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THE ANTILEUKEMIC ACTIVITY OF 5-AZA-2 DEOXYCYTIDINE (AZA-DC) IN PATIENTS WITH RELAPSED AND RESISTANT LEUKEMIA
被引:67
|作者:
RICHEL, DJ
COLLY, LP
KLUINNELEMANS, JC
WILLEMZE, R
机构:
[1] Department of Haematology, University Medical Centre, Leiden
关键词:
5-AZA-2'-DEOXYCYTIDINE;
LEUKEMIA;
DNA;
DIFFERENTIATION;
INHIBITION;
INDUCTION;
CYTOSINE;
CELLS;
MICE;
D O I:
10.1038/bjc.1991.258
中图分类号:
R73 [肿瘤学];
学科分类号:
100214 ;
摘要:
In the present study we demonstrate that Aza-dC in combination with Amsacrine has major antileukaemic properties in patients who have not already received extensive Ara-C therapy. Eight out of 11 patients in their first relapse of acute leukaemia achieved complete remission. Cross resistance between Ara-C and Aza-dC was revealed by the lack of antileukaemic activity in five patients with with Ara-C resistant leukaemia. Combination therapy with Aza-dC/Ams-acrine induced a considerable period of a granulo-cytopenia (28-35 days), while the toxic effect on erythro- and megakaryopoiesis was comparable to that reported for high dose Ara-C/Amsacrine chemotherapy. Remarkable is the long disappearance time for leukaemic blast cells in bone marrow, i.e. 3-5 weeks in some cases. Analysis of cell membrane markers showed a loss of the early differentiation antigens CD34 and CD33 from leukaemic bone marrow cells after 7 days of Aza-dC treatment, which is suggestive of leukaemic cell differentiation. In the small group of patients tested for DNA hypomethylation no association existed between the degree of hypomethylation and clinical response. Non-haematologic side effects were considerable in patients receiving the highest dosages of Aza-dC and consisted of severe, although usually reversible, gastrointestinal and neurological complications. In comparison with Ara-C, Aza-dC causes less nausea and vomiting and is therefore better tolerated.
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页码:144 / 148
页数:5
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