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Dive into the research topics where Robert P. Curtain is active.

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Featured researches published by Robert P. Curtain.


Human Genetics | 2000

Familial typical migraine: significant linkage and localization of a gene to Xq24-28

Dale R. Nyholt; Robert P. Curtain; Lyn R. Griffiths

Abstract. In a previous study we found evidence for an X-linked genetic component for familial typical migraine in two large Australian white pedigrees, designated MF7 and MF14. Significant excess allele sharing was indicated by nonparametric linkage (NPL) analysis using GENEHUNTER (P=0.031 and P=0.012, respectively), with a combined analysis of the two pedigrees showing further increased evidence for linkage, producing a maximum NPL score of 2.87 (P=0.011) at DXS1123 on Xq27. The present study was aimed at refining the localization of the migraine X-chromosomal component by typing additional markers, performing haplotype analysis and applying a more powerful technique in the analysis of linkage data from these two pedigrees. Results from the haplotype analyses, coupled with linkage analyses that produced a peak GENEHUNTER-PLUS LOD* score of 2.388 (P=0.0005), provide compelling evidence for the presence of a migraine susceptibility locus on chromosome Xq24–28.


Cephalalgia | 1996

MIGRAINE ASSOCIATION AND LINKAGE ANALYSES OF THE HUMAN 5-HYDROXYTRYPTAMINE(5HT2A) RECEPTOR GENE

Nyholt; Robert P. Curtain; Philip Thomas Gaffney; Peter J. Brimage; Peter J. Goadsby; Lyn R. Griffiths

5-Hydroxytryptamine (5HT), commonly known as serotonin, which predominantly serves as an inhibitory neurotransmitter in the brain, has long been implicated in migraine pathophysiology. This study tested an Mspl polymorphism in the human 5HT2A receptor gene (HTR2A) and a closely linked microsatellite marker (D13S126), for linkage and association with common migraine. In the association analyses, no significant differences were found between the migraine and control populations for both the Mspl polymorphism and the D13S126 microsatellite marker. The linkage studies involving three families comprising 36 affected members were analysed using both parametric (FASTLINK) and non-parametric (MFLINK and APM) techniques. Significant close linkage was indicated between the Mspl polymorphism and the D13S126 microsatellite marker at a recombination fraction (θ) of zero (lod score=7.15). Linkage results for the Mspl polymorphism were not very informative in the three families, producing maximum and minimum lod scores of only 0.35 and 0.39 at recombination fractions (θ) of 0.2 and 0.00, respectively. However, linkage analysis between the D13S126 marker and migraine indicated significant non-linkage (lod2) up to a recombination fraction (θ) of 0.028. Results from this study exclude the HTR2A gene, which has been localized to chromosome 13q14-q21, for involvement with common migraine.


International Journal of Obesity | 1997

Association of a low density lipoprotein receptor microsatellite variant with obesity.

Sue Rutherford; Dale R. Nyholt; Robert P. Curtain; Quinlan; Philip Thomas Gaffney; B. J. Morris; Lyn R. Griffiths

OBJECTIVE: To determine whether a microsatellite polymorphism located towards the 3’ end of the low density lipoprotein receptor gene (LDLR) is associated with obesity. DESIGN: A cross-sectional case-control study. SUBJECTS: One hundred and seven obese individuals, defined as a body mass index (BMI)≥26 kg/m2, and 163 lean individuals, defined as a BMI<26 kg/m2. MEASUREMENTS: BMI, blood pressure, serum lipids, alleles of LDLR microsatellite (106 bp, 108 bp and 112 bp). RESULTS: There was a significant association between variants of the LDLR microsatellite and obesity, in the overall tested population, due to a contributing effect in females (χ2=12.3, P=0.002), but not in males (χ2=0.3, P=0.87). In females, individuals with the 106 bp allele were more likely to be lean, while individuals with the 112 bp and/or 108 bp alleles tended to be obese. CONCLUSIONS: These results suggest that in females, LDLR may play a role in the development of obesity.


Clinical and Experimental Pharmacology and Physiology | 1995

CROSS-SECTIONAL STUDY OF A MICROSATELLITE MARKER IN THE LOW DENSITY LIPOPROTEIN RECEPTOR GENE IN OBESE NORMOTENSIVES

Lyn R. Griffiths; Dale R. Nyholt; Robert P. Curtain; Philip Thomas Gaffney; Brian J. Morris

1. The low density lipoprotein receptor is an important regulator of serum cholesterol which may have implications for the development of both hypertension and obesity. In this study, genotypes for a low density lipoprotein receptor gene (LDLR) dinucleotide polymorphism were determined in both lean and obese normotensive populations.


Neurogenetics | 2002

A typical migraine susceptibility region localizes to chromosome 1q31

Rod A. Lea; Graeme A. Shepherd; Robert P. Curtain; Dale R. Nyholt; Sharon Anne Quinlan; Peter J. Brimage; Lyn R. Griffiths


Pediatric Neurology | 2006

Minor Head Trauma–Induced Sporadic Hemiplegic Migraine Coma

Robert P. Curtain; Robert L. Smith; Mick Ovcaric; Lyn R. Griffiths


American Journal of Medical Genetics | 2001

Investigation of the CACNA1A gene as a candidate for typical migraine susceptibility

Rod A. Lea; Robert P. Curtain; Colin M. Hutchins; Peter J. Brimage; Lyn R. Griffiths


American Journal of Medical Genetics | 2001

No evidence for involvement of the human inducible nitric oxide synthase (iNOS) gene in susceptibility to typical migraine.

Rod A. Lea; Robert P. Curtain; A. Graeme Shepherd; Peter J. Brimage; Lyn R. Griffiths


Hypertension | 1997

Influence of family history on frequency of glucagon receptor Gly40Ser mutation in hypertensive subjects.

B. J. Morris; Jeyasingam Cl; Weihua Zhang; Robert P. Curtain; Lyn R. Griffiths


Human Mutation | 2000

Identification of a novel mutation C144F in the notch3 gene in an Australian CADASIL pedigree

Rachel Grigg; Rod A. Lea; A.A. Sullivan; Robert P. Curtain; John MacMillian; Lyn R. Griffiths

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Lyn R. Griffiths

Queensland University of Technology

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Dale R. Nyholt

Queensland University of Technology

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Rod A. Lea

Queensland University of Technology

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John MacMillan

Royal Children's Hospital

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Sue Rutherford

Texas Biomedical Research Institute

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A.A. Sullivan

University of Queensland

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