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Solutions for Antibody-Drug Conjugates (ADCs) Development

Antibody-Drug Conjugates (ADCs) are an innovative class of biopharmaceuticals that deliver potent cytotoxic agents directly to tumor cells via monoclonal antibodies and specialized linkers. Each component—antibody, linker, and payload—plays a critical role in ensuring ADC stability, efficacy, and safety.
An ideal ADC should selectively target cancer cells, prevent premature payload release, and minimize toxicity to healthy tissues. Successful development requires optimizing target selection, antibody design, linker stability, payload properties, conjugation technology, drug-to-antibody ratio (DAR), and resistance mechanisms.
To support ADC research, we offer a comprehensive range of products and services covering early discovery, CMC quality control, and both preclinical and clinical development. Our solutions help researchers accelerate innovation and optimize ADC design for maximum therapeutic impact.

Antibody Screening

In an Ideal ADC, antibody is a crucial vehicle for the specific binding with target antigen. The antibody must have high binding affinity towards target antigen and low immunogenicity. Additionally, an antibody should have ability to maintain a long plasma half-life and fast internalization.
At present, the conventional technologies widely used include hybridoma technology, antibody library screening technology, B cell cloning technology and other screening technologies. Common methods include ELISA and FACS cell level binding and blocking, SPR/BLI affinity detection, etc.

ADC Target Proteins

  • ADC Target Proteins
  • AGLink® Site-specific Conjugation Kit

ADC Target Proteins

The target antigen expressed on the surface of tumor cells is a key factor for ADCs to recognize tumor cells and guide the cytotoxic payload into the cancer cells. Therefore, selecting an appropriate target antigen is a primary consideration in ADCs design. Ideal antigens should exhibit specific expression, non-secretion, and favorable internalization properties.

We have successfully developed a suite of over 90 high-quality ADCs target proteins, encompassing a variety of species including Human, Mouse, Cynomolgus Monkey, and Rat, each equipped with diverse tags. These proteins with high purity and robust bioactivity, suitable for immunization, Antibody Screening, species validation, quality control, pharmacokinetic studies, and diverse applications.

Learn more about ADC target proteins and validation data

Internalization Mechanism Characterization

ADC targets cancer cell antigens through antibodies, delivering cytotoxic drugs directly into tumor cells via internalization, which significantly reduces side effects. The internalization efficiency directly impacts the amount of payload delivered, making it a key evaluation criterion in drug design, including antibody screening and linker optimization. Therefore, screening antibodies with high internalization efficiency is essential in the early stages of development.

To support ADC internalization research, we have developed a specialized Antibody Internalization Detection Reagent (Cat. No. IGG-PZF2001), featuring a pH-sensitive red fluorescent dye that labels the human IgG Fc region. The reagent forms a stable fluorescent complex that enables detection of antibody endocytosis within cells. It delivers enhanced fluorescence in acidic compartments with minimal background, supporting flow cytometry, cell imaging, and other cellular analysis techniques.

Schematic of antibody internalization detection reagent principle

Schematic of antibody internalization detection reagent principle

Cat. No. Product Description Tests
IGG-PZF2001 Antibody Internalization Detection reagent 100tests/500tests

Learn more about Internalization Mechanism Characterization

Fc Effector Function Validation

The efficacy of antibody-drug conjugates (ADCs) is determined not only by the ability of their Fab fragments to bind tumor-associated antigens but also by the interaction between their Fc fragments and Fc receptors. Fc-mediated effector functions—such as antibody-dependent cellular cytotoxicity (ADCC), complement-dependent cytotoxicity (CDC), and antibody-dependent cellular phagocytosis (ADCP)—play a crucial role in the elimination or suppression of tumor cells.

Additionally, the affinity of the Fc fragment for the neonatal Fc receptor (FcRn) is a key predictor of an antibody’s half-life. Therefore, optimizing antibody structures and selecting candidates with ideal Fc receptor affinity are essential strategies in the development of therapeutic antibodies.

We offer a comprehensive collection of Fc receptor products, including FcRn, FcγR, and their commonly studied mutants. Leveraging our extensive protein product resources and activity analysis experience, we can also provide high-quality SPR & BLI affinity testing services upon receiving your sample. To support your research, we also supply all necessary high-quality Fc receptor proteins free of charge for these experiments.

Learn more about Fc receptor proteins and validation data

Linker Screening and Validation

In the development of ADCs, the linker structure impacts stability, homogeneity, cytotoxic potency, tolerability, and pharmacokinetics (PK). Therefore, selecting the appropriate linker is crucial for optimizing the therapeutic potential and safety of ADCs.

