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Cy5.5-N-羥基琥珀酰亞胺酯

貨號(hào):AGF1345A
包裝:1mg,5mg,25mg,50mg
  • 英文名:Cyanine5.5 NHS ester
  • 分子式:C44H46ClN3O4
  • 分子量:716.31
  • 品牌:Lumiprobe

*西寶提示:我司所銷(xiāo)售的化學(xué)試劑、原料等所有產(chǎn)品(包括但不限于抗生素類(lèi)、蛋白質(zhì)類(lèi)、試劑盒類(lèi)產(chǎn)品等)僅限用于科學(xué)研究用途,不得作用于人體。

訂購(gòu)熱線:400-021-8158
訂購(gòu)貨號(hào) 產(chǎn)品名稱及規(guī)格
17020 Cyanine5.5 NHS ester, 1 mg
27020 Cyanine5.5 NHS ester, 5 mg
47020 Cyanine5.5 NHS ester, 25 mg
57020 Cyanine5.5 NHS ester, 50 mg
67020 Cyanine5.5 NHS ester, 100 mg
 
Cy5.5 NHS是近紅外胺類(lèi)活性染料。

CY5.5 NHS ester是用于標(biāo)記多肽、蛋白和寡核苷酸的氨基基團(tuán)的活性染料。CY5.5屬于是近紅外熒光染料,當(dāng)背景熒光有干擾時(shí)適宜用它來(lái)做標(biāo)記以進(jìn)行熒光分析。它也可以用于活體成像實(shí)驗(yàn)。該染料可以替代Alexa Fluor 680和DyLight 680。

推薦手冊(cè):
氨基分子的NHS酯標(biāo)記(請(qǐng)聯(lián)系西寶生物獲取)
Cy® is a trademark of GE Healthcare.

General properties

Appearance: dark blue powder
Molecular weight: 716.31
Molecular formula: C44H46ClN3O4

 

Solubility: soluble in organic solvents (DMSO, DMF, dichloromethane), low solubility in water
Quality control: NMR 1H (95%) and 13C, TLC, functional testing
Storage conditions: Storage: 24 months after receival at -20°C in the dark. Transportation: at room temperature for up to 3 weeks. Avoid prolonged exposure to light. Desiccate.
MSDS:

Download

Spectral properties

 

Excitation maximum, nm: 673
209000  
Emission maximum, nm: 707
Fluorescence quantum yield: 0.2

 

 

Product citations

  1. Jiang, X.; Bugno, J.; Hu, C.; Yang, Y.; Herold, T.; Qi, J.; Chen, P.; Gurbuxani, S.; Arnovitz, S.; Strong, J.; Ferchen, K.; Ulrich, B.; Weng, H.; Wang, Y.; Huang, H.; Li, S.; Neilly, M.B.; Larson, R.A.; Le Beau, M.M.; Bohlander, S.K.; Jin, J.; Li, Z.; Bradner, J.E.; Hong, S.; Chen, J. Eradication of acute myeloid leukemia with FLT3 ligand-targeted miR-150 nanoparticles. Cancer Research, in press. doi: 10.1158/0008-5472.CAN-15-2949
  2. Sun, Y.; Hong, S.; Ma, X.; Cheng, K.; Wang, J.; Zhang, Z.; Yang, M.; Jiang, Y.; Hong, X.; Cheng, Z. Recyclable Cu(I)/Melanin Dots for Cycloadditions, Bioconjugation and Cell Labeling. Chemical Science. doi: 10.1039/c6sc01536k
  3. Kim, K.-M.; Kim, M.K.; Paek, H.-J.; Choi, S.-J.; Oh, J.-M. Stable fluorescence conjugation of ZnO nanoparticles and their size dependent cellular uptake. Colloids and Surfaces B: Biointerfaces2016, 145, 870–877. doi: 10.1016/j.colsurfb.2016.06.006
  4. Geng, L.; Wang, Z.; Jia, X.; Han, Q.; Xiang, Z.; Li, D.; Yang, X.; Zhang, D.; Bu, X.; Wang, W.; Hu, Z.; Fang, Q. HER2 Targeting Peptides Screening and Applications in Tumor Imaging and Drug Delivery. Theranostics2016, 6(8), 1261–1273. doi:10.7150/thno.14302
  5. Yang, Q.; Li, L.; Sun, W.; Zhou, Z.; Huang, Y. Dual Stimuli-Responsive Hybrid Polymeric Nanoparticles Self-Assembled from POSS-Based Star-Like Copolymer-Drug Conjugates for Efficient Intracellular Delivery of Hydrophobic Drugs. ACS Applied Materials & Interfaces2016, 8(21), 13251–13261. doi: 10.1021/acsami.6b02403
  6. Brinkman, A.M.; Chen, G.; Wang, Y.; Hedman, C.J.; Sherer, N.M.; Havighurst, T.C.; Gong, S.; Xu, W. Aminoflavone-Loaded EGFR-Targeted Unimolecular Micelle Nanoparticles Exhibit Anti-Cancer Effects in Triple Negative Breast Cancer. Biomaterials,2016, 101, 20–31. doi: 10.1016/j.biomaterials.2016.05.041
  7. Bygd, H.C.; Bratlie, K.M. The effect of chemically modified alginates on macrophage phenotype and biomolecule transport. Journal of Biomedical Materials Research2016, 104(7), 1707–1719. doi: 10.1002/jbm.a.35700
  8. Zhao, L.; Yuan, W.; Ang, C.Y.; Qu, Q.; Dai, Y.; Gao, Y.; Luo, Z.; Wang, J.; Chen, H.; Li, M.; Li, F.; Zhao, Y. Silica-Polymer Hybrid with Self-Assembled PEG Corona Excreted Rapidly via a Hepatobiliary Route. Advanced Functional Materials2016, 26(18), 3036–3047. doi: 10.1002/adfm.201505155
  9. Al-Hilal, T.A.; Chung, S.W.; Choi, J.U.; Alam, F.; Park, J.; Kim, S.W.; Kim, S.Y.; Ahsan, F.; Kim, I.-S.; Byun, Y. Targeting prion-like protein doppel selectively suppresses tumor angiogenesis. Journal of Clinical Investigation2016, 126(4), 1251–1266. doi:10.1172/JCI83427
  10. Jiang, X.; Hu, C.; Arnovitz, S.; Bugno, J.; Yu, M.; Zuo, Z.; Chen, P.; Huang, H.; Ulrich, B.; Gurbuxani, S.; Weng, H.; Strong, J.; Wang, Y.; Li, Y.; Salat, J.; Li, S.; Elkahloun, A.G.; Yang, Y.; Neilly, M.B.; Larson, R.A.; Le Beau, M.M.; Herold, T.; Bohlander, S.K.; Liu, P.P.; Zhang, J.; Li, Z.; He, C.; Jin, J.; Hong, S.; Chen, J.;. miR-22 has a potent anti-tumour role with therapeutic potential in acute myeloid leukaemia. Nature Communications2016, 7, 11452. doi: 10.1038/ncomms11452
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