July 20, 2004 - The African clawed frog, Xenopus laevis , begins development as a compact ball
of cells that undergoes a dramatic transformation through cell migrations and positional rearrangements
that result in the separation of the embryo into three distinct germ layers, which go on to give rise
to all of the tissues and structures in the adult animal's body. During this transformation, known as
gastrulation, the embryo changes from a roughly spherical shape to an elongated, streamlined form through
a process called convergent extension (CE), in which polarized cells migrate to and merge at the embryo's
midline, driving it to lengthen along its anterior-posterior axis.
A number of genes involved in the regulation of convergent extension have been identified in amphibians
and other vertebrates, such as zebrafish, but the picture of the underlying molecular mechanisms remains
incomplete. In a report published in Nature Cell Biology , Noriaki Sasai and colleagues in
the RIKEN CDB Laboratory for Organogenesis and Neurogenesis (Kobe, Japan) show that the product of the
gene NRH1 is essential to the regulation of CE movements in the frog.
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Expression of NRH1 at the neurula stage (dorsal view;
anterior at top) |
While performing a screen of genes expressed in the posterior neuroectoderm, Sasai et al. identified
a gene encoding a protein that showed similarities to p75 NTR , a neurotrophin receptor. (Neurotrophins
are molecules that function in the survival, growth and migration of neurons.) However, on testing its
affinity for neurotrophin ligands, the group found that, unlike p75 NTR , NRH1 did not bind with neurotrophins,
which led them to seek other biological roles for the protein.
Experiments in which NRH1 was overexpressed by injecting its messenger RNA directly into very early
(4-cell stage) embryos resulted in shortening of the body axis and the failure of mesodermal and neural
plate marker gene expression to converge on the midline or extend axially. Interestingly, interfering
with NRH1 function by introducing morpholinos to block production of the NRH1 protein had
similar effects - the inhibition of convergent extension. That both gain and loss of NRH1 function
resulted in the failure of CE activity suggested that the gene's function in this process is tightly
regulated.
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Embryo injected with NRH1 morpholino
(top) shows shortened body axis due to
failure of convergent extension. Wild type embryo is shown below. |
These first findings led Sasai to investigate possible interactions between NRH1 and genes
involved in the Wnt/PCP (planar cell polarity) signaling pathway, which is also known to play
an important role in the regulation of CE movements in both fish and frog through the activity
of downstream small GTPases. This protein family, which includes Rho, Rac and Cdc42, interacts
with the cytoskeleton and plays important roles in the dynamics of cell morphology and motility.
Overexpression and loss-of-function of NRH1 in the marginal zone (where convergent extension originates)
respectively resulted in increased and decreased Rho, Rac and Cdc42 activity, confirming the link
between NRH1 and Rho-family small GTPases. Loss of NRH1 function could be rescued by the co-injection
of Frz7, a Wnt receptor functioning upstream of Rho, Rac and Cdc42 in the PCP pathway and, similarly,
NRH1 complemented a dominant-negative Frz7 phenotype, indicating the two proteins play compensatory
and mutually independent roles in the activation of small GTPases.
Further experiments showed that NRH1's effects on CE movements are also mediated by a second
branch of the Wnt/PCP pathway, in which MKK7 and JNK work to phosphorylate c-Jun in the animal
cap (a region of prospective ectoderm located on the roof of the blastocoel, a hollow in the spherical
early embryo). As with the small GTPases, the activation of the MKK7-JNK cascade could also be
effected by either Frz7 or NRH1, but it was found that NRH1 functioned independently of Xdsh ,
another upstream regulator of Rho-family small GTPase activity in the Wnt/PCP pathway. The transduction
mechanisms by which NRH1 interacts with Wnt/PCP signaling factors remain to be worked out, as
do the specifics of the inter-related but apparently independent roles of NRH1 and PCP signaling
in the control of cell movements within the developing embryo.
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