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Literature DB >> 24838312

Crosstalk between Agrin and Wnt signaling pathways in development of vertebrate neuromuscular junction.

Arnab Barik¹, Bin Zhang, Gurkirpal S Sohal, Wen-Cheng Xiong, Lin Mei.

Abstract

Neuromuscular junction (NMJ) is a cholinergic synapse where motor neurons elicit muscle contraction. Agrin and its coreceptors LRP4 and MuSK are critical for vertebrate NMJ formation. This paper reviews recent evidence for Wnts and Wnt signaling molecules in NMJ formation including a possible retrograde mechanism by muscle β-catenin. We also present data that Wnt3a, 7a, 8a and 10b could inhibit agrin-mediated AChR clustering. Together with the stimulating effect of Wnt9a, 9b, 10b, 11 and 16 on AChR clustering in the absence of agrin, these results suggest diverse roles for Wnt ligands in NMJ development.

Entities: Disease Gene

Keywords: LRP4; NMJ; WNT; aneural clusters; musk

Mesh：

Substances：
Agrin

Year: 2014 PMID： 24838312 DOI： 10.1002/dneu.22190

Source DB: PubMed Journal: Dev Neurobiol ISSN： 1932-8451 Impact factor: 3.964

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Cited

28 in total

1. Muscle Yap Is a Regulator of Neuromuscular Junction Formation and Regeneration.

Authors: Kai Zhao; Chengyong Shen; Yisheng Lu; Zhihui Huang; Lei Li; Christopher D Rand; Jinxiu Pan; Xiang-Dong Sun; Zhibing Tan; Hongsheng Wang; Guanglin Xing; Yu Cao; Guoqing Hu; Jiliang Zhou; Wen-Cheng Xiong; Lin Mei
Journal: J Neurosci Date: 2017-02-17 Impact factor: 6.167

Crosstalk between Agrin and Wnt signaling pathways in development of vertebrate neuromuscular junction.

1. Muscle Yap Is a Regulator of Neuromuscular Junction Formation and Regeneration.

Review 2. Moving forward with the neuromuscular junction.

3. Schwann Cells in Neuromuscular Junction Formation and Maintenance.

Review 4. Mechanical regulation of musculoskeletal system development.

5. iPSC-derived functional human neuromuscular junctions model the pathophysiology of neuromuscular diseases.

Review 6. Neuromuscular junction degeneration in muscle wasting.

7. LRP4 is critical for neuromuscular junction maintenance.

8. Phosphorylation of α-dystrobrevin is essential for αkap accumulation and acetylcholine receptor stability.

9. Diverging roles for Lrp4 and Wnt signaling in neuromuscular synapse development during evolution.

10. Slit2 as a β-catenin/Ctnnb1-dependent retrograde signal for presynaptic differentiation.