SEBOV GP Antikörper (AA 1-637)
SEBOV GP
Reaktivität: Sudan ebolavirus
WB
Wirt: Kaninchen
Polyclonal
unconjugated
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- Target Alle SEBOV GP Produkte
- SEBOV GP (Sudan Ebola Virus Envelope Glycoprotein (SEBOV GP))
- Bindungsspezifität
- AA 1-637
- Reaktivität
- Sudan ebolavirus
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Wirt
- Kaninchen
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Klonalität
- Polyklonal
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Konjugat
- Dieser SEBOV GP Antikörper ist unkonjugiert
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Applikation
- Western Blotting (WB)
- Spezifität
- Anti-Ebola virus EBOV(Subtype Sudan, strain Gulu) Glycoprotein/GP Polyclonal Antibody
- Aufreinigung
- Antigen Affinity
- Immunogen
- Recombinant EBOV (Subtype Sudan, strain Gulu) Glycoprotein / GP Protein (aa:Met1-Asn637, His Tag), ABIN7198907
- Isotyp
- IgG
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- Applikationshinweise
- WB 1:1000-1:5000
- Beschränkungen
- Nur für Forschungszwecke einsetzbar
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- Konzentration
- 1 mg/mL
- Buffer
- 0.2 μm filtered solution in PBS
- Lagerung
- -20 °C
- Informationen zur Lagerung
- Store at -20°C. Avoid freeze / thaw cycles.
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- Target
- SEBOV GP (Sudan Ebola Virus Envelope Glycoprotein (SEBOV GP))
- Andere Bezeichnung
- SEBOV Glycoprotein/GP (SEBOV GP Produkte)
- Hintergrund
- Glycoprotein,GP,The fourth gene of the EBOV genome encodes a 16- kDa envelope-attached glycoprotein (GP) and a 11 kDa secreted glycoprotein (sGP). Both GP and sGP have an identical 295-residue N-terminus, however, they have different C-terminal sequences. Recently, great attention has been paid to GP for vaccines design and entry inhibitors isolation. GP is a class I fusion protein which assembles as trimers on viral surface and plays an important role in virus entry and attachment. Mature GP is a disulfide-linked heterodimer formed by two subunits, GP1 and GP2, which are generated from the proteolytical process of GP precursor (pre-GP) by cellular furin during virus assembly . The GP1 subunit contains a mucin domain and a receptor-binding domain (RBD), the GP2 subunit has a fusion peptide, a helical heptad-repeat (HR) region, a transmembrane (TM) domain, and a 4-residue cytoplasmic tail. The RBD of GP1 mediates the interaction of EBOV with cellular receptor (e.g. DC-SIGN/LSIGN, TIM-1, hMGL, NPC1, β-integrins, folate receptor-α, and Tyro3 family receptors), of which TIM1 and NPC1 are essential for EBOV entry, the mucin domain having N- and O-linked glycans enhances the viral attachment to cellular hMGL, and participates in shielding key neutralization epitopes, which helps the virus evades immune elimination. There are large conformation changes of GP2 during membrane fusion, which enhance the insertion of fusion loop into cellular membrane and facilitate the release of viral nucleocapsid core to cytoplasm.
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