Tumors acquiring resistance is one of the major barriers to successful
cancer therapy. Feng Fu, Sebastian Bonhoeffer (ETH Zurich) and their
collaborator Martin Nowak (Harvard) use mathematical models to
characterize how important aspects of tumor micro-environment can impair
the efficacy of targeted cancer therapies.Failure of cancer therapy
is commonly attributed to pre-existing resistant mutants already
present prior to treatment. The research highlights the important role of tumor sanctuaries in the rapid acquisition of resistance.
The authors offer an in silico model for predicting treatment outcomes that depend on the tumor micro-environment
within a solid tumor or across metastases. The results show that
resistance in non-sanctuary sites is likely originated from sanctuaries
with little drug exposure.
There is increasing evidence that the tumor microenvironment influences cell sensitivity to drugs mediating the evolution of drug resistance.
The results provide new insights into understanding why cancers tend to
quickly become resistant, and that cell migration and the presence of
sanctuary sites with little drug exposure are essential to this end.
"In order to improve our ability to fight
against cancer, not only we should search for more effective therapies
that sufficiently target tumor genetic heterogeneity, but also such
efforts will have to be paralleled with finding novel delivery
approaches aimed at eliminating potential tumor sanctuaries."
No comments:
Post a Comment