Vc-MMAE ADCs for Research Only CAS:646502-53-6

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Home > Product > Vc-MMAE ADCs for Research Only CAS:646502-53-6
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Vc-MMAE ADCs for Research Only CAS:646502-53-6
Posting date : Jul 25, 2017
Membership
Free Member Scince Jul 25, 2017
FOB Price
USD100
Min. Order Quantity
100mg
Supply Abillity
10g/month
Port
SHANGHAI
Payment Terms
MoneyGram,Western Union,T/T
Package
Aluminum foil bag
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Product Detail
Company Info
 
Quick Detail
Place of Origin
China [CN]
Brand Name
Demeikai
HS-CODE
2811-11
Package & Delivery Lead Time
Package
Aluminum foil bag
Delivery Lead Time
7 days
Detailed Description
Vc-MMAE Basic Info.
Name:Vc-MMAESynonyms:Maleimidocaproyl-valine-citrulline-p-aminobenzoyloxycarbonyl-monomethyl auristatin E; Vedotin
CAS:646502-53-6
Molecular Formula:C68H105N11O15
Molecular Weight:1316.6
VcMMAE, Maleimidocaproyl-valine-citrulline-p-aminobenzoyloxycarbonyl-monomethyl auristatin E, Vedotin3
 
Antibody-drug conjugates (ADCs) require thorough characterization and understanding of product quality attributes. The framework of many ADCs comprises one molecule of antibody that is usually conjugated with multiple drug molecules at various locations. It is unknown whether the drug release rate from the ADC is dependent on drug location, and/or local environment, dictated by the sequence and structure of the antibody carrier. This study addresses these issues with valine-citrulline-monomethylauristatin E (vc-MMAE)-based ADC molecules conjugated at reduced disulfide bonds, by evaluating the cathepsin B catalyzed drug release rate of ADC molecules with different drug distributions or antibody carriers. MMAE drug release rates at different locations on ADC I were compared to evaluate the impact of drug location. No difference in rates was observed for drug released from the VH, VL, or CH2 domains of ADC I. Furthermore, four vc-MMAE ADC molecules were chosen as substrates for cathepsin B for evaluation of Michaelis-Menten parameters. There was no significant difference in KM or kcat values, suggesting that different sequences of the antibody carrier do not result in different drug release rates. Comparison between ADCs and small molecules containing vc-MMAE moieties as substrates for cathepsin B suggests that the presence of IgG1 antibody carrier, regardless of its bulkiness, does not impact drug release rate. Finally, a molecular dynamics simulation on ADC II revealed that the val-cit moiety at each of the eight possible conjugation sites was, on average, solvent accessible over 50% of its maximum solvent accessible surface area (SASA) during a 500 ns trajectory. Combined, these results suggest that the cathepsin cleavage sites for conjugated drugs are exposed enough for the enzyme to access and that the drug release rate is rather independent of drug location or monoclonal antibody carrier. Therefore, the distribution of drug conjugation at different sites is not a critical parameter to control in manufacturing of the vc-MMAE-based ADC conjugated at reduced disulfide bonds.
 

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