2008
DOI: 10.1111/j.1399-0004.2008.00992.x
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Severe mandibuloacral dysplasia caused by novel compound heterozygous ZMPSTE24 mutations in two Japanese siblings

Abstract: Mandibuloacral dysplasia (MAD) is a rare autosomal recessive progeroid syndrome, characterized by mandibular hypoplasia, acroosteolysis affecting distal phalanges and clavicles, delayed closure of the cranial sutures, atrophic skin, and lipodystrophy. Recently, mutations in lamin A/C (LMNA) and zinc metalloprotease (ZMPSTE24), involved in post-translational processing of prelamin A to mature lamin A, have been identified in MAD kindreds. We now report novel compound heterozygous mutations in exon 1 (c.121C>T; … Show more

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Cited by 46 publications
(54 citation statements)
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“…Missense mutations such as p.Trp340Arg or p.Asn265Ser lead to a reduced catalytic ZMPSTE24 activity. 13,27 All the reported cases of MAD-B phenotypes followed this pathophysiological rule. 22,23,25,27 An apparent exception to this general rule has been reported by Denecke et al 26 but is explained by a digenic mechanism involving both ZMPSTE24 and LMNA.…”
Section: Pathogenicity Of Splice Site Mutationsmentioning
confidence: 82%
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“…Missense mutations such as p.Trp340Arg or p.Asn265Ser lead to a reduced catalytic ZMPSTE24 activity. 13,27 All the reported cases of MAD-B phenotypes followed this pathophysiological rule. 22,23,25,27 An apparent exception to this general rule has been reported by Denecke et al 26 but is explained by a digenic mechanism involving both ZMPSTE24 and LMNA.…”
Section: Pathogenicity Of Splice Site Mutationsmentioning
confidence: 82%
“…13,27 All the reported cases of MAD-B phenotypes followed this pathophysiological rule. 22,23,25,27 An apparent exception to this general rule has been reported by Denecke et al 26 but is explained by a digenic mechanism involving both ZMPSTE24 and LMNA. The case reported in this study was described as a HGPS patient but, according to molecular findings and our current knowledge, it should be classified as a severe MAD-B.…”
Section: Pathogenicity Of Splice Site Mutationsmentioning
confidence: 82%
See 1 more Smart Citation
“…9,32-34 These ZMPSTE24 mutations result not only in the presence of traces of prelamin A but also that of mature lamin A 33 because of partial residual ZMPSTE24 activity. 9,32,33 All these reports strongly suggest a link between phenotype severity, prelamin A accumulation levels and ZMPSTE24 residual activity. Complete prelamin A accumulation with null ZMPSTE24 enzyme activity can be correlated to the most severe progeroid syndrome, RD; null ZMPSTE24 activity rescued by a heterozygous LMNA null mutation causes a severe, HGPS-like, MADB phenotype, whereas partial accumulation of prelamin A with reduced ZMPSTE24 enzyme activity is associated with milder MADB phenotypes.…”
Section: Discussionmentioning
confidence: 99%
“…Such calcifications have been reported in four ZMPSTE24-related MADB cases, two of them requiring surgical removal, 9,36 but not in the two others. 33 Similarly, a homozygous LMNA mutation c.1718C4T leading to the missense substitution p.Ser573Leu has been reported to result in progeroid features associated with arthropathy and tendinous calcinosis 37 without any prelamin A accumulation. Furthermore, renal artery calcifications and chronic kidney disease were responsible for pharmacoresistant high blood pressure as observed in ZMPSTE24-related MADB.…”
Section: Discussionmentioning
confidence: 99%