Genomic Variation in Multigenic Traits: Hirschsprung Disease

  1. A.S. MCCALLION,
  2. E.S. EMISON,
  3. C.S. KASHUK,
  4. R.T. BUSH,
  5. M. KENTON,
  6. M.M. CARRASQUILLO,
  7. K.W. JONES,
  8. G.C. KENNEDY,
  9. M.E. PORTNOY,
  10. E.D. GREEN, and
  11. A. CHAKRAVARTI
  1. *McKusick-Nathans Institute of Genetic Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205; Affymetrix, Santa Clara, California 95051; Genome Technology Branch, National Human Genome Research Institute, National Institutes of Health, Bethesda, Maryland 20892

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Excerpt

Recent advances in genomic technology and the availability of a finished human genome sequence havegreatly facilitated the identification of genes underlyinghuman Mendelian disorders. The contemporary challenge lies in the elucidation of complex disorders. Classically, the transmission of a Mendelian disorder is explained by the exact co-segregation of a single mutationwith the phenotype. Such mutations are absent in controlsand, most frequently, involve conserved coding sequences. These observations are in stark contrast to thecomplex non-Mendelian diseases, wherein mutations atsingle genes do occur in unaffecteds, and variants withweak or moderate quantitative effects on the phenotypeplay a significant role. Consequently, such mutationsmay exist at relatively high frequency in the generalpopulation...

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This Article

  1. doi:10.1101/sqb.2003.68.373 Cold Spring Harb Symp Quant Biol 68: 373-382

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