Linkers are typically classified as cleavable or non-cleavable based on their cleavage mechanism. Current ADCs research primarily focuses on cleavable linkers, with cathepsin-cleavable linkers being the most widely used and extensively studied. Additionally, several other linker-cleaving enzymes are under investigation.

For the screening and validation of linkers for ADCs, we have developed a series of proteases specialized in linker cleavage, encompassing Cathepsin B, Cathepsin L, Cathepsin S, MMP-2, MMP-7, MMP-9, β-glucuronidase, β-galactosidase.

Molecule Cat. No. Product Description Preorder/Order
Cathepsin B CTB-H5222 Human Cathepsin B / CTSB Protein, His Tag (MALS verified)

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Cathepsin B CTB-M52H9 Mouse Cathepsin B / CTSB Protein, His Tag (MALS verified)

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Cathepsin L CAL-H52H3 Human Cathepsin L / CTSL1 Protein, His Tag (active enzyme)

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Cathepsin L CAL-M52H3 Mouse Cathepsin L / CTSL1 Protein, His Tag (MALS verified)

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Cathepsin S CTS-H52H9 Human Cathepsin S / CTSS Protein, His Tag (active enzyme, MALS verified)

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MMP-9 MM9-C52H3 Cynomolgus MMP-9 Protein, His Tag (active enzyme)

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MMP-9 MM9-H5221 Human MMP-9 Protein, His Tag (active enzyme)

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MMP-9 MM9-H5229 Human MMP-9 Protein, His Tag (active enzyme) (MALS verified)

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MMP-9 MM9-H52H8 Human MMP-9 (107-707) Protein, His Tag (active enzyme)

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MMP-9 MM9-H52H9 Human MMP-9 (20-707) Protein, His Tag (active enzyme, MALS verified)

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MMP-9 MM9-M52H1 Mouse MMP-9 (20-471) Protein, His Tag (active enzyme, MALS verified)

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MMP-2 MM2-M52H9 Mouse MMP-2 (30-460) Protein, His Tag (active enzyme)

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MMP-7 MM7-C53H3 Cynomolgus MMP-7 Protein, His Tag (active enzyme, HPLC verified)

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MMP-7 MM7-H5249 Human MMP-7 / PUMP1 Protein, His Tag (active enzyme)

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beta-Glucuronidase/GUSB BEB-H52H3 Human beta-Glucuronidase/GUSB Protein, His Tag (active enzyme)

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beta-Galactosidase-1 BG1-H52H3 Human beta-Galactosidase-1 Protein, His Tag (active enzyme)

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Learn more about proteases for ADC screening and validation

Clinical/Preclinical PK Analysis

ADCs have a more complex structure compared to traditional small molecule drugs and antibody drugs, resulting in higher drug heterogeneity, which makes its PK studies more complex. Analytes for ADCs typically encompass total antibodies (both conjugated and unconjugated with cytotoxic payloads, DAR≥0); conjugated antibodies (antibody conjugated to payload, DAR≥1), the antibody-conjugated drug, free drugs, and their analogs. The quantification of total antibodies and conjugated antibodies commonly employs ELISA (Enzyme-linked Immunosorbent Assay), while the analysis of antibody-conjugated drugs, free drugs, and their metabolites frequently involves LC-MS (Liquid Chromatograph Mass Spectrometer).

In order to tackle the challenges and complexities associated with the PK analysis of ADCs, we have introduced a comprehensive range of products and services tailored for PK research. These offerings encompass biotinylated proteins, streptavidin (SA) series products, anti-Payload antibodies, anti-idiotypic antibodies, anti-idiotypic antibodies development services, PK method development, validation and transfer, kit development services and more.

Featured Products: Anti-payload Antibodies

Molecule Cat. No. Product Description Preorder/Order
DM-1 DM1-BLY73 Biotinylated Monoclonal Anti-DM-1&DM-4 Antibody, Mouse IgG1

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DM-1 DM1-PLY73 HRP conjugated Monoclonal Anti-DM-1&DM-4 Antibody,Mouse IgG1

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DM-1 DM1-Y73 Monoclonal Anti-DM-1&DM-4 Antibody, Mouse IgG1

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Doxorubicin APA-05 Anti-Doxorubicin Antibody Screening Panel

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Doxorubicin DON-MY2215 Monoclonal Anti-Doxorubicin specific Antibody, Rabbit IgG (1M2B1)

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Doxorubicin DON-MY2216 Monoclonal Anti-Doxorubicin specific Antibody, Rabbit IgG (1M2C3)

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DXD DXD-BVM807 Biotinylated Anti-DXD&Exatecan Antibody, Mouse IgG1, Avitag™ (MALS verified)

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DXD DXD-M684 Monoclonal Anti-DXD&Exatecan Antibody, Mouse IgG1

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DXD DXD-PLM684 HRP conjugated Monoclonal Anti-DXD&Exatecan Antibody, Mouse IgG1

