Jerusalem, ⁵ Department of Neurology, Rabin Medical Center, Petah-Tikva, ⁶ Clalit Health Services, Jerusalem and ⁷ Department of Community Genetics, Public Health Services, Ministry of Health, Jerusalem Israel, ⁸ Department of Genetics, INSERM U-393, Hopital Necker-Enfants Malades, Paris, France and ⁹ Department of Medical Genetics, INH, Rabat, Morocco

Correspondence to: Dr A. Lossos, Department of Neurology, Hadassah University Hospital, POB 12000, Jerusalem 91120, Israel E-mail: alos{at}hadassah.org.il

We describe a new autosomal recessive myopathy of early onsetand very slow progression distinguished by the prominent externalophthalmoplegia in 16 subjects of eight families from a largeand highly inbred Arab community. Characteristic clinical featuresinclude mild facial and skeletal muscle weakness and atrophymore pronounced proximally in the upper limbs, facial dysmorphismand scoliosis associated with conjugate, non-restrictive ocularmotility impairment greatest in the upgaze and without ptosisor aberrant eye movements. Orbital MRI in the patients demonstratedatrophy with fatty replacement of the oculorotatory muscles.The major pathological alteration on skeletal muscle biopsywas a marked type 1 fibre predominance with core-like formations.A genome wide search for regions of homozygosity in the affectedmembers from two informative families identified linkage withchromosome 17p13.1-p12 markers. Maximum two-point logarithmof odds scores were obtained at loci D17S1803 and AFMA070WD1(Zmax = 3.74 at ${theta}$ = 0). Two independent recombination eventsat D17S1812 and D17S947 further defined a critical region of12 cM. Several genes map to this interval, including a clusterof sarcomeric myosin heavy chain genes. One of these genes,MYH2, is involved in inclusion body myopathy 3, but no exonicmutations were found by direct sequencing. The molecular basisfor this new myopathy remains to be identified.

^# Deceased

This work is dedicated to the memory of our dear colleague andfriend, the late Dr Lea Averbuch-Heller. Her enthusiasm andwisdom made this work possible.

^* These authors contributed equally to this work.

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