Khan Arif O, Aldahmesh Mohammad A, Al-Amri Abdullah
Pediatric Ophthalmology Division, King Khaled Eye Specialist Hospital, Riyadh, Saudi Arabia.
Ophthalmic Genet. 2008 Jun;29(2):67-71. doi: 10.1080/13816810801908152.
To report the genetic basis for congenital glaucoma with clinical aniridia in an infant and a milder phenotype in her mother.
Prospective case series.
An infant girl with almost complete lack of iris tissue was referred and treated for congenital glaucoma. Although the presumed clinical diagnosis was aniridia (On-line Mendelian Inheritance in Man [OMIM] AN2, # 106210), PAX6 sequencing was normal. Examination of the infant's mother was significant for Axenfeld-Rieger malformation (ARM): prominent Schwabe line, subtle iris hypoplasia, iris stands bridging the angle, increased intraocular pressure, and glaucomatous optic nerve cupping. Both parents and the infant underwent diagnostic FOXC1 DNA sequencing. A heterozygous M161K FOXC1 mutation was found in the infant and her mother but not in the father, who had a normal ocular examination.
The spectrum of intrafamilial phenotypic variation associated with heterozygous FOXC1 mutation can be wide. FOXC1 mutation can be a cause of congenital glaucoma with clinical aniridia. Although such infants resemble the AN2 phenotype, the glaucoma of AN2 due to PAX6 mutation is typically secondary with onset several years after birth.
报告一名患有先天性青光眼合并临床无虹膜的婴儿及其母亲较轻表型的遗传基础。
前瞻性病例系列研究。
一名几乎完全缺乏虹膜组织的女婴因先天性青光眼前来就诊并接受治疗。尽管临床初步诊断为无虹膜(《人类孟德尔遗传在线》[OMIM] AN2,#106210),但PAX6基因测序结果正常。对婴儿母亲的检查发现有Axenfeld-Rieger畸形(ARM):Schwabe线明显、虹膜轻度发育不全、虹膜条索跨越房角、眼压升高以及青光眼性视神经凹陷。父母及婴儿均接受了FOXC1基因诊断性DNA测序。在婴儿及其母亲中发现了杂合的M161K FOXC1突变,而眼部检查正常的父亲未发现该突变。
与杂合FOXC1突变相关的家族内表型变异范围可能很广。FOXC1突变可能是先天性青光眼合并临床无虹膜的病因。尽管此类婴儿与AN2表型相似,但因PAX6突变导致的AN2型青光眼通常为继发性,出生后数年发病。