1. that increasing NMNAT1 levels can slow the progression of symptoms and neuropathological features of tauopathy PMID: 29175372
2. Using steady-state and flux analysis of NAD(+) metabolites in healthy and injured mouse dorsal root ganglion axons, we find that rather than altering NAD(+) synthesis, NMNAT1 instead blocks the injury-induced, SARM1-dependent NAD(+) consumption that is central to axon degeneration. PMID: 27735788
3. Mouse-non nuclear-nicotinamide mononucleotide adenylyltransferase type 1 maintains mitochondrial nicotinamide levels and thereby supports mitochondrial unfolded protein response function and mitochondrial proteostasis in injured neurons. PMID: 26913604
4. NMNAT1 overexpression enhanced AMPK activity in oxygen-glucose deprivation treated cortical neurons PMID: 25841561
5. An increased level of Nmnat protein in hiw mutants is both required and sufficient to inhibit axonal degeneration. PMID: 23226106
6. Overexpression of Nmnat1 in the cytoplasm and axons of RGCs robustly protected against both ischemic and glaucomatous loss of RGC axonal integrity, as well as loss of RGC soma. PMID: 23211826
7. Findings reveal a novel role for NMNAT1 in the morphogenesis of developing cortical neurons, which indicate that the loss of function of NMNAT1 may contribute to different neurodegenerative disorders in central nervous system. PMID: 22088538
8. Nicotinamide mononucleotide adenylyl transferase 1 protects against acute neurodegeneration in developing CNS by inhibiting excitotoxic-necrotic cell death. PMID: 22058226
9. NMNAT1 is indispensable for the normal development of the embryo. Decreased NMNAT1 activity in heterozygous null mice does not affect the rate of Wallerian degeneration, suggesting that endogenous NMNAT1 does not have a primary role in axon maintenance. PMID: 21615689
10. nicotinamide mononucleotide adenylyltransferase (Nmnat) protein transduction into transected axons blocks axonal degeneration PMID: 21071441
11. Through NAMPT activity, visfatin contributes to vascular inflammation, causing atherothrombotic diseases linked to metabolic disorders. PMID: 19727662
12. demonstrated that increased Nmnat activity is responsible for the axon-sparing activity of the Wlds protein; also demonstrated that SIRT1 is the downstream effector of increased Nmnat activity that leads to PMID: 15310905
13. Nmnat1 is significantly weaker than Wld(S) at protecting axons against traumatic or toxic injury in vitro, and has no detectable effect in vivo PMID: 16645633
14. results suggest that axonal protection by NMNAT expression in neurons is provided by modifying mitochondrial function PMID: 19439605
15. This study provided the evidence that Nmnat1 protein manifest robust delay in axonal degeneration. PMID: 19458223

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KEGG: mmu:66454

STRING: 10090.ENSMUSP00000030845

UniGene: Mm.76062