Clinical Cancer Research

2005

DOI: 10.1158/1078-0432.ccr-04-1756

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MEN4901/T-0128, a New Camptothecin Derivative–Carboxymethyldextran Conjugate, Has Potent Antitumor Activities in a Panel of Human Tumor Xenografts in Nude Mice

Francisco Eiichi Fujita

¹

,

²

,

Masahide Fujita

³

et al.

Abstract: Purpose: The purpose of the present study was to evaluate the antitumor activity and pharmacokinetic profile of MEN4901/T-0128 in nude mice bearing human tumor xenografts in comparison with irinotecan (CPT-11) and T-2513. Experimental Design: We have determined the antitumor activity of MEN4901/T-0128, CPT-11, and T-2513 in BALB/cA Jcl nude mice bearing human gastric (H-81), colon (H-110), lung (Mqnu-1, H-74), esophageal (H-204), liver (H-181), and pancreatic (H-48) cancer lines, which had been … Show more

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Macromolecular Architectures For Passive Drug Delivery1

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Cited by 12 publications

(11 citation statements)

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“…In contrast, a single treatment of MEN4901/T-0128 had less effective antitumor activity unless a higher dose was used, indicating repeated treatment regimens were superior to single bolus drug administration. Furthermore, all MEN4901/T-0128 treated animals had tumor regression efficacy against the primary human colon tumor, which was consistent with antitumor activity in human tumor subcutaneous xenografts (9). …”

Section: Discussionsupporting

confidence: 73%

“…T-0128 has demonstrated a strong antitumor activity against a panel of human tumor subcutaneously implanted in nude mice that were mostly refractory to CPT-11, T-2513, and topotecan (9). These studies could not evaluate antimetastatic efficacy, since they involved subcutaneously-growing tumors which do not metastasize.…”

Section: Discussionmentioning

confidence: 99%

“…The evaluation of the in vivo antitumor activity of MEN4901/T-0128 against a panel of human tumors implanted subcutaneously in nude mice has demonstrated enhanced antitumor activity and a broad range of therapeutic doses. Pharmacokinetic analysis showed that MEN4901/T-0128 had an extended plasma half-life with sustained tumor levels, which may explain the superior activity of MEN4901/T-0128 in vivo (9). However, these subcutaneous-transplant models generally do not metastasize and could not evaluate the anti-metastatic activity of MEN4901/T0128.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

High Antimetastatic Efficacy of MEN4901/T-0128, a Novel Camptothecin Carboxymethyldextran Conjugate

¹

,

²

,

³

et al. 2011

Journal of Surgical Research

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The antimetastatic activity of a novel camptothecan conjugate. MEN4901/T-0128, in which 7-ethyl-10-aminopropyloxy-camptothecin (T-2513) is bound to a biodegradable carboxymethyldextran via a Gly-Gly-Gly linker, was observed in this study. High antimetastatic activity of MEN4901/T-0128 was demonstrated in a clinically-relevant orthotopic mouse model of human colon cancer. MEN4901/T-0128 and irinotecan were compared for anti-metastatic activity as well as efficacy against the primary tumor. An imageable, metastatic model was made by surgical orthotopic implantation (SOI) of the green fluorescent protein (GFP)-expressing HT-29 tumor in nude mice. MEN4901/T-0128 and irinotecan were administered intravenously at various doses and schedules. MEN4901/T-0128, with treatment beginning on day 49 after SOI, was highly effective on lymph node metastasis as well as against the primary tumor. Both GFP imaging and histology demonstrated a markedly lower metastatic incidence of lymph nodes in all MEN4901/ T-0128 treated mice compared to irinotecan-treated and untreated mice. At the most efficacious dose of MEN4901/T-0128, only 1 of 12 animals had lymph node metastasis compared to 19 of 24 in the control group. The present study demonstrates the principle that when a camptothecan is conjugated to an appropriate polymer, the drug can become extremely effective with important clinical potential for antimetastatic therapy, a most urgent need.

“…In contrast, a single treatment of MEN4901/T-0128 had less effective antitumor activity unless a higher dose was used, indicating repeated treatment regimens were superior to single bolus drug administration. Furthermore, all MEN4901/T-0128 treated animals had tumor regression efficacy against the primary human colon tumor, which was consistent with antitumor activity in human tumor subcutaneous xenografts (9). …”

Section: Discussionsupporting

confidence: 73%

“…T-0128 has demonstrated a strong antitumor activity against a panel of human tumor subcutaneously implanted in nude mice that were mostly refractory to CPT-11, T-2513, and topotecan (9). These studies could not evaluate antimetastatic efficacy, since they involved subcutaneously-growing tumors which do not metastasize.…”

Section: Discussionmentioning

confidence: 99%

“…The evaluation of the in vivo antitumor activity of MEN4901/T-0128 against a panel of human tumors implanted subcutaneously in nude mice has demonstrated enhanced antitumor activity and a broad range of therapeutic doses. Pharmacokinetic analysis showed that MEN4901/T-0128 had an extended plasma half-life with sustained tumor levels, which may explain the superior activity of MEN4901/T-0128 in vivo (9). However, these subcutaneous-transplant models generally do not metastasize and could not evaluate the anti-metastatic activity of MEN4901/T0128.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

High Antimetastatic Efficacy of MEN4901/T-0128, a Novel Camptothecin Carboxymethyldextran Conjugate

