TY - JOUR
T1 - Meier-Gorlin syndrome genotype-phenotype studies
T2 - 35 individuals with pre-replication complex gene mutations and 10 without molecular diagnosis
AU - de Munnik, Sonja A
AU - Bicknell, Louise S
AU - Aftimos, Salim
AU - Al-Aama, Jumana Y
AU - van Bever, Yolande
AU - Bober, Michael B
AU - Clayton-Smith, Jill
AU - Edrees, Alaa Y
AU - Feingold, Murray
AU - Fryer, Alan
AU - van Hagen, Johanna M
AU - Hennekam, Raoul C
AU - Jansweijer, Maaike C E
AU - Johnson, Diana
AU - Kant, Sarina G
AU - Opitz, John M
AU - Ramadevi, A Radha
AU - Reardon, Willie
AU - Ross, Alison
AU - Sarda, Pierre
AU - Schrander-Stumpel, Constance T R M
AU - Schoots, Jeroen
AU - Temple, I Karen
AU - Terhal, Paulien A
AU - Toutain, Annick
AU - Wise, Carol A
AU - Wright, Michael
AU - Skidmore, David L
AU - Samuels, Mark E
AU - Hoefsloot, Lies H
AU - Knoers, Nine V A M
AU - Brunner, Han G
AU - Jackson, Andrew P
AU - Bongers, Ernie M H F
PY - 2012
Y1 - 2012
N2 - Meier-Gorlin syndrome (MGS) is an autosomal recessive disorder characterized by microtia, patellar aplasia/hypoplasia, and short stature. Recently, mutations in five genes from the pre-replication complex (ORC1, ORC4, ORC6, CDT1, and CDC6), crucial in cell-cycle progression and growth, were identified in individuals with MGS. Here, we report on genotype-phenotype studies in 45 individuals with MGS (27 females, 18 males; age 3 months-47 years). Thirty-five individuals had biallelic mutations in one of the five causative pre-replication genes. No homozygous or compound heterozygous null mutations were detected. In 10 individuals, no definitive molecular diagnosis was made. The triad of microtia, absent/hypoplastic patellae, and short stature was observed in 82% of individuals with MGS. Additional frequent clinical features were mammary hypoplasia (100%) and abnormal genitalia (42%; predominantly cryptorchidism and hypoplastic labia minora/majora). One individual with ORC1 mutations only had short stature, emphasizing the highly variable clinical spectrum of MGS. Individuals with ORC1 mutations had significantly shorter stature and smaller head circumferences than individuals from other gene categories. Furthermore, compared with homozygous missense mutations, compound heterozygous mutations appeared to have a more severe effect on phenotype, causing more severe growth retardation in ORC4 and more frequently pulmonary emphysema in CDT1. A lethal phenotype was seen in four individuals with compound heterozygous ORC1 and CDT1 mutations. No other clear genotype-phenotype association was observed. Growth hormone and estrogen treatment may be of some benefit, respectively, to growth retardation and breast hypoplasia, though further studies in this patient group are needed.
AB - Meier-Gorlin syndrome (MGS) is an autosomal recessive disorder characterized by microtia, patellar aplasia/hypoplasia, and short stature. Recently, mutations in five genes from the pre-replication complex (ORC1, ORC4, ORC6, CDT1, and CDC6), crucial in cell-cycle progression and growth, were identified in individuals with MGS. Here, we report on genotype-phenotype studies in 45 individuals with MGS (27 females, 18 males; age 3 months-47 years). Thirty-five individuals had biallelic mutations in one of the five causative pre-replication genes. No homozygous or compound heterozygous null mutations were detected. In 10 individuals, no definitive molecular diagnosis was made. The triad of microtia, absent/hypoplastic patellae, and short stature was observed in 82% of individuals with MGS. Additional frequent clinical features were mammary hypoplasia (100%) and abnormal genitalia (42%; predominantly cryptorchidism and hypoplastic labia minora/majora). One individual with ORC1 mutations only had short stature, emphasizing the highly variable clinical spectrum of MGS. Individuals with ORC1 mutations had significantly shorter stature and smaller head circumferences than individuals from other gene categories. Furthermore, compared with homozygous missense mutations, compound heterozygous mutations appeared to have a more severe effect on phenotype, causing more severe growth retardation in ORC4 and more frequently pulmonary emphysema in CDT1. A lethal phenotype was seen in four individuals with compound heterozygous ORC1 and CDT1 mutations. No other clear genotype-phenotype association was observed. Growth hormone and estrogen treatment may be of some benefit, respectively, to growth retardation and breast hypoplasia, though further studies in this patient group are needed.
U2 - 10.1038/ejhg.2011.269
DO - 10.1038/ejhg.2011.269
M3 - Article
C2 - 22333897
VL - 20
SP - 598
EP - 606
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 6
ER -