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Fig. 3. Depletion of gata5 and gata6 from the YSL causes
cardia bifida but does not affect myelopoiesis. (A) The YSL
expression of gata5 and gata6 was depleted by injection of
gata5+gata6 morpholinos into the YSL at the 1000-cell stage. To trace
the correctly targeted embryos, a fluorescent control morpholino was
co-injected. Embryos positive for fluorescence in the YSL alone (+YSL) were
selected at several time points and harvested as YSL
gata5+gata6-depleted embryos. The embryos showing no fluorescence
(-YSL) were collected as negative injection controls and should express
wild-type levels of gata5 and gata6. To ensure the
efficiency of the morpholinos, positive control embryos were injected with
gata5+gata6 morpholinos at the one-cell stage and were fluorescent
throughout the embryo (+embryos). To assess heart formation, cmlc2
and nkx2.5 expression was analysed. Depletion of gata5 and
gata6 in the YSL (+YSL) showed normal levels of expression of both
cmlc2 and nkx2.5, indicating that specification occurs
normally in these embryos. However, cardia bifida was observed in the +YSL
embryos, demonstrating that gata5 and gata6 are required in
the YSL for the correct migration of the cardiac precursors to the midline. By
contrast, l-plastin expression was the same as in the wild-type
embryos, indicating that gata5 and gata6 expression in the
YSL is dispensable for myelopoiesis. Embryos injected at the one-cell stage
(+embryos) showed complete absence of cmlc2, nkx2.5 and
l-plastin expression, thereby validating morpholino effectiveness.
Views are anterior. For each gene and type (±YSL, +embryo) analysed,
n=28-38, and the images shown depict the findings for >95% of the
embryos. (B,C) Loss of endoderm in casanova morphant embryos
but no defects in myelopoiesis. To establish whether endoderm plays a role in
myelopoiesis, endodermless embryos were created by injection of
casanova morpholinos. Casanova morphants (casmo)
were assessed for endoderm formation and myelopoiesis. Myelopoiesis was not
affected in cas morphants as l-plastin and mpx
remained unaffected (B). Gene expression in the ALM of cas morphants
was examined at 5 and 10 somites (C). The formation of myeloid precursors
occurred as normal in cas morphants. Expression of pu1 at 5
somites, and runx1, ikaros and cmyb at 10 somites, was
unaffected in cas morphants. Views are anterior-dorsal. For each gene
analysed n=38-67, and the images shown depict the findings for
>95% of the embryos.
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