The columnar gene vnd is required for tritocerebral neuromere formation during embryonic brain development of Drosophila.

6533b838fe1ef96bd12a4840

RESEARCH PRODUCT

The columnar gene vnd is required for tritocerebral neuromere formation during embryonic brain development of Drosophila.

Filippo M. Rijli Rolf Urbach Heinrich Reichert Simon G. Sprecher Simon G. Sprecher Gerhard M. Technau Frank Hirth

subject

Nervous system Mutant Apoptosis 0302 clinical medicine MESH: Gene Expression Regulation Developmental Drosophila Proteins MESH: Animals Axon Hox gene MESH: Melatonin Genetics 0303 health sciences MESH: Pineal Gland Brain Gene Expression Regulation Developmental MESH: Transcription Factors Neuromere Phenotype Biological Evolution Cell biology medicine.anatomical_structure Drosophila melanogaster Phenotype MESH: Photic Stimulation MESH: Body Patterning MESH: Mutation MESH: Drosophila Proteins Biology MESH: Phenotype MESH: Drosophila melanogaster 03 medical and health sciences MESH: Brain Neuroblast MESH: Evolution MESH: Homeodomain Proteins medicine Animals MESH: Circadian Rhythm Molecular Biology 030304 developmental biology Body Patterning Homeodomain Proteins MESH: Humans MESH: Apoptosis Embryogenesis [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry Molecular Biology/Molecular biology MESH: Light Mutation MESH: Serotonin MESH: Seasons 030217 neurology & neurosurgery Developmental Biology Transcription Factors

description

International audience; In Drosophila, evolutionarily conserved transcription factors are required for the specification of neural lineages along the anteroposterior and dorsoventral axes, such as Hox genes for anteroposterior and columnar genes for dorsoventral patterning. In this report, we analyse the role of the columnar patterning gene ventral nervous system defective (vnd) in embryonic brain development. Expression of vnd is observed in specific subsets of cells in all brain neuromeres. Loss-of-function analysis focussed on the tritocerebrum shows that inactivation of vnd results in regionalized axonal patterning defects, which are comparable with the brain phenotype caused by mutation of the Hox gene labial (lab). However, in contrast to lab activity in specifying tritocerebral neuronal identity, vnd is required for the formation and specification of tritocerebral neural lineages. Thus, in early vnd mutant embryos, the Tv1-Tv5 neuroblasts, which normally express lab, do not form. Later in embryogenesis, vnd mutants show an extensive loss of lab-expressing cells because of increased apoptotic activity, resulting in a gap-like brain phenotype that is characterized by an almost complete absence of the tritocerebral neuromere. Correspondingly, genetic block of apoptosis in vnd mutant embryos partially restores tritocerebral cells as well as axon tracts. Taken together, our results indicate that vnd is required for the genesis and proper identity specification of tritocerebral neural lineages during embryonic brain development of Drosophila.

year	journal	country	edition	language
2006-11-01

10.1242/dev.02606 https://hal.archives-ouvertes.fr/hal-00188150