| Abstract | dc.description.abstract | Mutations in the gene encoding the phosphoinositide
phosphatase myotubularin 1 protein (MTM1) are
usually associated with severe neonatal X-linked myotubular
myopathy (XLMTM). However, mutations in MTM1
have also been recognized as the underlying cause of “atypical”
forms of XLMTM in newborn boys, female infants,
female manifesting carriers and adult men. We reviewed
systematically the biopsies of a cohort of patients with an
unclassiWed form of centronuclear myopathy (CNM) and
identiWed four patients presenting a peculiar histological
alteration in some muscle Wbers that resembled a necklace
(“necklace Wbers”). We analyzed further the clinical and
morphological features and performed a screening of the
genes involved in CNM. Muscle biopsies in all four
patients demonstrated 4–20% of Wbers with internalized
nuclei aligned in a basophilic ring (necklace) at 3 m
beneath the sarcolemma. Ultrastructurally, such necklaces
consisted of myoWbrils of smaller diameter, in oblique orientation,
surrounded by mitochondria, sarcoplasmic reticulum
and glycogen granules. In the four patients (three
women and one man), myopathy developed in early childhood
but was slowly progressive. All had mutations in the
MTM1 gene. Two mutations have previously been
reported (p.E404K and p.R241Q), while two are novel; a
c.205_206delinsAACT frameshift change in exon 4 and a
c.1234A>G mutation in exon 11 leading to an abnormal
splicing and the deletion of nine amino acids in the catalytic
domain of MTM1. Necklace Wbers were seen neither in DNM2- or BIN1-related CNM nor in males with classical
XLMTM. The presence of necklace Wbers is useful as a
marker to direct genetic analysis to MTM1 in CNM. | en_US |
