Type I C1 inhibitor deficiency with a small messenger RNA resulting from deletion of one exon.

Ariga, Tadashi; Igarashi, Tomoko; Ramesh, Narayanaswamy; Parad, Richard B.; Cicardi, Marco; Davis, Alvin E.

doi:10.1172/jci114095

Cited by 42 publications

(16 citation statements)

References 41 publications

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“…In both cases, 1 mg of total RNA was amplified in a one-step reaction with the SuperScriptt One-Step RT-PCR with Platinum Taq kit (Invitrogen; Life Technologies, Carlsbad, CA) in a final volume of 50 ml. In order to amplify a fragment from exons 6-8, the forward primer 5 0 aactcagttataaaagtgcccatgatgaat 3 0 [Ariga et al, 1989] and the reverse primer 5 0 gtgctgcatcgcagaaacctgaagatctgg 3 0 were used, and cDNA synthesis was achieved in a 45-min incubation at 501C after a hot start. The amplification of the cDNA was performed using 25 pmol of each primer and 35 cycles in a Perkin Elmer 9700 thermocycler (Applied Biosystems), comprising 15 sec at 941C, 30 sec at 531C, and 1 min at 721C, followed by a final extension of 10 min at 721C.…”

Section: Rt-pcrmentioning

confidence: 99%

Hereditary angioedema: The mutation spectrum ofSERPING1/C1NHin a large Spanish cohort

et al. 2005

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Hereditary angioedema (HAE) is a disease caused by defects in the C1 inhibitor gene (SERPING1/C1NH). We screened the entire C1NH gene for mutations in a large series of 87 Spanish families (77 with type I, and 10 with type II HAE) by SSCP, sequencing, Southern blotting, and quantitative multiplex PCR of short fluorescent fragments (QMPSF), and we characterized several defects at the mRNA level. We found large rearrangements in 13 families, and point mutations or microdeletions/insertions in 74 families. The 13 large rearrangements included nine exon deletions, of which at least eight were distinct, two were distinct exon duplications, and two were rearrangements whose precise nature could not be determined. We confirmed that exon 4 is particularly prone to rearrangements. Thirty-six mutations were unreported, and included 10 microdeletions/insertions, 10 missense, five nonsense, eight splicing, and three splicing or missense mutations. Moreover, we detected six novel uncharacterized sequence variants (USV). RT-PCR studies showed that in addition to several intronic splice site mutations tested, the exonic mutations c.882C>G and c.884T>G, located near the 3' end of exon 5, also produced exon skipping. This is the first evidence of SERPING1/C1NH mutations in coding regions that differ from the canonical splice sites that affect splicing, which suggests the presence of an exonic splicing enhancer (ESE) in exon 5.

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Section: Rt-pcrmentioning

confidence: 99%

Hereditary angioedema: The mutation spectrum ofSERPING1/C1NHin a large Spanish cohort

et al. 2005

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“…Four of the mutations previously had not been reported: (1) The first mutation, in patient P1, is a splice site error at nucleotide 8721, which changes the 3Ј acceptor splice site AG to GG at the end of intron 5 at nucleotide 8721-8722. This patient has a family history of HAE and typical symptoms (C1INH, 8 mg/ dL; normal range, [11][12][13][14][15][16][17][18][19][20][21][22][23][24]. (2) The second mutation, in patient P2, is a single base insertion in exon 3 between nucleotides 2467 and 2468.…”

Section: New C1inh Gene Defectsmentioning

confidence: 99%

“…In our patient, a T16827C substitution changes the Phe at amino acid 457 to Leu. This patient has no family history of HAE but typical symptoms; she developed symptoms initially at age 74 (C1INH, 7 mg/dL; normal range, [11][12][13][14][15][16][17][18][19][20][21][22][23][24].…”

Section: New C1inh Gene Defectsmentioning

confidence: 99%

A Review of the Reported Defects in the Human C1 Esterase Inhibitor Gene Producing Hereditary Angioedema Including Four New Mutations

Bowen

Hawk

Sibunka

et al. 2001

Clinical Immunology

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“…Differences occur between serum levels ofC I INH in types I and II HANE. In most type I patients there is no restriction fragment length polymorphism, but deletions in either exon 4 or exon 7 have been identified in some type I kindreds (3,22,23). In type II HANE, mutations occur mostly in the P1 reactive center at amino acid 444 (24), but may also occur at 251 (Ta kindred) (13).…”

Section: Introductionmentioning

confidence: 99%

Synthesis of C1 inhibitor in fibroblasts from patients with type I and type II hereditary angioneurotic edema.

Kramer¹,

Katz²,

Rosen³

et al. 1991

J. Clin. Invest.

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Type I C1 inhibitor deficiency with a small messenger RNA resulting from deletion of one exon.

Cited by 42 publications

References 41 publications

Hereditary angioedema: The mutation spectrum ofSERPING1/C1NHin a large Spanish cohort

Hereditary angioedema: The mutation spectrum ofSERPING1/C1NHin a large Spanish cohort

A Review of the Reported Defects in the Human C1 Esterase Inhibitor Gene Producing Hereditary Angioedema Including Four New Mutations

Synthesis of C1 inhibitor in fibroblasts from patients with type I and type II hereditary angioneurotic edema.

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