L1 is an important protein for the development of the
nervous system affecting both cell adhesion and motility.
Cell adhesion L1 has a static function as a
cell adhesion molecule which connects different cells. It is involved in the
adhesion between
neurons and in the growth and association of neurites called neurite fasciculation.
Cell motility Motility promoting functions are related to the regulation of the movement of nerve cells during
neural development. L1 is present in developing neurons and plays an important role in guiding new neurons into the correct positions and helping axons grow and make connections with other neurons. L1 is also involved in
synaptic plasticity, which is the ability of synapses to strengthen or weaken, and it also plays a role in regeneration after trauma. Some studies have proved that L1 has a role in tumor growth, tumor cell invasion, metastasis of melanoma, ovarian and colon cancer due to an overexpression of the protein L1 that improves cell motion of the malignant cells. The domains of this protein promote homophilic interactions, where adhesion molecules on one cell interact with identical molecules on the other cell. And also heterophilic interactions, where an adhesion molecule on one cell works as a receptor that connects with a different molecule on the other cell. These interactions promote
cell adhesion and regulation of
signal transduction. In addition, L1 participates in myelination processes, which are involved in the proliferation of myelin through the nervous system (specifically the progressive myelination of nerve axon fibers), by mediating the elongation of
Schwann cells along the axon.
Nervous system L1 is involved in neuron-neuron adhesion, neurite fasciculation, outgrowth of neurites, cerebellar granule cell migration, neurite outgrowth on
Schwann cells and interactions among epithelial cells of intestinal crypts. As a consequence, mutations in the L1CAM gene cause the
Nervous System to malfunction. The main disorders linked to this mutation are known by the acronym CRASH or can be also referred as
L1 syndrome. This includes disorders such as
HSAS,
MASA syndrome,
agenesis of the corpus callosum and
spastic paraplegia. Lower limb spasticity,
mental retardation,
hydrocephalus and flexion deformity of the thumbs are some of the symptoms expressed mostly in male individuals who suffer from this condition. Although the pathological mechanisms leading to L1 syndrome are still unknown, about 200 mutations of the L1CAM gene have been identified and then associated with the syndrom. These mutations mostly affect structurally important key residues in the extracellular region of L1 causing alterations in the protein binding properties, which correlate to the impairment of neuronal physiological mechanisms such as
cell adhesion or specific interacting with other molecules.
Ankyrin interaction with L1CAM is an example of a protein binding that fails in CRASH patients due to a mutation that causes
leucine and
histidine to replace
serine and
tyrosine respectively, in the SFIGQY motif, where ankyrin should be bound in the L1CAM family cytoplasmic terminus. Ankyrin-L1CAM interaction is involved in the
growth cone initiation, consequently, a failure in this interaction causes neurites to not reach synaptic target. Furthermore, evidence shows there is a correlation between
fetal alcohol spectrum disorder and L1 protein since
ethanol inhibits L1-mediated adhesion and neurite outgrowth.
Hirschsprung's disease has also been linked to a L1CAM malfunction. ==Transcription and synthesis==