. Binding to SEP3 was usually withi

. Binding to SEP3 was usually within a few
hundred bp upstream or downstream of coding sequences, 72% of
which were differentially expressed during flower development or
in floral homeoticmutants, suggesting that themajority of SEP3 targets
were functionally relevant. There was a large overlap between
sites bound in the wt and in the ag mutant, suggesting that many
SEP3 targets are shared between perianth and reproductive organs,
although the regulatory outcome (activation or repression) might
vary in different organs. Finally, gene ontology analysis revealed
that the direct targets of SEP3 had a functional bias similar to that
found in the transcriptome of early buds, with enrichment for genes
encoding transcription factors, genes involved in the synthesis and
response to hormones (particularly auxin) and in lipid metabolism.
In summary, early and direct targets of organ identity targets are
enriched for genes encoding transcription factors and include the
organ identity genes themselves, whose expression is maintained
by auto-regulatory loops. Genes involved in hormone synthesis and
responses also feature prominently among the target genes. The
sets of targets change as development progresses and ultimately
organ identity genes modify the expression of thousands of genes,
particularly in reproductive organs.