Consensus on the use and interpretation of cystic fibrosis mutation analysis in clinical practice

Castellani, Carlo; Cuppens, Harry; Maçek, Milan; Cassiman, Jean Jacques; Kerem, Eitan; Durie, Peter R.; Tullis, Elizabeth; Assael, B.M.; Bombieri, Cristina; Brown, Anthony; Casals, Teresa; Claustres, Mireille; Cutting, Garry R.; Dequeker, Elisabeth; Dodge, J A; Doull, Iolo; Farrell, Philip M.; Férec, Claude; Girodon, Emmanuelle; Johannesson, Marie; Kerem, Batsheva; Knowles, Michael R.; Munck, À.; Pignatti, Pierfranco; Radojković, Dragica; Rizzotti, Paolo; Schwarz, Martin; Stuhrmann, Manfred; Tzetis, Maria; Zielenski, Julian; Elborn, J. Stuart

doi:10.1016/j.jcf.2008.03.009

Cited by 507 publications

(495 citation statements)

References 143 publications

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“…Strom et al 7 advocate against adding these variants to CF panels, stating that detection of D1152H and L206W during carrier screening may increase the rate of pregnancy termination among parents who fear having a child with classic CF, not to mention inflating the mutation detection rate among Hispanic Americans. 7 It is acknowledged now in the literature that the D1152H variant belongs to both the CF-causing and CFTR-related disorder groups, [19][20][21] and, in conjunction with an established CF-causing mutation, it could still manifest as typical CF. 19,22 Burgel et al 23 studied 42 patients with D1152H mutations and reported that the variant, in conjunction with a CF-causing mutation, can cause significant pulmonary disease, albeit with longer survival.…”

Section: Discussionmentioning

confidence: 99%

“…7 It is acknowledged now in the literature that the D1152H variant belongs to both the CF-causing and CFTR-related disorder groups, [19][20][21] and, in conjunction with an established CF-causing mutation, it could still manifest as typical CF. 19,22 Burgel et al 23 studied 42 patients with D1152H mutations and reported that the variant, in conjunction with a CF-causing mutation, can cause significant pulmonary disease, albeit with longer survival. One of the authors of this article observed similar results (K.J.F., unpublished data).…”

Section: Discussionmentioning

confidence: 99%

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Cystic fibrosis carrier screening in a North American population

Zvereff¹,

Faruki²,

Edwards³

et al. 2014

Genetics in Medicine

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Methods:Patients referred for cystic fibrosis screening from January 2005 through December 2010 were tested using either a 32-mutation panel (n = 1,601,308 individuals) or a 69-mutation panel (n = 109,830). Results:The carrier frequencies observed for the 69-mutation panel study population (1/36) and Caucasian (1/27) and African-American individuals (1/79) agree well with published cystic fibrosis carrier frequencies; however, a higher carrier frequency was observed for Hispanic-American individuals (1/48) using the 69-mutation panel as compared with the 32-mutation panel (1/69). The 69-mutation panel detected ~20% more mutations than the 32-mutation panel for both African-American and Hispanic-American individuals. Conclusion:Expanded panels using race-specific variants can improve cystic fibrosis carrier detection rates within specific populations. However, it is important that the pathogenicity and the relative frequency of these variants are confirmed. Genet Med advance online publication 19 December 2013

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Cystic fibrosis carrier screening in a North American population

Zvereff¹,

Faruki²,

Edwards³

et al. 2014

Genetics in Medicine

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“…Their decisions are based on expert consensus and best practice guidelines, and depend on the clinical indication in the case. [13][14][15][16] Two assessors independently evaluate genotypes and interpretation in the submitted reports. Results are also discussed during an assessment meeting.…”

Section: Context and Setting Of The Studymentioning

confidence: 99%

“…Interpretation could additionally be influenced by external factors such as the availability of best practice guidelines and publications. [13][14][15] Second, the presence in clinical reports of all investigated interpretation elements improved over the years. Two elements increased remarkably more (430%) than others: stating the need to test the parents of a CF patient to confirm homozygosity or compound heterozygosity (need for qualification of the genotype) and Interpretation in CF laboratory reports S Berwouts et al mentioning the possibility of testing the relatives.…”

Section: Principal Findingsmentioning

confidence: 99%

Improvement of interpretation in cystic fibrosis clinical laboratory reports: longitudinal analysis of external quality assessment data

et al. 2012

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Participation in external quality assessment (EQA) is a key element of quality assurance in medical laboratories. In genetics EQA, both genotyping and interpretation are assessed. We aimed to analyse changes in the completeness of interpretation in clinical laboratory reports of the European cystic fibrosis EQA scheme and to investigate the effect of the number of previous participations, laboratory accreditation/certification status, setting and test volume. We distributed similar versions of mock clinical cases to eliminate the influence of the difficulty of the clinical question on interpretation performance: a cystic fibrosis patient (case 1) and a cystic fibrosis carrier (case 2). We then performed a retrospective longitudinal study of reports over a 6-year period from 298 participants for case 1 (2004, 2008, 2009) and from 263 participants for case 2 (2006, 2008, 2009). The number of previous participations had a positive effect on the interpretation score (Po0.0001), whereas the laboratory accreditation/certification status, setting and test volume had no effect. Completeness of interpretation improved over time. The presence of the interpretation element 'requirement for studying the parents to qualify the genotype' increased most (from 49% in 2004 to 93% in 2009). We still observed room for improvement for elements that concerned offering testing for familial mutations in relatives and prenatal/preimplantation diagnosis (16% and 24% omission, respectively, for case 1 in 2009). Overall, regular participation in external quality assessment contributes to improved interpretation in reports, with potential value for quality of care for patients and families by healthcare professionals involved in genetic testing.

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“…Mutations in the cystic fibrosis transmembrane conductance regulator gene (CFTR/ABCC7; MIM #602421) induce a wide spectrum of clinical phenotypes from classic CF characterized by pancreatic insufficiency and positive sweat chloride values, to milder forms of the disease with pancreatic sufficiency, to CFTR related disorders (CFTR-RDs), where a diagnosis of CF cannot be established because the individual does not meet standard diagnostic criteria (Farrell et al 2008;Castellani et al 2008). …”

mentioning

confidence: 99%