OBSL1 mutations in 3‐M syndrome are associated with a modulation of IGFBP2 and IGFBP5 expression levels

3‐M syndrome is an autosomal recessive disorder characterized by severe pre‐ and postnatal growth retardation and minor skeletal changes. We have previously identified CUL7 as a disease‐causing gene but we have also provided evidence of genetic heterogeneity in the 3‐M syndrome. By homozygosity mapping in two inbred families, we found a second disease locus on chromosome 2q35–36.1 in a 5.2‐Mb interval that encompasses 60 genes. To select candidate genes, we performed microarray analysis of cultured skin fibroblast RNA from one patient, looking for genes with altered expression; we found decreased expression of IGFBP2 and increased expression of IGFBP5. However, direct sequencing of these two genes failed to detect any anomaly. We then considered other candidate genes by their function/location and found nine distinct mutations in the OBSL1 gene in 13 families including eight nonsense and one missense mutations. To further understand the links between OBSL1, CUL7, and insulin‐like growth factor binding proteins (IGFBPs), we performed real‐time quantitative PCR (RT‐PCR) analysis for OBSL1, CUL7, IGFBP2, and IGFBP5, using cultured fibroblast RNAs from two patients with distinct OBSL1 mutations (p.F697G; p.H814RfsX15). We found normal CUL7 mRNA levels but abnormal IGFBP2 and IGFBP5 mRNA levels in the two patients, suggesting that OBSL1 modulates the expression of IGFBP proteins. Hum Mutat 30:1–7, 2009. © 2009 Wiley‐Liss, Inc.

[1]  A. Munnich,et al.  The 3M syndrome. , 2011, Best practice & research. Clinical endocrinology & metabolism.

[2]  D. Sillence,et al.  A large-scale mutation search reveals genetic heterogeneity in 3M syndrome , 2009, European Journal of Human Genetics.

[3]  Z. Pan,et al.  The Cullin7 E3 ubiquitin ligase: A novel player in growth control , 2008, Cell cycle.

[4]  Yonghong Xiao,et al.  Disruption of the Fbxw8 Gene Results in Pre- and Postnatal Growth Retardation in Mice , 2007, Molecular and Cellular Biology.

[5]  M. Russell,et al.  Obscurin-like 1, OBSL1, is a novel cytoskeletal protein related to obscurin. , 2007, Genomics.

[6]  Frank McCormick,et al.  A Critical Role for FBXW8 and MAPK in Cyclin D1 Degradation and Cancer Cell Proliferation , 2006, PloS one.

[7]  A. Munnich,et al.  Identification of mutations in CUL7 in 3-M syndrome , 2005, Nature Genetics.

[8]  C. Holding,et al.  Insulin-like growth factor-binding protein 5 (Igfbp5) compromises survival, growth, muscle development, and fertility in mice , 2004, Proceedings of the National Academy of Sciences of the United States of America.

[9]  D. C. Dias,et al.  CUL7: A DOC domain-containing cullin selectively binds Skp1⋅Fbx29 to form an SCF-like complex , 2002, Proceedings of the National Academy of Sciences of the United States of America.

[10]  B. Otten,et al.  3-M syndrome: description of six new patients with review of the literature. , 2001, Clinical dysmorphology.

[11]  R. Hennekam,et al.  Further delineation of the 3-M syndrome with review of the literature. , 1987, American journal of medical genetics.

[12]  R. Winter,et al.  The 3-M syndrome. , 1984, Journal of medical genetics.

[13]  J. Opitz,et al.  A new familial intrauterine growth retardation syndrome the “3-M syndrome” , 1976, European Journal of Pediatrics.

[14]  M. Bissell The Primordial Growth Disorder 3-M Syndrome Connects Ubiquitination to the Cytoskeletal Adaptor OBSL1 , 2010 .

[15]  A. Hoeflich,et al.  Overexpression of insulin-like growth factor-binding protein-2 in transgenic mice reduces postnatal body weight gain. , 1999, Endocrinology.