Antibody-Drug Conjugates-Evolution and Perspectives.
Adriana Aurelia Aurelia ChisCarmen Maximiliana Maximiliana DobreaAnca Maria ArseniuAdina FrumLuca-Liviu RusGabriela CormosCecilia GeorgescuClaudiu MorgovanAnca ButucaFelicia Gabriela Gabriela GligorAndreea Loredana Vonica-TincuPublished in: International journal of molecular sciences (2024)
Antineoplastic therapy is one of the main research themes of this century. Modern approaches have been implemented to target and heighten the effect of cytostatic drugs on tumors and diminish their general/unspecific toxicity. In this context, antibody-drug conjugates (ADCs) represent a promising and successful strategy. The aim of this review was to assess different aspects regarding ADCs. They were presented from a chemical and a pharmacological perspective and aspects like structure, conjugation and development particularities alongside effects, clinical trials, safety issues and perspectives and challenges for future use of these drugs were discussed. Representative examples include but are not limited to the following main structural components of ADCs: monoclonal antibodies (trastuzumab, brentuximab), linkers (pH-sensitive, reduction-sensitive, peptide-based, phosphate-based, and others), and payloads (doxorubicin, emtansine, ravtansine, calicheamicin). Regarding pharmacotherapy success, the high effectiveness expectation associated with ADC treatment is supported by the large number of ongoing clinical trials. Major aspects such as development strategies are first discussed, advantages and disadvantages, safety and efficacy, offering a retrospective insight on the subject. The second part of the review is prospective, focusing on various plans to overcome the previously identified difficulties.
Keyphrases
- clinical trial
- cancer therapy
- randomized controlled trial
- systematic review
- drug delivery
- phase ii
- oxidative stress
- stem cells
- epidermal growth factor receptor
- open label
- current status
- hodgkin lymphoma
- smoking cessation
- study protocol
- bone marrow
- diffusion weighted imaging
- mesenchymal stem cells
- phase iii
- magnetic resonance
- tyrosine kinase
- finite element
- contrast enhanced