abstract
IMPLICATIONS FOR PRACTICE:
Microsatellite
instability
(MSI-H) colorectal tumors exhibit hypermethylation in tumor
mismatch repair genes, or have mutations in one or more of these genes
resulting from a germ-line defect (
Lynch syndrome).
PARP inhibitors such
as olaparib are most effective in tumors associated with inability to
repair DNA damage. However, in this trial, single agent
olaparib failed
to elicit responses in patients with
MSI-H colorectal tumors, and in
those with microsatellite-stable tumors. It is possible that by adding
olaparib to radiation therapy, or to a systemic DNA damaging agent,
tumor lethality could be obtained. However, the price would be
increased
toxicity.
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