Ritanserin, a potent serotonin 2A receptor antagonist, represses MEK/ERK signalling pathway to restore PAX6 production and function in aniridia-like cellular model.

Aniridia is a panocular inherited rare eye disease linked to heterozygous mutations on the PAX6 gene, which fail to properly produce sufficient protein essential for normal eye development and function. Most of the patients suffer from aniridia-related keratopathy, a progressive opacification of the cornea. There is no effective treatment for this blinding disease. Here we screen for small compounds and identified Ritanserin, a serotonin 2A receptor antagonist, that can rescue PAX6 haploinsufficiency of mutant limbal cells, defective cell migration and PAX6-target gene expression. We further demonstrated that Ritanserin activates PAX6 production through the selective inactivation of the MEK/ERK signaling pathway. Our data strongly suggest that repurposing this therapeutic molecule could be effective in preventing or treating existing blindness by restoring corneal transparency.

Heterozygous FOXC1 mutation (M161K) associated with congenital glaucoma and aniridia in an infant and a milder phenotype in her mother.

PURPOSE: To report the genetic basis for congenital glaucoma with clinical aniridia in an infant and a milder phenotype in her mother. METHODS: Prospective case series. RESULTS: 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. DISCUSSION: 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.

Aniridia: estudio de los tratamientos y costes orientativos / Aniride: study of the treatments and orientative costs

El objeto de este trabajo ha sido el estudio del tratamiento de las principales alteraciones oculares asociadas a aniridia susceptibles de ser tratadas farmacológicamente (glaucoma y ojo seco) así como de las ayudas a la baja visión necesarias para mejorar la calidad de vida de los pacientes. El estudio se realizó desde un punto de vista tanto terapéutico como económico (cálculo aproximado de los costes de tratamiento). Asimismo se realizó una aproximación a las prestaciones ofertadas por la administración para los afectados

The aim of the present work was the study of the treatment of the main ocular diseases associated to aniridia able to be treated with drugs (glaucoma and dry eye) as well as the helps to the low vision which are needed to improve the quality of life of pacients. The study was performed from a therapeutic and economic point of view (estimated treatment cost). A little overview about the helps offered by the administration were considered as well