Sylvia A. Rayner scite author profile

Mutations in the two-handed zinc-finger homeodomain transcription factor gene (TCF8) have been associated with posterior polymorphous corneal dystrophy (PPCD) and extraocular developmental abnormalities. We performed screening of TCF8 in 32 affected, unrelated probands, affected and unaffected family members of probands identified with a TCF8 mutation, and in 100 control individuals. Eight different pathogenic mutations were identified in eight probands: four frameshift (c.953_954insA, c.1506dupA, c.1592delA, and c.3012_3013delAG); three nonsense (Gln12X, Gln214X, Arg325X); and one missense (Met1Arg). Screening of TCF8 in affected and unaffected family members in six families demonstrated that each identified mutation segregated with the disease phenotype in each family; two probands did not have additional family members available for analysis. None of the eight TCF8 mutations was identified in 200 control chromosomes. The prevalence of hernias of the abdominal region in affected individuals with PPCD associated with TCF8 mutations was significantly higher than the prevalence in both individuals with PPCD not associated with a TCF8 mutation and in unaffected individuals. Therefore, PPCD is associated with TCF8 mutations in one quarter of affected families in this study, or about one third of all PPCD families that have been screened thus far. In these families, the presence of apparently causative TCF8 mutations is associated with abdominal and inguinal hernias.

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A comparison of rhodamine 123 accumulation and efflux in cells with P-glycoprotein-mediated and MRP-associated multidrug resistance phenotypes

Twentyman

Rhodes

Rayner

1994

European Journal of Cancer

116

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Mitigation of Neutrophil Infiltration in a Rat Model of EarlyStaphylococcus aureusEndophthalmitis

Giese¹,

Rayner²,

Fardin³

et al. 2003

Invest. Ophthalmol. Vis. Sci.

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NoVSX1Gene Mutations Associated with Keratoconus

Aldave¹,

Yellore²,

Salem³

et al. 2006

Invest. Ophthalmol. Vis. Sci.

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Only one of the presumed pathogenic mutations in the VSX1 gene, Asp144Glu, was identified in a single member of the cohort of affected patients. However, as previously demonstrated, Asp144Glu is a non-disease-causing polymorphism. The absence of pathogenic mutations in the VSX1 gene in a large number of unrelated KTCN patients indicates that other genetic factors are involved in the development of this disorder.

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Autosomal Recessive CHED Associated With Novel Compound Heterozygous Mutations in SLC4A11

Aldave¹,

Yellore²,

Bourla³

et al. 2007

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Sylvia A. Rayner

Posterior polymorphous corneal dystrophy is associated with TCF8 gene mutations and abdominal hernia

A comparison of rhodamine 123 accumulation and efflux in cells with P-glycoprotein-mediated and MRP-associated multidrug resistance phenotypes

Mitigation of Neutrophil Infiltration in a Rat Model of EarlyStaphylococcus aureusEndophthalmitis

NoVSX1Gene Mutations Associated with Keratoconus

Autosomal Recessive CHED Associated With Novel Compound Heterozygous Mutations in SLC4A11

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