¹

,

²

,

³

et al. 2011

Journal of Surgical Research

Self Cite

View full text Add to dashboard Cite

The antimetastatic activity of a novel camptothecan conjugate. MEN4901/T-0128, in which 7-ethyl-10-aminopropyloxy-camptothecin (T-2513) is bound to a biodegradable carboxymethyldextran via a Gly-Gly-Gly linker, was observed in this study. High antimetastatic activity of MEN4901/T-0128 was demonstrated in a clinically-relevant orthotopic mouse model of human colon cancer. MEN4901/T-0128 and irinotecan were compared for anti-metastatic activity as well as efficacy against the primary tumor. An imageable, metastatic model was made by surgical orthotopic implantation (SOI) of the green fluorescent protein (GFP)-expressing HT-29 tumor in nude mice. MEN4901/T-0128 and irinotecan were administered intravenously at various doses and schedules. MEN4901/T-0128, with treatment beginning on day 49 after SOI, was highly effective on lymph node metastasis as well as against the primary tumor. Both GFP imaging and histology demonstrated a markedly lower metastatic incidence of lymph nodes in all MEN4901/ T-0128 treated mice compared to irinotecan-treated and untreated mice. At the most efficacious dose of MEN4901/T-0128, only 1 of 12 animals had lymph node metastasis compared to 19 of 24 in the control group. The present study demonstrates the principle that when a camptothecan is conjugated to an appropriate polymer, the drug can become extremely effective with important clinical potential for antimetastatic therapy, a most urgent need.

“…A subsequent study in mice bearing human tumor xenografts found significant tumor inhibition at one third the MTD of 80 mg/kg once a week for four weeks (H81 gastric, 97.5%; H-110 colon, 98.5%; Mqnu-1 lung, 99.7%; H-74 lung, 90.7%; H-204 esophageal, 78.8%; H-181 liver, 81.2%; H48 pancreatic, 98.8%). 292 Pharmacokinetic evaluation of polymer bound SN-38 in nude mice bearing St-4 xenografts found plasma AUC values of 23,900 μg•h/mL and a 30 h half-life after a 40 mg/kg i.v. injection.…”

Section: Macromolecular Architectures For Passive Drug Deliverymentioning

confidence: 99%

Cancer Therapies Utilizing the Camptothecins: A Review of the in Vivo Literature

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²

2010

Mol. Pharmaceutics

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This review summarizes the in vivo assessment--preliminary, preclinical, and clinical--of chemotherapeutics derived from camptothecin or a derivative. Camptothecin is a naturally occurring, pentacyclic quinoline alkaloid that possesses high cytotoxic activity in a variety of cell lines. Major limitations of the drug, including poor solubility and inactivity at physiological conditions, prevent full clinical utilization. Camptothecin remains at equilibrium in an active lactone form and inactive hydrolyzed carboxylate form. The active lactone binds to DNA topoisomerase I cleavage complex, believed to be the single site of activity inhibiting DNA religation, resulting in apoptosis. A series of small molecule camptothecin derivatives have been developed that increase solubility, lactone stability and bioavailability to varying levels of success. A number of macromolecular agents have also been described wherein camptothecin(s) are covalently appended or non-covalently associated with the goal of improving solubility and lactone stability, while taking advantage of the tumor physiology to deliver larger doses of drug to the tumor with lower systemic toxicity. With the increasing interest in drug delivery and polymer therapeutics, additional constructs are anticipated. The goal of this review is to summarize the relevant literature for others interested in the field of camptothecin-based therapeutics, specifically in the context of biodistribution, dosing regimens, and pharmacokinetics with the desire of providing a useful source of comparative data. To this end, only constructs where in vivo data is available are reported. The review includes published reports in English through mid-2009.

“…On the contrary, the treatment with irinotecan and T-2513 was pharmacologically ineffective. The therapeutic treatment with the conjugate did not induce either animal death or weight loss indicating the high therapeutic index with respect to the parent drug [128].…”

Section: Camptothecinmentioning

confidence: 93%

Polysaccharide-Based Anticancer Prodrugs

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³

2009

Macromolecular Anticancer Therapeutics

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So far, polysaccharides have been widely used in pharmaceutical technology as first choice excipients for production of traditional formulations. Nevertheless, in the recent years these natural and semisynthetic macromolecules have been addressed for new challenging applications as functional materials for innovative formulations. Their peculiar physicochemical and biological properties have been exploited to develop macromolecular prodrugs which can exhibit favorable biopharmaceutical properties and enforce the therapeutic performance of the parent drugs. These polymers display, in fact, high biocompatibility and biodegradability, multiple insertion points, and biological properties that can be advantageously exploited in drug delivery. In particular, the multifunctional structures of these polymers are anchoring points for conjugation of several anticancer drugs, which usually suffer from poor physicochemical, biopharmaceutical, and therapeutic properties that limit their therapeutic performance and proper use in anticancer treatment. Polysaccharide-based anticancer prodrugs can be designed to endow derivatives with new bioresponse, targeting, or environmental triggering properties or to combine molecules with synergistic therapeutic effect. Over the years, a variety of synthetic protocols have been set up to conjugate anticancer drugs to the polysaccharide backbone via specific linkages or through spacers which convey to the conjugates selective drug-delivery properties. Furthermore, the intrinsic antitumor activity and cell-targeting properties of few polysaccharides represent an additional value to the final therapeutic systems. Anticancer drugs with different pharmacodynamic, pharmacokinetic, and physicochemical properties have been successfully conjugated to various natural and semisynthetic polysaccharides highlighting the interesting perspectives for exploitation of new promising anticancer polymer therapeutics.

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