Investigation of Hydrophilic Auristatin Derivatives for Use in Antibody Drug Conjugates.
Brian A MendelsohnStuart D BarnscherJosh T SnyderZili AnJennifer M DoddJulien Dugal-TessierPublished in: Bioconjugate chemistry (2017)
Antibody drug conjugates offer a targeted cancer treatment for the delivery of potent cytotoxic drugs. Derivatives of the natural product dolastatin 10 containing pyridines and other basic amines were examined with the objective of determining if a more hydrophilic auristatin derivative would be potent enough for use as part of an ADC. This may be advantageous if a less hydrophobic drug makes a better ADC. A pyridine derivative, monomethyl auristatin PYE, showed the greatest potency when tested in vivo. While only a modest tumor growth inhibition was observed when the HCC1954 human breast cancer xenografts were treated with"non-cleavable" linker ADCs, tumor regression was seen when treated with an enzymatically degradable "cleavable" linker ADC when conjugated to trastuzumab. Based on these studies, monomethyl auristatin PYE shows promise for use as an ADC payload.
Keyphrases
- diffusion weighted imaging
- diffusion weighted
- cancer therapy
- contrast enhanced
- endothelial cells
- liquid chromatography
- magnetic resonance imaging
- anti inflammatory
- photodynamic therapy
- ionic liquid
- computed tomography
- water soluble
- magnetic resonance
- epidermal growth factor receptor
- induced pluripotent stem cells
- big data
- machine learning
- adverse drug
- drug induced
- high resolution
- breast cancer risk