Melissa Claire Rhodes
University of Maryland, Baltimore
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Anti-Cancer Drugs | 2007
Rocio Alejandra Lopez; Amanda Beth Goodman; Melissa Claire Rhodes; Jessica Andrea Loduca Blomberg; Jonathan Heller
Terameprocol (meso-tetra-O-methyl nordihydroguaiaretic acid, formerly known as EM-1421 and M4N) is a semi-synthetic small molecule with antitumor activity occurring via selective targeting of Sp1-regulated proteins, including survivin and cdc2 that control cell cycle and apoptosis. Terameprocol is in clinical development as a site-specific transcription inhibitor in solid refractory tumors. The present studies were designed to investigate the in-vitro and in-vivo anticancer activity of terameprocol in a novel hydroxypropyl &bgr;-cyclodextrin and polyethylene glycol solvent formulation (designated CPE) designed for safe parenteral administration. Terameprocol powder was dissolved in CPE (20% hydroxypropyl &bgr;-cyclodextrin and 50% polyethylene glycol 300 or 30% hydroxypropyl &bgr;-cyclodextrin and 25% polyethylene glycol 300) or dimethyl sulfoxide and used for in-vitro cell proliferation assays, and in human carcinoma xenograft studies using female athymic nude mice injected with SW-780 human bladder cells. Terameprocol (50 and 100 mg/kg), paclitaxel (5 mg/kg), terameprocol and paclitaxel or vehicle was administered intraperitoneally daily for 21 days. Stock solutions of the CPE formulation were stable for up to 12 months. Terameprocol CPE formulation showed concentration-dependent inhibition of HeLa and C33A cell proliferation, and was less toxic than terameprocol dimethyl sulfoxide formulation. The terameprocol CPE formulation showed no overt toxicities in tumor-bearing mice. Terameprocol alone reduced the rate of tumor growth, and a combination of terameprocol/paclitaxel reduced both the rate and extent of tumor growth. These preclinical results confirm the tumoricidal activity of terameprocol formulated in a solvent suitable for parenteral administration and suggest that terameprocol has improved efficacy when coadministered with paclitaxel.
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller
Archive | 2005
Neil Frazer; Jonathan Heller; Rocio Alejandra Lopez; Melissa Claire Rhodes; Ru Chih C Huang; Richard N. Dalby; Niharika Khanna
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller; Amanda Beth Goodman
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller; Amanda Beth Goodman
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller; Amanda Beth Goodman
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller
Archive | 2006
Rocio Alejandra Lopez; Jessica Andrea Loduca Blomberg; Melissa Claire Rhodes; Jonathan D. Heller; Amanda Beth Goodman