Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics

Gabriele Wildhardt; Birgit Zirn; Luitgard M Graul-Neumann; Juliane Wechtenbruch; Markus Suckfüll; Annegret Buske; Axel Bohring; Christian Kubisch; Stefanie Vogt; Gertrud Strobl-Wildemann; Marie Greally; Oliver Bartsch; Daniela Steinberger

doi:10.1136/bmjopen-2012-001917

Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics

Standard

Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics. / Wildhardt, Gabriele; Zirn, Birgit; Graul-Neumann, Luitgard M; Wechtenbruch, Juliane; Suckfüll, Markus; Buske, Annegret; Bohring, Axel; Kubisch, Christian; Vogt, Stefanie; Strobl-Wildemann, Gertrud; Greally, Marie; Bartsch, Oliver; Steinberger, Daniela.

In: BMJ OPEN, Vol. 3, No. 3, 01.01.2013.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Wildhardt, G, Zirn, B, Graul-Neumann, LM, Wechtenbruch, J, Suckfüll, M, Buske, A, Bohring, A, Kubisch, C, Vogt, S, Strobl-Wildemann, G, Greally, M, Bartsch, O & Steinberger, D 2013, 'Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics', BMJ OPEN, vol. 3, no. 3. https://doi.org/10.1136/bmjopen-2012-001917

APA

Wildhardt, G., Zirn, B., Graul-Neumann, L. M., Wechtenbruch, J., Suckfüll, M., Buske, A., Bohring, A., Kubisch, C., Vogt, S., Strobl-Wildemann, G., Greally, M., Bartsch, O., & Steinberger, D. (2013). Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics. BMJ OPEN, 3(3). https://doi.org/10.1136/bmjopen-2012-001917

Vancouver

Wildhardt G, Zirn B, Graul-Neumann LM, Wechtenbruch J, Suckfüll M, Buske A et al. Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics. BMJ OPEN. 2013 Jan 1;3(3). https://doi.org/10.1136/bmjopen-2012-001917

Bibtex

@article{2671f693f7224e64b53eca7a16eabe98,

title = "Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics",

abstract = "OBJECTIVES: Till date, mutations in the genes PAX3 and MITF have been described in Waardenburg syndrome (WS), which is clinically characterised by congenital hearing loss and pigmentation anomalies. Our study intended to determine the frequency of mutations and deletions in these genes, to assess the clinical phenotype in detail and to identify rational priorities for molecular genetic diagnostics procedures.DESIGN: Prospective analysis.PATIENTS: 19 Caucasian patients with typical features of WS underwent stepwise investigation of PAX3 and MITF. When point mutations and small insertions/deletions were excluded by direct sequencing, copy number analysis by multiplex ligation-dependent probe amplification was performed to detect larger deletions and duplications. Clinical data and photographs were collected to facilitate genotype-phenotype analyses.SETTING: All analyses were performed in a large German laboratory specialised in genetic diagnostics.RESULTS: 15 novel and 4 previously published heterozygous mutations in PAX3 and MITF were identified. Of these, six were large deletions or duplications that were only detectable by copy number analysis. All patients with PAX3 mutations had typical phenotype of WS with dystopia canthorum (WS1), whereas patients with MITF gene mutations presented without dystopia canthorum (WS2). In addition, one patient with bilateral hearing loss and blue eyes with iris stroma dysplasia had a de novo missense mutation (p.Arg217Ile) in MITF. MITF 3-bp deletions at amino acid position 217 have previously been described in patients with Tietz syndrome (TS), a clinical entity with hearing loss and generalised hypopigmentation.CONCLUSIONS: On the basis of these findings, we conclude that sequencing and copy number analysis of both PAX3 and MITF have to be recommended in the routine molecular diagnostic setting for patients, WS1 and WS2. Furthermore, our genotype-phenotype analyses indicate that WS2 and TS correspond to a clinical spectrum that is influenced by MITF mutation type and position.",

author = "Gabriele Wildhardt and Birgit Zirn and Graul-Neumann, {Luitgard M} and Juliane Wechtenbruch and Markus Suckf{\"u}ll and Annegret Buske and Axel Bohring and Christian Kubisch and Stefanie Vogt and Gertrud Strobl-Wildemann and Marie Greally and Oliver Bartsch and Daniela Steinberger",

