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EasySep™ Release人CD4正选试剂盒

采用可解离磁珠的免疫磁珠正选

产品号 #(选择产品)

产品号 #17752_C

采用可解离磁珠的免疫磁珠正选

产品优势

  • 在30分钟内分离出高纯度的人CD4+细胞
  • 无需清洗去除EasySep™ Releasable RapidSpheres™可解离磁珠     

产品组分包括

  • EasySep™ Release人CD4正选试剂盒(产品号 #17752)
    • EasySep™ Release人CD4正选抗体混合物,1 mL
    • EasySep™ Releasable RapidSpheres™ 50201磁珠,1 mL
    • EasySep™ Release缓冲液(浓缩),3 x 1 mL
  • RoboSep™ Release人CD4正选试剂盒(产品号 #17752RF)
    • EasySep™ Release人CD4正选抗体混合物,1 mL
    • EasySep™ Releasable RapidSpheres™ 50201磁珠,1 mL
    • EasySep™ Release缓冲液(浓缩),3 x 1 mL
    • RoboSep™ 缓冲液(产品号 #20104)
    • RoboSep™ 过滤吸头(产品号 #20125)
    • EasySep™ EasyTube™-14(产品号 #20128)
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总览

EasySep™ Release人CD4正选试剂盒用于从新鲜或冻存的外周血单个核细胞或洗涤的白细胞单采术样本中通过免疫磁珠正选分离出CD4+细胞。

目的细胞经抗体复合物和磁珠标记,并通过 EasySep™ 磁极进行无柱分选。非目的细胞通过简单倾倒或吸取弃去,而目的细胞则保留在管中。随后,结合在EasySep™分离的CD4+细胞上的磁珠被解离,分选后的细胞可立即用于下游应用。使用该EasySep™ Release试剂盒分选之后,细胞表面仍结合有抗体复合物,并可能与Brilliant Violet™偶联的抗体、聚乙二醇修饰的蛋白质或其他化学相关配体相互作用。CD4抗原在辅助性T细胞上强表达,在外周血单核细胞和组织巨噬细胞上弱表达。

目的细胞经抗体复合物和磁珠标记,并通过 EasySep™ 磁极进行无柱分选。非目的细胞通过简单倾倒或吸取弃去,而目的细胞则保留在管中。随后,结合在EasySep™分离的CD4+细胞上的磁珠被解离,分选后的细胞可立即用于下游应用。使用该EasySep™ Release试剂盒分选之后,细胞表面仍结合有抗体复合物,并可能与Brilliant Violet™偶联的抗体、聚乙二醇修饰的蛋白质或其他化学相关配体相互作用。CD4抗原在辅助性T细胞上强表达,在外周血单核细胞和组织巨噬细胞上弱表达。

目的细胞经抗体复合物和磁珠标记,并通过 EasySep™ 磁极进行无柱分选。非目的细胞通过简单倾倒或吸取弃去,而目的细胞则保留在管中。随后,结合在EasySep™分离的CD4+细胞上的磁珠被解离,分选后的细胞可立即用于下游应用。使用该EasySep™ Release试剂盒分选之后,细胞表面仍结合有抗体复合物,并可能与Brilliant Violet™偶联的抗体、聚乙二醇修饰的蛋白质或其他化学相关配体相互作用。CD4抗原在辅助性T细胞上强表达,在外周血单核细胞和组织巨噬细胞上弱表达。

目的细胞经抗体复合物和磁珠标记,并通过 EasySep™ 磁极进行无柱分选。非目的细胞通过简单倾倒或吸取弃去,而目的细胞则保留在管中。随后,结合在EasySep™分离的CD4+细胞上的磁珠被解离,分选后的细胞可立即用于下游应用。使用该EasySep™ Release试剂盒分选之后,细胞表面仍结合有抗体复合物,并可能与Brilliant Violet™偶联的抗体、聚乙二醇修饰的蛋白质或其他化学相关配体相互作用。CD4抗原在辅助性T细胞上强表达,在外周血单核细胞和组织巨噬细胞上弱表达。

