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  Česky / Czech version Čes.-slov. Pediat., 2007, roč. 62, č. 4, s. 187-195.
 
Newborn Screening for Cystic Fibrosis in the Czech Republic: Results of a Pilot Study  
Holubová A.1*, Balaščáková M.1*, Skalická V.2, Kračmar P.3, Piskáčková T.1, Vávrová V.2, Zemkova D.2, Gonsorčíková L.3, Lebl J.2, Macek M.111I.1, Votava F.3 

Ústav biologie a lékařské genetiky UK 2. LF a FN Motol, Praha1 přednosta prof. MUDr. M. Macek ml., DrSc. Pediatrická klinika UK 2. LF a FN Motol, Praha2 přednosta prof. MUDr. J. Lebl, CSc. Klinika dětí a dorostu UK 3. LF a FN Královské Vinohrady, Praha3 přednosta doc. MUDr. F. Votava, PhD.
 


Summary:

       Early diagnosis of cystic fibrosis (CF) is considered as a favorable prognostic factor and as a hallmark of a properly functioning health care systém. During the last deca-de evidence for deterioration of early clinical diagnosis of CF in the Czech Republic became evident. This alarming fact led us to commence a CF newborn screening (NBS) pilot project in order to assess its feasibility as an efficient tool for uniform and early diagnosis of CF in our country. Concentrations of immunoreactive trypsin (IRT) in dried blood spots (Guthrie cards) were examined in 76438 newborns born between 1. 2. 2005 and 2. 11. 2006 within a region comprising 62% of the entire Czech populati-on. IRT concentration of 75 ng/ml and higher was found in 799 newborns, i.e. 1.05% of the total. Since these newborns were considered at high risk of CF and panels of popu-lation specific mutations of the gene CFTR were analysed from respective blood spots. The five most common mutations of gene CFTR (comprising 83.8% of alleles in CF pa-tients in CR) were investigated if the concentration of IRT was within the range of 75-150 ng/ml. In addition, 38 CFTR gene mutations (comprising 90.8% of CF alleles in CR) were examined in blood spots where the concentration of IRT was more than 150 ng/ml and/or if one CFTR gene mutation was found in a dried blood spot with a lower IRT concentration. Two CFTR gene mutations were found in 11 newborns, confirming the diagnosis of CF. A single CFTR mutation was found in 53 newborns. All such cases were subjected to sweat testing, which was finished in all but 6 newborns. The sweat test was positi¬ve (ď level >60 mmol/1) in one newborn with one CFTR gene mutation, in one newborn borderline levels were detected (Cl" level 30-40 mmol/1, which indicated his long-term follow-up) and in other 45 newborns the sweat test was negative (Cl" level <30 mmol/1) - unaffected carries. Over the course of our project 12 infants were diagnosed as having CF. The medián of age at diagnosis was 37 days. Interestingly, 4 of these cases were diagnosed clinical-ly prior the results of NBS. If data of NBS would háve been ušed alone the extrapola-ted incidence of the disease (1:6369 newborns) was surprisingly lower than that estab-lished epidemiologically (1:2736 newborns). This discrepancy could be explained by: 1. a relatively small number of examined newborns, i.e. error due to a small number of studied subjects; 2. falše negativity of utilised screening algorithm, which is however unlikely; 3. impact of prenatal diagnosis where parents háve opted for selected termination of pregnancy. Authors conclude that the NBS for CF in conditions of the Czech Republic is an effective tool for early and broad based diagnosis of CF. It also complements the cur-rent deterioration of early clinical diagnosis of the disease. Nevertheless, an unanswe-red question remains if really all cases of incident CF were ascertained, which neces-sitates further studies.

        Key words: cystic fibrosis (OMIM 219700), newborn screening, immunoreactive tryp-sin/trypsinogen, CFTR gene, molecular genetic testing
       

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