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- 英文名:
/
- 库存:
现货库存
- 供应商:
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- 肿瘤类型:
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- 细胞类型:
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- 品系:
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- 组织来源:
ATCC/DSMZ/ECACC
- 相关疾病:
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- 物种来源:
人或动物
- 免疫类型:
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- 细胞形态:
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- 是否是肿瘤细胞:
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- 器官来源:
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- 运输方式:
常温或干冰
- 年限:
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- 生长状态:
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| 种属 | 小鼠 |
| 别称 | B16-F10+OVA |
| 组织来源 | 皮肤 |
| 疾病 | 小鼠黑色素瘤 |
| 传代比例/细胞消化 | 1:2传代 ,消化1-2分钟 |
| 完全培养基配置 | RPMI1640培养基; 10%胎牛血清; 1%双抗 |
| 简介 | B16 - F10细胞是B16 - F0细胞的亚系 |
| 形态 | 上皮细胞样 ,梭形 |
Results: Twenty-one patients were investigated, including 11 adenocarcinoma and 10 squamous cell carcinoma cases. Anti-programmed cell death protein-1 (PD-1) antibody (n=18) and anti-PD-L1 antibody (n=3) were administered. The clinical responses were graded as follows:
Results: A total of 122 patients were included in this study. GTF2I was the most common gene mutation. Higher TMB was significantly associated with the later stage, more advanced pathological type, and older age. The overall survival (OS) of patients in the low-TMB group was The mice with a disruption of Rank or Rankl exhibit normal mammary development during puberty, but their mammary epithelium fails to proliferate and form lobuloalveolar structures during pregnancy, resulting in the death of newborns. Hormone replacement therapy is associated with an increased risk of breast cancer. Importantly, specific deletion of RANK in mammary epithelium cells prevents both the onset and progression of medroxyprogesterone acetate (MPA) -driven mammary cancer and impairs self-renewal of breast cancer stem cells. Furthermore, RANK is highly expressed in several cancer cells. Functionally, it has been shown that RANKL can stimulate the directed migration of mammary epithelial cells as well as prostate cancer and melanoma cells toward a source of RANKL. In an in vivo metastasis model, OPG reduced the tumor burden in bones and ameliorated clinical paralysis, but did not affect the frequency of the spread of metastases into other tissues. These findings show that the RANK/RANKL system is crucial for mammary development, breast tumorigenesis and bone metastasis.
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文献和实验/histocompatibility complex (MHC) class I and programmed cell death-ligand 1 (PD-L1) expression of cancer cells, and the PD-L1, CD8 and CD103 expression of tumor infiltrating immune cells in lung cancer tissue before the administration of ICI were confirmed by immunohistochemistry (IHC).
魔高一尺,道高一丈!清华大学徐萌团队发现能量代谢与肿瘤免疫逃逸的关系
, GZMB, and PRF1)定义了 cytotoxic T lymphocyte (CTL) score,反映肿瘤浸润 CD8+ T 细胞的功能。 研究发现在表观转录组调控因子中,RNA 去甲基化酶 FTO 与 CTL score 呈现负相关。为了检测肿瘤细胞的 FTO 表达是否影响 T 细胞介导的抗肿瘤功能,研究人员在 B16-OVA 黑色素瘤细胞和肺癌细胞系 LLC 中对 FTO 进行敲降。研究人员将 B16-OVA 和 LLC 接种到小鼠体内,发现 Fto-Kd 细胞产生的肿瘤生长速度明显减慢
模型建立方法:将体外原代培养处于对数生长期的B16-F10黑色素瘤细胞,胰酶消化,用RPMI-1640培养液洗2遍,调至1×106/ml悬浮于RPMI-1640培养液中(台盼兰染色检测活性95%以上)。经眼球后静脉丛每鼠注射0.1ml含0.1ml 1×105个B16-F10黑色素瘤细胞悬液。模型特点及功用:可用于研究黑素瘤肺转移的治疗研究。模型建立和使用注意事项:1、本课题组选用两种肿瘤细胞株建立了实验性肺转移及自发肺转移模型,发现:眼球后静脉注入2.5×104以上B16黑色素瘤活细胞/鼠
「CAR-T 之父」Carl June 引领抗癌风向标!挑战
RN7SL1,发现其可诱导 B16-F10 黑色素瘤细胞或人树突状细胞干扰素刺激基因(IFN-stimulated genes, ISGs)的表达,如主要组织相容性复合体 I 类(MHC I 类)、PDL1 和 CD86。为了确定 RN7SL1 和对照 RNA(Scrambled RNA, Scr RNA)在体内的效应,他们将 B16 肿瘤植入野生型小鼠的侧壁,并在瘤内注射脂质体包裹的 RNA。结果发现,瘤内注射 RN7SL1 促进肿瘤生长,并降低了小鼠体内的 CD4 和 CD8 T
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