Pregled bibliografske jedinice broj: 98393
The relevance of multidrug resistance-associated Pgp expression and function in responses to Gleevec
The relevance of multidrug resistance-associated Pgp expression and function in responses to Gleevec // The Hematology Journal, 3 (Suppl 1)
Firenca, Italija, 2002. str. 313-313 (poster, međunarodna recenzija, sažetak, znanstveni)
CROSBI ID: 98393 Za ispravke kontaktirajte CROSBI podršku putem web obrasca
Naslov
The relevance of multidrug resistance-associated Pgp expression and function in responses to Gleevec
Autori
Svoboda-Beusan, Ivna ; Bulum, Joško ; Ajduković, Radmila ; Rabatić, Sabina ; Gačić, Maja ; Labar, Boris
Vrsta, podvrsta i kategorija rada
Sažeci sa skupova, sažetak, znanstveni
Izvornik
The Hematology Journal, 3 (Suppl 1)
/ - , 2002, 313-313
Skup
7th Annual Meeting of the European Haematology Association
Mjesto i datum
Firenca, Italija, 06.06.2002. - 09.06.2002
Vrsta sudjelovanja
Poster
Vrsta recenzije
Međunarodna recenzija
Sažetak
Gleevec is among the most promising highly selective inhibitors of fusion Bcr-Abl tyrosine kinase activity in chronic myeloid leukemia (CML) cells. A possible mechanisms of resistance to Gleevec are yet unknown. Although published data are very limited, the overexpressed P-glycoprotein (Pgp) in some resistant cells may indicate that Pgp can operate in response and be another reason for the reduced sensitivity (1). Objective: To evaluate the influence of Gleevec on the expression level and function and its correlation to the treatment outcome. Design and methods: Fourteen patients aged >22 yrs with advanced CML /4 blast crisis (BC), 9 accelerated phase (AP) and 1 in chronic phase/ were monitored in 3 months intervals. Previous treatment included cytoreductive HU and Ara-C followed by progressive doses of IFN-alpha. Patients were eligible if they were in the chronic phase of Ph+CML and had not responded or showed intolerance to IFN-alpha therapy, or if they were in accelerated phase and blast crisis of Ph+CML. Gleevec was administered as oral monotherapy: 600 mg daily for BC and AP and 400 mg/day for patients in chronic phase, respectively. Due to toxicity reaction in 6 patients the dose was reduced. To determine the changes in Pgp phenotype, bone marrow and peripheral blood cells were stained simultaneously with anti-HLA-DR and Pgp monoclonal antibodies (Becton Dickinson) and the results were expressed as the ratio of mean fluorescences (RMF) of specific anti-Pgp and FL2 isotype control fluorescence. Pgp activity was assessed by comparing the uptake/efflux rates of Pgp-related rhodamine dye (Rh123) together with Pgp-reversing agent Cyclosporine A. Results: Our preliminary results indicate that the changes in Pgp phenotype and function may influence the response to Gleevec treatment. Although none of Pgp-inactive patients underwent clinical relapse while Pgp+ and active patients did relapse, due to short-term follow-up those differences did not reach statistical significance. Conclusion: One of the new mechanisms of resistance to Gleevec therapy in CML can be Pgp-associated. From the prognostic point of view, screening of changes in Pgp phenotype and function may be helpful in determination of Gleevec-resistant phenotypes. (1) Blood 2000; 96:1070-9
Izvorni jezik
Engleski
Znanstvena područja
Temeljne medicinske znanosti
