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B6-hKLB Mouse
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B6-hKLB Mouse
製品名
B6-hKLB Mouse
製品ID
C001622
系統名
C57BL/6NCya-Klbem1(hKLB)/Cya
背景情報
C57BL/6NCya
状況
このマウス系統を論文で使用する場合は、「B6-hKLB Mouse(カタログ番号C001622)はサイアジェンから購入しました。」と引用してください。
Metabolic Target Humanized Mouse Models
Obesity and Diabetes Mellitus
MASH and Fibrosis
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。
お見積もりについてはこちらまでご連絡ください
Metabolic Target Humanized Mouse Models
Obesity and Diabetes Mellitus
MASH and Fibrosis
基本情報
関連リソース
基本情報
遺伝子名
遺伝子別名
BKL
NCBI ID
染色体
Chr 4
MGI ID
さらに
系統詳細
The KLB gene encodes β-Klotho, a transmembrane protein that functions as an obligate co-receptor for fibroblast growth factor (FGF) receptors, specifically for the endocrine FGF ligands FGF19 and FGF21 [1]. Expressed across metabolic tissues, including adipose, liver, and pancreas, KLB is a critical regulator of FGF19 and FGF21 signaling, impacting glucose homeostasis, energy balance, and bile acid metabolism [1-3]. β-Klotho facilitates FGF19 and FGF21 signaling through direct interaction with FGF receptors [1]. KLB gene expression is observed across various tissues, encompassing metabolic, haematopoietic, foetal, and adult tissues [1]. Perturbations in KLB function and genetic variants have been implicated in a range of disorders, including hypogonadotropic hypogonadism, male infertility, obesity, non-alcoholic fatty liver disease, irritable bowel syndrome, and potentially certain malignancies [1-4]. Thus, KLB emerges as a pivotal gene in FGF signaling, exerting pleiotropic effects on metabolic physiology and disease [1-4].
The B6-hKLB mouse is a humanized model generated using gene editing technology by integrating the Chimeric cDNA and the 3'UTR of the mouse Klb gene into the mouse Klb gene locus. The mouse Klb endogenous extracellular domain was replaced with the human KLB domain, and the murine transmembrane-cytoplasmic region was remained. Homozygous B6-hKLB mice are viable and fertile. This model can be used for research on the pathological mechanisms and treatment methods of metabolic diseases such as obesity, diabetes, metabolic-associated steatohepatitis (MASH), inflammatory diseases, and potentially selected malignancies and the development of KLB-targeted drugs.
参考文献
Aaldijk AS, Verzijl CRC, Jonker JW, Struik D. Biological and pharmacological functions of the FGF19- and FGF21-coreceptor beta klotho. Front Endocrinol (Lausanne). 2023 May 16;14:1150222.
Lu W, Li X, Luo Y. FGF21 in obesity and cancer: New insights. Cancer Lett. 2021 Feb 28;499:5-13.
Shao W, Jin T. Hepatic hormone FGF21 and its analogues in clinical trials. Chronic Dis Transl Med. 2022 Feb 23;8(1):19-25.
G. Schumann,C. Liu,P. O’Reilly,H. Gao,P. Song,B. Xu,B. Ruggeri,N. Amin,T. Jia,S. Preis,M. Segura Lepe,S. Akira,C. Barbieri,S. Baumeister,S. Cauchi,T. Clarke,S. Enroth,K. Fischer,J. Hällfors,[...]& P. Elliott, KLB is associated with alcohol drinking, and its gene product β-Klotho is necessary for FGF21 regulation of alcohol preference, Proc. Natl. Acad. Sci. U.S.A. 2016; 113 (50) 14372-14377.
系統作製戦略
The coding sequences of exon 1 plus partial intron 1 of mouse Klb were replaced with the “Kozak-Chimeric cDNA-3'UTR of mouse Klb-WPRE-BGH pA" cassette. The mouse Klb endogenous extracellular domain was replaced with the human KLB domain, and the murine transmembrane-cytoplasmic region was remained.

Figure 1. Gene editing strategy of B6-hKLB mice.
*Kozak-Chimeric cDNA (human KLB extracellular-mouse Klb transmembrane-cytoplasmic)
適用分野
KLB-targeted drug screening, development, and evaluation;
Research on the pathological mechanisms and therapeutic approaches of metabolic diseases such as obesity, diabetes, and metabolic-associated steatohepatitis (MASH);
Research on the pathological mechanisms and therapeutic approaches of inflammatory diseases and potentially selected malignancies.
関連リソース
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