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產(chǎn)品資料

pCMV-IκBα

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產(chǎn)品名稱: pCMV-IκBα
產(chǎn)品型號(hào):
產(chǎn)品展商: HZbscience
產(chǎn)品文檔: 無(wú)相關(guān)文檔

簡(jiǎn)單介紹

pCMV-IκBα的各批次質(zhì)粒菌株發(fā)貨前均經(jīng)過(guò)嚴(yán)格的多重驗(yàn)證,如存在質(zhì)量問題,請(qǐng)?jiān)谑盏疆a(chǎn)品的三個(gè)月內(nèi)通知我司。收到pCMV-IκBα后請(qǐng)短暫離心,取2μl轉(zhuǎn)化至對(duì)應(yīng)感受態(tài)中,挑取單克隆重新提取質(zhì)粒后使用。


pCMV-IκBα  的詳細(xì)介紹

pCMV-IκBα載體基本信息

載體名稱: pCMV-IκBα 、 IκBα Dominant-Negative Vector
質(zhì)粒類型: 信號(hào)通路分析載體;顯性抑制載體
克隆方法: --
啟動(dòng)子: CMV
載體大小: 4.9kb
5' 測(cè)序引物及序列: --
3' 測(cè)序引物及序列: --
載體標(biāo)簽: --
載體抗性: Kanamycin.html' target='_blank'>卡那霉素
篩選標(biāo)記: G418
克隆菌株: DH5a 或 HB101
宿主細(xì)胞(系): --
備注: pCMV-IκBα載體是信號(hào)通路分析載體;
IκBα是信號(hào)轉(zhuǎn)導(dǎo)蛋白,IκBα的突變體是顯性負(fù)性突變體,抑制信號(hào)轉(zhuǎn)導(dǎo)過(guò)程。
產(chǎn)品目錄號(hào): 631923
穩(wěn)定性: 瞬表達(dá)
組成型/誘導(dǎo)型: 組成型
病毒/非病毒: 非病毒

pCMV-IκBα載體質(zhì)粒圖譜和多克隆位點(diǎn)信息

pCMV-IκBα



pCMV-IκBα

pCMV-IκBα載體簡(jiǎn)介

IkappaBalpha (IKBA) The IkappaBalpha Dominant-Negative Vector Set provides a convenient way to examine NFkappaB regulation by manipulating its inhibitor, IkappaBalpha, which normally keeps NFkappaB inactive and sequestered in the cytosol. This vector set gives you the ability to compare the effects of overexpressed IkappaBalpha (phosphorylated specifically by your agent) to those of IkappaBalphaM (unable to be phosphorylated under any conditions). By combining these vectors with cis-acting NFkappaB Vectors, you have a complete assay system to study and measure activation of the NFkappaB pathway. 載體描述 The IκBα Dominant-Negative Vector Set consists of two vectors, pCMV-IκBα and pCMV-IκBαM. These vectors are convenient tools for examining NFκB regulation by manipulating its inhibitor, IκBα. In uninduced cells, IκBα binds NFκB and inhibits its activation by preventing NFκB from translocating to the nucleus. However, upon activation of NFκB by agents like TNF, IκBα can be phosphorylated, thus leading to the disassociation of IκBα from NFκB. pCMV-IκBαM contains two mutations that prevent this phosphorylation step; therefore, cells expressing IκBαM block the NFκB pathway (1–3). The IκBα gene and IκBαM gene differ by serine to alanine mutations at residues 32 and 36 (1). Both proteins are expressed at high levels from the constitutive CMV promoter.
The SV40 polyadenylation sequence directs proper processing of the 3' end of the mRNAs. The vector backbone contains an SV40 origin for replication in mammalian cells expressing the SV40 T antigen. A neomycin-resistance cassette (Neor)—consisting of the SV40 early promoter, the Tn5 neomycin/kanamycin resistance gene, and polyadenylation signals from the
Herpes simplex virus thymidine kinase (HSV TK) gene—allows kanamycin selection in E. coli and neomycin selection in eukaryotic cells. The vector backbone also provides a pUC origin of replication for propagation in E. coli and an f1 origin for single-stranded DNA production. 使用 pCMV-IκBα can be used to screen drug candidates for their effects on NFκB pathway or to study the involvement of upstream kinases which precede IκBα degradation. IκBα overexpression eliminates any low-level stimulation produced from the culture medium, and ensures that any NFκB stimulation measured is due to the agent you are testing. pCMV-IκBαM can be used to "knock down" expression of endogenous IκBα or block NFκB signaling in a particular cell line.
In conjunction with one of our NFκB cis-acting reporter vectors, such as pNFκB-SEAP, pNFκBLuc, or pNFκB-d2EGFP (Cat. Nos. 631905, 631904, and 631803, resp.), you can measure the activation of NFκB in your system by measuring the expression of the reporter gene (4).
Both vectors can be transfected into mammalian cells using any standard method. Stable transformants can be selected using G418 (5).

