Highly Recurrent RET Mutations and Novel Mutations in Genes of the Receptor Tyrosine Kinase and Endothelin Receptor B Pathways in Chinese Patients with Sporadic Hirschsprung Disease

doi:10.1373/clinchem.2003.022061

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Clinical Chemistry 50: 93-100, 2004. First published November 18, 2003; 10.1373/clinchem.2003.022061

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	Molecular Diagnostics and Genetics

(Clinical Chemistry. 2004;50:93-100.)
© 2004 American Association for Clinical Chemistry, Inc.

Molecular Diagnostics and Genetics

Highly Recurrent RET Mutations and Novel Mutations in Genes of the Receptor Tyrosine Kinase and Endothelin Receptor B Pathways in Chinese Patients with Sporadic Hirschsprung Disease

Mercè Garcia-Barceló¹^,2, Mai-Har Sham², Wing-Shan Lee¹, Vincent Chi-Hang Lui¹, Benedict Ling-Sze Chen¹, Kenneth Kak-Yuen Wong¹, Joyce Suet-Wan Wong¹ and Paul Kwong-Hang Tam¹^,3^,a

¹ Division of Paediatric Surgery, Department of Surgery, University of Hong Kong Medical Center, Queen Mary Hospital, Hong Kong SAR, China.
² Department of Biochemistry and ³ Genome Research Centre, The University of Hong Kong, Hong Kong SAR, China.

^aAuthor for correspondence: Fax 852-2817-3155; e-mail paultam{at}hkucc.hku.hk.

Background: Hirschsprung disease (HSCR) is a congenital disordercharacterized by an absence of ganglion cells in the nerve plexusesof the lower digestive tract. HSCR has a complex pattern ofinheritance and is sometimes associated with mutations in genesof the receptor tyrosine kinase (RET) and endothelin receptorB (EDNRB) signaling pathways, which are crucial for developmentof the enteric nervous system.

Methods: Using PCR amplification and direct sequencing, we screenedfor mutations and polymorphisms in the coding regions and intron/exonboundaries of the RET, GDNF, EDNRB, and EDN3 genes of 84 HSCRpatients and 96 ethnically matched controls.

Results: We identified 10 novel and 2 previously described mutationsin RET, and 4 and 2 novel mutations in EDNRB and in EDN3, respectively.Potential disease-causing mutations were detected in 24% ofthe patients. The overall mutation rate was 41% in females and19% in males (P = 0.06). RET mutations occurred in 19% of thepatients. R114H in RET was the most prevalent mutation, representing7% of the patients or 37% of the patients with RET mutations.To date, such a high frequency of a single mutation has neverbeen reported in unrelated HSCR patients. Mutations in EDNRB,EDN3, and GDNF were found in four, two, and none of the patients,respectively. Two patients with mutations in genes of the EDNRBpathway also harbored a mutation in RET. Three novel and threereported polymorphisms were found in EDNRB, EDN3, and GDNF.

Conclusion: This study identifies additional HSCR disease-causingmutations, some peculiar to the Chinese population, and representsthe first comprehensive genetic analysis of sporadic HSCR diseasein Chinese.

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				M. Garcia-Barcelo, R. W. Ganster, V. C.H. Lui, T. Y.Y. Leon, M.-T. So, A. M.F. Lau, M. Fu, M.-H. Sham, J. Knight, M. S. Zannini, et al. TTF-1 and RET promoter SNPs: regulation of RET transcription in Hirschsprung's disease Hum. Mol. Genet., January 15, 2005; 14(2): 191 - 204. [Abstract] [Full Text] [PDF]

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