TY - JOUR
T1 - Insights into genetics, human biology and disease gleaned from family based genomic studies
AU - Centers for Mendelian Genomics
AU - Posey, Jennifer E.
AU - O’Donnell-Luria, Anne H.
AU - Chong, Jessica X.
AU - Harel, Tamar
AU - Jhangiani, Shalini N.
AU - Coban Akdemir, Zeynep H.
AU - Buyske, Steven
AU - Pehlivan, Davut
AU - Carvalho, Claudia M.B.
AU - Baxter, Samantha
AU - Sobreira, Nara
AU - Liu, Pengfei
AU - Wu, Nan
AU - Rosenfeld, Jill A.
AU - Kumar, Sushant
AU - Avramopoulos, Dimitri
AU - White, Janson J.
AU - Doheny, Kimberly F.
AU - Witmer, P. Dane
AU - Boehm, Corinne
AU - Sutton, V. Reid
AU - Muzny, Donna M.
AU - Boerwinkle, Eric
AU - Günel, Murat
AU - Nickerson, Deborah A.
AU - Mane, Shrikant
AU - MacArthur, Daniel G.
AU - Gibbs, Richard A.
AU - Hamosh, Ada
AU - Lifton, Richard P.
AU - Matise, Tara C.
AU - Rehm, Heidi L.
AU - Gerstein, Mark
AU - Bamshad, Michael J.
AU - Valle, David
AU - Lupski, James R.
N1 - Publisher Copyright:
© 2019, American College of Medical Genetics and Genomics.
PY - 2019/4/1
Y1 - 2019/4/1
N2 - Identifying genes and variants contributing to rare disease phenotypes and Mendelian conditions informs biology and medicine, yet potential phenotypic consequences for variation of >75% of the ~20,000 annotated genes in the human genome are lacking. Technical advances to assess rare variation genome-wide, particularly exome sequencing (ES), enabled establishment in the United States of the National Institutes of Health (NIH)-supported Centers for Mendelian Genomics (CMGs) and have facilitated collaborative studies resulting in novel “disease gene” discoveries. Pedigree-based genomic studies and rare variant analyses in families with suspected Mendelian conditions have led to the elucidation of hundreds of novel disease genes and highlighted the impact of de novo mutational events, somatic variation underlying nononcologic traits, incompletely penetrant alleles, phenotypes with high locus heterogeneity, and multilocus pathogenic variation. Herein, we highlight CMG collaborative discoveries that have contributed to understanding both rare and common diseases and discuss opportunities for future discovery in single-locus Mendelian disorder genomics. Phenotypic annotation of all human genes; development of bioinformatic tools and analytic methods; exploration of non-Mendelian modes of inheritance including reduced penetrance, multilocus variation, and oligogenic inheritance; construction of allelic series at a locus; enhanced data sharing worldwide; and integration with clinical genomics are explored. Realizing the full contribution of rare disease research to functional annotation of the human genome, and further illuminating human biology and health, will lay the foundation for the Precision Medicine Initiative.
AB - Identifying genes and variants contributing to rare disease phenotypes and Mendelian conditions informs biology and medicine, yet potential phenotypic consequences for variation of >75% of the ~20,000 annotated genes in the human genome are lacking. Technical advances to assess rare variation genome-wide, particularly exome sequencing (ES), enabled establishment in the United States of the National Institutes of Health (NIH)-supported Centers for Mendelian Genomics (CMGs) and have facilitated collaborative studies resulting in novel “disease gene” discoveries. Pedigree-based genomic studies and rare variant analyses in families with suspected Mendelian conditions have led to the elucidation of hundreds of novel disease genes and highlighted the impact of de novo mutational events, somatic variation underlying nononcologic traits, incompletely penetrant alleles, phenotypes with high locus heterogeneity, and multilocus pathogenic variation. Herein, we highlight CMG collaborative discoveries that have contributed to understanding both rare and common diseases and discuss opportunities for future discovery in single-locus Mendelian disorder genomics. Phenotypic annotation of all human genes; development of bioinformatic tools and analytic methods; exploration of non-Mendelian modes of inheritance including reduced penetrance, multilocus variation, and oligogenic inheritance; construction of allelic series at a locus; enhanced data sharing worldwide; and integration with clinical genomics are explored. Realizing the full contribution of rare disease research to functional annotation of the human genome, and further illuminating human biology and health, will lay the foundation for the Precision Medicine Initiative.
KW - Centers for Mendelian Genomics (CMG)
KW - Mendelian conditions
KW - disease traits
KW - genetic models for disease
KW - rare variant phenotypes
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U2 - 10.1038/s41436-018-0408-7
DO - 10.1038/s41436-018-0408-7
M3 - Review article
C2 - 30655598
AN - SCOPUS:85060245235
SN - 1098-3600
VL - 21
SP - 798
EP - 812
JO - Genetics in Medicine
JF - Genetics in Medicine
IS - 4
ER -