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Research ArticleExperimental Studies

Comparative Effects of PP242 and Rapamycin on mTOR Signalling and NOTCH Signalling in Leukemia Cells

AYA ONO, RYO OIKE, YUKI OKUHASHI, YUSUKE TAKAHASHI, MAI ITOH, NOBUO NARA and SHUJI TOHDA
Anticancer Research March 2013, 33 (3) 809-813;
AYA ONO
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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RYO OIKE
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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YUKI OKUHASHI
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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YUSUKE TAKAHASHI
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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MAI ITOH
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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NOBUO NARA
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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SHUJI TOHDA
Department of Laboratory Medicine, Tokyo Medical and Dental University, Yushima, Tokyo, Japan
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  • For correspondence: tohda.mlab@tmd.ac.jp
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Abstract

Aim: PP242 is a compound which inhibits both mammalian target of rapamycin complex-1 (mTORC1) and mTORC2. We examined the effects of PP242 and rapamycin on mTOR signalling and evaluated potential crosstalk with the NOTCH signalling in eight leukemia cell lines. Materials and Methods: We examined the effects of treatment with these inhibitors on cell growth and protein expression. Results: PP242 suppressed growth more potently than did rapamycin. In two cell lines poorly sensitive to PP242, PP242 failed to inhibit v-akt murine thymoma viral oncogene homolog (AKT) phosphorylation. Suppression of mTOR phosphorylation was weaker in myeloid cell lines. Rapamycin induced eukaryotic initiation factor 4E-binding protein 1 (4E-BP1) hyperphosphorylation in three cell lines. Phosphorylation of both isoforms (p70 and p85) of S6 kinase (S6K) was suppressed in three cell lines; only p70 was suppressed in the others. NOTCH1 expression and activation were up-regulated by PP242 in one cell line but down-regulated in another. Conclusion: PP242 is a candidate for molecular-targeted leukemia therapy, although its effects must be evaluated on a case-by-case basis. Crosstalk was found between the mTOR and NOTCH signalling pathways.

  • mTOR
  • rapamycin
  • NOTCH
  • leukemia
  • Received December 25, 2012.
  • Revision received February 5, 2013.
  • Accepted February 5, 2013.
  • Copyright© 2013 International Institute of Anticancer Research (Dr. John G. Delinassios), All rights reserved
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Anticancer Research: 33 (3)
Anticancer Research
Vol. 33, Issue 3
March 2013
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Comparative Effects of PP242 and Rapamycin on mTOR Signalling and NOTCH Signalling in Leukemia Cells
AYA ONO, RYO OIKE, YUKI OKUHASHI, YUSUKE TAKAHASHI, MAI ITOH, NOBUO NARA, SHUJI TOHDA
Anticancer Research Mar 2013, 33 (3) 809-813;

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Comparative Effects of PP242 and Rapamycin on mTOR Signalling and NOTCH Signalling in Leukemia Cells
AYA ONO, RYO OIKE, YUKI OKUHASHI, YUSUKE TAKAHASHI, MAI ITOH, NOBUO NARA, SHUJI TOHDA
Anticancer Research Mar 2013, 33 (3) 809-813;
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Keywords

  • mTOR
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