Treatment of Colorectal Cancer Using a Combination of Liposomal Irinotecan (Irinophore C™) and 5-Fluorouracil

Abstract: PurposeTo investigate the use of liposomal irinotecan (Irinophore C™) plus or minus 5-fluorouracil (5-FU) for the treatment of colorectal cancer.Experimental DesignThe effect of irinotecan (IRI) and/or 5-FU exposure times on cytotoxicity was assessed in vitro against HT-29 or LS174T human colon carcinoma cells. The pharmacokinetics and biodistribution of Irinophore C™ (IrC™) and 5-FU, administered alone or in combination, were compared in vivo. A subcutaneous model of HT-29 human colorectal cancer in Rag2-M mi… Show more

“…Hence, 40 mM lipid initial concentration appears to be an optimum between good encapsulation and excipient cost. Passive encapsulation allows to yield a 5-FU concentration of up to 3.6 mg 5-FU/mL compatible with an efficient treatment in vivo on HT-29 xenograft tumors in mice (injection of 20-40 mg 5-FU/kg) (17,32). These results are in agreement with literature, where similar encapsulation efficacy of 5-FU has been reported for DPPC liposomes (14).…”

Formulation and Pharmacokinetics of Thermosensitive Stealth® Liposomes Encapsulating 5-Fluorouracil

“…Hence, 40 mM lipid initial concentration appears to be an optimum between good encapsulation and excipient cost. Passive encapsulation allows to yield a 5-FU concentration of up to 3.6 mg 5-FU/mL compatible with an efficient treatment in vivo on HT-29 xenograft tumors in mice (injection of 20-40 mg 5-FU/kg) (17,32). These results are in agreement with literature, where similar encapsulation efficacy of 5-FU has been reported for DPPC liposomes (14).…”

Formulation and Pharmacokinetics of Thermosensitive Stealth® Liposomes Encapsulating 5-Fluorouracil

“…The data show that any therapeutic potential of the combination is compromised by an unexpected increase in toxicity [22]. The reasons for the enhanced toxicity are not well-understood although it may be due to IrC™ treatment prolonging the circulation lifetime of 5-FU [22]. The observed improvements in tumor perfusion following IrC™ treatment [20,21,23] suggest the possibility that combination treatments with IrC™ and 5-FU might be more efficacious if 5-FU was administered after IrC™ treatment in a sequential, rather than concurrent, manner.…”

“…Recognizing that IrC™, if approved for clinical use, will be used in combination with other drugs, our research team has examined the therapeutic effects when IrC™ and 5-FU are administered concurrently [22]. The data show that any therapeutic potential of the combination is compromised by an unexpected increase in toxicity [22].…”

“…The data show that any therapeutic potential of the combination is compromised by an unexpected increase in toxicity [22]. The reasons for the enhanced toxicity are not well-understood although it may be due to IrC™ treatment prolonging the circulation lifetime of 5-FU [22].…”

Irinophore C™, a lipid nanoparticulate formulation of irinotecan, improves vascular function, increases the delivery of sequentially administered 5-FU in HT-29 tumors, and controls tumor growth in patient derived xenografts of colon cancer

“…The primary method currently used to treat all stages of colon cancer is surgery. After tumor excision, chemotherapeutic drugs, such as irinotecan (CPT-11), 5-fluorouracil (5-FU), and oxaliplatin, are typically used to further eradicate any residual tumor cells [2,3] . However, in the majority of cancer patients, currently available chemotherapies have had only partial success, owing to chemoresistance and side effects [4] .…”

New benzimidazole acridine derivative induces human colon cancer cell apoptosis in vitro via the ROS-JNK signaling pathway