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Hyperlipidemia and hepatitis in liver-specific CREB3L3 knockout mice generated using a one-step CRISPR/Cas9 system

机译：使用一步式CRISPR / Cas9系统产生的肝脏特异性CREB3L3基因敲除小鼠的高脂血症和肝炎

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cAMP responsive element binding protein 3-like 3 (CREB3L3), a transcription factor expressed in the liver and small intestine, governs fasting-response energy homeostasis. Tissue-specific CREB3L3 knockout mice have not been generated till date. To our knowledge, this is the first study using the one-step CRISPR/Cas9 system to generate CREB3L3 floxed mice and subsequently obtain liver- and small intestine-specific Creb3l3 knockout (LKO and IKO, respectively) mice. While LKO mice as well as global KO mice developed hypertriglyceridemia, LKO mice exhibited hypercholesterolemia in contrast to hypocholesterolemia in global KO mice. LKO mice demonstrated up-regulation of hepatic Srebf2 and its corresponding target genes. No phenotypic differences were observed between IKO and floxed mice. Severe liver injury was observed in LKO mice fed a methionine-choline deficient diet, a model for non-alcoholic steatohepatitis. These results provide new evidence regarding the hepatic CREB3L3 role in plasma triglyceride metabolism and hepatic and intestinal CREB3L3 contributions to cholesterol metabolism.

机译：cAMP反应元件结合蛋白3样3（CREB3L3）是在肝脏和小肠中表达的转录因子，控制着空腹反应能量的体内平衡。迄今为止尚未产生组织特异性CREB3L3基因敲除小鼠。据我们所知，这是第一项使用一步式CRISPR / Cas9系统生成CREB3L3荷瘤小鼠并随后获得肝和小肠特异性Creb3l3基因敲除小鼠（分别为LKO和IKO）的研究。尽管LKO小鼠和整体KO小鼠均发生高甘油三酯血症，但与整体KO小鼠的低胆固醇血症相比，LKO小鼠表现出高胆固醇血症。 LKO小鼠表现出肝Srebf2及其相应靶基因的上调。在IKO和肥胖小鼠之间未观察到表型差异。在喂食甲硫氨酸-胆碱缺乏饮食（一种非酒精性脂肪性肝炎的模型）的LKO小鼠中观察到严重的肝损伤。这些结果提供了有关肝CREB3L3在血浆甘油三酸酯代谢中的作用以及肝和肠CREB3L3对胆固醇代谢的贡献的新证据。

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Nakagawa Yoshimi; Oikawa Fusaka; Mizuno Seiya; Ohno Hiroshi; Yagishita Yuka; Satoh Aoi; Osaki Yoshinori; Takei Kenta; Kikuchi Takuya; Han Song-iee; Matsuzaka Takashi; Iwasaki Hitoshi; Kobayashi Kazuto; Yatoh Shigeru; Yahagi Naoya; Isaka Masaaki; Suzuki Hiroaki; Sone Hirohito; Takahashi Satoru; Yamada Nobuhiro; Shimano Hitoshi;
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1. Hyperlipidemia and hepatitis in liver-specific CREB3L3 knockout mice generated using a one-step CRISPR/Cas9 system [J] . Yoshimi Nakagawa, Fusaka Oikawa, Seiya Mizuno, Scientific reports. . 2016,第1期

机译：高脂血症和使用单步骤CRISPR生成肝炎中肝特异性CREB3L3敲除小鼠/ Cas9系统
2. One-step Generation of Phenotype-expressing Triple-knockout Mice with Heritable Mutated Alleles by the CRISPR/Cas9 System (vol 60, pg 326, 2014) [J] . Fujii Wataru, Onuma Asuka, Sugiura Koji, The Journal of Reproduction and Development . 2014,第5期

机译：通过CRISPR / Cas9系统一步生成具有可遗传突变的等位基因的表型表达三敲除小鼠（vol 60，pg 326，2014）
3. One-step Generation of Phenotype-expressing Triple-knockout Mice with Heritable Mutated Alleles by the CRISPR/Cas9 System [J] . Fujii W, Onuma A, Sugiura K, The Journal of Reproduction and Development . 2014,第4期

机译：通过CRISPR / Cas9系统一步生成具有可遗传突变等位基因的表型表达三联敲除小鼠
4. Homology-lntegrated CRISPR-Cas (HI-CRISPR) System for One-Step Multigene Disruption in Saccharomyces cerevisiae [C] . Zehua Bao, Han Xiao, Jing Liang AIChE Annual Meeting . 2014

机译：同源性-LN的CRAP-CAS（HI-CRISPR）Saccharomyces酿酒酵母中的一步多岛破坏系统
5. Generation of Double Mutant, Permanent Knockout LTP3/LTP4 Arabidopsis thaliana Plants Using CRISPR/CAS9 Gene Editing [D] . Avellan, Mark Edward. 2021

机译：双突变体，永久敲除LTP3 / LTP4拟南芥拟南芥使用CRISPR / CAS9基因编辑
6. Hyperlipidemia and hepatitis in liver-specific CREB3L3 knockout mice generated using a one-step CRISPR/Cas9 system [O] . Yoshimi Nakagawa, Fusaka Oikawa, Seiya Mizuno, -1

机译：使用一步式CRISPR / Cas9系统产生的肝脏特异性CREB3L3基因敲除小鼠的高脂血症和肝炎
7. One-step Generation of Phenotype-expressing Triple-knockout Mice with Heritable Mutated Alleles by the CRISPR/Cas9 System [O] . Wataru FUJII, Asuka ONUMA, Koji SUGIURA, 2014

机译：通过CRISPR / CAS9系统具有遗传突变等位基因的表型表达三重敲除小鼠的一步生成

Hyperlipidemia and hepatitis in liver-specific CREB3L3 knockout mice generated using a one-step CRISPR/Cas9 system

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