Kidney Cancer Clinical Trial
Official title:
Evaluation of a Promising New Combination of Protein Kinase Inhibitors on Organotypic Cultures of Human Renal Tumors
The investigators objective is to test the combination directly on organotypic cultures of
tumors from patients after their excision in the Department of Urology and Renal
Transplantation of the University Hospital of Grenoble and to compare their efficacy with
that of currently selected treatments in the clinic.
The population targeted by the combination for use in clinical practice is patients with
metastatic clear cell renal cell carcinoma.
Current treatments for these patients are Sunitinib, Pazopanib and Temsirolimus.
Given the failure of conventional therapies in kidney cancer, both chemo and radio resistant,
it was necessary to seek therapeutic alternatives.
Thus, in 2005, the first targeted therapies in kidney cancer came with protein kinase
inhibitors including mTOR (mammilian target of rapamycin) inhibitors (Temsirolimus and
Everolimus) and VEGFR inhibitors (Sunitinib, Sorafenib, Pazopanib and Axitinib).
Nevertheless resistance to these treatments appeared with their prolonged use as monotherapy
in all cases. One of the main mechanisms of this therapeutic escape is the adaptation of the
tumor cell via the use of an alternative pathway of deregulation of cell signaling.
Thus emerged the idea of simultaneously treating multiple targets to prevent the tumor cell
from adapting. Phase I / II therapeutic trials have already been initiated with the
combination of anti-BRAF (proto-oncogene B-Raf) and anti-MEK (MAP-ERK kinase) in metastatic
melanoma or with the combination of anti-EGFR (epidermal growth factor receptor) and anti-MET
in lung and breast cancer. The results are very promising since we observe a synergistic
effect of two targeted therapies combined.
In kidney cancer, this escape phenomenon is also observed (example of the mTORC2 (mammilian
target of rapamycin complex 2) crosstalk on AKT which limits the effect of mTORC1 (mammilian
target of rapamycin complex 1) inhibitors at the level of the PI3 kinase signaling pathway).
It is therefore time to check if this strategy is applicable in kidney cancer. The
investigators have, through a chemo-genomic screening of a hundred molecules stored in the
CEA (French Alternative Energies and Atomic Energy Commission) chemical bank, found a
combination of inhibitors targeting the kinases CK2 and ATM very effective on a human cell
line of renal cell carcinoma clear. This combination has been tested on conventional cultures
as well as on more innovative 3D cultures, better reproducing the tumor environment. The
preliminary results obtained show that the combination is clearly more efficient in a 3D
model as well as on the VHL-line (von Hippel-Lindau) in hypoxic condition, which is very
encouraging.
In the context of preclinical validation, it is now essential to evaluate the therapeutic
potential of these molecules by comparing their efficiency with those currently selected.
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