Your search keyword '"Yates, John R W"' showing total 3 results

1. CASK mutations are frequent in males and cause X-linked nystagmus and variable XLMR phenotypes.

Author

Hackett, Anna, Tarpey, Patrick S., Licata, Andrea, Cox, James, Whibley, Annabel, Boyle, Jackie, Rogers, Carolyn, Grigg, John, Partington, Michael, Stevenson, Roger E., Tolmie, John, Yates, John R. W., Turner, Gillian, Wilson, Meredith, Futreal, Andrew P., Corbett, Mark, Shaw, Marie, Gecz, Jozef, Raymond, F. Lucy, and Stratton, Michael R.

Subjects

GENETIC mutation, NYSTAGMUS, EYE movement disorders, PHENOTYPES, PATHOLOGICAL psychology

Abstract

Mutations of the calcium/calmodulin-dependent serine protein kinase (CASK) gene have recently been associated with X-linked mental retardation (XLMR) with microcephaly, optic atrophy and brainstem and cerebellar hypoplasia, as well as with an X-linked syndrome having some FG-like features. Our group has recently identified four male probands from 358 probable XLMR families with missense mutations (p.Y268H, p.P396S, p.D710G and p.W919R) in the CASK gene. Congenital nystagmus, a rare and striking feature, was present in two of these families. We screened a further 45 probands with either nystagmus or microcephaly and mental retardation (MR), and identified two further mutations, a missense mutation (p.Y728C) and a splice mutation (c.2521-2A>T) in two small families with nystagmus and MR. Detailed clinical examinations of all six families, including an ophthalmological review in four families, were undertaken to further characterise the phenotype. We report on the clinical features of 24 individuals, mostly male, from six families with CASK mutations. The phenotype was variable, ranging from non-syndromic mild MR to severe MR associated with microcephaly and dysmorphic facial features. Carrier females were variably affected. Congenital nystagmus was found in members of four of the families. Our findings reinforce the CASK gene as a relatively frequent cause of XLMR in females and males. We further define the phenotypic spectrum and demonstrate that affected males with missense mutations or in-frame deletions in CASK are frequently associated with congenital nystagmus and XLMR, a striking feature not previously reported. [ABSTRACT FROM AUTHOR]

Published

2010

2. Expanding the tuberous sclerosis phenotype: mild disease caused by a TSC1 splicing mutation.

Author

Blyth, Moira, Raponi, Michela, Treacy, Rebecca, Raymond, F. Lucy, Yates, John R. W., and Baralle, Diana

Subjects

TUBEROUS sclerosis, ERYTHEMA, RNA splicing, PHENOTYPES, INTELLECTUAL disabilities, EPILEPSY, PATIENTS

Abstract

The article focuses on the tuberous sclerosis phenotype expansion, an autosomal dominant disorder that causes mental retardation and epilepsy. It references the case of a family with an unusually mild phenotype due to TSC1 splice site (SS) mutation wherein the proband had generalised tonic-clonic seizures when he was 11, his brother had nocturnal seizues, and his father has mild facial erythema with no definite angiofibromas. It adds the classification of the proband and father as possible TS.

Published

2010

3. The Gene Encoding Collagen ∝1(V) (COL5A1) Is Linked to Mixed Ehlers-Danlos Syndrome Type I/II.

Author

Burrows, Nigel P., Nicholls, Alan C., Yates, John R. W., Gatward, Graham, Sarathachandra, Padmini, Richards, Allan, and Pope, F. Michael

Subjects

*COLLAGEN, *CONNECTIVE tissue diseases, *EHLERS-Danlos syndrome, *GENETIC mutation, *PHENOTYPES, *DERMATOLOGY

Abstract

The Ehlers-Danlos syndrome (EDS) is a heterogeneo US group of inherited connective tissue disorders in which cutaneous fragility and ligamentous laxity often combine with vascular, gastrointestinal, and skeletal deformities. There is considerable phenotypic overlap between the more common fonas of EDS (types I and II), in which specific molecular defects have not yet been identified. Recently, genetic linkage has been demonstrated between the COL5A1 gene, which encodes the α1 chain of type V collagen, and EDS type II in a large British kindred. Using a polymorphic intragenic simple sequence repeat at the COL5A1 locus, we now demonstrate tight linkage to EDS type I/II in a three-generation family, giving a LOD score (log10 of the odds for linkage) of 4.07 at zero recombination. The variation in expression in this family suggests that EDS types I and II are allelic, and the linkage data support the hypothesis that mutation in COL5A1 can cause both phenotypes. [ABSTRACT FROM AUTHOR]

Published

1996