Abstract
Small-molecule protein kinase inhibitors are used for the treatment of various diseases. Although their effect(s) on the respective kinase are generally quite well understood, surprisingly, their interaction with membranes is only barely investigated; even though these drugs necessarily come into contact with the plasma and intracellular membranes. Using biophysical methods such as NMR, ESR, and fluorescence spectroscopy in combination with lipid vesicles, we studied the membrane interaction of the kinase inhibitors sunitinib, erlotinib, idelalisib, and lenvatinib; these drugs are characterized by medium log p values, a parameter reflecting the overall hydrophobicity of the molecules, which is one important parameter to predict the interaction with lipid membranes. While all four molecules tend to embed in a similar region of the lipid membrane, their presence has different impacts on membrane structure and dynamics. Most notably, sunitinib, exhibiting the lowest log p value of the four inhibitors, effectively influences membrane integrity, while the others do not. This shows that the estimation of the effect of drug molecules on lipid membranes can be rather complex. In this context, experimental studies on lipid membranes are necessary to (i) identify drugs that may disturb membranes and (ii) characterize drug–membrane interactions on a molecular level. Such knowledge is important for understanding the efficacy and potential side effects of respective drugs.
Highlights
In order to understand the impact of therapeutically applied drugs on cells, the knowledge about interactions of the molecules with cellular membranes is of high relevance.Firstly, plasma membranes can be defined as the primary contact site of the drug with the cell
One obvious approach to anticipate the membrane interaction of membrane active molecules is to consider their log p value, which quantitatively reflects the partition of the respective compound between octanol and water
ESR assay, which does not does depend light on light absorption, found in the of presence of asunitinib a significant of the absorption, we foundwe in the presence sunitinib significant increase ofincrease the ascorbate ascorbate permeation rate
Summary
In order to understand the impact of therapeutically applied drugs on cells, the knowledge about interactions of the molecules with cellular membranes is of high relevance.Firstly, plasma membranes can be defined as the primary contact site of the drug with the cell. In order to understand the impact of therapeutically applied drugs on cells, the knowledge about interactions of the molecules with cellular membranes is of high relevance. It can be presumed that this aspect of cellular drug effect(s) is important for understanding the efficacy and side effects of the respective substances. Despite this significance, drug–membrane interactions have not been investigated in detail for many existing medications. One obvious approach to anticipate the membrane interaction of membrane active molecules is to consider their log p value, which quantitatively reflects the partition of the respective compound between octanol and water. Focusing on log p values is a very simplified method and more (physico-chemical) parameters have
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