Pregled bibliografske jedinice broj: 596375
BCR-ABL KINASE DOMAIN MUTATIONS IN PRIMARY AND SECONDARY RESISTANT IMATINIB-TREATED CHRONIC MYELOID LEUKEMIA
BCR-ABL KINASE DOMAIN MUTATIONS IN PRIMARY AND SECONDARY RESISTANT IMATINIB-TREATED CHRONIC MYELOID LEUKEMIA // PROGRAM AND ABSTRACTS THE SEVENTH CONFERENCE IN FORENSICS, ANTHROPOLOGIC AND MEDICAL GENETICS AND MAYO CLINIC LECTURES IN TRANSLATIONAL MEDICINE
Bol, Hrvatska, 2011. (poster, međunarodna recenzija, sažetak, znanstveni)
CROSBI ID: 596375 Za ispravke kontaktirajte CROSBI podršku putem web obrasca
Naslov
BCR-ABL KINASE DOMAIN MUTATIONS IN PRIMARY AND SECONDARY RESISTANT IMATINIB-TREATED CHRONIC MYELOID LEUKEMIA
Autori
Marusic Vrsalovic, Maruška ; Livun, Ana ; Duic, Ivana ; Ajdukovic, Radmila ; Hariš, Višnja, Jakšić, Ozren ; Pejša, Vlatko ; Kušec, Rajko Kušec R
Vrsta, podvrsta i kategorija rada
Sažeci sa skupova, sažetak, znanstveni
Izvornik
PROGRAM AND ABSTRACTS THE SEVENTH CONFERENCE IN FORENSICS, ANTHROPOLOGIC AND MEDICAL GENETICS AND MAYO CLINIC LECTURES IN TRANSLATIONAL MEDICINE
/ - , 2011
Skup
ISABS – International Society for Applied Biological Sciences
Mjesto i datum
Bol, Hrvatska, 20.06.2011. - 24.06.2011
Vrsta sudjelovanja
Poster
Vrsta recenzije
Međunarodna recenzija
Ključne riječi
CML; imatinib therapy; KD mutations; imatinib resistance; ASO-PCR
Sažetak
Mutations of BCR-ABL tyrosine kinase domain are the major cause of resistance to imatinib in patients with chronic myeloid leukemia. However, it is not known whether KD mutant clones that are detectable prior to therapy are selected in the presence of imatinib, and whether they may predict for therapy outcome. We sought to investigate the occurrence and dynamics of 4 common KD mutations (T315I, F311L, E255K, E255V) in imatinib-treated patients lacking predicted therapy response (by ELN criteria). Eleven of 41 imatinib-treated CML patients showed primary resistance to imatinib with inadequate CgR and consistently high levels of BCR-ABL transcripts monitored by real-time PCR. Using ASO-PCR we investigated the prevalence and the evolution of the above mentioned mutations in pretherapeutic diagnostic samples and in follow-up samples collected throughout imatinib therapy. In 3 patients F311L mutation was detected in imatinib-naive pretherapeutic leukemic samples. Eight patients showed no mutations at the time of diagnosis. After 24 months of imatinib therapy identical mutation status was identified in 5/12 patients (41.6%). Two patients acquired additional mutation (E255K, E255V, one each) and had approximately 10 times higher BCR-ABL transcripts compared to patients with single KD mutation. T315I mutation was not detected. We conclude that: (1) increased proportion of mutated sequences during treatment detected by ASO-PCR suggests clonal evolution of mutated cells, (2) KD mutations are not restricted to the accelerated phase of the disease, and in some cases, mutations occur in chronic phase of the disease and prior to imatinib therapy.
Izvorni jezik
Engleski
Znanstvena područja
Temeljne medicinske znanosti
POVEZANOST RADA
Ustanove:
Klinička bolnica "Dubrava"
Profili:
Višnja Hariš
(autor)
Ana Livun
(autor)
Vlatko Pejša
(autor)
Maruška Marušić Vrsalović
(autor)
Rajko Kušec
(autor)
