Publication Date:
2009-11-20
Description:
Abstract 2374 Poster Board II-351 ABT-263 is a first-in-class BH3 mimetic inhibitor of 3 pro-survival members of the BCL2 protein family (BCL2, BCLXL, BCLW). Consistent with potent activity against BCL2-overexpressing cell lines and primary CLL cells in vitro, and BCL2-overexpressing lymphoid murine tumors in vivo, ABT-263 demonstrated significant antitumor activity in pts with relapsed, refractory CLL and small lymphocytic lymphoma (SLL) in 2 phase 1/2a studies. To date, 42 pts (35 evaluable) with CLL/SLL have been treated with ABT-263 (40-440 mg/d). 51% (18/35) with a baseline lymphocytosis 〉5,000 have achieved '50% reduction in lymphocytosis, while 34% (12/35; 5 bulky disease) with measurable nodal disease at initiation have achieved a partial response. Overall, some manifestation of antitumor activity was observed in 60% (21/35). Responses tend to be durable, with the median PFS not reached as yet while the median time on study for M06-873 pts is 9 mos for pts on the M06-873 study. Responses were observed in pts who received 〉4 lines of prior therapy and in those who were fludarabine refractory and/or had bulky disease. BCL2 is highly expressed in all CLL/SLL, yet only a subset of pts responded. We tested whether additional intrinsic biological characteristics of CLL were associated with response to ABT-263 in vivo. Potential biomarkers, both standard (FISH for 17p13, 11q22.3) and investigational (in vitro sensitivity; quantitative expression of BCL2, MCL1, BIM, BAX) were measured at study entry, during therapy and where possible at progression in a subset of pts treated in the phase 1 study in CLL (M06-873). Of 21 pts receiving 〉40mg/d ABT-263 for 〉7d, FISH data for 17p13 and 11q22.3 were available for 16, of which only 5 were normal; 4 and 6 had deleted 17p13 or 11q22.3 respectively, and 2 had deletions for both in 〉5% of cells examined. Similar majorities of pts with del17p13 (4/6) or del11q22.3 (5/8), or with neither abnormality (4/5), achieved either a 〉50% fall in peripheral blood lymphocytes, reduction in nodal size, or both. None of the pts without del17p13 or del11q22.3 have progressed after median 285 d (range 167-484 d) on drug, while only 1/6 with del17p13 and 2/8 with del11q22.3 have progressed (all 3 within 3 mos). CLL cells from 12 pts were tested for in vitro sensitivity to ABT-737, a BH3 mimetic with the same specificity and activity in vitro as ABT-263. LC50 were all
Print ISSN:
0006-4971
Electronic ISSN:
1528-0020
Topics:
Biology
,
Medicine
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