PLoS ONE (Jan 2012)

Rhodacyanine derivative selectively targets cancer cells and overcomes tamoxifen resistance.

  • John Koren,
  • Yoshinari Miyata,
  • Janine Kiray,
  • John C O'Leary,
  • Lana Nguyen,
  • Jianping Guo,
  • Laura J Blair,
  • Xiaokai Li,
  • Umesh K Jinwal,
  • Jin Q Cheng,
  • Jason E Gestwicki,
  • Chad A Dickey

DOI
https://doi.org/10.1371/journal.pone.0035566
Journal volume & issue
Vol. 7, no. 4
p. e35566

Abstract

Read online

MKT-077, a rhodacyanine dye, was shown to produce cancer specific cell death. However, complications prevented the use of this compound beyond clinical trials. Here we describe YM-1, a derivative of MKT-077. We found that YM-1 was more cytotoxic and localized differently than MKT-077. YM-1 demonstrated this cytotoxicity across multiple cancer cell lines. This toxicity was limited to cancer cell lines; immortalized cell models were unaffected. Brief applications of YM-1 were found to be non-toxic. Brief treatment with YM-1 restored tamoxifen sensitivity to a refractory tamoxifen-resistant MCF7 cell model. This effect is potentially due to altered estrogen receptor alpha phosphorylation, an outcome precipitated by selective reductions in Akt levels (Akt/PKB). Thus, modifications to the rhodocyanine scaffold could potentially be made to improve efficacy and pharmacokinetic properties. Moreover, the impact on tamoxifen sensitivity could be a new utility for this compound family.