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HOXA13 regulates Aldh1a2 expression in the autopod to facilitate interdigital programmed cell death
Author(s) -
Shou Siming,
Carlson Hanqian L.,
Perez Wilma D.,
Stadler H. Scott
Publication year - 2013
Publication title -
developmental dynamics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.634
H-Index - 141
eISSN - 1097-0177
pISSN - 1058-8388
DOI - 10.1002/dvdy.23966
Subject(s) - biology , retinoic acid , limb development , microbiology and biotechnology , mutant , transcription factor , genetics , gene
Background : Retinoic acid (RA), plays an essential role in the growth and patterning of vertebrate limb. While the developmental processes regulated by RA are well understood, little is known about the transcriptional mechanisms required to precisely control limb RA synthesis. Here, Aldh1a2 functions as the primary enzyme necessary for RA production which regulates forelimb outgrowth and hindlimb digit separation. Because mice lacking HOXA13 exhibit similar defects in digit separation as Aldh1a2 mutants, we hypothesized that HOXA13 regulates Aldh1a2 to facilitate RA‐mediated interdigital programmed cell death (IPCD) and digit separation. Results: In this report, we identify Aldh1a2 as a direct target of HOXA13. In absence of HOXA13 function, Aldh1a2 expression, RA signaling, and IPCD are reduced. In the limb, HOXA13 binds a conserved cis ‐regulatory element in the Aldh1a2 locus that can be regulated by HOXA13 to promote gene expression. Finally, decreased RA signaling and IPCD can be partially rescued in the Hoxa13 mutant hindlimb by maternal RA supplementation. Conclusions: Defects in IPCD and digit separation in Hoxa13 mutant mice may be caused in part by reduced levels of RA signaling stemming from a loss in the direct regulation of Aldh1a2 . These findings provide new insights into the transcriptional regulation of RA signaling necessary for limb morphogenesis. Developmental Dynamics 242:687–698, 2013 . © 2013 Wiley Periodicals, Inc.

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