Molecular and clinical analysis of patients with classic and Duarte galactosemia in western Hungary

Milánkovics, Ilona; Schuler, Ágnes; Kámory, Enikő; Csókay, Béla; Fodor, F; Somogyi, Csilla; Németh, Krisztína; Fekete, György

doi:10.1007/s00508-010-1311-7

Cited by 10 publications

(11 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…The frequency of the mutations (between 45 and 93.6%) was reported to be as follows in different countries: Ireland, 93.6%; 17 Great Britain, 77%; 3 Portugal, 57.8%; 18 The Netherlands, 58.5%; 19 Spain, 50%; 18 Germany, 69%; 20 Austria, 60%; 21 Poland, 51.3%; 22 the Czech Republic and the Slovak Republic, 46%; 7 and Hungary, 45%. 23 As in these European countries, it was also found to be the most common disease-causing mutation in the Turkish population, and presented data strengthen the observed pattern that the frequency of the Q188R mutation decreases from the west to the east and from the north to the south in the European continent. 24 In the present study on the Turkish population, K285N is seen only in 3.57% of the population.…”

Section: Discussionsupporting

confidence: 79%

“…The frequency of this mutant allele varies from 19 to 33.8% in different European populations. 7,[20][21][22][23] In contrast to these high frequencies observed and reported above, some populations have a low allele frequency for this mutation, with distribution between 2.4 and 9.8% in European countries. 18,19,25 These three mutant alleles, A320T (7.14%), E340* (10.71%) and M142K (6.25%), are the second in terms of frequency in Turkish patients and are observed more commonly than in other populations.…”

Section: Discussionmentioning

confidence: 93%

See 1 more Smart Citation

Galactosemia in the Turkish population with a high frequency of Q188R mutation and distribution of Duarte-1 and Duarte-2 variations

et al. 2013

View full text Add to dashboard Cite

Classical galactosemia is an inherited recessive disorder of galactose metabolism caused by deficiency of the enzyme galactose-1-phosphate uridyl transferase (GALT), which is caused by mutations in the GALT gene. In this study, 56 Turkish patients diagnosed with galactosemia were screened for GALT gene mutations using Affymetrix resequencing microarrays. Eleven types of mutations were detected in these patients, including two novel mutations (R258G and G310fsX49) and nine recurrent mutations. We detected six patients who were homozygous for the E340* mutation and for N314D, L218L silent substitutions (Duarte-1 variant) in this study. The haplotype E340*, N314D and L218L has been reported only in Turkish patients, which suggests that the E340* mutation is specific for our population and might be spread by a Turk ancestor. In patients, the Duarte-1 allele was found with a frequency of 10.71%, whereas the Duarte-2 allele was not detected. Duarte-1 and Duarte-2 alleles were found to be present at a frequency of 2.3% and 1.4%, respectively, in the screening of 105 healthy individuals. Considering all detected mutations, it is a very important finding that exons 6 and 10 of the GALT gene account for 79% of all mutant alleles in the Turkish population. The most common mutation is Q188R, with a frequency of 55.35%.

show abstract

Section: Discussionsupporting

confidence: 79%

Section: Discussionmentioning

confidence: 93%

Galactosemia in the Turkish population with a high frequency of Q188R mutation and distribution of Duarte-1 and Duarte-2 variations

et al. 2013

View full text Add to dashboard Cite

show abstract

“…Step 5 Greber-Platzer et al 1997;Itemetal.2002;Kozak et al 2000;Milankovics et al 2010;Murphyetal.1999;Ng et al 1994;Ounap et al 2010;Suzuki et al 2001;Tyfield et al 1999;V i g g i a n oe ta l .2015; Zekanowski et al 1999 (Kozak et al 2000;Milankovics et al 2010;Zekanowskietal.1999). Two studies coming from these countries showed that subjects homozygous for p.Q188R or p.K285N exhibit nil enzyme activity, severe newborn symptoms and long-term complications.…”

