Diverse Developmental Disorders from The One Ring: Distinct Molecular Pathways Underlie the Cohesinopathies

Horsfield, Julia A.; Print, Cristin G.; Mönnich, Maren

doi:10.3389/fgene.2012.00171

Cited by 86 publications

(90 citation statements)

References 158 publications

(249 reference statements)

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“…Recurrent mutations could delineate clusters for genotype-phenotype correlations that may either predict disease outcome and evolution, or disclose the actions of modifiers. Individuals carrying novel mutations could enhance the understanding of the mechanisms by which altered SMC1A proteins dysregulate multiple downstream genes [Revenkova et al, 2009;Gimigliano et al, 2012;Horsfield et al, 2012].…”

Section: Introductionmentioning

confidence: 99%

Cornelia de Lange individuals with new and recurrent SMC1A mutations enhance delineation of mutation repertoire and phenotypic spectrum

Gervasini

Russo

Cereda

et al. 2013

American J of Med Genetics Pt A

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We report on the clinical and molecular characterization of eight patients, one male and seven females, with clinical diagnosis of Cornelia de Lange syndrome (CdLS), who were found to carry distinct mutations of the SMC1A gene. Five of the eight mutations are novel, with two involving amino acid residues previously described as altered in a different way. The other three have been reported each in a single case. Comparison of pairs of individuals with the same mutation indicates only partial overlap of their clinical phenotypes. The following novel missense mutations, all affecting highly conserved amino acid residues, were found: p.R398G in the N‐terminal coiled‐coil domain, p.V651M in the C‐terminal coiled‐coil/hinge junction, p.R693G in the C‐terminal coiled‐coil, and p.N1166T and p.L1189F in the C‐terminal ABC cassette. The latter is localized in the H‐loop, and represents the first mutation involving a functional motif of SMC1A protein. The effect of the mutations on SMC1A protein function has been predicted using four bioinformatic tools. All mutations except p.V651M were scored as pathogenic by three or four of the tools. p.V651M was found in the only male individual of our cohort, who presented with the most severe phenotype. This raises the issue of gender effect when addressing mutation‐phenotype correlation for genes such as SMC1A, which incompletely escapes X‐inactivation. Our clinical and molecular findings expand the total number of characterized SMC1A‐mutated patients (from 44 to 52) and the restricted repertoire of SMC1A mutations (from 29 to 34), contributing to the molecular and clinical signature of SMC1A‐based CdLS. © 2013 Wiley Periodicals, Inc.

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Section: Introductionmentioning

confidence: 99%

Cornelia de Lange individuals with new and recurrent SMC1A mutations enhance delineation of mutation repertoire and phenotypic spectrum

Gervasini

Russo

Cereda

et al. 2013

American J of Med Genetics Pt A

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“…Finally, the collection of related developmental disorders known as cohesinopathies that include Cornelia de Lange syndrome and Roberts syndrome are linked to misregulation of MYC (Horsfield et al 2012). Cohesinopathies are caused by mutations in components of the cohesin complex, including the cohesin subunits NIPPED-B, SMC1 and SMC3, RAD21, and the cohesin acetyltransferase ESCO2 (Horsfield et al 2012).…”

Section: Myc In Developmental Disordersmentioning

confidence: 99%

“…Cohesinopathies are caused by mutations in components of the cohesin complex, including the cohesin subunits NIPPED-B, SMC1 and SMC3, RAD21, and the cohesin acetyltransferase ESCO2 (Horsfield et al 2012). Cohesinopathies show considerable overlapping pathology with VACTERAL association and Feingold syndromes, suggesting potential involvement of MYCN.…”

Section: Myc In Developmental Disordersmentioning

confidence: 99%

“…For example, these disorders typically feature short stature, dysmorphic facial features including micrognathia, limb defects, hearing loss, gastrointestinal defects including atresia, cardiac defects, genitourinary defects, and mental retardation (van Bokhoven et al 2005;ShawSmith 2006;Horsfield et al 2012). Interestingly, the cohesin complex, which is best known for its functions in sister chromatid exchange (Horsfield et al 2012), shares with MYC the property of preferentially binding to genes being actively transcribed (Misulovin et al 2008). Furthermore, cohesin has been linked to stimulation of transcription elongation through release of paused RNA polymerase II complexes (Fay et al 2011).…”

Section: Myc In Developmental Disordersmentioning

confidence: 99%

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Control of Vertebrate Development by MYC

