TP53基因敲除HCT116细胞

TP53基因敲除HCT116细胞
货号:

EDC07854

物种:

细胞名称:

HCT 116

基因名称:

TP53

基因ID:

7157

规格:

1×10⁶ cells

TP53基因敲除细胞HCT116是由EVO视讯 EVO真人生命基因优化的CRISPR/Cas9编辑而成,采用Sanger测序法验证敲除,保证单克隆,活性良好。
货号 EDC07854
细胞 HCT116
Cellosaurus ID CVCL_0291
细胞别名 HCT-116, HCT.116, HCT_116, HCT116, HCT116wt, HCT-116/P, HCT-116/parental, CoCL2
基因 TP53
基因ID
7157
基因别名 BCC7|BMFS5|LFS1|P53|TRP53
摘要
This gene encodes a tumor suppressor protein containing transcriptional activation, DNA binding, and oligomerization domains. The encoded protein responds to diverse cellular stresses to regulate expression of target genes, thereby inducing cell cycle arrest, apoptosis, senescence, DNA repair, or changes in metabolism. Mutations in this gene are associated with a variety of human cancers, including hereditary cancers such as Li-Fraumeni syndrome. Alternative splicing of this gene and the use of alternate promoters result in multiple transcript variants and isoforms. Additional isoforms have also been shown to result from the use of alternate translation initiation codons from identical transcript variants (PMIDs: 12032546, 20937277). [provided by RefSeq, Dec 2016]
癌症类型 Colorectal Carcinoma
细胞形态 Adherent
传代比率 1/5-1/4,2days
完全培养基 mcCoy5A+10% FBS
冻存培养基 90% FBS/完培+10% DMSO
* 仅供科研使用,不适用于人体或动物,包括临床、治疗或诊断用途。
Loci送检细胞STR信息
送检细胞名: HCT 116
细胞库细胞STR信息
细胞库细胞名: HCT 116
Allele1Allele2Allele3Allele4Allele1 Allele2 Allele3 Allele4
AmelogeninXX
CSF1PO710791011
D2S13381616
D3S135812171819121819
D5S81810111011
D7S82011121112
D8S11791012141510121415
D13S31710121012
D16S539111311121314
D18S5116171617
D19S433121312
D21S1129302930
FGA18231823
Penta D913913
Penta E121314121314
TH018989
TPOX88
vWA1721222317212223
D6S104313
D12S391172122
D2S4411112
* 该细胞系与收录于ATCC, DSMZ, JCRB 和 RIKEN数据库的细胞系STR数据匹配。
结论:该细胞 STR 鉴定正确。
* 研究用途免责声明:本内容基于公开的研究数据、生物信息学资源及计算分析生成,仅供研究参考。

相关文献

IF=2.6
PloS one
The p53 protein is crucial for regulating cell survival and apoptosis in response to DNA damage. However, its influence on therapy effectiveness is controversial: when DNA damage is high p53 directs cells toward apoptosis, while under moderate genotoxic stress it saves the cells from death and promote DNA repair. Furthermore, these processes are influenced by the metabolism of transition metals, particularly copper since they serve as cofactors for critical enzymes. The metallochaperone Atox1 is under intensive study in this context because it serves as transcription factor allegedly mediating described effects of copper. Investigating the interaction between p53 and Atox1 could provide insights into tumor cell survival and potential therapeutic applications in oncology. This study explores the relationship between p53 and Atox1 in HCT116 and A549 cell lines with wild type and knockout TP53. The study found an inverse correlation between Atox1 and p53 at the transcriptional and translational levels in response to genotoxic stress. Atox1 expression decreased with increased p53 activity, while cells with inactive p53 had significantly higher levels of Atox1. Suppression of both genes increased apoptosis, while suppression of the ATOX1 gene prevented apoptosis even under the treatment with chemotherapeutic drugs. The findings suggest that Atox1 may act as one of key elements in promotion of cell cycle under DNA-damaging conditions, while p53 works as an antagonist by inhibiting Atox1. Understanding of this relationship could help identify potential targets in cell signaling pathways to enhance the effectiveness of combined antitumor therapy, especially in tumors with mutant or inactive p53.
该敲除模型可用于: - 研究 p53 介导的 Atox1 铜伴侣蛋白抑制作为调节基因毒性应激下肿瘤细胞存活的机制 - 阐明在 p53 失活或突变时 Atox1 在 DNA 损伤期间促进细胞周期进程的作用 - 测试靶向 p53-Atox1 轴的联合抗肿瘤疗法以增强 TP53 缺失或突变肿瘤的凋亡 - 研究 p53 和 Atox1 在化疗药物反应中的转录和翻译负相关 - 评估 Atox1 作为预防 p53 功能障碍癌症中凋亡逃逸的潜在治疗靶点

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