Section: Aetiology and Pathophysiologymentioning

confidence: 99%

“…Duarte 2, variant galactosaemia (heterozygocity for the Duarte muation p. Asn314Asp (pN314D) and a classic galactosaemia allele), were found in 2-15 % of populations (Greber-Platzer et al 1997;Kozak et al 2000;Milankovics et al 2010;Suzuki et al 2001). Patients with Duarte 2 galactosaemia presented reduced enzyme activity (≤25 %) and 0 or mild symptomatology and good long-term prognosis in the study performed by Milankovics et al (2010). This study identified two siblings with p.Gln188Arg/ p.Glu146Asp heterozygous genotypes, who also showed approximately 25 % of normal activity and mild symptomatology.…”

Section: Aetiology and Pathophysiologymentioning

confidence: 99%

“…Schweitzer et al (1993)alsoreported that exchange transfusion was necessary in 36 % of the 134 patients identified in 25 children's hospitals in Germany (30 %-40 % potential number of galactosaemia cases). In Hungary (Milankovics et al 2010) and Italy (Viggiano et al 2015) > 90 % of newborns presented symptomatology before screening (day 4-5), 72.7 % of a severe nature. In Estonia, the mean age at hospitalisation of the nine symptomatic cases detected through screening was 12 days, with final diagnosis at 19 days (Ounap et al 2010).…”

Section: Clinical Presentation Of the Diseasementioning

confidence: 99%

See 1 more Smart Citation

Appropriateness of newborn screening for classic galactosaemia: a systematic review

Varela-Lema¹,

Paz-Valiñas²,

Atienza-Merino³

et al. 2016

J of Inher Metab Disea

View full text Add to dashboard Cite

Currently, there is no universal agreement on galactosaemia screening, fundamentally because of the risk-benefit uncertainties. We conducted two exhaustive systematic searches in the main electronic databases (PubMed, Embase, Cochrane, etc.) to recover relevant information about the disease and screening test/s in order to support decision making in Spain. All of the 45 studies identified that covered disease issues were retrospective case series or cross-sectional analysis (level-4 evidence). Studies consistently found that the majority of patients presented characteristic symptomatology before diagnosis. Long term disabilities were not significantly correlated with age of diagnosis, onset of dietary restriction or strict diet compliance. The five studies that provided accuracy data used different cut-off points and verification tests, and thus differed in their definitions of a positive case (level-3b evidence). The estimated sensitivity was 100 % and the specificity 99.9 %. The false-positive rate ranged from 0.0005 % to 0.25 %, and the PPV from 0 % to 64.3 %. The comparative clinical effectiveness in relation to not screening or implementation of other programs is unknown. In summary, existing evidence remains insufficient to establish the appropriateness of newborn screening for galactosaemia screening, although health benefits could be expected if early diagnosis and treatment is achieved. If screening is implemented in Spain, it would be important that a pilot programme be implemented to assess false positive rate and ensure that early diagnosis is not delayed.

show abstract

Alterations of galactose metabolism caused by deficit of galactose-1-phosphate uridylyltransferase activity: An overview of galactosemia type I

Lucca

Casique

Cornejo

2019

Molecular Nutrition: Carbohydrates

View full text Add to dashboard Cite

Molecular and clinical analysis of patients with classic and Duarte galactosemia in western Hungary

Abstract: The most serious clinical phenotypes in our population were associated with mutations p. Q188R, p.K285N, p.X380R, p.S297P, p.M142K, p.R.204X, p.Q169K and p.R407P, but manifestations depend on other genetic and environmental factors.

Cited by 10 publications

References 29 publications

Galactosemia in the Turkish population with a high frequency of Q188R mutation and distribution of Duarte-1 and Duarte-2 variations

Galactosemia in the Turkish population with a high frequency of Q188R mutation and distribution of Duarte-1 and Duarte-2 variations

Appropriateness of newborn screening for classic galactosaemia: a systematic review

Alterations of galactose metabolism caused by deficit of galactose-1-phosphate uridylyltransferase activity: An overview of galactosemia type I

Contact Info

Product

Resources

About