2009
DOI: 10.1182/blood.v114.22.1123.1123
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Large Granular Lymphocyte (LGL) Expansions Comprising Oligoclonal T Cell or NK Cell Populations in Dasatinib Treated Patients Are Associated with HLA-A*0201, CMV Reactivation and Enhanced Anti-Leukemic Control.

Abstract: 1123 Poster Board I-145 Introduction Immunosuppressive effects of the second generation tyrosine kinase inhibitor dasatinib (Sprycel®) on T cells and NK cells have been described in vitro. In contrast, in some CML or Ph+ ALL patients receiving dasatinib, the development of a chronic, oscillating lymphocytosis has been observed in vivo. We previously showed that dasatinib-induced lymphocytosis typically comprises of oligoclonal NK or CD8+ cytoto… Show more

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“…Previous investigations have not identified the predictive factors for lymphocytosis. Mustijoki et al [22] suggested the role of host and environmental factor by reporting that HLA‐A*0201 and CMV reactivation was linked to the clonal expansion of leukemia patients. In our study, interestingly, the LC + group showed a relatively higher mutation ratio, although this was not statistically significant.…”
Section: Discussionmentioning
confidence: 99%
“…Previous investigations have not identified the predictive factors for lymphocytosis. Mustijoki et al [22] suggested the role of host and environmental factor by reporting that HLA‐A*0201 and CMV reactivation was linked to the clonal expansion of leukemia patients. In our study, interestingly, the LC + group showed a relatively higher mutation ratio, although this was not statistically significant.…”
Section: Discussionmentioning
confidence: 99%
“…Efekt ten okazał się niezależny od dobowej dawki stosowanego leku, a także sposobu jego podawania (raz/d., 2 razy/d.) [23]. W 2011 roku opisano wzrost bezwzględnej limfocytozy we krwi u 23 spośród 50 pacjentów z 9 koreańskich ośrodków hematologicznych oraz u 4 spośród 15 chorych z Detroit, leczonych DAZA z powodu CML [24,25].…”
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“…W jednym z doniesień Mustjoki i wsp. [23] sugerują rolę obecności antygenu zgodności tkankowej HLA*0201 oraz udział w patogenezie limfocytozy u chorych na CML reaktywacji infekcji wirusem cytomegalii (CMV, cytomegalovirus).…”
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