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Featured researches published by Diane Lawson.


Molecular Psychiatry | 2001

Genomic structure and localisation within a linkage hotspot of Disrupted In Schizophrenia 1 , a gene disrupted by a translocation segregating with schizophrenia

J. K. Millar; Sheila Christie; Stuart Anderson; Diane Lawson; D Hsiao-Wei Loh; Rebecca S. Devon; Benoit Arveiler; Walter J. Muir; Douglas Blackwood; David J. Porteous

Two overlapping and antiparallel genes on chromosome 1, Disrupted In Schizophrenia 1 and 2 (DISC1 and DISC2), are disrupted by a (1;11)(q42.1;q14.3) translocation which segregates with schizophrenia through at least four generations of a large Scottish family. Consequently, these genes are worthy of further investigation as candidate genes potentially involved in the aetiology of major psychiatric illness. We have constructed a contiguous clone map of PACs and cosmids extending across at least 400u2009kb of the chromosome 1 translocation breakpoint region and this has provided the basis for examination of the genomic structure of DISC1. The gene consists of thirteen exons, estimated to extend across at least 300u2009kb of DNA. The antisense gene DISC2 overlaps with exon 9. Exon 11 contains an alternative splice site that removes 66 nucleotides from the open reading frame. The final intron of DISC1 belongs to the rare AT-AC class of introns. We have also mapped marker DIS251 in close proximity to DISC1, localising the gene within a critical region identified by several independent studies. Information regarding the structure of the DISC1 gene will facilitate assessment of its involvement in the aetiology of major mental illness in psychotic individuals unrelated to carriers of the translocation.


Human Genetics | 1995

Multi-PRINS: multiple sequential oligonucleotide primed in situ DNA synthesis reactions label specific chromosomes and produce bands

Ernst J. M. Speel; Diane Lawson; Anton H. N. Hopman; John R. Gosden

A fast method for identifying several chromosomes with chromosome-specific oligonucleotide primers directing an in situ labeling reaction is described. Up to three reactions distinguished by different fluorochromes (fluorescein isothiocyanate, rhodamine/Texas red, p-aminomethyl-cyclohexane carboxylic acid) can currently be performed. Prospects for increasing this up to seven colors, and for the future of the process in prenatal diagnosis are discussed.


American Journal of Medical Genetics | 2000

Mutational analysis of the Wolfram syndrome gene in two families with chromosome 4p-linked bipolar affective disorder.

Kathryn L. Evans; Diane Lawson; Thomas Meitinger; Douglas Blackwood; David J. Porteous

Bipolar affective disorder (BPAD) is a complex disease with a significant genetic component. Heterozygous carriers of Wolfram syndrome (WFS) are at increased risk of psychiatric illness. A gene for WFS (WFS1) has recently been cloned and mapped to chromosome 4p, in the general region we previously reported as showing linkage to BPAD. Here we present sequence analysis of the WFS1 coding sequence in five affected individuals from two chromosome 4p-linked families. This resulted in the identification of six polymorphisms, two of which are predicted to change the amino acid sequence of the WFS1 protein, however none of the changes segregated with disease status. Am. J. Med. Genet. (Neuropsychiatr. Genet.) 96:158-160, 2000.


Psychiatric Genetics | 1998

A long-range restriction map across 3 Mb of the chromosome 11 breakpoint region of a translocation linked to schizophrenia: localization of the breakpoint and the search for neighbouring genes

J. K. Millar; John Brown; John C. Maule; Yoshiro Shibasaki; Sheila Christie; Diane Lawson; Stuart Anderson; Julie C. Wilson-Annan; Rebecca S. Devon; D. St Clair; D. H. R. Blackwood; W. J. Muir; David J. Porteous

A balanced t(1;11)(q42.1;q14.3) translocation segregates with schizophrenia and related mental illness in a single large Scottish pedigree. We have constructed a long-range restriction map covering at least 3 Mb of the chromosome 11 breakpoint region and conducted searches for genes whose expression could be altered by the translocation, resulting in schizophrenia. Novel transcribed sequences of unknown function clustered around putative CpG islands, located approximately 500 kb and 700 kb above the breakpoint, represent the only evidence to date for expressed genes within the mapped region.


Human Molecular Genetics | 1994

Rapid chromosome identification by oligonucleotide-primed in situ DNA synthesis (PRINS)

John R. Gosden; Diane Lawson


Genomics | 1996

Characterization of a chromosome-specific chimpanzee alpha satellite subset: Evolutionary relationship to subsets on human chromosomes

Peter E. Warburton; Thomas Haaf; John R. Gosden; Diane Lawson; Huntington F. Willard


Genomics | 2001

A 6.9-Mb high-resolution BAC/PAC contig of human 4p15.3-p16.1, a candidate region for bipolar affective disorder

Kathryn L. Evans; Stephanie Le Hellard; Stewart W. Morris; Diane Lawson; Claire Whitton; Colin A. Semple; Judith A. Fantes; Helen S. Torrance; M. Pat Malloy; John C. Maule; Sean Humphray; Mark T. Ross; David R. Bentley; Walter J. Muir; Douglas Blackwood; David J. Porteous


Methods of Molecular Biology | 1997

PRINS DNA Synthesis on Frozen Tissue Sections

Ernst J. M. Speel; Diane Lawson; Frans C. S. Ramaekers; John R. Gosden; Anton H. N. Hopman


Genome Research | 1995

Human repeat-mediated integration of selectable markers into somatic cell hybrids.

Janet Elizabeth Vivienne Watson; E.M. Slorach; John C. Maule; Diane Lawson; David J. Porteous; Anthony J. Brookes


Methods of Molecular Biology | 1997

Multiple Sequential Oligonucleotide Primed In Situ DNA Syntheses (MULTI-PRINS)

John R. Gosden; Diane Lawson

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John R. Gosden

Western General Hospital

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John C. Maule

Western General Hospital

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