Integrating cell-level kinetic modeling into the optimization of cancer 
therapeutics

Krippendorff, Ben-Fillippo

Item

ITEM ACTIONSEXPORT

Add to Basket

Local TagsRelease HistoryDetailsSummary

Released

Thesis

Integrating cell-level kinetic modeling into the optimization of cancer therapeutics

MPS-Authors

Krippendorff, Ben-Fillippo
Max Planck Society;

External Resource

No external resources are shared

Fulltext (restricted access)

There are currently no full texts shared for your IP range.

Fulltext (public)

Krippendorff.pdf
(Any fulltext), 12MB

Supplementary Material (public)

There is no public supplementary material available

Citation

Krippendorff, B.-F. (2010). Integrating cell-level kinetic modeling into the optimization of cancer therapeutics. PhD Thesis, National University of Ireland, Maynooth.

Cite as: https://hdl.handle.net/11858/00-001M-0000-0010-7C68-6

Abstract

Cancer therapy bene ts today from the availability of new promising classes of drugs such as therapeutic proteins. Due to their ability to speci cally bind targets in the body they allow to modulate speci c chemical reactions and ultimately to modify the functional response of the cell, such as cell growth or cell division. Targeting receptor systems by competitive inhibition is the objective of various protein drugs in development and on the market. Many targeted receptor systems also constitute a degradation mechanism for the drug via endocytosis and a thorough understanding of the complex interplay between the drug's pharmacokinetics and its e ect, is largely missing. For complex diseases such as cancer, systems biology models of therapeutically relevant cellular processes have proven valuable for identifying potent drug targets. So far, such information about the dynamics of the targeted system is neglected in later stages of the drug development process when pharmacokinetic modeling is used to guide dose nding and analyze preclinical or clinical in vivo data. This is especially critical for therapeutic proteins where, due to the degradation mediated by the targeted receptor, drug e ect and pharmacokinetics are inherently interdependent. This thesis combines the points of view of systems biology and pharmacokinetics. We present a detailed mechanistic model of the targeted cellular system that explicitly takes into account receptor binding and tra cking inside the cell and that is used to derive reduced models of drug degradation which retain a mechanistic interpretation. By integrating celllevel models with established pharmacokinetic models, we translate biophysical properties of protein drugs into a transient drug e ect in vivo. We illustrate the approach for antibodies against the epidermal growth factor receptor used in cancer therapy. The cell-level pharmacokinetic/pharmacodynamic model identi es options and limits for future therapeutic antibodies and links their inhibitory e ect with genomic alteration of tumor cells.