AIM OF THE STUDY: The tumor metastases targeting ruthenium complex NAMI-A synergistically improves the activity of gemcitabine in combination therapies. High-throughput screening was used to identify other potential drug combinations from a library of FDA approved drugs. Doxorubicin was identified as a hit compound and was therefore evaluated in combination with NAMI-A in vitro and in a preclinical in vivo model. RESULTS: High-throughput screening identified eight structurally diverse compounds that synergize with NAMI-A including doxorubicin. The combination index on MCF-7 cells showed synergism as the concentration of NAMI-A increases independent of the doxorubicin concentration. In MCa mammary carcinoma of CBA mice, NAMI-A (35 mg/kg/day i.p. on days 7-12) followed by doxorubicin (10 mg/kg i.p. on day 16), significantly increased the effects of the individual drugs on metastases with 70 % animals resulting free of macroscopically detectable tumor nodules in the lungs at sacrifice. NAMI-A, unlike doxorubicin, cured 60 % of the treated mice but the combination therapy was toxic to the animals. CONCLUSIONS: The combined therapy of NAMI-A with doxorubicin synergizes on lung metastasis in a preclinical mouse model. The combination therapy at the maximum tolerated doses of the two drugs is toxic. Hence, this combination is not suitable for clinical studies using maximum tolerated doses.
AIM OF THE STUDY: The tumor metastases targeting ruthenium complex NAMI-A synergistically improves the activity of gemcitabine in combination therapies. High-throughput screening was used to identify other potential drug combinations from a library of FDA approved drugs. Doxorubicin was identified as a hit compound and was therefore evaluated in combination with NAMI-A in vitro and in a preclinical in vivo model. RESULTS: High-throughput screening identified eight structurally diverse compounds that synergize with NAMI-A including doxorubicin. The combination index on MCF-7 cells showed synergism as the concentration of NAMI-A increases independent of the doxorubicin concentration. In MCa mammary carcinoma of CBA mice, NAMI-A (35 mg/kg/day i.p. on days 7-12) followed by doxorubicin (10 mg/kg i.p. on day 16), significantly increased the effects of the individual drugs on metastases with 70 % animals resulting free of macroscopically detectable tumor nodules in the lungs at sacrifice. NAMI-A, unlike doxorubicin, cured 60 % of the treated mice but the combination therapy was toxic to the animals. CONCLUSIONS: The combined therapy of NAMI-A with doxorubicin synergizes on lung metastasis in a preclinical mouse model. The combination therapy at the maximum tolerated doses of the two drugs is toxic. Hence, this combination is not suitable for clinical studies using maximum tolerated doses.
Authors: M C Alley; D A Scudiero; A Monks; M L Hursey; M J Czerwinski; D L Fine; B J Abbott; J G Mayo; R H Shoemaker; M R Boyd Journal: Cancer Res Date: 1988-02-01 Impact factor: 12.701
Authors: M Vadori; C Florio; B Groppo; M Cocchietto; S Pacor; S Zorzet; L Candussio; G Sava Journal: J Biol Inorg Chem Date: 2015-05-16 Impact factor: 3.358
Authors: Joji Iida; Elisabeth T Bell-Loncella; Marc L Purazo; Yifeng Lu; Jesse Dorchak; Rebecca Clancy; Julianna Slavik; Mary Lou Cutler; Craig D Shriver Journal: J Transl Med Date: 2016-02-12 Impact factor: 5.531
Authors: Robert H Berndsen; Andrea Weiss; U Kulsoom Abdul; Tse J Wong; Patrick Meraldi; Arjan W Griffioen; Paul J Dyson; Patrycja Nowak-Sliwinska Journal: Sci Rep Date: 2017-02-22 Impact factor: 4.379
Authors: Yi Gou; Zhenlei Zhang; Dongyang Li; Lei Zhao; Meiling Cai; Zhewen Sun; Yongping Li; Yao Zhang; Hamid Khan; Hongbing Sun; Tao Wang; Hong Liang; Feng Yang Journal: Drug Deliv Date: 2018-11 Impact factor: 6.419