Chromosome 7p disruptions in Silver Russell syndrome: delineating an imprinted candidate gene region.

Monk, David; Bentley, Louise; Hitchins, Megan P.; Myler, Rachael A.; Clayton‐Smith, Jill; Ismail, Samira; Price, Sue; Preece, M A; Stanier, Philip; Moore, Gudrun E.

doi:10.1007/s00439-002-0777-4

Cited by 78 publications

(59 citation statements)

References 45 publications

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“…In addition, the duplication of pre-existing pathogenic mutations by isodisomy can lead to the clinical expression of recessive disorders (such as cystic fibrosis) in patients with upd(7)mat [38][39][40] . Candidate SRS regions have been suggested through identification of patients with segmental upd(7)mat or CNVs (see Supplementary information S3 (table)); the primary candidate SRS genes on chromosome 7 are currently GRB10 (7p12.1) and MEST (7q32) [41][42][43][44][45][46][47][48] . Microsatellite analysis was the first diagnostic test for upd(7)mat 35,36 ; however, this analysis cannot detect imprinting defects (epimutations) and requires DNA from at least one parent.…”

Section: Chromosomementioning

confidence: 99%

Diagnosis and management of Silver–Russell syndrome: first international consensus statement

et al. 2016

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Section: Chromosomementioning

confidence: 99%

Diagnosis and management of Silver–Russell syndrome: first international consensus statement

et al. 2016

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“…1 As inferred earlier, mitochondrial disorders can manifest in various phenotypic classifications. We see in Tables 1 and 2 that MRP genes are candidates for dwarfism, growth retardation, and limb deformity disorders such as Russell-Silver Syndrome, 49,50 Stuve-Wiedemann Syndrome, 51 and Moebius Syndrome I. 52 Metabolic disorders for which MRP genes associate by map position are Multiple Mitochondrial Dysfunctions, 53 Stuve-Wiedemann Syndrome, 51 Leigh Syndrome, 54 and diabetes.…”

Section: Mrp Characterization Gene Identification and Mappingmentioning

confidence: 99%

Mitochondrial ribosomal proteins: Candidate genes for mitochondrial disease

Sylvester

Fischel‐Ghodsian

Mougey

et al. 2004

Genetics in Medicine

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Most of the energy requirement for cell growth, differentiation, and development is met by the mitochondria in the form of ATP produced by the process of oxidative phosphorylation. Human mitochondrial DNA encodes a total of 13 proteins, all of which are essential for oxidative phosphorylation. The mRNAs for these proteins are translated on mitochondrial ribosomes. Recently, the genes for human mitochondrial ribosomal proteins (MRPs) have been identified. In this review, we summarize their refined chromosomal location. It is well known that mutations in the mitochondrial translation system, i.e., ribosomal RNA and transfer RNA cause various pathologies. In this review, we suggest possible associations between clinical conditions and MRPs based on coincidence of genetic map data and chromosomal location. These MRPs may be candidate genes for the clinical condition or may act as modifiers of existing known gene mutations (mt-tRNA, mt-rRNA, etc.). Genet Med 2004:6(2):73-80.

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“…14 The role of genomic imprinting in IUGR pregnancies has been investigated, but systematic studies are sparse. 15,16 A recent study comparing gene expression profiles of normal and IUGR placentas using microarrays which included 27 imprinted genes demonstrated that 22% of the imprinted genes were differentially expressed, far in excess of the non-imprinted genes. 7 These results strongly demonstrate a critical role of genomic imprinting in placental/fetal growth and suggest that IUGR may be a result of altered expression of critical imprinted genes.…”

Section: Introductionmentioning

confidence: 99%

Differential expression of imprinted genes in normal and IUGR human placentas

Diplas¹,

Lambertini²,

Lee³

et al. 2009

Epigenetics

173

124

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Genomic imprinting refers to silencing of one parental allele in the zygotes of gametes depending upon the parent of origin. Loss of imprinting (LOI) is the gain of function from the silent allele that can have a maximum effect of doubling the gene dosage. LOI may play a significant role in the etiology of intrauterine growth restriction (IUGR). Using placental tissue from ten normal and seven IUGR pregnancies, we conducted a systematic survey of the expression of a panel of 74 "putatively" imprinted genes using quantitative RT-PCR. We found that 52/74 (~70%) of the genes were expressed in human placentas. Nine of the 52 (17%) expressed genes were significantly differentially expressed between normal and IUGR placentas; five were upregulated (PHLDA2, ILK2, NNAT, CCDC86, PEG10) and four downregulated (PLAGL1, DHCR24, ZNF331, CDKAL1). We also assessed LOI profile of 14 imprinted genes in 14 normal and 24 IUGR placentas using a functional and sensitive assay developed in our laboratory. Little LOI was observed in any placentas for five of the genes (PEG10, PHLDA2, MEG3, EPS15, CD44). With the 149 heterozygosities examined, 40 (26.8%) exhibited LOI >3%. Some genes exhibited frequent LOI in placentas regardless of the disease status (IGF2, TP73, MEST, SLC22A18, PEG3), while others exhibited LOI only in IUGR placentas (PLAGL1, DLK1, H19, SNRPN). Importantly, there was no correlation between gene expression and LOI profile. Our study suggests that genomic imprinting may play a role in IUGR pathogenesis, but mechanisms other than LOI may contribute to dysregulation of imprinted genes. IntroductionGenomic imprinting refers to silencing of one parental allele in the zygotes of gametes depending upon the parent of origin; this silencing occurs via epigenetic processes such as DNA methylation and/or histone modification. 1 It has been hypothesized in the "parental conflict" theory that paternally expressed genes favors the utilization of maternal resources for the benefit of the offspring while the maternally expressed genes act to preserve such resources. Thus, imprinted genes that are paternally expressed (maternally imprinted) are predicted to promote growth of the offspring, either in utero or in perinatal period, whilst maternally expressed (paternally imprinted) genes would act as growth suppressors to assure appropriate allocation of limited maternal resources to each conceptus. 2 Consequently, imprinted genes play critical roles in regulation of growth and development; disruption of this critical process, such as loss of imprinting (LOI), has been associated with a wide range of human diseases including birth defects neurodevelopmental disorders and cancer. [3][4][5][6][7] Compared to other mammalian genomes such as that of the mouse, the human genome is imprinted to a much lesser degree, possibly due to a lack of competition for maternal resources because human pregnancies are typically singletons. 8 The estimated number of imprinted genes is ~100-200 (<1% of the genome). This limited number of imprinted genes affo...

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Chromosome 7p disruptions in Silver Russell syndrome: delineating an imprinted candidate gene region.

Cited by 78 publications

References 45 publications

Diagnosis and management of Silver–Russell syndrome: first international consensus statement

Diagnosis and management of Silver–Russell syndrome: first international consensus statement

Mitochondrial ribosomal proteins: Candidate genes for mitochondrial disease

Differential expression of imprinted genes in normal and IUGR human placentas

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