E. E. Roberts scite author profile

A family with X-linked amelogenesis imperfecta (XAI) is described in which the disease is associated with a nonsense mutation in exon 5 of the amelogenin gene. This mutation involves a single base deletion (CCCC-->CCC) in the exon in an affected male, his sister and his mother. The effect of this deletion is to alter the reading frame and to introduce an inappropriate TGA stop codon (an opal mutation) into the exonic sequence of the amelogenin gene immediately 3' of the mutation. The clinical features in the examined members of this family indicate that, in some individuals, the most noticeable defect is of enamel hypoplasia. In others, the hypoplastic changes are subtle and might have been overlooked on cursory examination; the most noticeable change is of enamel colour, indicating a degree of hypomineralisation. We propose that the amelogenin gene is implicated in both the formation of enamel of normal thickness and in the normal mineralisation process.

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No evidence for allelic association between bipolar disorder and monoamine oxidase a gene polymorphisms

Craddock

Daniels

Roberts

et al. 1995

Am. J. Med. Genet.

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We have tested the hypothesis that DNA markers in the MAOA gene show allelic association with bipolar affective disorder. Eighty-four unrelated Caucasian patients with DSM III-R bipolar disorder and 84 Caucasian controls were typed for three markers in MAOA: a dinucleotide repeat in intron 2, a VNTR in intron 1, and an Fnu4HI RFLP in exon 8. No evidence for allelic association was observed between any of the markers and bipolar disorder.

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Follow‐up of a report of a potential linkage for schizophrenia on chromosome 22q12‐q13.1: Part 2

et al. 1994

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A collaboration involving four groups of investigators (Johns Hopkins University/Massachusetts Institute of Technology; Medical College of Virginia/The Health Research Board, Dublin; Institute of Psychiatry, London/University of Wales, Cardiff; Centre National de la Recherche Scientifique, Paris) was organized to confirm results suggestive of a schizophrenia susceptibility locus on chromosome 22 identified by the JHU/MIT group after a random search of the genome. Diagnostic, laboratory, and analytical reliability exercises were conducted among the groups to ensure uniformity of procedures. Data from genotyping of 3 dinucleotide repeat polymorphisms (at the loci D22S268, IL2RB, D22S307) for a combined replication sample of 256 families, each having 2 or more affected individuals with DNA, were analysed using a complex autosomal dominant model. This study provided no evidence for linkage or heterogeneity for the region 22q12-q13 under this model. We conclude that if this region confers susceptibility to schizophrenia, it must be in only a small proportion of families. Collaborative efforts to obtain large samples must continue to play an important role in the genetic search for clues to complex psychiatric disorders such as schizophrenia.

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Constipation and reversible urinary tract abnormalities.

Dohil

Roberts

Jones

et al. 1994

Archives of Disease in Childhood

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Urinary tract anomalies were prospectively investigated with ultrasound in 29 children with functional constipation. These children were compared before and after treatment with 451 age matched healthy controls without constipation. The bladder residue and upper renal tract dilatation after micturition were significantly increased in the group with constipation and improved after treatment. (Arch Dis Child 1994; 70: 56-57) Functional constipation, defined as constipation without evidence of an underlying abnormality, is a common and underdiagnosed paediatric problem. A number of reports have linked constipation with urinary tract problems, including urinary tract infection, enuresis, vesicoureteric reflux, and upper renal tract dilatation,l1 though a mechanism for the increased incidence of these abnormalities has not been clearly defined.With the aim of investigating this relation we undertook a prospective controlled study to evaluate the urinary tract in a series of children with constipation using ultrasound. We observed the effects of treatment and compared the children with controls. Ethical approval was obtained from the local research ethics committee.

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Genetic heterogeneity in X-linked amelogenesis imperfecta

et al. 1992

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E. E. Roberts

Identification of a nonsense mutation in the amelogenin gene (AMELX) in a family with X-linked amelogenesis imperfecta (AIH1)

No evidence for allelic association between bipolar disorder and monoamine oxidase a gene polymorphisms

Follow‐up of a report of a potential linkage for schizophrenia on chromosome 22q12‐q13.1: Part 2

Constipation and reversible urinary tract abnormalities.

Genetic heterogeneity in X-linked amelogenesis imperfecta

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