搜索结果: 'methocult media formulations for human hematopoietic cells serum containing'
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Martinelli P et al. (JUN 2011) Blood 117 24 6617--26The lymphoma-associated NPM-ALK oncogene elicits a p16INK4a/pRb-dependent tumor-suppressive pathway.
Oncogene-induced senescence (OIS) is a barrier for tumor development. Oncogene-dependent DNA damage and activation of the ARF/p53 pathway play a central role in OIS and,accordingly,ARF and p53 are frequently mutated in human cancer. A number of leukemia/lymphoma-initiating oncogenes,however,inhibit ARF/p53 and only infrequently select for ARF or p53 mutations,suggesting the involvement of other tumor-suppressive pathways. We report that NPM-ALK,the initiating oncogene of anaplastic large cell lymphomas (ALCLs),induces DNA damage and irreversibly arrests the cell cycle of primary fibroblasts and hematopoietic progenitors. This effect is associated with inhibition of p53 and is caused by activation of the p16INK4a/pRb tumor-suppressive pathway. Analysis of NPM-ALK lymphomagenesis in transgenic mice showed p16INK4a-dependent accumulation of senescent cells in premalignant lesions and decreased tumor latency in the absence of p16INK4a. Accordingly,human ALCLs showed no expression of either p16INK4a or pRb. Up-regulation of the histone-demethylase Jmjd3 and de-methylation at the p16INK4a promoter contributed to the effect of NPM-ALK on p16INK4a,which was transcriptionally regulated. These data demonstrate that p16INK4a/pRb may function as an alternative pathway of oncogene-induced senescence,and suggest that the reactivation of p16INK4a expression might be a novel strategy to restore the senescence program in some tumors. View Publication产品类型:
产品号#:
03434
03444
产品名:
MethoCult™ GF M3434
MethoCult™ GF M3434
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Zhou L et al. (JUL 2011) The Journal of biological chemistry 286 28 25211--23Aberrant epigenetic and genetic marks are seen in myelodysplastic leukocytes and reveal Dock4 as a candidate pathogenic gene on chromosome 7q.
Myelodysplastic syndromes (MDS) are characterized by abnormal and dysplastic maturation of all blood lineages. Even though epigenetic alterations have been seen in MDS marrow progenitors,very little is known about the molecular alterations in dysplastic peripheral blood cells. We analyzed the methylome of MDS leukocytes by the HELP assay and determined that it was globally distinct from age-matched controls and was characterized by numerous novel,aberrant hypermethylated marks that were located mainly outside of CpG islands and preferentially affected GTPase regulators and other cancer-related pathways. Additionally,array comparative genomic hybridization revealed that novel as well as previously characterized deletions and amplifications could also be visualized in peripheral blood leukocytes,thus potentially reducing the need for bone marrow samples for future studies. Using integrative analysis,potentially pathogenic genes silenced by genetic deletions and aberrant hypermethylation in different patients were identified. DOCK4,a GTPase regulator located in the commonly deleted 7q31 region,was identified by this unbiased approach. Significant hypermethylation and reduced expression of DOCK4 in MDS bone marrow stem cells was observed in two large independent datasets,providing further validation of our findings. Finally,DOCK4 knockdown in primary marrow CD34(+) stem cells led to decreased erythroid colony formation and increased apoptosis,thus recapitulating the bone marrow failure seen in MDS. These findings reveal widespread novel epigenetic alterations in myelodysplastic leukocytes and implicate DOCK4 as a pathogenic gene located on the 7q chromosomal region. View Publication产品类型:
产品号#:
04434
04444
84434
84444
产品名:
MethoCult™ H4434 Classic
MethoCult™ H4434 Classic
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- 研究领域 干细胞生物学 删除该内容
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- ALDEFLUOR 68
- AggreWell 58
- ArciTect 11
- BrainPhys 9
- CellAdhere 1
- CloneR 5
- CryoStor 14
- EC-Cult 1
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- MyoCult 6
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- RSeT 8
- ReLeSR 6
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- STEMdiff 57
- STEMvision 3
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细胞类型
- B 细胞 4
- B细胞 43
- CD4+ T细胞 14
- CD8+ T细胞 11
- CHO细胞 1
- NK 细胞 2
- NK细胞 26
- PSC衍生 9
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- PSC衍生造血细胞 15
- T 细胞 5
- T细胞 53
- 上皮细胞 19
- 乳腺细胞 33
- 先天性淋巴细胞 3
- 全血 1
- 其他亚群 1
- 内皮细胞 2
- 内胚层 2
- 前列腺细胞 8
- 单个核细胞 12
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- 多能干细胞 1567
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- 巨噬细胞 7
- 巨核细胞 1
- 成骨细胞 5
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- 杂交瘤细胞 1
- 树突状细胞(DCs) 22
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- 癌细胞及细胞系 40
- 癌细胞和细胞系 2
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- 神经元 5
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- 神经干祖细胞 98
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- 粒细胞及其亚群 36
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- 肌源干祖细胞 5
- 肝细胞 5
- 肠道细胞 6
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- 骨髓基质细胞 1
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- PSC衍生中胚层 11
- PSC衍生内皮细胞 8
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- PSC衍生心肌细胞 19
- PSC衍生神经细胞 47
- PSC衍生肝细胞 8
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- 其他T细胞亚型 2
- 呼吸道细胞 1
- 小鼠胚胎成纤维细胞 1
- 神经元 48
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耦连
- Biotin 或 生物素 13
- PerCP-Cyanine5.5 4
- 未偶联的 29
- APC 14
- APC-Cyanine7 2
- Alexa Fluor 488 9
- FITC 14
- PE 19
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反应性物种
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- IL-17A
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目标抗原
- CD105 (Endoglin) 2
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- CD69 1
- CD71 (Transferrin Receptor) 1
- Human Epithelial Cell 1
- MAP2 (Microtubule-Associated Protein-2) 1
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- TBR1 1
- CD326 (EpCAM) 2
- CD34 3
- CD38 2
- CD45RO 1
- CD5 1
- CD73 1
- CD90 (Thy-1) 1
- MUC1 (CD227) 1
- Nestin 1
- OCT4 (OCT3) 1
- SSEA-5 1
- TRA-1-60 (Podocalyxin) 1
- TRA-1-81 1
- TRA-2-54 1
- p63 (deltaN) 1
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