Marfan syndrome with neonatal progeroid syndrome‐like lipodystrophy associated with a novel frameshift mutation at the 3′ terminus of the <i>FBN1</i>‐gene

Graul‐Neumann, Luitgard; Kienitz, Tina; Robinson, Peter N.; Baasanjav, Sevjidmaa; Karow, Benjamin; Gillessen‐Kaesbach, Gabriele; Fahsold, Raimund; Schmidt, Hartmut; Hoffmann, Katrin; Passarge, Eberhard

doi:10.1002/ajmg.a.33690

Cited by 70 publications

(63 citation statements)

References 40 publications

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“…In addition, the intracellular retention caused by the single amino acid L2780P substitution (20), which affects a highly conserved leucine, suggests that the function of the propeptide is dependent on its native structure and/or interactions. Recently a correlation has been established between a subset of mutations affecting the fibrillin-1 C terminus and a neonatal, progeroid form of MFS (30)(31)(32)(33)(34). All of these mutations result in a frameshift with the introduction of a stop codon before the sequence encoding the C-terminal furin cleavage site (33).…”

Section: Discussionmentioning

confidence: 99%

C-terminal propeptide is required for fibrillin-1 secretion and blocks premature assembly through linkage to domains cbEGF41-43

Jensen

Aspinall

Handford

2014

Proc. Natl. Acad. Sci. U.S.A.

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Fibrillin microfibrils are 10-12 nm diameter, extracellular matrix assemblies that provide dynamic tissues of metazoan species with many of their biomechanical properties as well as sequestering growth factors and cytokines. Assembly of fibrillin monomers into microfibrils is thought to occur at the cell surface, with initial steps including proprotein processing, multimerization driven by the C terminus, and the head-to-tail alignment of adjacent molecules. At present the mechanisms that regulate microfibril assembly are still to be elucidated. We have used structure-informed protein engineering to create a recombinant, GFP-tagged version of fibrillin-1 (GFP-Fbn) to study this process. Using HEK293T cells transiently transfected with GFP-Fbn constructs, we show that (i) the C-terminal propeptide is an essential requirement for the secretion of fulllength fibrillin-1 from cells; (ii) failure to cleave off the C-terminal propeptide blocks the assembly of fibrillin-1 into microfibrils produced by dermal fibroblasts; and (iii) the requirement of the propeptide for secretion is linked to the presence of domains cbEGF41-43, because either deletion or exchange of domains in this region leads to cellular retention. Collectively, these data suggest a mechanism in which the propeptide blocks a key site at the C terminus to prevent premature microfibril assembly.

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Section: Discussionmentioning

confidence: 99%

C-terminal propeptide is required for fibrillin-1 secretion and blocks premature assembly through linkage to domains cbEGF41-43

Jensen

Aspinall

Handford

2014

Proc. Natl. Acad. Sci. U.S.A.

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“…Primär ein Protein der extrazellulären Matrix, Fibrillin 1, ist beim progeroiden Marfan-Syndrom betroffen, bei dem der vorgealterte Aspekt v. a. auf eine starke Lipodystrophie zurückgeht [17]. Ebenso durch eine starke Beteiligung der extrazellulären Matrix gekennzeichnet sind die Cutis-laxa-Syndrome, von denen v. a. die autosomal-rezessive Cutis laxa (ARCL) progeroide Züge zeigt.…”

Section: Defekte Kernlaminaunclassified

Progeroide Erkrankungen und ihre Mechanismen

Wollnik

Kornak

2012

Medizinische Genetik

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“…6,7 Six recent reports describe seven patients with a newly recognized syndrome, the clinical features of which overlap with those of congenital MFS, progeroid syndromes, and lipodystrophy. [8][9][10][11][12][13] All seven individuals harbor a disease-causing mutation in exon 64, the penultimate exon of the FBN1 gene (Table 1).…”

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confidence: 99%

“…8 Recognizable mutations in seven known lipodystrophy-associated genes (APGAT2, BSCL2, CAV1, LMNA, PPARG, LMNB2, and PTRF-CAVIN) and two progeroid-associated genes (LMNA/C and ZMPSTE24) were ruled out by extensive molecular analysis. Additional sequencing of the coding regions of the MFSassociated genes (FBN1, TGFBR1, and TGFBR2) revealed a de novo heterozygous 2-bp deletion c.8155_8156delAA in the coding exon 64 of the FBN1 gene.…”

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confidence: 99%

“…Additional sequencing of the coding regions of the MFSassociated genes (FBN1, TGFBR1, and TGFBR2) revealed a de novo heterozygous 2-bp deletion c.8155_8156delAA in the coding exon 64 of the FBN1 gene. 8 (The annotation of this and all the following FBN1 variants is with respect to NM_000138.4.) This mutation was absent in both parents, the patient's unaffected sister, and in 150 unrelated controls.…”

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confidence: 99%

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Marfanoid–progeroid–lipodystrophy syndrome: a newly recognized fibrillinopathy

2016

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We review six previous reports between 2000 and 2014 of seven unrelated patients with mutations in the FBN1 gene affecting function. All mutations occurred in exon 64 of the FBN1 gene. A distinctive phenotype consisting of partial manifestations of Marfan syndrome, a progeroid facial appearance, and clinical features of lipodystrophy was present in all individuals. We suggest that this previously unknown genotype/phenotype relationship constitutes a new fibrillinopathy for which the name marfanoid-progeroid-lipodystrophy syndrome would be appropriate.

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Marfan syndrome with neonatal progeroid syndrome‐like lipodystrophy associated with a novel frameshift mutation at the 3′ terminus of the FBN1‐gene

Cited by 70 publications

References 40 publications

C-terminal propeptide is required for fibrillin-1 secretion and blocks premature assembly through linkage to domains cbEGF41-43

C-terminal propeptide is required for fibrillin-1 secretion and blocks premature assembly through linkage to domains cbEGF41-43

Progeroide Erkrankungen und ihre Mechanismen

Marfanoid–progeroid–lipodystrophy syndrome: a newly recognized fibrillinopathy

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