ライフサイエンスコーパス: NgR2

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1 he Nogo-66 receptor-1 (NgR1) and its homolog NgR2.

2 outgrowth but fail to associate with NgR1 or NgR2.

3 -66, and MAG compared with wild-type NgR1 or NgR2.

4 son of NgR surface residues not conserved in NgR2 and NgR3, identifies potential protein interaction

5 e similarity with NgR, two related proteins, NgR2 and NgR3, which we have identified, do not bind Nog

6 Nogo receptors (NgR1, NgR2, and NgR3) are growth cone directive molecules know

7 receptors of the Nogo Receptor family (NgR1, NgR2, and NgR3) restrict excitatory synapse formation.

8 of the structurally related molecules NgR1, NgR2, and NgR3.

9 In postnatal brain NgR1 and NgR2 are strongly enriched in Triton X-100-insoluble lip

10 The Nogo receptor family members NgR1 and NgR2 bind to MAIs and have been implicated in neuronal i

11 The CT-cap domain and stalk region of NgR2, but not NgR1, are sufficient for MAG binding, and

12 We also confirmed here that MAG binds to NgR2, but not to NgR3.

13 MAG binds NgR2 directly and with greater affinity than NgR1.

14 Soluble NgR2 has MAG antagonistic capacity and promotes neuronal

15 Neural expression studies of NgR1 and NgR2 have revealed broad and overlapping, yet distinct,

16 e first evidence for a physiological role of NgR2 in the peripheral nervous system.

17 Here we show that NgR2 is a novel receptor for MAG and acts selectively to

18 nt with its role as a neuronal MAG receptor, NgR2 is an axonassociated glycoprotein.

19 e we report that the Nogo66 receptor homolog NgR2 is essential for proper cutaneous innervation.

20 Forced expression of NgR2 is sufficient to impart MAG inhibition to neonatal

21 Structural studies have revealed that the NgR2 leucine-rich repeat cluster and the NgR2 "unique" d

22 NgR2(-/-) mice display increased density of nonpeptiderg

23 f total measured area in APP(swe)/PS1DeltaE9/NgR2(-/-) mice vs. 0.76% of total measured area in APP(s

24 gr3 (Ngr1(-/-); Ngr3(-/-)), but not Ngr1 and Ngr2 (Ngr1(-/-); Ngr2(-/-)), was sufficient to mimic the

25 Nogo receptor triple mutants (Ngr1(-/-); Ngr2(-/-); Ngr3(-/-); which are also known as Rtn4r, Rtn

26 ly and with high affinity to NgR1 but not to NgR2 or NgR3.

27 However, deletion of NgR2 renders nociceptive nonpeptidergic sensory neurons

28 The data suggest that Versican/NgR2 signaling at the dermo-epidermal junction acts in v

29 Biochemical evidence shows that NgR2 specifically interacts with the G3 domain of Versic

30 followed by a 13 aa MAG-binding motif of the NgR2 stalk, shows superior binding of OMgp, Nogo-66, and

31 In neurons NgR1 and NgR2 support MAG binding in a sialic acid-dependent Vibr

32 the NgR2 leucine-rich repeat cluster and the NgR2 "unique" domain are necessary for high-affinity MAG

33 When NgR2 was ablated in AD transgenic mice expressing Swedis

34 gr3(-/-)), but not Ngr1 and Ngr2 (Ngr1(-/-); Ngr2(-/-)), was sufficient to mimic the triple mutant re

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