Open AccessMitf-family transcription factor function is required within cranial neural crest cells to promote choroid fissure closure
Author(s) -
Katie L. Sinagoga,
Alessandra Larimer-Picciani,
Stephanie M. George,
Samantha A. Spencer,
James Lister,
Jeffrey M. Gross
Publication year - 2020
Publication title -
development
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.754
H-Index - 325
eISSN - 1477-9129
pISSN - 0950-1991
DOI - 10.1242/dev.187047
Subject(s) - microphthalmia associated transcription factor , biology , zebrafish , neural crest , coloboma , transcription factor , microbiology and biotechnology , genetics , pitx2 , anatomy , gene , homeobox
A critical step in eye development is closure of the choroid fissure (CF), a transient structure in the ventral optic cup through which vasculature enters the eye and ganglion cell axons exit. While many factors have been identified that function during CF closure, the molecular and cellular mechanisms mediating this process remain poorly understood. Failure of CF closure results in colobomas. Recently, MITF was shown to be mutated in a subset of human coloboma patients, but how MITF functions during CF closure is unknown. To address this question, zebrafish with mutations in mitfa and tfec, two members of the Mitf-family of transcription factors, were analyzed and their functions during CF closure determined. mitfa;tfec mutants possess severe colobomas and our data demonstrate that Mitf activity is required within cranial neural crest cells (cNCCs) during CF closure. In the absence of Mitf function, cNCC migration and localization in the optic cup are perturbed. These data shed light on the cellular mechanisms underlying colobomas in patients with MITF mutations and identify a novel role for Mitf function in cNCCs during CF closure.