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- 2025年12月24日
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- 详细信息
- 文献和实验
- 技术资料
- 英文名:
Immortalized mouse adipose derived mesenchymal stem cells
- 库存:
10
- 供应商:
欣润生物
- 肿瘤类型:
NO
- 细胞类型:
永生化
- ATCC Number:
11222
- 品系:
ICR小鼠
- 组织来源:
脂肪干
- 相关疾病:
无
- 物种来源:
小鼠
- 免疫类型:
不详
- 细胞形态:
成纤维细胞样
- 是否是肿瘤细胞:
否
- 器官来源:
/
- 运输方式:
常温
- 年限:
5年
- 生长状态:
贴壁生长
- 规格:
T25方瓶
永生化小鼠脂肪间充质干细胞简介:
产品描述:小鼠脂肪间充质干细胞分离自成年小鼠腹股沟皮下脂肪组织,体外培养的脂肪干细胞呈纤维细胞样生长,为短梭形、小三角形以及多角形等。来源于中胚层的脂肪组织的干细胞具有向成脂肪、成软骨、成骨、心肌细胞和神经源细胞分化的多分化潜能。因此脂肪组织可以作为小鼠干细胞库的重要来源,并可作为多种组织工程的种子细胞,有非常重要的研究和应用价值。
产品货号:IM2028
产品类型: 永生化细胞
传代能力: 30代左右
产品形态: 成纤维细胞形态
培养基:永生化小鼠脂肪间充质干细胞专用完全培养基
支原体质控:检测阴性
产品培养条件:37℃,5%CO2
发货方式:T25瓶子常温发货
货期:7天货期
永生化小鼠脂肪间充质干细胞白光及脂肪诱导分化图
Suppression of human peripheral blood lymphocyte proliferation by immortalized mesenchymal stem cells derived from bone marrow of Banna Minipig inbred-line
This study sought to investigate whether mesenchymal stem cells (MSC) derived from Banna Minipig Inbred-line (BMI-MSC) suppressed human peripheral blood lymphocyte (hPBLs) proliferation in a one-way mixed lymphocyte reaction system. BMI-MSC failed to stimulate proliferative responses by hPBLs, which were activated by allogenic endothelial cells, BMI-PBLs and non-specific mitogenic stimuli. Furthermore, BMI-MSC also suppressed proliferation of hPBLs stimulated by mismatched allogenic, as well as xenogenic PBLs, and the mitogenic stimulus ConA. The suppression occurred in dose-dependent fashion when the ratio of hPBLs to BMI-MSC varied from 1 to 5 fold; fewer, BMI-MSC (0.001 to 0.01 times) showed no obvious suppression. When BMI-MSC were added to hPBLs stimulated for 72 hours, the proliferative suppression was still evident. Addition of anti-FasL or anti-TGF-β1 antibody attenuated the proliferative suppression, while antibody against IL-10 had no effect on it. Further immunofluorescence analysis demonstrated that FasL and TGF-β1 constitutively expressed BMI-MSC.
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文献和实验Chicken intestinal epithelial cells were obtained from NEWGAINBIO company. Cells were cultured on 37℃, with 5% CO2, in the Ham’s F-12 Nutrient (DMEM/12) that contained the following supplementations: fetal bovine serum (5%), in-sulin (5 µg/mL), transferrin (5 µg/mL), selenium (5 ng/mL), epidermal growth factor (5 ng/mL) and penicillin-streptomycin (100–100 U/mL) for cell culturing (full DMEM/12). Experiments were performed with chicken intestinal epithelial cells and working solutions were prepared with plain DMEM/12 without supplementation. For the investigations, cells were seeded onto 96-well, 24-well or 6-well polystyrene cell culture plates.
Primary hVICs (passage 2) were cultured to 50–60% confluence and infected with pGMLV-SV40T-puro lentivirus (NewgainBio, Wuxi, China) at a multiplicity of infection of 80 supplemented with 5 µg/mL polybrene (Sigma-Aldrich, Buchs, Switzerland).
Tissue was cultured until cells became visible around the tissue, and when the fusion reached 90% (FIGURE 1A) §ask ¦lled with the prepared culturing medium was sent to the company for further immortalisation. Cell immortalisation was done for cell stability and longer-term use. Immortalised cells were cultured with 10% FBS and 1% PS in the DMEM medium. After the cells multiplied and merged, they were routinely passed and grown ( NEWGAINBIO Inc. Wuxi, Jiangsu, China) (FIGURE 1B-C).
Mouse primary cultured renal vascular ECs and VSMCs were obtained from Newgainbio company, which were tested by Factor VIII and α-smooth muscle actin (α-SMA), the marker of ECs and VSMCs. RNeasy Mini Kit was used for RNA extraction, and the above protocols were repeated.
Porcine primary colon epithelial cells (Newgainbio company, Wuxi,China) were cultured in Dulbecco's Modified Eagle's Medium (Solarbio, Beijing, China) containing 10 % fetal bovine serum (BioInd, Kiryat shmona, Lsrael) at 37 ◦C and 5 % CO2 humidity.
成功逆转衰老!来自年轻身体的多种物质,可让衰老小鼠「重返青春」
:Nature Cell Biology 2022 年 10 月 19 日,又有一篇新的研究发现,给老年小鼠注射来自年轻小鼠脂肪间充质干细胞的小细胞外囊泡,即可减少老年小鼠的衰老迹象,改善其协调能力、肌肉力量,增强抗疲劳性。注射了小细胞外囊泡的老年小鼠如同服用「返老还童」药丸一般,一些组织表观遗传上似乎变得更年轻 [4]。 该研究以 Small extracellular vesicles from young adipose-derived stem cells prevent frailty
,CD146 在 HFD(高脂饲喂)、ob/ob(瘦素缺失)、年老小鼠脂肪组织中显著高表达。分析了肥胖和健康受试者内脏脂肪中 CD146 的表达,发现肥胖受试者的内脏脂肪中 CD146 的表达明显更高,并且与 BMI(体重指数) 呈正相关关系。 图片来源:Advanced Science 2. CD146 全身敲除和脂肪组织特异性敲除小鼠均可抵抗肥胖。 作者构建 CD146 敲除基因型(CD146 KO)小鼠,饲喂高脂饲料过程中发现 CD146 KO 小鼠的脂肪量显著降低,改善了胰岛素敏感
饥饿使人健康又长寿?新研究揭示,减少热量摄入还不够,适当「饿肚子」或是发挥作用的关键
CD 对 C57BL/6 系小鼠进行了 90 天的能量限制,观察并比较了在能量限制期间两种限制方法下小鼠的体重、脂肪重量、各个器官组织应对能量匮乏的响应、代谢生理指标、动物行为的差异以及在能量限制后两组小鼠下丘脑的基因表达谱的差异以及与对照组的差异。实验结果表明经历饥饿的过程似乎是 CR 限食延长寿命和改善健康状况背后机制的一个关键因素。 该研究成果于 2022 年 5 月 17 日在国际主流期刊 Cell Reports 上发表,研究论文题为 Calorie restriction
技术资料