Mitsuyo Uesawa scite author profile

Bendamustine has shown considerable clinical activity against indolent lymphoid malignancies as a single agent or in combination with rituximab, but combination with additional anti-cancer drugs may be required for refractory and/or relapsed cases as well as other intractable tumors. In this study, we attempted to determine suitable anti-cancer drugs to be combined with bendamustine for the treatment of mantle cell lymphoma, diffuse large B-cell lymphoma, aggressive lymphomas and multiple myeloma, all of which are relatively resistant to this drug, and investigated the mechanisms underlying synergism. Isobologram analysis revealed that bendamustine had synergistic effects with alkylating agents (4-hydroperoxy-cyclophosphamide, chlorambucil and melphalan) and pyrimidine analogues (cytosine arabinoside, gemcitabine and decitabine) in HBL-2, B104, Namalwa and U266 cell lines, which represent the above entities respectively. In cell cycle analysis, bendamustine induced late S-phase arrest, which was enhanced by 4-hydroperoxy-cyclophosphamide, and potentiated early S-phase arrest by cytosine arabinoside (Ara-C), followed by a robust increase in the size of sub-G1 fractions. Bendamustine was able to elicit DNA damage response and subsequent apoptosis faster and with shorter exposure than other alkylating agents due to rapid intracellular incorporation via equilibrative nucleoside transporters (ENTs). Furthermore, bendamustine increased the expression of ENT1 at both mRNA and protein levels and enhanced the uptake of Ara-C and subsequent increase in Ara-C triphosphate (Ara-CTP) in HBL-2 cells to an extent comparable with the purine analog fludarabine. These purine analog-like properties of bendamustine may underlie favorable combinations with other alkylators and pyrimidine analogues. Our findings may provide a theoretical basis for the development of more effective bendamustine-based combination therapies.

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Combination of tipifarnib and rapamycin synergistically inhibits the growth of leukemia cells and overcomes resistance to tipifarnib via alteration of cellular signaling pathways

Nagai

Ohmine

Fujiwara

et al. 2010

Leukemia Research

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Bone Marrow Metastasis of Malignant Melanoma

et al. 2006

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A 67-year-old woman was admitted to our hospital with a 3-month history of lower back pain. One year earlier, the patient was diagnosed with malignant melanoma of the right maxillary bone and underwent an operation followed by adjuvant chemotherapy. (Fig. 1) A bone marrow aspirate revealed that the marrow was infiltrated by tumors composed of nests of poorly differentiated cells. These tumor cells were large and round shaped, and the cellular outlines within clumps of tumor cells were indistinct. Although these findings were not specific for any group of metastatic tumors, the cytoplasm of tumor cells was filled with numerous granules of melanin

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Plasmapheresis‐Refractory Transplantation‐Associated Thrombotic Microangiopathy Successfully Treated With Pravastatin and Limaprost Alfadex

2013

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Mitsuyo Uesawa

Mechanisms of resistance to azacitidine in human leukemia cell lines

Purine Analog-Like Properties of Bendamustine Underlie Rapid Activation of DNA Damage Response and Synergistic Effects with Pyrimidine Analogues in Lymphoid Malignancies

Combination of tipifarnib and rapamycin synergistically inhibits the growth of leukemia cells and overcomes resistance to tipifarnib via alteration of cellular signaling pathways

Bone Marrow Metastasis of Malignant Melanoma

Plasmapheresis‐Refractory Transplantation‐Associated Thrombotic Microangiopathy Successfully Treated With Pravastatin and Limaprost Alfadex

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