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Query: UMLS:C0344329 (
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28,634
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Close homolog of L1
(
CHL1
) is a transmembrane cell adhesion molecule with unique developmental functions in cortical neuronal positioning and dendritic projection within the L1 family, as well as shared functions in promotion of integrin-dependent neurite outgrowth and semaphorin3A (Sema3A)-mediated axon repulsion. The molecular mechanisms by which
CHL1
mediates these diverse functions are obscure. Here it is demonstrated using a cytofluorescence assay that
CHL1
is able to recruit ezrin, a member of the ezrin-radixin-moesin (ERM) family of filamentous actin binding proteins to the plasma membrane, and that this requires a membrane-proximal motif (RGGKYSV) in the
CHL1
cytoplasmic domain. This sequence in
CHL1
is shown to have novel functions necessary for Sema3A-induced growth cone
collapse
and
CHL1
-dependent neurite outgrowth and branching in cortical embryonic neurons. In addition, stimulation of haptotactic cell migration and cellular adhesion to fibronectin by
CHL1
depends on the
CHL1
/ERM recruitment motif. These findings suggest that a direct or indirect interaction between
CHL1
and ERM proteins mediates Sema3A-induced growth cone
collapse
as well as neurite outgrowth and branching, which are essential determinants of axon guidance and connectivity in cortical development.
...
PMID:CHL1 promotes Sema3A-induced growth cone collapse and neurite elaboration through a motif required for recruitment of ERM proteins to the plasma membrane. 1799 39
We report a cooperation between the neural adhesion molecule
close homolog of L1
(
CHL1
) and the semaphorin 3A (Sema3A) receptor, neuropilin 1 (Npn1), important for establishment of area-specific thalamocortical projections.
CHL1
deletion in mice selectively disrupted the projection of somatosensory thalamic axons from the ventrobasal (VB) nuclei, causing them to shift caudally and target the visual cortex. At the ventral telencephalon, an intermediate target with graded Sema3A expression, VB axons were caudally shifted in
CHL1
- embryos and in Npn1(Sema-/-) mutants, in which axons are nonresponsive to Sema3A.
CHL1
colocalized with Npn1 on thalamic axons, and associated with Npn1 through a sequence in the
CHL1
Ig1 domain that was required for Sema3A-induced growth cone
collapse
. These results identify a novel function for
CHL1
in thalamic axon responsiveness to ventral telencephalic cues, and demonstrate a role for
CHL1
and Npn1 in establishment of proper targeting of specific thalamocortical projections.
...
PMID:Close homolog of L1 and neuropilin 1 mediate guidance of thalamocortical axons at the ventral telencephalon. 1807 78
Neural cell adhesion molecule
close homolog of L1
(
CHL1
) is a regulator of topographic targeting of thalamic axons to the somatosensory cortex (S1) but little is known about its cooperation with other L1 class molecules. To investigate this,
CHL1
(-/-)/L1(-/y) double mutant mice were generated and analyzed for thalamocortical axon topography. Double mutants exhibited a striking posterior shift of axons from motor thalamic nuclei to the visual cortex (V1), which was not observed in single mutants. In wild-type (WT) embryos, L1 and
CHL1
were coexpressed in the dorsal thalamus (DT) and on fibers along the thalamocortical projection in the ventral telencephalon and cortex. L1 and
CHL1
colocalized on growth cones and neurites of cortical and thalamic neurons in culture. Growth cone
collapse
assays with WT and mutant neurons demonstrated a requirement for L1 and
CHL1
in repellent responses to EphrinA5, a guidance factor for thalamic axons. L1 coimmunoprecipitated with the principal EphrinA5 receptors expressed in the DT (EphA3, EphA4, and EphA7), whereas
CHL1
associated selectively with EphA7. These results implicate a novel mechanism in which L1 and
CHL1
interact with individual EphA receptors and cooperate to guide subpopulations of thalamic axons to distinct neocortical areas essential for thalamocortical connectivity.
...
PMID:L1 and CHL1 Cooperate in Thalamocortical Axon Targeting. 2057 28