Your search keyword '"István Sziklai"' showing total 4 results

1. GJB2 mutations in patients with non-syndromic hearing loss from Northeastern Hungary

Author

Tímea, Tóth, Susan, Kupka, Birgit, Haack, Kathrin, Riemann, Simone, Braun, Ferenc, Fazakas, Hans-Peter, Zenner, László, Muszbek, Nikolaus, Blin, Markus, Pfister, and István, Sziklai

Subjects

Adult, Male, Hungary, Adolescent, DNA Mutational Analysis, Infant, Middle Aged, Connexins, Pedigree, Connexin 26, Gene Frequency, Child, Preschool, Mutation, Humans, Female, Child, Hearing Loss, Aged

Abstract

Mutations in the GJB2 gene encoding the gap-junction protein connexin 26 have been identified in many patients with childhood hearing impairment (HI). One single mutation, c.35delG, accounts for the majority of mutations in Caucasian patients with HI. In the present study we screened 500 healthy control individuals and a group of patients with HI from Northeastern Hungary for GJB2 mutations. The patients' group consisted of 102 familial from 28 families and 92 non-familial cases. The most common mutation in the Hungarian population is the c.35delG, followed by the c.71GA (p.W24X) mutation. 34.3% of the patients in the familial group were homozygous, and 17.6% heterozygous for 35delG. In the non-familial group the respective values were 37% and 18% (allele frequency: 46.2%). In the general population an allele frequency of 2.4% was determined. Several patients were identified with additional, already described or new GJB2 mutations, mostly in heterozygous state. The mutation c.380GA (p.R127H) was formerly found only in heterozygous state and its disease relation was controversial. We demonstrated the presence of this mutation in a family with three homozygous patients and 4 heterozygous unaffected family members, a clear indication of recessively inherited HI. Furthermore, we provided evidence for the pathogenic role of two new mutations, c.51CA (p.S17Y) and c.177GT (p.G59V), detected in the present study. In the latter case the pattern of inheritance might be dominant. Our results confirm the importance of GJB2 mutations in the Hungarian population displaying mutation frequencies that are comparable with those in the Mediterranean area.

Published

2004

2. Mutation A1555G in the 12S rRNA gene and its epidemiological importance in German, Hungarian, and Polish patients

Author

Susan, Kupka, Tímea, Tóth, Maciej, Wróbel, Ulrike, Zeissler, Witold, Szyfter, Krzysztof, Szyfter, Grazyna, Niedzielska, Jerzy, Bal, Hans-Peter, Zenner, István, Sziklai, Nikolaus, Blin, and Markus, Pfister

Subjects

Adult, Male, Hungary, Alanine, Hearing Loss, Sensorineural, Glycine, Infant, Middle Aged, Pedigree, Amino Acid Substitution, RNA, Ribosomal, Child, Preschool, Germany, Mutation, Humans, Female, Genetic Predisposition to Disease, Genetic Testing, Poland, Child, Aged

Abstract

The A1555G mutation in the 12SrRNA gene has been associated with aminoglycoside induced and nonsyndromic sensorineural hearing impairment. In this study we analyzed Hungarian, Polish and German patients with nonsyndromic severe to profound hearing impairment of unknown origin for this mutation. The frequency of the A1555G mutation in the Hungarian hearing impaired population was below 1.8 %. Three out of 125 Polish patients carrying the A1555G mutation were identified. Among German patients one carrier was found (0.7 %) revealing a homoplastic A1555G mutation, whereas no mutation was detected in control individuals with normal hearing (frequency0.6%). In summary the frequencies of the A1555G mutation are low in the hearing impaired as well as in the normal population in Hungary, Poland and Germany. Since the importance of this mutation and its relationship with aminoglycoside exposure is not well understood yet, patients with nonsyndromic hearing impairment should be routinely screened for this mutation to avoid aminoglycoside induced hearing impairment due to increased sensitivity of maternal relatives.

Published

2002

3. GJB2mutations in patients with non-syndromic hearing loss from Northeastern Hungary

Author

István Sziklai, Nikolaus Blin, Simone Braun, Tímea Tóth, Hans-Peter Zenner, László Muszbek, Birgit Haack, Susan Kupka, Markus Pfister, Kathrin Riemann, and Ferenc Fazakas

Subjects

Genetics, education.field_of_study, Hearing loss, Population, Disease, Biology, Gjb2 gene, Mutation (genetic algorithm), medicine, In patient, medicine.symptom, education, Allele frequency, Genetics (clinical), Non syndromic

Abstract

Mutations in the GJB2 gene encoding the gap-junction protein connexin 26 have been identified in many patients with childhood hearing impairment (HI). One single mutation, c.35delG, accounts for the majority of mutations in Caucasian patients with HI. In the present study we screened 500 healthy control individuals and a group of patients with HI from Northeastern Hungary for GJB2 mutations. The patients' group consisted of 102 familial from 28 families and 92 non-familial cases. The most common mutation in the Hungarian population is the c.35delG, followed by the c.71G>A (p.W24X) mutation. 34.3% of the patients in the familial group were homozygous, and 17.6% heterozygous for 35delG. In the non-familial group the respective values were 37% and 18% (allele frequency: 46.2%). In the general population an allele frequency of 2.4% was determined. Several patients were identified with additional, already described or new GJB2 mutations, mostly in heterozygous state. The mutation c.380G>A (p.R127H) was formerly found only in heterozygous state and its disease relation was controversial. We demonstrated the presence of this mutation in a family with three homozygous patients and 4 heterozygous unaffected family members, a clear indication of recessively inherited HI. Furthermore, we provided evidence for the pathogenic role of two new mutations, c.51C>A (p.S17Y) and c.177G>T (p.G59V), detected in the present study. In the latter case the pattern of inheritance might be dominant. Our results confirm the importance of GJB2 mutations in the Hungarian population displaying mutation frequencies that are comparable with those in the Mediterranean area.

Published

2004

4. Mutation A1555G in the 12S rRNA gene and its epidemiological importance in German, Hungarian, and Polish patients

Author

Markus Pfister, Grazyna Niedzielska, István Sziklai, Ulrike Zeissler, Maciej Wróbel, Jerzy Bal, Nikolaus Blin, Krzysztof Szyfter, Tímea Tóth, Hans-Peter Zenner, Witold Szyfter, and Susan Kupka

Subjects

Genetics, Pediatrics, medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, Hearing loss, Aminoglycoside, Population, Biology, humanities, Mutation (genetic algorithm), Epidemiology, otorhinolaryngologic diseases, medicine, Profound hearing impairment, medicine.symptom, education, Gene, Genetics (clinical), Genetic testing

Abstract

The A1555G mutation in the 12SrRNA gene has been associated with aminoglycoside induced and nonsyndromic sensorineural hearing impairment. In this study we analyzed Hungarian, Polish and German patients with nonsyndromic severe to profound hearing impairment of unknown origin for this mutation. The frequency of the A1555G mutation in the Hungarian hearing impaired population was below 1.8 %. Three out of 125 Polish patients carrying the A1555G mutation were identified. Among German patients one carrier was found (0.7 %) revealing a homoplastic A1555G mutation, whereas no mutation was detected in control individuals with normal hearing (frequency < 0.6%). In summary the frequencies of the A1555G mutation are low in the hearing impaired as well as in the normal population in Hungary, Poland and Germany. Since the importance of this mutation and its relationship with aminoglycoside exposure is not well understood yet, patients with nonsyndromic hearing impairment should be routinely screened for this mutation to avoid aminoglycoside induced hearing impairment due to increased sensitivity of maternal relatives.

Published

2002