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C57BL/6JCya-Nmnat1em1flox/Cya
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C57BL/6JCya-Nmnat1em1flox/Cya

Common Name
Nmnat1-flox
Product ID
S-CKO-13095
Backgroud
C57BL/6JCya
Strain ID
CKOCMP-66454-Nmnat1-B6J-VA
Status
Research and Development
When using this mouse strain in a publication, please cite “Nmnat1-flox Mouse (Catalog S-CKO-13095) were purchased from Cyagen.”
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Basic Information
Strain Name
Nmnat1-flox
Strain ID
CKOCMP-66454-Nmnat1-B6J-VA
Gene Name
Nmnat1
Product ID
S-CKO-13095
Gene Alias
nmnat, D4Cole1e, 2610529L11Rik, 5730441G13Rik
Background
C57BL/6JCya
Gene Full Name
nicotinamide nucleotide adenylyltransferase 1
Modification
Conditional knockout
NCBI ID
66454 (Mouse)
Phenotype
MGI:1913704
Chromosome
Chr 4 (Mouse)
Application
--
Datasheet
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Rare Disease Data Center >>
Strain Description
Ensembl Transcript ID
ENSMUST00000030845
NCBI Transcript ID
NM_133435
Target Region
Exon 3
Size of Effective Region
~1.3 kb
Overview of Gene Research
Nmnat1, encoding nicotinamide mononucleotide adenylyltransferase 1, is a key enzyme in the synthesis of nicotinamide adenine dinucleotide (NAD+), an essential cofactor in redox reactions involved in multiple cellular processes. NAD+ salvage pathway mediated by Nmnat1 is crucial, and Nmnat1 is vital to embryonic development [3]. Genetic models, such as knockout (KO) and conditional knockout (CKO) mice, have been instrumental in studying its functions.

In PT-specific Nmnat1 CKO mice, Nmnat1 deficiency led to mitoribosome excess, hindered mitoribosomal translation of oxidative phosphorylation complex proteins, and caused mitoribosomal dysfunction in the context of diabetic nephropathy, suggesting its protective role in this disease [1]. In human iPS cell-derived retinal organoid differentiation, NMNAT1-KO cells showed reduced induction of genes for retinal early development and failure of retinal primordial structure formation, indicating NMNAT1 is essential for retinal fate differentiation [2]. Hepatic Nmnat1 KO mice had lower NAD+ levels but comparable metabolic activity and similar phenotypes in diet-induced fatty liver disease models, suggesting redundancy in obesity-induced hepatic disorders [3]. Adipocyte-specific Nmnat1 KO mice had a marked reduction in nuclear NAD+ concentration in brown adipose tissue, yet no impact on thermogenic and metabolic responses [4].

In conclusion, Nmnat1 is essential for maintaining normal cellular functions, especially in relation to NAD+ synthesis. Studies using Nmnat1 KO/CKO mouse models have provided insights into its role in diseases like diabetic nephropathy, retinal degeneration, and have also shown its dispensability in certain metabolic contexts such as diet-induced fatty liver disease and regulation of thermogenesis in adipose tissue.

References:
1. Hasegawa, Kazuhiro, Tamaki, Masanori, Sakamaki, Yusuke, Wakino, Shu. 2024. Nmnat1 Deficiency Causes Mitoribosome Excess in Diabetic Nephropathy Mediated by Transcriptional Repressor HIC1. In International journal of molecular sciences, 25, . doi:10.3390/ijms25126384. https://pubmed.ncbi.nlm.nih.gov/38928090/
2. Kuribayashi, Hiroshi, Iwagawa, Toshiro, Murakami, Akira, Suzuki, Yutaka, Watanabe, Sumiko. . NMNAT1 Is Essential for Human iPS Cell Differentiation to the Retinal Lineage. In Investigative ophthalmology & visual science, 65, 37. doi:10.1167/iovs.65.12.37. https://pubmed.ncbi.nlm.nih.gov/39446354/
3. Iqbal, Tooba, Nawaz, Allah, Karim, Mariam, Matsumoto, Michihiro, Nakagawa, Takashi. 2022. Loss of hepatic Nmnat1 has no impact on diet-induced fatty liver disease. In Biochemical and biophysical research communications, 636, 89-95. doi:10.1016/j.bbrc.2022.10.072. https://pubmed.ncbi.nlm.nih.gov/36332487/
4. Yamaguchi, Shintaro, Kojima, Daiki, Iqbal, Tooba, Nakagawa, Takashi, Yoshino, Jun. 2023. Adipocyte NMNAT1 expression is essential for nuclear NAD+ biosynthesis but dispensable for regulating thermogenesis and whole-body energy metabolism. In Biochemical and biophysical research communications, 674, 162-169. doi:10.1016/j.bbrc.2023.07.007. https://pubmed.ncbi.nlm.nih.gov/37421924/
Quality Control Standard
Sperm Test

Pre-cryopreservation: Measurement of sperm concentration, determination of sperm viability.

Post-cryopreservation: A vial of cryopreserved sperms is selected for in-vitro fertilization from each batch.

Environmental Standards:SPF
Available Region:Global
Source:Cyagen
Publications
Science Advances
2025-05-31
Hepatic NMNAT1 is required to defend against alcohol-associated fatty liver disease
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The industry is undergoing a rapid transformation driven by next-generation modalities, globalized markets, and upstream technological innovations.
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