Irgm1-flox Mouse
一般名
Irgm1-flox
製品ID
S-CKO-03038
背景情報
C57BL/6NCya
系統ID
CKOCMP-15944-Irgm1-B6N-VA
状況
このマウス系統を論文で使用する場合は、「Irgm1-flox Mouse(カタログ番号S-CKO-03038)はサイアジェンから購入しました。」と引用してください。
製品タイプ
年齢
遺伝子型
性別
数量
標準的な配送方法では、少なくとも3匹のヘテロ接合体キャリアを保証しています。ホモ接合体キャリアや指定された性別の個体の繁殖サービスも利用可能です。
基本情報
系統名
Irgm1-flox
系統ID
CKOCMP-15944-Irgm1-B6N-VA
遺伝子名
製品ID
S-CKO-03038
遺伝子別名
Ifi1, Irgm, Iigp3, Iipg3, Ifggd3
遺伝子別名
C57BL/6NCya
NCBI ID
修正
Conditional knockout
染色体
Chr 11
表現型
アプリケーション
--
さらに
系統詳細
EnsemblトランスクリプトID
ENSMUST00000049519
NCBIトランスクリプトID
NM_008326
ターゲット領域
Exon 3
有効領域の大きさ
~2.5 kb
遺伝子研究の概要
Irgm1, the mouse orthologue of human IRGM (Immunity-related GTPase family M protein), is a GTPase that plays crucial roles in processes like autophagy, mitophagy, and immune-related responses. It is associated with pathways such as the cGAS-STING-dependent type I interferon pathway, MAPK signaling, and the PI3K/AKT/mTOR pathway. Its functions are vital for maintaining normal cellular homeostasis, host defense, and are linked to various diseases [1-10].
In gene-knockout (KO) mouse models, Irgm1 deficiency leads to multiple phenotypes. Mice lacking Irgm1 exhibit a type I interferonopathy with autoimmune features, impaired mitophagy, and tissue-selective autoimmune pathologies, suggesting a connection between mitochondrial quality control and autoimmunity [1]. Irgm1+/- mice show increased atherosclerotic plaque stability due to inhibited macrophage apoptosis via reduced ROS generation and MAPK signaling [2]. In ulcerative colitis, berberine's anti-inflammatory effect is related to its targeting of Irgm1, reducing its overexpression and blocking the PI3K/AKT/mTOR pathway [3]. T cell-specific KO of Irgm1 causes changes in T cell numbers, function, metabolism, and increased apoptosis [4]. In acute liver failure, Irgm1 knockdown decreases autophagy and upregulates NLRP3 inflammasome activation [5]. Irgm1 knockdown in early-atherosclerotic mice reduces plaque burden by promoting lymphangiogenesis through LEC autophagy [6]. Also, Irgm1-deficient mice have a longer occlusion time and lower growth rate in thrombosis models, with inhibited neutrophil-platelet interactions [7]. Irgm1 knockout in mice indirectly inhibits skeletal muscle regeneration after injury due to a high interferon-gamma microenvironment [8].
In conclusion, Irgm1 is essential for processes like autophagy, mitophagy, and immune responses. KO and CKO mouse models have revealed its significance in autoimmune diseases, atherosclerosis, ulcerative colitis, liver failure, thrombosis, and muscle regeneration. Understanding Irgm1's functions through these models provides insights into disease mechanisms and potential therapeutic targets.
References:
1. Rai, Prashant, Janardhan, Kyathanahalli S, Meacham, Julie, Taylor, Gregory A, Fessler, Michael B. 2021. IRGM1 links mitochondrial quality control to autoimmunity. In Nature immunology, 22, 312-321. doi:10.1038/s41590-020-00859-0. https://pubmed.ncbi.nlm.nih.gov/33510463/
2. Fang, Shaohong, Sun, Song, Cai, Hengxuan, Yu, Bo, Sun, Bo. 2021. IRGM/Irgm1 facilitates macrophage apoptosis through ROS generation and MAPK signal transduction: Irgm1+/- mice display increases atherosclerotic plaque stability. In Theranostics, 11, 9358-9375. doi:10.7150/thno.62797. https://pubmed.ncbi.nlm.nih.gov/34646375/
3. Meng, Guibing, Li, Pengyan, Du, Xuemei, Feng, Xinchi, Qiu, Feng. 2024. Berberine alleviates ulcerative colitis by inhibiting inflammation through targeting IRGM1. In Phytomedicine : international journal of phytotherapy and phytopharmacology, 133, 155909. doi:10.1016/j.phymed.2024.155909. https://pubmed.ncbi.nlm.nih.gov/39068762/
4. Alwarawrah, Yazan, Danzaki, Keiko, Nichols, Amanda G, Taylor, Gregory A, MacIver, Nancie J. 2022. Irgm1 regulates metabolism and function in T cell subsets. In Scientific reports, 12, 850. doi:10.1038/s41598-021-04442-x. https://pubmed.ncbi.nlm.nih.gov/35039539/
5. Zhang, Xing, Hu, Yangyang, Wang, Wei, Wang, Yadong, Zhao, Caiyan. 2024. IRGM/Irgm1 increases autophagy to inhibit activation of NLRP3 inflammasome in inflammatory injury induced acute liver failure. In Cell death discovery, 10, 272. doi:10.1038/s41420-024-02052-w. https://pubmed.ncbi.nlm.nih.gov/38849356/
6. Cai, Hengxuan, Ma, Guanpeng, Zhang, Zhenming, Fang, Shaohong, Yu, Bo. 2024. A potential early-atheroprotective target: Irgm1 mediates lymphangiogenesis through LEC autophagy by Tfeb translocation. In Biochimica et biophysica acta. Molecular basis of disease, 1870, 167238. doi:10.1016/j.bbadis.2024.167238. https://pubmed.ncbi.nlm.nih.gov/38759815/
7. Sun, Song, Zou, Xiaoyi, Wang, Duo, Fu, Jin, Fang, Shaohong. 2022. IRGM/Irgm1 deficiency inhibits neutrophil-platelet interactions and thrombosis in experimental atherosclerosis and arterial injury. In Biomedicine & pharmacotherapy = Biomedecine & pharmacotherapie, 158, 114152. doi:10.1016/j.biopha.2022.114152. https://pubmed.ncbi.nlm.nih.gov/36580725/
8. Zhang, Liulei, Wang, Guangyou, Chen, Xin, Mu, Lili, Wang, Jinghua. 2020. Irgm1 knockout indirectly inhibits regeneration after skeletal muscle injury in mice. In International immunopharmacology, 84, 106515. doi:10.1016/j.intimp.2020.106515. https://pubmed.ncbi.nlm.nih.gov/32311672/
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