Ctnnb1 Mouse shRNA Plasmid (Locus ID 12387)
CAT#: TL500280
Ctnnb1 - Mouse, 4 unique 29mer shRNA constructs in lentiviral GFP vector, 5µg of each construct provided
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CNY 5,740.00
货期*
现货
规格
Cited in 1 publication. |
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经常一起买 (3)
Specifications
Product Data | |
Product Name | Ctnnb1 Mouse shRNA Plasmid (Locus ID 12387) |
Locus ID | 12387 |
UniProt ID | Q02248 |
Synonyms | Bfc; Cat; Catnb; Mesc |
Vector | pGFP-C-shLenti |
Format | Lentiviral plasmids |
Kit Components | Ctnnb1 - Mouse, 4 unique 29mer shRNA constructs in lentiviral GFP vector(Gene ID = 12387). 5µg purified plasmid DNA per construct29-mer scrambled shRNA cassette in pGFP-C-shLenti Vector, TR30021, included for free. |
RefSeq | BC048153, BC053065, NM_001165902, NM_007614, NM_007614.1, NM_007614.2, NM_007614.3, NM_001165902.1, BC053065.1, BC006739, BC043078, BC043481 |
Summary | This gene encodes not only an important cytoplasmic component of the classical cadherin adhesion complex that forms the adherens junction in epithelia and mediates cell-cell adhesion in many other tissues but also a key signaling molecule in the canonical Wnt signaling pathway that controls cell growth and differentiation during both normal development and tumorigenesis. The gene product contains a central armadillo-repeat containing domain through which it binds the cytoplasmic tail of classical cadherins; meanwhile, it also binds alpha-catenin, which further links the cadherin complex to the actin cytoskeleton either directly or indirectly. Beta-catenin is therefore necessary for the adhesive function of classical cadherins. Another key function of this protein is to mediate the canonical Wnt signaling pathway and regulate gene transcription. Without Wnt signal, cytoplasmic beta-catenin that is not associated with the cadherin complex is quickly phosphorylated at the N-terminal Ser/Thr residues by the so called degradation complex containing axin, adenomatous polyposis coli (APC), casein kinase I, and GSK3B, then ubiquitylated by beta-TrCP, and degraded by the proteasome. However, in the presence of Wnt signal, the degradation complex is disrupted and the stabilized cytoplasmic beta-catenin translocates into the nucleus, where it binds various transcription factors and, together with these factors, regulates the transcription of many downstream genes. Mutations of this gene have been linked with various types of tumors. Alternatively spliced variants have been found for this gene. [provided by RefSeq, Sep 2009] |
shRNA Design | These shRNA constructs were designed against multiple splice variants at this gene locus. To be certain that your variant of interest is targeted, please contact techsupport@origene.com. If you need a special design or shRNA sequence, please utilize our custom shRNA service. |
Performance Guaranteed | OriGene guarantees that the sequences in the shRNA expression cassettes are verified to correspond to the target gene with 100% identity. One of the four constructs at minimum are guaranteed to produce 70% or more gene expression knock-down provided a minimum transfection efficiency of 80% is achieved. Western Blot data is recommended over qPCR to evaluate the silencing effect of the shRNA constructs 72 hrs post transfection. To properly assess knockdown, the gene expression level from the included scramble control vector must be used in comparison with the target-specific shRNA transfected samples. For non-conforming shRNA, requests for replacement product must be made within ninety (90) days from the date of delivery of the shRNA kit. To arrange for a free replacement with newly designed constructs, please contact Technical Services at techsupport@origene.com. Please provide your data indicating the transfection efficiency and measurement of gene expression knockdown compared to the scrambled shRNA control (Western Blot data preferred). |
Citations (1)
The use of this RNAi has been cited in the following citations: |
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MDMX acts as a pervasive preleukemic-to-acute myeloid leukemia transition mechanism
,Ueda, K;Kumari, R;Schwenger, E;Wheat, JC;Bohorquez, O;Narayanagari, SR;Taylor, SJ;Carvajal, LA;Pradhan, K;Bartholdy, B;Todorova, TI;Goto, H;Sun, D;Chen, J;Shan, J;Song, Y;Montagna, C;Xiong, S;Lozano, G;Pellagatti, A;Boultwood, J;Verma, A;Steidl, U;,
Cancer cell
,PubMed ID 33667384
[CTNNB1]
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