Cxcl17-KO Mouse
一般名
Cxcl17-KO
製品ID
S-KO-06588
背景情報
C57BL/6JCya
系統ID
KOCMP-232983-Cxcl17-B6J-VA
状況
このマウス系統を論文で使用する場合は、「Cxcl17-KO Mouse(カタログ番号S-KO-06588)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
Cxcl17-KO
系統ID
KOCMP-232983-Cxcl17-B6J-VA
遺伝子名
製品ID
S-KO-06588
遺伝子別名
Vcc1, VCC-1
遺伝子別名
C57BL/6JCya
NCBI ID
修正
Conventional knockout
染色体
Chr 7
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
ENSMUST00000200880
NCBIトランスクリプトID
NM_153576
ターゲット領域
Exon 2~3
有効領域の大きさ
~1.7 kb
遺伝子研究の概要
CXCL17 is the last described chemokine, which is abundantly and specifically expressed in mucosal sites [1]. It is thought to potentially exhibit chemotactic, anti-inflammatory, and antimicrobial activities under multiple biological conditions, and may be involved in processes like recruiting myeloid cells, regulating angiogenesis, and defending against pathogenic microorganisms [4]. Its receptor is still not well-determined, though GPR35 has been suggested as a putative receptor, though this has been questioned [3].
In a mouse model of liver ischemia-reperfusion injury, endothelial YAP/TEAD1-CXCL17 signaling was found to recruit myeloid-derived suppressor cells (MDSCs), which alleviated liver IRI-induced inflammation and damage by inhibiting M1 macrophage polarization [2]. In a mouse model of aerosol infection with the hypervirulent Mycobacterium tuberculosis HN878 strain, CXCL17 production increased in the lung during acute and chronic stages of infection, but CXCL17-/-mice were not more susceptible to TB than wild-type animals, suggesting a dispensable role during pulmonary TB [6]. In C57BL/6 male mice exposed to diesel exhaust emissions (DEE), AAV5-CXCL17 enhanced macrophage recruitment and clearance of DEE in the lungs, improving respiratory parameters, airway injury, and airway remodeling [5].
In conclusion, CXCL17 appears to play roles in inflammation-related processes such as liver ischemia-reperfusion injury, DEE-induced lung damage, and potentially in anti-microbial defense during tuberculosis infection. The use of gene knockout mouse models in these studies has provided insights into the specific functions of CXCL17 in these disease-relevant biological processes, highlighting its potential as a therapeutic target in certain disease areas.
References:
1. Xiao, Shiyu, Xie, Wenhui, Zhou, Liya. 2020. Mucosal chemokine CXCL17: What is known and not known. In Scandinavian journal of immunology, 93, e12965. doi:10.1111/sji.12965. https://pubmed.ncbi.nlm.nih.gov/32869346/
2. Zhang, Sitong, Sun, Zhongquan, Chen, Zhenhua, Ding, Yuan, Wang, Weilin. 2024. Endothelial YAP/TEAD1-CXCL17 signaling recruits myeloid-derived suppressor cells against liver ischemia-reperfusion injury. In Hepatology (Baltimore, Md.), 81, 888-902. doi:10.1097/HEP.0000000000000773. https://pubmed.ncbi.nlm.nih.gov/38407233/
3. Giblin, Sean Patrick, Pease, James Edward. 2023. What defines a chemokine? - The curious case of CXCL17. In Cytokine, 168, 156224. doi:10.1016/j.cyto.2023.156224. https://pubmed.ncbi.nlm.nih.gov/37210967/
4. Hashemi, Seyyede Fatemeh, Khorramdelazad, Hossein. 2022. The cryptic role of CXCL17/CXCR8 axis in the pathogenesis of cancers: a review of the latest evidence. In Journal of cell communication and signaling, 17, 409-422. doi:10.1007/s12079-022-00699-7. https://pubmed.ncbi.nlm.nih.gov/36352331/
5. Yin, Yize, Mu, Chaohui, Wang, Jiahui, Li, Qinghai, Han, Wei. 2023. CXCL17 Attenuates Diesel Exhaust Emissions Exposure-Induced Lung Damage by Regulating Macrophage Function. In Toxics, 11, . doi:10.3390/toxics11080646. https://pubmed.ncbi.nlm.nih.gov/37624152/
6. Choreño-Parra, José Alberto, Dunlap, Micah D, Swanson, Rosemary, Zúñiga, Joaquín, Khader, Shabaana A. 2021. CXCL17 Is Dispensable during Hypervirulent Mycobacterium tuberculosis HN878 Infection in Mice. In ImmunoHorizons, 5, 752-759. doi:10.4049/immunohorizons.2100048. https://pubmed.ncbi.nlm.nih.gov/34561226/
品質管理基準
精子検査
凍結前の精子濃度を測定し、精子の生存能力の判定します。
凍結後の精子では、各バッチから1本の凍結保存された精子を選び出し、体外受精に使用します。
環境基準:
SPF対応地域:
グローバル由来:
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