Genetic history of cystic fibrosis mutations in Italy. I. Regional distribution

Rendine, S.; CALAFELL, F.; CAPPELLO, N.; Gagliardini, R.; CARAMIA, G.; Rigillo, N; SILVETTI, M.; ZANDA, M.; MIANO, A.; Battistini, F; MARIANELLI, L.; Taccetti, Giovanni; Diana, M.; ROMANO, L.; ROMANO, C.; Giunta, Anna; Padoan, Rita; PIANAROLI, A.; Raia, Valeria; RITIS, G. DE; BATTISTINI, A.; GRZINCICH, G.; JAPICHINO, L.; PARDO, F.; Antonelli, M.; Quattrucci, Serena; Lucidi, Vincenzina; CASTRO, M.; SANTINI, B.; CASTELLO, M.; Guanti, Ginevra; LEONI, G. B.; Cao, Antonio; TOFFOLI, C.; LUCCI, E.; VULLO, C.; TORRICELLI, F.; SBERNINI, F.; ROMEO, G.; Ronchetto, Patrizia; Seia, Manuela; ROSSI, A.; FERRARI, M.; CREMONESI, L.; Salvatore, Francesco; Castaldo, Giuseppe; D'ALCAMO, E.; MAGGIO, A.; Sangiuolo, Federica; Dallapiccola, Bruno; MACERATESI, P.; Bisceglia, Luigi; GASPARINI, P.; Carbonara, A.O.; Bonizzato, Alberto; CABRINI, G.; Bombieri, Cristina; Pignatti, Pier Franco; BORGO, G.; Castellani, Carlo; VILLANI, A.; Arduino, Carlo; Salvatore, Donatello; Mastella, G; Piazza, Alberto

doi:10.1017/s0003480097006477

Cited by 58 publications

(47 citation statements)

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“…This condition is fulfilled if f obs -2.5SE is greater than the threshold. In the case of CF in southern Europe, the threshold is 0.004, since the global frequency of CF mutations in Europe is about 0.02, that of ∆F508 is about 0.01 in Italy (Bonizzato et al 1994;Rendine et al 1997), in Southern France (Claustres et al 1993), and in Spain (Estivill et al 1997), and the combined frequency of the other most common CF mutations is about 0.006. Therefore the probability that a C mutation is classified as being common (hence non-CF-causing) was calculated as follows: f obs must be at least equal to 0.004+2.5SE; this value f minimal is 0.025, 0.015, 0.012, and 0.009 when N is 380, 1000, 1500, and 3000, respectively.…”

Section: Discussionmentioning

confidence: 99%

A new approach for identifying non-pathogenic mutations. An analysis of the cystic fibrosis transmembrane regulator gene in normal individuals

Bombieri¹,

Giorgi²,

Carles³

et al. 2000

Human Genetics

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Given q as the global frequency of the alleles causing a disease, any allele with a frequency higher than q minus the cumulative frequency of the previously known disease-causing mutations (threshold) cannot be the cause of that disease. This principle was applied to the analysis of cystic fibrosis transmembrane conductance regulator (CFTR) mutations in order to decide whether they are the cause of cystic fibrosis. A total of 191 DNA samples from random individuals from Italy, France, and Spain were investigated by DGGE (denaturing gradient gel electrophoresis) analysis of all the coding and proximal non-coding regions of the gene. The mutations detected by DGGE were identified by sequencing. The sample size was sufficient to select essentially all mutations with a frequency of at least 0.01. A total of 46 mutations was detected, 20 of which were missense mutations. Four

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Section: Discussionmentioning

confidence: 99%

A new approach for identifying non-pathogenic mutations. An analysis of the cystic fibrosis transmembrane regulator gene in normal individuals

Bombieri¹,

Giorgi²,

Carles³

et al. 2000

Human Genetics

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“…Therefore, analysis of numerous mutations is required to obtain satisfactory carrier detection levels. 4 Based on published manuscripts [5][6][7] and the results of a survey of the various CF molecular genetic laboratories (European Concerted Action BMH4-CT96-0462, unpublished data (M Macek Jr, C Deltas, P Pachecco, (1999), personal communication)) we recommend a minimal number of mutations be assembled for each ethnic population (or region) to ensure detection of disease mutations in at least 80% of all carriers and patients (Tables 1 and 2). CF mutation detection methods can be divided into two groups: mutation detection (test DNA sample for presence or absence of one specific mutation), and mutation scanning methods (screen sample for any deviation from the standard sequence).…”

Section: Methodsmentioning

confidence: 99%

Recommendations for quality improvement in genetic testing for cystic fibrosis European Concerted Action on Cystic Fibrosis

et al. 2000

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These recommendations for quality improvement of cystic fibrosis genetic diagnostic testing provide general guidelines for the molecular genetic testing of cystic fibrosis in patients/individuals. General strategies for testing as well as guidelines for laboratory procedures, internal and external quality assurance, and for reporting the results, including the requirements of minimal services in mutation testing, the nomenclature for describing mutations, procedures to control false-positive amplification reactions and to validate tests, and guidelines to implement a quality system in a molecular diagnostic laboratory are reviewed.

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“…N1303K and G542X occur at a frequency of around 5% in Italy. 11 In Germany, a study of 658 CF families revealed mutation frequencies of R553X (1.8%), N1303K (1.3%), G542X (1.1%), G551D (0.8%) and R347P (0.8%). 12 The frequency of CFTR mutations recorded for just over 1000 patients for the Irish CF Database include G551D in 7%, R117H in 2% and DF508 in 72% of patients.…”

Section: Cftr Mutations In Caucasiansmentioning

confidence: 99%

Demographics of the UK cystic fibrosis population: implications for neonatal screening

et al. 2002

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Genetic history of cystic fibrosis mutations in Italy. I. Regional distribution

Cited by 58 publications

References 0 publications

A new approach for identifying non-pathogenic mutations. An analysis of the cystic fibrosis transmembrane regulator gene in normal individuals

A new approach for identifying non-pathogenic mutations. An analysis of the cystic fibrosis transmembrane regulator gene in normal individuals

Recommendations for quality improvement in genetic testing for cystic fibrosis European Concerted Action on Cystic Fibrosis

Demographics of the UK cystic fibrosis population: implications for neonatal screening

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