Antibody-drug conjugates (ADCs) are made up of a monoclonal antibody linked to a cytotoxic drug (payload) through a stable chemical linker, enabling targeted delivery of the drug to specific cancer cells. The ideal ADC payload should have sufficient toxicity, low immunogenicity, high stability, and modifiable functional groups. All approved ADC therapeutics currently possess a single-drug payload, such as monomethyl auristatin E (MMAE), monomethyl auristatin F (MMAF), or maytansinoids like DM1 and DM4. A recent review by Journeaux & Bernardes describes how researchers are now attempting to develop homogenous ADCs with multiple unique payloads to improve the efficacy of targeted therapy. However, due to the many reactive functional groups on the surface of an antibody, this task has been difficult.
Most of the research in this field focuses on dual-payload ADCs. Another review by Wang et al. highlights how dual-payload ADCs can have greater therapeutic effects and survival benefits than just two single-agent combinations. Just a few weeks ago, Hummingbird Bioscience presented promising data on their dual-payload ADC to overcome severe side effects and the intrinsic or acquired resistance seen in patients with earlier generation single payload ADCs.
The problem with heterogeneity within tumors such as breast cancer, is that multiple cells with different gene expression profiles results in drug resistance, recurrence, and metastasis after chemotherapy. Researchers from The University of Texas Health Science Center developed a homogeneous ADC containing two distinct payloads with HER2-specific cell killing potency by chemoenzymatic conjugation. Unlike other methods, their linker systems allowed for the generation of a panel of homogeneous dual-drug ADCs with flexible combined drug-to-antibody ratios (DARs) of 2 + 2, 4 + 2, and 2 + 4. DARs are typically maintained under a value of 4 to avoid monoclonal antibody aggregation and limit hydrophobicity, as they have been linked to toxicity, reduced half-life and a narrow therapeutic index.
This report aims to explore the events and trends of the biopharmaceutical industry in Q2 (April, May, June). Besides crovalimab and Vyloy, two more novel antibody drugs have been approved this year
The start of 2024 has seen leaps in deals for antibody therapeutics, especially ADCs (antibody-drug conjugates). This report aims to explore the events and trends of the biopharmaceutical industry in Q1. As of now, only two novel antibody drugs have been approved this year, but many more in regulatory review are expected to be fully approved.
Alzheimer’s research has undergone transformative changes in recent years, characterized by breakthroughs, controversies, and a reevaluation of long-held theories. Recently, BioArctic announced a global license agreement with Bristol Myers Squibb for BioArctic’s PyroGlutamate-
The FDA has revoked Emergency Use Authorizations (EUAs) for multiple COVID-19 monoclonal antibody (mAb) therapies, including those developed by Eli Lilly, AstraZeneca, Vir Biotechnology, and Regeneron. This decision reflects the challenges of targeting rapidly mutating viruses like SARS-CoV-2, which
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