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Apoe-KO(2)

品系全名

C57BL/6Smoc-Apoe^em5Smoc

目錄號

NM-KO-190565

品系狀態(tài)

活體

導(dǎo)出PDF

基因信息

基因名
Apoe

基因曾用名

Apo-E; AI255918

染色體位置

NCBI ID

MGI ID

Ensembl ID

Pubmed

人類同源基因

APOE

品系描述

通過敲除Apoe基因exon 2-4，建立Apoe-KO(2)小鼠模型。原Apoe-KO(NM-KO-00033)小鼠模型因技術(shù)原因已下架。

應(yīng)用領(lǐng)域：動脈粥樣硬化、高脂血癥、血膽脂醇過多、心臟功能損傷、腦梗塞、老年癡呆癥及慢性乙型肝炎等

*使用本品系發(fā)表的文獻(xiàn)需注明: Apoe-KO(2) mice (Cat. NO. NM-KO-190565) were purchased from Shanghai Model Organisms Center, Inc..

疾病預(yù)測

腹部肥胖代謝綜合癥
Abdominal Obesity-Metabolic Syndrome

近似模型的表型

MGI:5428435
注：該品系需與Cyp19A1-KO(NM-KO-2102244)交配才可能獲得預(yù)期表型

參考文獻(xiàn)

Scott NJ, Cameron VA, Raudsepp S, Lewis LK, Simpson ER, Richards AM, Ellmers LJ, Generation and characterization of a mouse model of the metabolic syndrome: apolipoprotein E and aromatase double knockout mice. Am J Physiol Endocrinol Metab. 2012 Mar;302(5):E576-84

冠狀動脈疾病
Coronary Artery Disease

近似模型的表型

MGI:5558016
注：該品系需與Scarb1-KO(NM-KO-201876)交配才可能獲得預(yù)期表型

參考文獻(xiàn)

Tsukamoto K, Mani DR, Shi J, Zhang S, Haagensen DE, Otsuka F, Guan J, Smith JD, Weng W, Liao R, Kolodgie FD, Virmani R, Krieger M, Identification of apolipoprotein D as a cardioprotective gene using a mouse model of lethal atherosclerotic coronary artery disease. Proc Natl Acad Sci U S A. 2013 Oct 15;110(42):17023-8

家族性合并高脂血癥
Familial Combined Hyperlipidemia

近似模型的表型

MGI:4354296
注：該品系需與Lpl-KO(NM-KO-201300)交配才可能獲得預(yù)期表型

參考文獻(xiàn)

Xian X, Ding Y, Zhang L, Wang Y, McNutt MA, Ross C, Hayden MR, Deng X, Liu G, Enhanced atherothrombotic formation after oxidative injury by FeCl3 to the common carotid artery in severe combined hyperlipidemic mice. Biochem Biophys Res Commun. 2009 Aug 7;385(4):563-9

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驗證數(shù)據(jù)

Fig 1. Lipid profile biochemical markers of male Apoe-KO mice and? WT mice CD conditions. Under CD conditions, male Apoe-KO mice exhibit elevated levels of total cholesterol (T-CHO), and low-density lipoprotein cholesterol (LDL-C) compared to WT mice, while high-density lipoprotein cholesterol (HDL-C) levels are decreased. (n=5-10)

Abbr. WT, wild type; CD, chow diet.

Fig 2. Oil Red O staining of aortic valve in male Apoe-KO mice and WT mice under CD conditions. The results indicate that no lipid accumulation was observed in the aortic valves of WT mice at 7 months of age. In contrast, all Apoe-KO mice (6/6) exhibited significant lipid accumulation in the aortic valves as early as 5 months of age, with the severity of this phenotype progressively worsening with age. (n=4-6)

Abbr. WT, wild type; CD, chow diet.

Fig 3. Oil Red O staining of aorta in male Apoe-KO mice and WT mice under CD conditions. The results indicate that at 5 months of age, WT mice exhibit no significant lesions in the aorta, while some Apoe-KO mice (4/6) show fat accumulation near the aortic arch. By 6 to 7 months of age, all Apoe-KO mice (4/4) exhibit fat accumulation, with the severity of this phenotype progressively increasing. (n=4-6)

Abbr. WT, wild type; CD, chow diet.

Fig 4. Masson staining of aortic valve in Apoe-KO mice and WT mice under CD conditions. Muscle fibers appear red, while collagen fibers are stained blue. Apoe-KO mice exhibit increased collagen content within plaques, suggesting enhanced plaque stability. (n=3)

Abbr. WT, wild type; CD, chow diet.

Fig 5. Representative pictures of aortic valve. In WT mice, no significant plaque formation, necrosis, or inflammatory cell infiltration is seen. However, in Apoe-KO mice, extensive plaque formation is observed in the aortic valve, protruding into the lumen. Numerous interwoven collagen fibers are present, along with abundant infiltration of foam cells (red arrows). A small amount of cholesterol crystals (black arrows), appearing as needle-shaped voids, are visible, accompanied by minor deposits of brown pigment (green arrows). A small number of infiltrating lymphocytes (yellow arrows) are also noted. Myocardial cells display loose and irregular arrangement. The black box indicates the location of the magnified view.