Note: The following list of features is based on the pCMV-IκBα Vector. pCMV-IκBαM differs from pCMV-IκBα by two mutations at residues 32 & 36 of IκBα. Due to different subcloning parameters, the pCMV-IκBαM Vector is 30 bp smaller than pCMV-IκBα. Propagation in E. coli Suitable host strains: DH5α, HB101 and other general purpose strains. Single-stranded DNA production requires a host containing an F plasmid such as JM101 or XL1-Blue.
 Selectable marker: plasmid confers resistance to kanamycin (50 μg/ml) to E. coli hosts.
 E. coli replication origin: pUC
 Copy number: ~500
 Plasmid incompatibility group: pMB1/ColE1 

pCMV-IκBα載體序列

hz-0096R AAT/Tryptase  α-1抗胰蛋白酶抗體
hz-1510R AATK  AATK細(xì)胞凋亡關(guān)聯(lián)酪氨酸激酶抗體
hz-2451R NMP-22  核基質(zhì)蛋白22
hz-1229R AATF  拮抗凋亡轉(zhuǎn)錄因子抗體
hz-1627R ABCA1/ABC1  腺苷三磷酸結(jié)合盒轉(zhuǎn)運(yùn)體A1抗體
hz-1761R ABCD1/CCL22  嗜酸粒細(xì)胞趨化蛋白22抗體
hz-1604R ABCB5  ATP結(jié)合蛋白家族5抗體
hz-1224R ABCB6  ATP結(jié)合蛋白家族6抗體
hz-1960R ABCF1  ATP結(jié)合盒蛋白家族GCN20F家族1抗體
hz-1231R ABCG1  三磷酸腺苷結(jié)合盒亞家族G1抗體
hz-0662R ABCG2/CD338  三磷酸腺苷結(jié)合轉(zhuǎn)運(yùn)蛋白G超家族成員2抗體
hz-2812R KAT4  細(xì)胞周期基因1蛋白抗體
hz-1727R ABCG4  ABC膜轉(zhuǎn)運(yùn)蛋白抗體
hz-5013R ABCG5  三磷酸腺苷結(jié)合轉(zhuǎn)運(yùn)蛋白G超家族成員5抗體
hz-5014R ABCG8  三磷酸腺苷結(jié)合轉(zhuǎn)運(yùn)蛋白G超家族成員8抗體
hz-0583R c-Abl/Abl1  非受體酪氨酸激酶c-Abl抗體
hz-4083R phospho-c-Abl(Tyr134)  磷酸化非受體酪氨酸激酶c-Abl抗體
hz-3032R phospho-c-Abl(Tyr412)  磷酸化非受體酪氨酸激酶c-Abl抗體
hz-3041R phospho-c-Abl(Tyr245)  磷酸化非受體酪氨酸激酶c-Abl抗體
hz-3042R phospho-c-Abl(Tyr204)  磷酸化非受體酪氨酸激酶c-Abl抗體
hz-3044R phospho-c-Abl(Ser735)  磷酸化非受體酪氨酸激酶c-Abl抗體
hz-3071R phospho-c-Abl(Tyr89)  磷酸化非受體酪氨酸激酶c-Abl抗體

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