year = "2013",

month = jan,

day = "1",

doi = "10.1136/bmjopen-2012-001917",

language = "English",

volume = "3",

journal = "BMJ OPEN",

issn = "2044-6055",

publisher = "British Medical Journal Publishing Group",

number = "3",

}

RIS

TY - JOUR

T1 - Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics

AU - Wildhardt, Gabriele

AU - Zirn, Birgit

AU - Graul-Neumann, Luitgard M

AU - Wechtenbruch, Juliane

AU - Suckfüll, Markus

AU - Buske, Annegret

AU - Bohring, Axel

AU - Kubisch, Christian

AU - Vogt, Stefanie

AU - Strobl-Wildemann, Gertrud

AU - Greally, Marie

AU - Bartsch, Oliver

AU - Steinberger, Daniela

PY - 2013/1/1

Y1 - 2013/1/1

N2 - OBJECTIVES: Till date, mutations in the genes PAX3 and MITF have been described in Waardenburg syndrome (WS), which is clinically characterised by congenital hearing loss and pigmentation anomalies. Our study intended to determine the frequency of mutations and deletions in these genes, to assess the clinical phenotype in detail and to identify rational priorities for molecular genetic diagnostics procedures.DESIGN: Prospective analysis.PATIENTS: 19 Caucasian patients with typical features of WS underwent stepwise investigation of PAX3 and MITF. When point mutations and small insertions/deletions were excluded by direct sequencing, copy number analysis by multiplex ligation-dependent probe amplification was performed to detect larger deletions and duplications. Clinical data and photographs were collected to facilitate genotype-phenotype analyses.SETTING: All analyses were performed in a large German laboratory specialised in genetic diagnostics.RESULTS: 15 novel and 4 previously published heterozygous mutations in PAX3 and MITF were identified. Of these, six were large deletions or duplications that were only detectable by copy number analysis. All patients with PAX3 mutations had typical phenotype of WS with dystopia canthorum (WS1), whereas patients with MITF gene mutations presented without dystopia canthorum (WS2). In addition, one patient with bilateral hearing loss and blue eyes with iris stroma dysplasia had a de novo missense mutation (p.Arg217Ile) in MITF. MITF 3-bp deletions at amino acid position 217 have previously been described in patients with Tietz syndrome (TS), a clinical entity with hearing loss and generalised hypopigmentation.CONCLUSIONS: On the basis of these findings, we conclude that sequencing and copy number analysis of both PAX3 and MITF have to be recommended in the routine molecular diagnostic setting for patients, WS1 and WS2. Furthermore, our genotype-phenotype analyses indicate that WS2 and TS correspond to a clinical spectrum that is influenced by MITF mutation type and position.

AB - OBJECTIVES: Till date, mutations in the genes PAX3 and MITF have been described in Waardenburg syndrome (WS), which is clinically characterised by congenital hearing loss and pigmentation anomalies. Our study intended to determine the frequency of mutations and deletions in these genes, to assess the clinical phenotype in detail and to identify rational priorities for molecular genetic diagnostics procedures.DESIGN: Prospective analysis.PATIENTS: 19 Caucasian patients with typical features of WS underwent stepwise investigation of PAX3 and MITF. When point mutations and small insertions/deletions were excluded by direct sequencing, copy number analysis by multiplex ligation-dependent probe amplification was performed to detect larger deletions and duplications. Clinical data and photographs were collected to facilitate genotype-phenotype analyses.SETTING: All analyses were performed in a large German laboratory specialised in genetic diagnostics.RESULTS: 15 novel and 4 previously published heterozygous mutations in PAX3 and MITF were identified. Of these, six were large deletions or duplications that were only detectable by copy number analysis. All patients with PAX3 mutations had typical phenotype of WS with dystopia canthorum (WS1), whereas patients with MITF gene mutations presented without dystopia canthorum (WS2). In addition, one patient with bilateral hearing loss and blue eyes with iris stroma dysplasia had a de novo missense mutation (p.Arg217Ile) in MITF. MITF 3-bp deletions at amino acid position 217 have previously been described in patients with Tietz syndrome (TS), a clinical entity with hearing loss and generalised hypopigmentation.CONCLUSIONS: On the basis of these findings, we conclude that sequencing and copy number analysis of both PAX3 and MITF have to be recommended in the routine molecular diagnostic setting for patients, WS1 and WS2. Furthermore, our genotype-phenotype analyses indicate that WS2 and TS correspond to a clinical spectrum that is influenced by MITF mutation type and position.

U2 - 10.1136/bmjopen-2012-001917

DO - 10.1136/bmjopen-2012-001917

M3 - SCORING: Journal article

C2 - 23512835

VL - 3

JO - BMJ OPEN

JF - BMJ OPEN

SN - 2044-6055

IS - 3

ER -