Introduction: Familial dilated cardiomyopathy with conduction system defects variably associated with skeletal muscle abnormalities is frequently caused by LMNA gene mutations. Methods: A family affected by cardiac abnormalities, either isolated or variably associated with skeletal muscle compromise, was identified. LMNA gene analysis was applied to all family members. Results: A novel intron 5 (c.937-11 C>G) mutation was identified. mRNA transcription analysis was subsequently performed, and cDNA was obtained from mutated patients. It displayed an aberrant splice product featuring the insertion of 40 nucleotides from intron 5, leading to a frameshift. Computational predictions identified a cryptic splice site 40 bp upstream from the canonical site; this alternative splicing event was elicited by intronic mutation, which seems to interfere with the polypyrimidine tract of the canonical site. Conclusions: We have described the first mutation on the LMNA gene interfering with the polypyrimidine tract. Our findings underline the importance of including introns in the search for mutations.

Aberrant splicing in lmna gene caused by a novel mutation on the polypyrimidine tract of the intron 5 / Carboni, N; Floris, Matteo; Mateddu, A; Porcu, M; Marrosu, G; Solla, E; Cocco, E; Mura, M; Marini, S; Maioli, Ma; Piras, R; Aste, R; Marrosu, Mg. - In: MUSCLE & NERVE. - ISSN 0148-639X. - 43:5(2011), pp. 688-693. [10.1002/mus.21937]

Aberrant splicing in lmna gene caused by a novel mutation on the polypyrimidine tract of the intron 5

FLORIS, Matteo
Formal Analysis
;
2011

Abstract

Introduction: Familial dilated cardiomyopathy with conduction system defects variably associated with skeletal muscle abnormalities is frequently caused by LMNA gene mutations. Methods: A family affected by cardiac abnormalities, either isolated or variably associated with skeletal muscle compromise, was identified. LMNA gene analysis was applied to all family members. Results: A novel intron 5 (c.937-11 C>G) mutation was identified. mRNA transcription analysis was subsequently performed, and cDNA was obtained from mutated patients. It displayed an aberrant splice product featuring the insertion of 40 nucleotides from intron 5, leading to a frameshift. Computational predictions identified a cryptic splice site 40 bp upstream from the canonical site; this alternative splicing event was elicited by intronic mutation, which seems to interfere with the polypyrimidine tract of the canonical site. Conclusions: We have described the first mutation on the LMNA gene interfering with the polypyrimidine tract. Our findings underline the importance of including introns in the search for mutations.
Aberrant splicing in lmna gene caused by a novel mutation on the polypyrimidine tract of the intron 5 / Carboni, N; Floris, Matteo; Mateddu, A; Porcu, M; Marrosu, G; Solla, E; Cocco, E; Mura, M; Marini, S; Maioli, Ma; Piras, R; Aste, R; Marrosu, Mg. - In: MUSCLE & NERVE. - ISSN 0148-639X. - 43:5(2011), pp. 688-693. [10.1002/mus.21937]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11388/175559
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