MA-PEG4-vc-PAB-DMEA-duocarmycin DM

MA-PEG4-vc-PAB-DMEA-duocarmycin DM Catalog number: BADC-00745

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MA-PEG4-vc-PAB-DMEA-duocarmycin DM is a drug-linker conjugate for ADC by using Duocarmycin DM (a potent antitumor antibiotic), linked via MA-PEG4-vc-PAB-DMEA.

Category
ADCs Cytotoxin with Linkers
Product Name
MA-PEG4-vc-PAB-DMEA-duocarmycin DM
Catalog Number
BADC-00745
Molecular Formula
C68H89ClN12O17
Molecular Weight
1381.98
MA-PEG4-vc-PAB-DMEA-duocarmycin DM

Ordering Information

Catalog Number Size Price Quantity
BADC-00745 -- $-- Inquiry
Description
MA-PEG4-vc-PAB-DMEA-duocarmycin DM is a drug-linker conjugate for ADC by using Duocarmycin DM (a potent antitumor antibiotic), linked via MA-PEG4-vc-PAB-DMEA.
Synonyms
Mal-PEG4-vc-PAB-DMEA-duocarmycin DM
Shipping
Room temperature
Storage
-20°C

MA-PEG4-vc-PAB-DMEA-duocarmycin DM is a potent targeted drug conjugate designed for cancer therapy. This compound incorporates the maleimide (MA) group, which facilitates its conjugation to biomolecules with thiol groups, such as monoclonal antibodies or peptides. The polyethylene glycol (PEG4) linker enhances the solubility, stability, and circulation half-life of the conjugate in vivo. The VC (Val-Cit) cleavable linker is designed to release the cytotoxic payload, duocarmycin DM, specifically inside the target cell. Duocarmycin DM is a highly potent DNA alkylating agent that disrupts DNA replication and induces cell death by forming covalent bonds with the DNA. This targeted delivery system minimizes systemic toxicity and maximizes therapeutic effects by ensuring that the cytotoxic drug is released only within cancer cells.

One of the major applications of MA-PEG4-vc-PAB-DMEA-duocarmycin DM is in the design of antibody-drug conjugates (ADCs) for targeted cancer treatment. The linker system is engineered to be cleaved by intracellular enzymes once the conjugate is internalized by the target cancer cell. Upon internalization, the VC linker is cleaved in the acidic environment of the endosome or lysosome, releasing duocarmycin DM inside the cell. This allows the highly toxic duocarmycin to act directly on cancerous cells, causing DNA damage and triggering apoptosis. The targeted nature of this conjugate helps to concentrate the drug at the tumor site, minimizing off-target effects and reducing the collateral damage that traditional chemotherapy often causes.

Another critical application of MA-PEG4-vc-PAB-DMEA-duocarmycin DM is in overcoming challenges associated with chemotherapy resistance. Cancer cells often develop resistance mechanisms, such as efflux pumps or DNA repair pathways, that prevent conventional chemotherapy drugs from being effective. However, by using a targeted delivery system like this one, the drug is specifically delivered to cancer cells, bypassing the mechanisms of resistance. This strategy helps to ensure that duocarmycin DM retains its efficacy in treating resistant tumors, making this conjugate a valuable tool for fighting hard-to-treat cancers.

Additionally, MA-PEG4-vc-PAB-DMEA-duocarmycin DM has potential applications in precision medicine. The maleimide-PEG4-vc-PAB linker system allows for conjugation to various targeting moieties, such as monoclonal antibodies or small peptides that bind to specific tumor markers. This flexibility makes the compound adaptable for a wide range of cancer types, enabling personalized therapy tailored to the unique molecular profile of a patient's tumor. Furthermore, its application in ADCs opens the possibility of combination therapies, where this conjugate could be used alongside other cancer treatments to enhance efficacy and overcome therapeutic resistance.

The molarity calculator equation

Mass (g) = Concentration (mol/L) × Volume (L) × Molecular Weight (g/mol)

The dilution calculator equation

Concentration (start) × Volume (start) = Concentration (final) × Volume (final)

This equation is commonly abbreviated as: C1V1 = C2V2

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