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Abstract :
Phase 2 multicentre trial investigating intermittent and continuous dosing schedules of the poly(ADP-ribose) polymerase inhibitor rucaparib in germline BRCA mutation carriers with advanced ovarian and breast cancer : British Journal of Cancer
Background:
Rucaparib is an orally
available potent selective small-molecule inhibitor of poly(ADP-ribose)
polymerase (PARP) 1 and 2. Rucaparib induces synthetic lethality in
cancer cells defective in the homologous recombination repair pathway
including BRCA-1/2. We investigated the efficacy
and safety of single-agent rucaparib in germline (g) BRCA mutation
carriers with advanced breast and ovarian cancers.
Methods:
Phase II, open-label, multicentre trial of rucaparib in proven BRCA-1/2
mutation carriers with advanced breast and or ovarian cancer, WHO PS
0–1 and normal organ function. Intravenous (i.v.) and subsequently oral
rucaparib were assessed, using a range of dosing schedules, to determine
the safety, tolerability, dose-limiting toxic effects and
pharmacodynamic (PD) and pharmacokinetic (PK) profiles.
Results:
Rucaparib was well tolerated in patients up to doses of 480 mg per day and is a potent inhibitor of PARP, with sustained inhibition 
24 h after single doses. The i.v. rucaparib (intermittent dosing schedule) resulted in an objective response rate (ORR) of only 2% but with 41% (18 out of 44) patients achieved stable disease for 12
weeks and 3 patients maintaining disease stabilisation for >52
weeks. The ORR for oral rucaparib (across all six dose levels) was 15%. In the oral cohorts, 81%
(22 out of 27) of the patients had ovarian cancer and 12 out of 13, who
were dosed continuously, achieved RECIST complete response/partial response (CR/PR) or stable disease (SD) 12 weeks, with a median duration of response of 179 days (range 84–567 days).
24 h after single doses. The i.v. rucaparib (intermittent dosing schedule) resulted in an objective response rate (ORR) of only 2% but with 41% (18 out of 44) patients achieved stable disease for 12
weeks and 3 patients maintaining disease stabilisation for >52
weeks. The ORR for oral rucaparib (across all six dose levels) was 15%. In the oral cohorts, 81%
(22 out of 27) of the patients had ovarian cancer and 12 out of 13, who
were dosed continuously, achieved RECIST complete response/partial response (CR/PR) or stable disease (SD) 12 weeks, with a median duration of response of 179 days (range 84–567 days).
Conclusions:
Rucaparib is well
tolerated and results in high levels of PARP inhibition in surrogate
tissues even at the lowest dose levels. Rucaparib is active in
gBRCA-mutant ovarian cancer and this activity correlates with
platinum-free interval. The key lessons learned from this study is that
continuous rucaparib dosing is required for optimal response, the
recommended phase 2 dose (RP2D) for continuous oral scheduling has not
been established and requires further exploration and, thirdly, the use
of a PD biomarker to evaluate dose–response has its limitations.
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