Hurlin

2013

Cold Spring Harbor Perspectives in Medicine

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The study of MYC has led to pivotal discoveries in cancer biology, induced pluripotency, and transcriptional regulation. In this review, continuing advances in our understanding of the function of MYC as a transcription factor and how its transcriptional activity controls normal vertebrate development and contributes to developmental disorders is discussed. During embryonic development, a great diversity of cell types are rapidly produced concomitant with their organization into the different functional tissues and organ structures needed to sustain life. A common theme underlying higher-order organ development is the initial establishment of stem cells or multipotent progenitor cells at distinct spatial locations. These stem and progenitor populations then respond to local environmental cues by implementing selective activation and/or silencing of specific transcription programs that drive the generation and ordered proliferative expansion of the different cell types and lineages responsible for organ-specific tissue formation. There is intense interest in how these transcriptional programs are established and maintained, both with respect to the signaling pathways and critical transcription factors involved, because their manipulation may permit the in vivo or ex vivo generation of diverse cell types for therapeutic purposes, and because their misregulation appears to be a root cause of diverse cancers and developmental disorders. Prominent among the transcription factors involved are members of the MYC family of proteins, particularly MYC and MYCN.MYC and MYCN, together with the other MYC gene family member, MYCL, encode basic-helix-loop-helix-leucine zipper (BHLHZIP) proteins that function primarily as nuclear transcription factors. However, additional activities of MYC have been identified in the control of DNA replication (Dominguez-Sola et al. 2007), and in the cytoplasm where a cleaved form of MYC that lacks the BHLHZIP region can promote differentiation (Conacci-Sorrell et al. 2010). MYC proteins are best known for their frequent involvement in a great variety of cancers and the ability of ectopic MYC to contribute to pluripotency (Cartwright et al. 2005;Takahashi and Yamanaka 2006;Wernig et al. 2007). The role of MYC family proteins in cancer and induced pluripotency is thought to stem from the appropriation of MYC activities that generally, but not universally, tend to maintain cells in a proliferative state and prevent differentiation. In the context of cancer, the activities

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“…Furthermore, studies have associated cohesin and condensin with several human developmental disorders and cancer. [9][10][11] Cohesin Cohesin is a four-subunit SMC complex that mediates sister chromatid cohesion, the process in which the newly replicated DNA strands, assembled into distinct chromatin fibers, are held together from the time of their formation until their separation during mitosis and meiosis ( Figure 1). Cohesion maintains the fidelity of chromosome segregation by ensuring the bipolar attachment of the sister chromatids centromeres to the spindle.…”

Section: Smc Complexesmentioning

confidence: 99%

Structural maintenance of chromosome complexes and bone development: the beginning of a wonderful relationship?

Cohen-Zinder¹,

Karasik

Onn

2013

BoneKEy Reports

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Bone development depends on environmental, nutritional and hormonal factors. Yet, an ordered and timed activation of genes and their associated molecular pathways are central for the growth and development of healthy bones. The correct expression of genes depends on both cis-and trans-regulatory elements. Of these, the elusive role of chromatin ultrastructure is just beginning to become appreciated. Changes in the higher-order structure of chromatin are affecting the expression of genes in response to intrinsic and environmental signals. Cohesin and condensin are members of the structural maintenance of chromosome (SMC) family of protein complexes, which mediate higher-order chromatin structure by tethering distinct regions of chromatin either inter-or intra-molecularly. In recent years, SMCs had been identified for their function in the regulation of gene expression and developmental processes, whereas malfunction of cohesin or condensin has an impact on human health. However, little is known about the specific roles of SMC complexes in bone development and their possible effect on bone health. Here, we review studies that suggest an intimate link between SMCs and bone development, as well as a plausible effect, direct or indirect, on the bone health. We describe genetic syndromes associated with SMCs with distinctive bone phenotypes and identify links between SMCs and bone-related molecular pathways. Future studies of the relationship between SMCs and bone development will reveal new understandings of both the cellular and molecular roles of SMC complexes and provide new insights into the growth and developmental processes in the bone.

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Diverse Developmental Disorders from The One Ring: Distinct Molecular Pathways Underlie the Cohesinopathies

Cited by 86 publications

References 158 publications

Cornelia de Lange individuals with new and recurrent SMC1A mutations enhance delineation of mutation repertoire and phenotypic spectrum

Cornelia de Lange individuals with new and recurrent SMC1A mutations enhance delineation of mutation repertoire and phenotypic spectrum

Control of Vertebrate Development by MYC

Structural maintenance of chromosome complexes and bone development: the beginning of a wonderful relationship?

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