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Our study did not repeatedly confirm the association of the rs2222973 or the rs11770843 SNP with adolescent idiopathic scoliosis in a Chinese Han population.
The most significant was DSCAM, a neurological gene expressed widely in the developing brain and in the amygdala and hippocampus of the adult brain.
DSCAM physically interacts with tubulin folding cofactor D (zeige TBCD ELISA Kits).
DSCAM as a Hirschsprung disease (HSCR (zeige EDNRB ELISA Kits)) susceptibility locus, both in Down syndrome and HSCR (zeige EDNRB ELISA Kits) isolated cases.
Down syndrome cell adhesion molecule interacts with PRKAG1 (zeige PRKAG1 ELISA Kits) subunit and plays an important role in netrin-1 (zeige NTN1 ELISA Kits) induced neurite outgrowth.
knockdown of DSCAM inhibits netrin-induced tyrosine phosphorylation of UNC5C (zeige Unc5c ELISA Kits) and Fyn (zeige FYN ELISA Kits) as well as the interaction of UNC5C (zeige Unc5c ELISA Kits) with Fyn (zeige FYN ELISA Kits). The double knockdown of both receptors abolishes the induction of Fyn (zeige FYN ELISA Kits) tyrosine phosphorylation by netrin-1 (zeige NTN1 ELISA Kits)
The specificity of Drosophila Dscam is due to complementarity of variable residues in epitope I.
Overall, our study found a significant association of IL-17RC (zeige IL17RC ELISA Kits) gene polymorphisms with AIS (zeige AR ELISA Kits) in a Chinese Han population, indicating IL-17RC (zeige IL17RC ELISA Kits) gene may be as a susceptibility gene for AIS (zeige AR ELISA Kits).
Dscam may be involved in the generation and development of intractable epilepsy.
functionally conserved with Drosophila Dscam[TM1] isoforms
Migrating cells utilize dscam to remodel the developing embryo
Together, these results demonstrate that different cell types have different dependencies on the PDZ-interacting C-termini of DSCAM and DSCAML1 for function, indicating multiple intracellular molecular mechanisms are involved.
work presents the correlation between DSCAM gene overexpression and a dysregulation of the P21-activated kinases pathway.
DSCAM mutation induces dystonic hypertonia and a disruption of locomotor gaits.
DSCAM mutation reduces or abolishes spinal reflexes in both neonatal isolated spinal cords and adult mice.
Results suggest that down syndrome cell adhesion molecule collaborates with deleted in colorectal cancer (zeige DCC ELISA Kits) to regulate microtubule dynamics via direct binding to dynamic TUBB3 (zeige TUBB3 ELISA Kits) in Netrin-1 (zeige NTN1 ELISA Kits)-induced axon branching.
Our results indicate an important role of DSCAM and DSCAML1 in the development of cortical neural network.
DSCAM colocalizes in developmentally dynamic patterns with adhesion and synaptic proteins in the mouse retina.
The findings of this study are as follows: (1) DSCAM is sufficient to drive cell death (2) dendrite avoidance defects in the Dscam loss-of-function retina do not reflect a role for DSCAM, and necessary and sufficient to target neurites.
A novel splice isoform of Dscam causes defects in lamination of type 2 and type 6 cone bipolar cells in Dscam mutant mice.
DSCAM contributes to pyramidal neuron morphogenesis by regulating dendrite arborization and spine formation during cortical circuit development
Dscam1, the role of which during heart development was previously unknown, is required for both normal migration of cardioblasts and luminal expansion.
Sema1a and Dscam1 might play essential roles in the Drosophila DA1 (zeige TPM2 ELISA Kits) ventral olfactory projection neurons morphogenesis.
Studies suggest that the somatic mutually alternative splicing within a single gene may offer a simplified way of expressing a large Dscam repertoire.
Protein production, crystallization and preliminary crystallographic analysis of the four N-terminal immunoglobulin domains of Dscam1 has been reported.
Dysregulated Dscam binds to Abl through its cytoplasmic domain to enlarge presynaptic arbors in the Drosophila fragile X (zeige FMR1 ELISA Kits) syndrome model.
As thousands of Dscam isoforms are needed for the self-avoidance of the neuron, we propose that an increase in self-binding affinity provides the basis for the successful evolution of the arthropod brain
Manipulation of the Dscam1 isoform pool in single neurons caused severe disruption of collateral formation of mechanosensory axons.
The data of this study suggested that Dscam1 is required cell autonomously for normal adult motoneuron dendrite growth in Drosophila.
Dscam1 splicing is probabilistic through the analysis of alternative exon 4 expression using splicing reporters; widespread probabilistic splicing supports a role for Dscam1 diversity in self-recognition throughout the developing nervous system.
The found uncover a function of Dscam in presynaptic size control and provide insights into how dysregulated Dscam may contribute to the pathogenesis of neurological disorders.
This gene is a member of the immunoglobulin superfamily of cell adhesion molecules (Ig-CAMs), and is involved in human central and peripheral nervous system development. This gene is a candidate for Down syndrome and congenital heart disease (DSCHD). A gene encoding a similar Ig-CAM protein is located on chromosome 11. Alternatively spliced transcript variants encoding multiple isoforms have been observed for this gene.
, human CHD2-52 down syndrome cell adhesion molecule
, Down syndrome cell adhesion molecule
, Down syndrome cell adhesion molecule homolog
, Down's syndrome cell adhesion molecule
, down syndrome cell adhesion molecule
, down syndrome cell-adhesion molecule
, drosophila down syndrome cell adhesion molecule
, drosophila down syndrome cell adhesion molecule 1
, down syndrome cell adhesion molecule-like