Dasatinib has been reported to potently inhibit juxtamembrane domain mutant KIT(D816V) autophosph... more Dasatinib has been reported to potently inhibit juxtamembrane domain mutant KIT(D816V) autophosphorylation and KIT-dependent activation of down stream signaling important for cell growth and survival of neoplastic cells. Additionally, dasatinib induced apoptosis in mast cell and leukemia cell lines expressing KIT(D816V). Here, we present the first case report of long-term hematologic and molecular remission achieved with combined treatment with chemotherapy and dasatinib in a patient with systemic mastocytosis (SM) and acute myeloid leukemia (AML) with mutant KIT(D816V) expression. A 50-year-old male presented with pancytopenia, organomegaly, lymphadenopathy, and lytic bone lesions in the pelvis. The patient was found to have systemic mastocytosis (SM) and acute myelogeneous leukemia (AML) positive for KIT(D816V) and therefore diagnosed with SM with an associated clonal hematological non-mast cell lineage disease (SM-AHNMD). Both primary CD34+ cells containing myeloblasts and CD34- cells containing mastocytes obtained from the diagnostic BM lost viability markedly by in vitro dasatinib treatment. In addition, dasatinib diminished activity of STAT5, STAT3, AKT and ERK and attenuated the levels of c-KIT. The patient achieved a hematologic complete remission (HCR) by two induction chemotherapies with residual mastocytes. Dasatinib (70mg PO bid, days 1-4) was added to consolidation treatments composed of four cycles of high dose cytarabine and was then continued as maintenance therapy (50mg PO bid). Periodic bone marrow (BM) aspirate/biopsies (eight over 18 months) were performed. The patient remained in HCR, and the mastocyte burden decreased by 50%. The bone lytic lesions improved. The KIT(D816V)mutation progressively decreased and became undetectable in the last three BM analyses. This result was confirmed by an independent laboratory showing a lack of c-KIT mutation in both CD34+ cells and CD34- cells in the last BM. No significant adverse effects of dasatinib occurred. Dasatinib has in vitro and in vivo efficacy in SM-AML patients with KIT(D816V) mutation. Along with chemotherapy, dasatinib should be considered in these patients particularly if they cannot undergo allogeneic stem cell transplantation for this poor prognostic AML.
« PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. ... more « PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. Co-segregation of BRCA1 185delAG mutation and BRCA2 6174delT in one single family. R. Gershoni-Baruch: Affiliations. Correspondence to R. Gershoni-Baruch. ...
« PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. ... more « PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. Co-segregation of BRCA1 185delAG mutation and BRCA2 6174delT in one single family. R. Gershoni-Baruch: Affiliations. Correspondence to R. Gershoni-Baruch. ...
Dasatinib has been reported to potently inhibit juxtamembrane domain mutant KIT(D816V) autophosph... more Dasatinib has been reported to potently inhibit juxtamembrane domain mutant KIT(D816V) autophosphorylation and KIT-dependent activation of down stream signaling important for cell growth and survival of neoplastic cells. Additionally, dasatinib induced apoptosis in mast cell and leukemia cell lines expressing KIT(D816V). Here, we present the first case report of long-term hematologic and molecular remission achieved with combined treatment with chemotherapy and dasatinib in a patient with systemic mastocytosis (SM) and acute myeloid leukemia (AML) with mutant KIT(D816V) expression. A 50-year-old male presented with pancytopenia, organomegaly, lymphadenopathy, and lytic bone lesions in the pelvis. The patient was found to have systemic mastocytosis (SM) and acute myelogeneous leukemia (AML) positive for KIT(D816V) and therefore diagnosed with SM with an associated clonal hematological non-mast cell lineage disease (SM-AHNMD). Both primary CD34+ cells containing myeloblasts and CD34- cells containing mastocytes obtained from the diagnostic BM lost viability markedly by in vitro dasatinib treatment. In addition, dasatinib diminished activity of STAT5, STAT3, AKT and ERK and attenuated the levels of c-KIT. The patient achieved a hematologic complete remission (HCR) by two induction chemotherapies with residual mastocytes. Dasatinib (70mg PO bid, days 1-4) was added to consolidation treatments composed of four cycles of high dose cytarabine and was then continued as maintenance therapy (50mg PO bid). Periodic bone marrow (BM) aspirate/biopsies (eight over 18 months) were performed. The patient remained in HCR, and the mastocyte burden decreased by 50%. The bone lytic lesions improved. The KIT(D816V)mutation progressively decreased and became undetectable in the last three BM analyses. This result was confirmed by an independent laboratory showing a lack of c-KIT mutation in both CD34+ cells and CD34- cells in the last BM. No significant adverse effects of dasatinib occurred. Dasatinib has in vitro and in vivo efficacy in SM-AML patients with KIT(D816V) mutation. Along with chemotherapy, dasatinib should be considered in these patients particularly if they cannot undergo allogeneic stem cell transplantation for this poor prognostic AML.
« PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. ... more « PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. Co-segregation of BRCA1 185delAG mutation and BRCA2 6174delT in one single family. R. Gershoni-Baruch: Affiliations. Correspondence to R. Gershoni-Baruch. ...
« PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. ... more « PreviousNext »European Journal of Cancer Volume 33, Issue 13 , Pages 2283-2284, November 1997. Co-segregation of BRCA1 185delAG mutation and BRCA2 6174delT in one single family. R. Gershoni-Baruch: Affiliations. Correspondence to R. Gershoni-Baruch. ...
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