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DXD & Exatecan DXD-MY2289 Monoclonal Anti-DXD & Exatecan Antibody, Rabbit IgG (M1D08)

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DXD & Exatecan DXD-MY2290 Monoclonal Anti-DXD & Exatecan Antibody, Rabbit IgG (M1B09)

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Eribuli* APA-03 Anti-Eribuli* Antibody Screening Panel

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Eribuli* ERN-BMY12b Biotinylated Rabbit Anti-Eribuli* Antibody, Rabbit IgG (1M1G11)

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Eribuli* ERN-MY2012b Monoclonal Anti-Eribuli* Antibody, Rabbit IgG (1M1G11)

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Eribuli* ERN-MY2062b Monoclonal Anti-Eribuli* Antibody, Rabbit IgG (1M1F5)

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Eribuli* ERN-MY2063b Monoclonal Anti-Eribuli* Antibody, Rabbit IgG (1M2B11)

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Eribuli* ERN-PLM12b HRP conjugated Monoclonal Anti-Eribuli* Antibody, Rabbit IgG (1M1G11)

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MMAE APA-01 Anti-MMAE Antibody Screening Panel

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MMAE MME-BLS104 Biotinylated Monoclonal Anti-MMAE&MMAF Antibody, Mouse IgG1

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MMAE MME-M5252 Monoclonal Anti-MMAE&MMAF Antibody, Mouse IgG1

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MMAE MME-MY2198a Monoclonal Anti-MMAE specific Antibody, Rabbit IgG (M1H05)

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MMAE MME-MY2209 Monoclonal Anti-MMAE specific Antibody, Rabbit IgG (M1H09)

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MMAE MME-MY2210 Monoclonal Anti-MMAE specific Antibody, Rabbit IgG (M1G04)

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MMAE MME-MY2211 Monoclonal Anti-MMAE specific Antibody, Rabbit IgG (M1D12)

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MMAE MME-PLS104 HRP conjugated Monoclonal Anti-MMAE&MMAF Antibody,Mouse IgG1

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MMAF APA-02 Anti-MMAF Antibody Screening Panel

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MMAF MMF-MY2213 Monoclonal Anti-MMAF specific Antibody, Rabbit IgG (1M1G10)

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MMAF MMF-MY2214 Monoclonal Anti-MMAF specific Antibody, Rabbit IgG (1M1E12)

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MMAF MMF-MY2219 Monoclonal Anti-MMAF specific Antibody, Rabbit IgG (M1E04)

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MMAF MMF-MY2220 Monoclonal Anti-MMAF specific Antibody, Rabbit IgG (M1B12)

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PBD APA-04 Anti-PBD Antibody Screening Panel

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PBD PAD-MY2212 Monoclonal Anti-Payload PBD Antibody, Rabbit IgG (1M1F9)

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PBD PAD-MY2221 Monoclonal Anti-Payload PBD Antibody, Rabbit IgG (M1D08)

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SN38 SN8-BVM808 Biotinylated Anti-SN38 Antibody, Mouse IgG1, Avitag™

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SN38 SN8-M685 Monoclonal Anti-SN38 Antibody, Mouse IgG1

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SN38 SN8-PLM685 HRP conjugated Monoclonal Anti-SN38 Antibody, Mouse IgG1

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Click to view more ADCs PK analysis solutions

Resources

Webinar playback and appointment

Addressing Challenges in Antibody-Drug Conjugate Development
Here is the brief recap of the webinar:ADCs have the potential to enable 'precision medicine' with a wide market reach.Challenges in ADCs include managing Target Affinity, enhancing payload conjugation, and assessing Payload Delivery in vivo Pharmacokinetics. We can provide high-quality solutions to address these challenges.
Addressing Challenges in Antibody-Drug Conjugate Development
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Building the Perfect Antibody-based Therapeutic from Selection to Engineering and Manufacturing
In this webinar, discover how advanced techniques such as Al-driven candidate selection optimization of antibody sequences, and precise conjugation methods come together to address some of the current challenges in antibody-based therapeutics.
Addressing Challenges in Antibody-Drug Conjugate Development
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Resource download

More core reagents for Antibody-drug conjugates (ADCs) development
AGLink® ADC site-specific conjugation kit: Powering your magic bullets
Fc Receptor Proteins - Partners for Antibody Drug Development
[Flyer]Fucntional Cell Lines and Development Service
Tools for ADC PK Analysis

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  • ADCs Development Solutions
  • Antibody Screening
  • ADC Target Proteins
  • Internalization Mechanism Characterization
  • Fc Effector Function Validation
  • Linker Screening and Validation
  • Clinical/Preclinical PK Analysis
  • Resources
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