Genetics. Published Articles Ahead of Print: May 27, 2008, Copyright © 2008
doi:10.1534/genetics.108.088948


A more recent version of this article appeared on June 1, 2008.

REGULAR RESEARCH PAPERS

The T-box gene tbx-2, the homeobox gene egl-5, and the asymmetric cell division gene ham-1 specify neural fate in the HSN/PHB lineage

Aakanksha Singhvi 1, C. Andrew Frank 1 and Gian Garriga 1*

1 University of California, Berkeley

* To whom correspondence should be addressed. E-mail: garriga{at}berkeley.edu.

Submitted on March 5, 2008
Revised on April 5, 2008
Accepted on 5 April 2008


Abstract

Understanding how neurons adopt particular fates is a fundamental challenge in developmental neurobiology. To address this issue, we have been studying a C. elegans lineage that produces the HSN motor neuron and the PHB sensory neuron, sister cells produced by the HSN/PHB precursor. We have previously shown that the novel protein HAM-1 controls the asymmetric neuroblast division in this lineage. In this study we examine tbx-2 and egl-5, genes that act in concert with ham-1 to regulate HSN and PHB fate. In screens for mutants with abnormal HSN development, we identified the T-box protein TBX-2 as being important for both HSN and PHB differentiation. TBX-2, along with HAM-1, regulates the migrations of the HSNs and prevents the PHB neurons from adopting an apoptotic fate. The homeobox gene egl-5 has been shown to regulate the migration and later differentiation of the HSN. While mutations that disrupt its function show no obvious role for EGL-5 in PHB development, loss of egl-5 in a ham-1 mutant background leads to PHB differentiation defects. Expression of EGL-5 in the HSN/PHB precursor but not in the PHB neuron suggests that EGL-5 specifies precursor fate. These observations reveal a role for both EGL-5 and TBX-2 in neural fate specification in the HSN/PHB lineage.

Key Words: Hox, T-box, apoptosis, asymmetric cell division, neural fate