Expression, Localization, and Biochemical Characterization of Nicotinamide Mononucleotide Adenylyltransferase 2

Mayer, Paul R.; Huang, Niu; Dewey, Colleen M.; Dries, Daniel R.; Zhang, Hong; Yu, Gang

doi:10.1074/jbc.m110.178913

Cited by 67 publications

(82 citation statements)

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“…At 1q25, rs2022013 located in the first intron of nicotinamide mononucleotide adenylyltransferase 2 ( NMNAT2 ) was associated with SLE in GWAS (p=1.1×10 −7 , OR=0.85) and in a large-scale replication study (p=1.5×10 −3 , OR=0.92) using European-derived subjects,2 3 thus suggesting NMNAT2 as a SLE risk locus. NMNAT2, mainly expressed in the brain, is a central enzyme in the nicotinamide adenine dinucleotide biosynthetic pathway that is known to delay axon degeneration 4 5. Given no apparent clues for its involvement in immune dysregulation, we fine-mapped NMNAT2 and its neighbouring genes in four major populations, confirmed NMNAT2 association with SLE in European American (EA) and Amerindian/Hispanic (HS) ancestries and identified independent association at SMG7 in EA only.…”

Section: Introductionmentioning

confidence: 85%

Decreased SMG7 expression associates with lupus-risk variants and elevated antinuclear antibody production

et al. 2016

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Objectives Following up the SLE GWAS identification of NMNAT2 at rs2022013, we fine-mapped its 150kb flanking regions containing NMNAT2 and SMG7 in a 15,292 case-control multi-ancestry population and tested functions of identified variants. Methods We performed genotyping using custom array, imputation by IMPUTE 2.1.2, and allele specific functions using qRT-PCR and luciferase reporter transfections. SLE PBMCs were cultured with siRNAs to measure antinuclear antibody (ANA) and cyto/chemokine levels in supernatants using ELISA. Results We confirmed association at NMNAT2 in European American (EA) and Amerindian/Hispanic ancestries, and identified independent signal at SMG7 tagged by rs2702178 in EA only (P=2.4×10−8, OR=1.23 [95%CI=1.14–1.32]). In complete linkage disequilibrium with rs2702178, rs2275675 in the promoter region robustly associated with SMG7 mRNA levels in multiple expression quantitative trait locus datasets. Its risk allele was dose-dependently associated with decreased SMG7 mRNA levels in PBMCs of 86 SLE patients and 119 controls (P=1.1×10−3 and 6.8×10−8, respectively) and conferred reduced transcription activity in transfected HEK-293 and Raji cells (P=0.0035 and 0.0037, respectively). As a critical component in the nonsense-mediated mRNA decay pathway, SMG7 could regulate autoantigens including RNP and Sm. We showed SMG7 mRNA levels in PBMCs correlated inversely with ANA titers of SLE patients (r=−0.31, P=0.01), and SMG7 knockdown increased levels of ANA IgG and CCL19 in SLE PBMCs (P=2.0×10−5 and 2.0×10−4, respectively). Conclusions We confirmed NMNAT2 and identified independent SMG7 association with SLE. The inverse relationship between levels of the risk-allele associated SMG7 mRNAs and ANA suggested the novel contribution of mRNA surveillance pathway to SLE pathogenesis.

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Section: Introductionmentioning

confidence: 85%

Decreased SMG7 expression associates with lupus-risk variants and elevated antinuclear antibody production

et al. 2016

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“…Other mouse strains and animal work C57BL/6OlaHsd-Wld (Wld S ) mice were obtained from Harlan UK, FLPe transgenic mice (Rodríguez et al, 2000) were obtained from Martin Turner (Babraham Institute), and Nmnat2 gtBay mice, derived from gene trap ES cell clone RRF238 (BayGenomics), were described previously (Mayer et al, 2010).…”

Section: Methodsmentioning

confidence: 99%

“…Nmnat2 gtBAY/gtE compound heterozygotes, with further reduced NMNAT2 levels, are also outwardly healthy up to this age. Given that NMNAT2 is a low abundance protein (Mayer et al, 2010), this sets a surprisingly low threshold of NMNAT2 for normal development and animal survival, although enzyme activity will amplify its effects. The finding that conditional silencing of a single Nmnat2 allele in primary culture is sufficient to trigger distal neurite degeneration was therefore both unexpected and intriguing.…”

Section: Nmnat2mentioning

confidence: 99%

“…Samples were microfuged at 10,000 ϫ g to pellet cell debris, and the supernatant was mixed with 2ϫ Laemmli sample buffer. This step was included to facilitate detection of NMNAT2, which is a nonabundant protein (Mayer et al, 2010). There was no significant loss of NMNAT2 in the pellet.…”

Section: Immunoblottingmentioning

confidence: 99%

“…We crossed Nmnat2 ϩ/gtE mice to mice heterozygous for an alternative gene-trapped Nmnat2 allele (termed Nmnat2 gtBay to distinguish it from the Nmnat2 gtE allele), which suppresses expression from the trapped allele by only ϳ50% (Mayer et al, 2010). This produced compound heterozygotes (Nmnat2 gtBay/gtE ) expressing Nmnat2 mRNA and NMNAT2 protein at ϳ25% of wild-type levels (Fig.…”

Section: Mice Expressing Subheterozygous Levels Of Nmnat2 Are Viablementioning

confidence: 99%

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Rescue of Peripheral and CNS Axon Defects in Mice Lacking NMNAT2

Gilley

Adalbert

Yu³

et al. 2013

J. Neurosci.

110

171

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NMNAT2 is an NADϩ -synthesizing enzyme with an essential axon maintenance role in primary culture neurons. We have generated an Nmnat2 gene trap mouse to examine the role of NMNAT2 in vivo. Homozygotes die perinatally with a severe peripheral nerve/axon defect and truncated axons in the optic nerve and other CNS regions. The cause appears to be limited axon extension, rather than dying-back degeneration of existing axons, which was previously proposed for the NMNAT2-deficient Blad mutant mouse. Neurite outgrowth in both PNS and CNS neuronal cultures consistently stalls at 1-2 mm, similar to the length of truncated axons in the embryos. Crucially, this suggests an essential role for NMNAT2 during axon growth. In addition, we show that the Wallerian degeneration slow protein (Wld S ), a more stable, aberrant NMNAT that can substitute the axon maintenance function of NMNAT2 in primary cultures, can also correct developmental defects associated with NMNAT2 deficiency. This is dose-dependent, with extension of life span to at least 3 months by homozygous levels of Wld S the most obvious manifestation. Finally, we propose that endogenous mechanisms also compensate for otherwise limiting levels of NMNAT2. This could explain our finding that conditional silencing of a single Nmnat2 allele triggers substantial degeneration of established neurites, whereas similar, or greater, reduction of NMNAT2 in constitutively depleted neurons is compatible with normal axon growth and survival. A requirement for NMNAT2 for both axon growth and maintenance suggests that reduced levels could impair axon regeneration as well as axon survival in aging and disease.

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Niacin

Penberthy

Kirkland

2012

Present Knowledge in Nutrition

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Expression, Localization, and Biochemical Characterization of Nicotinamide Mononucleotide Adenylyltransferase 2

Cited by 67 publications

References 68 publications

Decreased SMG7 expression associates with lupus-risk variants and elevated antinuclear antibody production

Decreased SMG7 expression associates with lupus-risk variants and elevated antinuclear antibody production

Rescue of Peripheral and CNS Axon Defects in Mice Lacking NMNAT2

Niacin

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