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CMV ICP36 Antikörper

Antigen

CMV ICP36

Klonalität Monoklonal (CH16)
Wirt
Applikation
Alternativen Western Blot (WB), Immunfluoreszenz (IF)
8 Publikationen vorhanden
Produktnummer ABIN265590
Menge 500 ug  (1.0 mg/ml)
Preis 357,14 €   Zzgl. Versandkosten €20,00, €20,00 Trockeneispauschale sowie MWSt
Lieferung nach
Verfügbarkeit Lieferbar innerhalb von 5 Werktagen

Produktbeschreibung

Format Affinity-purified
Isotyp IgG2b-kappa  (Passende Sekundärantikörper)
Klon CH16
Beschreibung Mouse monoclonal antibody to ICP36 of Cytomegalovirus. This antibody originates from ascites fluids and is purified by protein G agarose affinity chromatography.

Anwendungen

Applikationshinweise Reactive with ICP36 of Cytomegalovirus in immunofluorescence (IFA) and western blot assays at 10 ug/ml. 
Konzentration 1.0 mg/ml
Reinigung Protein G agarose affinity chromatography
Buffer Phosphate Buffered Saline pH 7.4 (no azide)
Lagerung This product is supplied frozen on dry ice. Upon receipt, store at -20°C. Avoid multiple freeze-thaw cycles as product degradation may result.
Forschungsgebiet Virologie
Beschränkungen Nur für Forschungszwecke einsetzbar

Publikationen

Publikationen Mocarski, Pereira, Michael: "Precise localization of genes on large animal virus genomes: use of lambda gt11 and monoclonal antibodies to map the gene for a cytomegalovirus protein family." in: Proceedings of the National Academy of Sciences of the United States of America, Vol. 82, Issue 4, pp. 1266-70, 1985 (PubMed).

Pereira, Hoffman, Gallo et al.: "Monoclonal antibodies to human cytomegalovirus: three surface membrane proteins with unique immunological and electrophoretic properties specify cross-reactive determinants." in: Infection and immunity, Vol. 36, Issue 3, pp. 924-32, 1982 (PubMed).

White, Del Rosario, Sanders et al.: "The IE2 60-kilodalton and 40-kilodalton proteins are dispensable for human cytomegalovirus replication but are required for efficient delayed early and late gene expression and production of infectious virus." in: Journal of virology, Vol. 81, Issue 6, pp. 2573-83, 2007 (PubMed).

Sanders, Clark, Morello et al.: "Development of cell lines that provide tightly controlled temporal translation of the human cytomegalovirus IE2 proteins for complementation and functional analyses of growth-impaired and nonviable IE2 mutant viruses." in: Journal of virology, Vol. 82, Issue 14, pp. 7059-77, 2008 (PubMed).

Sanders, Del Rosario, White et al.: "Internal deletions of IE2 86 and loss of the late IE2 60 and IE2 40 proteins encoded by human cytomegalovirus affect the levels of UL84 protein but not the amount of UL84 mRNA or the loading and distribution of the mRNA on polysomes." in: Journal of virology, Vol. 82, Issue 22, pp. 11383-97, 2008 (PubMed).

Kapasi, Clark, Tran et al.: "Recruitment of cdk9 to the immediate-early viral transcriptosomes during human cytomegalovirus infection requires efficient binding to cyclin T1, a threshold level of IE2 86, and active transcription." in: Journal of virology, Vol. 83, Issue 11, pp. 5904-17, 2009 (PubMed).

Tran, Kamil, Coen et al.: "Inactivation and disassembly of the anaphase-promoting complex during human cytomegalovirus infection is associated with the degradation of the APC5 and APC4 subunits and does not require UL97-mediated phosphorylation of Cdh1." in: Journal of virology, 2010 (PubMed).

Fiorentini, Luganini, Delloste et al.: "Human Cytomegalovirus productively infects lymphatic endothelial cells and induces a secretome that promotes angiogenesis and lymphangiogenesis through IL-6 and GM-CSF." in: The Journal of general virology, 2010 (PubMed).

Alternativen

Alternativen zu Antigen "CMV ICP36", Typ "Antikörper" finden
Wirte Maus (1)
Applikationen Immunfluoreszenz (IF) (1), Western Blot (WB) (1)