Birth defects are preventable[1]

 

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Birth defects - or by according to the World Health Organization’s term: congenital anomalies - are structural, functional and/or biochemical-molecular defects present at birth whether detected at that time or not. Among different categories of birth defects, congenital abnormalities (CAs), i. e. structural-morphological defects represent the largest one.

CAs have two main characteristics: (i) defect conditions with a limited chance for complete recovery and (ii) the earliest (fetal or birth) onset. Thus, there is only one optimal medical solution for CAs and this is prevention. It is worth differentiating three levels of prevention (Tab. [1]), however, the efficacy of primary prevention was limited before 1990 [1].

There was a breakthrough in the primary prevention of CAs in the 1990 s and it was connected with the introduction of periconceptional folic acid or folic acid-containing multivitamin supplementation. First the prevention of recurrent neural-tube defects (NTD) by a folic acid (0.36mg)-containing multivitamin preparation used during at least one month before and three months after conception (i. e. periconceptional period) was shown in a non-randomized intervention study (Tab. [2]) [2] [3]. However, the results of this study were not accepted by some experts due to the possible social selection. Thus, the Medical Research Council (UK) organized a multicenter international randomized controlled trial (RCT) in which 43 % of participants came from Hungary. This trial indicated the efficacy of a large pharmacological dose (4 mg) of folic acid in the prevention of recurrent NTD (Tab. [2]) [4].

Table 1 Prevention of congenital abnormalities (CAs) Primary: avoidance of the causes of CAs- rubella vaccination- avoidance of teratogens (alcohol, drug, diabetes)- genetic counselling (reduction of recurrent CAs) Secondary: early detection and medical treatment- neonatal PKU, etc. and orthopaedic screening- prenatal diagnosis and selective abortion (?) = chromosomal aberrations, gene mutations, CAs- specific postnatal treatment = undescended testis, patent ductus arteriosus Tertiary: early surgical correction without residual effect e. g., cardiovascular CAs, pyloric stenosis, etc.

Table 2 Data and results of previous intervention studies for the reduction of recurrent NTD Type Method Location Supplement Risk Reduction Recurrence non-randomized Yorkshire 2 North. Ireland 3 Multivitamin(0.36 mg Folic Acid) 91 %83 % randomized Multicenter MRC 4 Folic Acid (4.0 mg) 71 %

1 Summary of a lecture held at the 9th symposium of Gesellschaft für angewandte Vitaminforschung e.V. - GVF. Bonn, 28.06.2006.

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1 Summary of a lecture held at the 9th symposium of Gesellschaft für angewandte Vitaminforschung e.V. - GVF. Bonn, 28.06.2006.

Prof. Andrew E. Czeizel

Scientific Director of the Foundation for the Community Control of Hereditary Diseases

Budapest, Hungary