Pharmacodynamics of the G-Quadruplex-Stabilizing Telomerase Inhibitor 3,11-Difluoro-6,8,13-trimethyl-8H-quino[4,3,2-kl]acridinium methosulfate (RHPS4) in Vitro: Activity in Human Tumor Cells Correlates with Telomere Length and Can Be Enhanced, or Antagonized, with Cytotoxic Agents

doi:10.1124/mol.105.013300

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First published on September 8, 2005; DOI: 10.1124/mol.105.013300

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Mol Pharmacol 68:1551-1558, 2005

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Pharmacodynamics of the G-Quadruplex-Stabilizing Telomerase Inhibitor 3,11-Difluoro-6,8,13-trimethyl-8H-quino[4,3,2-kl]acridinium methosulfate (RHPS4) in Vitro: Activity in Human Tumor Cells Correlates with Telomere Length and Can Be Enhanced, or Antagonized, with Cytotoxic Agents

Jennifer C. Cookson, Fangping Dai, Victoria Smith, Robert A. Heald, Charles A. Laughton, Malcolm F. G. Stevens, and Angelika M. Burger¹

Centre for Biomolecular Sciences, School of Pharmacy, University of Nottingham, Nottingham, United Kingdom (J.C.C., R.A.H., C.A.L., M.F.G.S); and Institute for Experimental Oncology, Freiburg, Germany (F.D., V.S., A.M.B)

Telomeric integrity is required to maintain the replicativeability of cancer cells and is a target for the G-quadruplex–stabilizingdrug 3,11-difluoro-6,8,13-trimethyl-8H-quino[4,3,2-kl]acridiniummethosulfate (RHPS4). We report a senescent-like growth arrestin MCF-7 breast cancer cells, within 14 to 17 days, and a reductionin telomere length (from 5.2 kilobases (kb) to 4.7 and 4.3 kbafter 17 days of treatment at 0.5 and 1 µM, respectively).These effects occurred at noncytotoxic drug concentrations (doses< 1 µM over a 14-day exposure) compatible with long-termdrug dosing. The telomere length of cancer cells influencestheir sensitivity to growth inhibition by RHPS4: mutant (mt)human telomerase reverse transcriptase (hTERT)-expressing MCF-7cells [short telomere restriction fragment (TRF) length, 1.9kb; IC₅₀, 0.2 µM] were 10 times more sensitive to RHPS4compared with wild-type (wt) hTERT-expressing, vector-transfectedcontrol cells (longer TRF-length 5.2 kb; IC₅₀ 2 µM) inthe 5 day SRB assay. This relationship was corroborated in apanel of 36 human tumor xenografts grown in vitro showing apositive correlation between telomere length and growth inhibitorypotency of RHPS4 (15-day clonogenic assay, r = 0.75). Theseobservations are consistent with loss of the protective cappingstatus of telomeres mediated by RHPS4 G-quadruplex-stabilization,thus leading to greater susceptibility of cells with shortertelomeres. In combination studies, paclitaxel (Taxol), doxorubicin(Adriamycin), and the experimental therapeutic agent 17-(allylamino)-17-demethoxygeldanamycin,which inhibits the 90-kDa heat shock protein, conferred enhancedsensitivity in RHPS4 treated MCF-7 cells, whereas the DNA-interactivetemozolomide and cisplatin antagonized the action of RHPS4.Our results support the combined use of certain classes of cytotoxicanticancer agents with RHPS4 to enhance potential clinical benefit.

Received March 30, 2005; accepted September 7, 2005

Address correspondence to: Malcolm F. G. Stevens, Centre for Biomolecular Sciences, School of Pharmacy, University of Nottingham, Nottingham NG7 2RD, United Kingdom. E-mail: malcolm.stevens{at}nottingham.ac.uk

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