磁体兼容性
• EasySep™ Magnet (Catalog #18000) • “The Big Easy” EasySep™ Magnet (Catalog #18001) • EasyPlate™ Magnet (Catalog #18102) • EasyEights™ Magnet (Catalog #18103) • RoboSep™-S (Catalog #21000)
 
亚型
细胞分选试剂盒
 
细胞类型
T 细胞,T 细胞,CD4+
 
种属

 
样本来源
Leukapheresis,PBMC
 
筛选方法
Positive
 
品牌
EasySep,RoboSep
 
研究领域
免疫,细胞治疗开发
 

实验数据

Starting with a single-cell suspension of human PBMCs, the CD4+ T cell content of the isolated fraction is typically 96.1 ± 4.1% (mean ± SD using the purple EasySep™ Magnet). In the above example, the purities of the start and final isolated fractions are 24.0% and 98.1%, respectively.

产品说明书及文档

请在《产品说明书》中查找相关支持信息和使用说明,或浏览下方更多实验方案。

Document Type
Product Name
Catalog #
Lot #
Language
Catalog #
17752RF
Lot #
All
Language
English
Catalog #
17752
Lot #
All
Language
English
Document Type
Safety Data Sheet 1
Catalog #
17752RF
Lot #
All
Language
English
Document Type
Safety Data Sheet 2
Catalog #
17752RF
Lot #
All
Language
English
Document Type
Safety Data Sheet 3
Catalog #
17752RF
Lot #
All
Language
English
Document Type
Safety Data Sheet 4
Catalog #
17752RF
Lot #
All
Language
English
Document Type
Safety Data Sheet 1
Catalog #
17752
Lot #
All
Language
English
Document Type
Safety Data Sheet 2
Catalog #
17752
Lot #
All
Language
English
Document Type
Safety Data Sheet 3
Catalog #
17752
Lot #
All
Language
English

应用领域

本产品专为以下研究领域设计,适用于工作流程中的高亮阶段。探索这些工作流程,了解更多我们为各研究领域提供的其他配套产品。

相关材料与文献

技术资料 (10)

文献 (1)

Regulatory Programs of B-cell Activation and Germinal Center Reaction Allow B-ALL Escape from CD19 CAR T-cell Therapy. N. G. Im et al. Cancer immunology research 2022 sep

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has led to tremendous successes in the treatment of B-cell malignancies. However, a large fraction of treated patients relapse, often with disease expressing reduced levels of the target antigen. Here, we report that exposing CD19+ B-cell acute lymphoblastic leukemia (B-ALL) cells to CD19 CAR T cells reduced CD19 expression within hours. Initially, CD19 CAR T cells caused clustering of CD19 at the T cell-leukemia cell interface followed by CD19 internalization and decreased CD19 surface expression on the B-ALL cells. CD19 expression was then repressed by transcriptional rewiring. Using single-cell RNA sequencing and single-cell assay for transposase-accessible chromatin using sequencing, we demonstrated that a subset of refractory CD19low cells sustained decreased CD19 expression through transcriptional programs of physiologic B-cell activation and germinal center reaction. Inhibiting B-cell activation programs with the Bruton's tyrosine kinase inhibitor ibrutinib increased the cytotoxicity of CD19 CAR T cells without affecting CAR T-cell viability. These results demonstrate transcriptional plasticity as an underlying mechanism of escape from CAR T cells and highlight the importance of combining CAR T-cell therapy with targeted therapies that aim to overcome this plasticity. See related Spotlight by Zhao and Melenhorst, p. 1040.

更多信息

更多信息
种属 Human
Magnet Compatibility • EasySep™ Magnet (Catalog #18000) • “The Big Easy” EasySep™ Magnet (Catalog #18001) • EasyPlate™ Magnet (Catalog #18102) • EasyEights™ Magnet (Catalog #18103) • RoboSep™-S (Catalog #21000)
样本来源 Leukapheresis, PBMC
Selection Method Positive
标记抗体
质量保证:

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