Poly( γ, l-glutamic acid)–cisplatin conjugate effectively inhibits human breast tumor xenografted in nude mice

Poly( γ, l-glutamic acid)–cisplatin conjugate effectively inhibits human breast tumor xenografted in nude mice

An easily administered cis-dichlorodiammineplatinum (II) (CDDP) formulation with less toxicity and greater antitumor effect would be extremely valuable. We describe PGA–CDDP, a water-soluble CDDP derivative. The hydrolyzed γ-PGA has a molecular weight between 45 and 60 kDa, and is a water-soluble, b...

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Veröffentlicht in:Biomaterials 2006-12, Vol.27 (35), p.5958-5965
Hauptverfasser: Ye, Haifeng, Jin, Li, Hu, Rongzhang, Yi, Zhengfang, Li, Jing, Wu, Yelin, Xi, Xuguang, Wu, Zirong
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Sprache:eng
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Animals
Antineoplastic Agents - pharmacology
Antitumor efficacy
Breast Neoplasms - pathology
Cis-dichlorodiammineplatinum(II)
Cisplatin - chemistry
Drug carriers
Humans
Mice
Mice, Nude
Neoplasm Transplantation
Poly( γ-glutamic acid)
Polyglutamic Acid - chemistry
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container_end_page 5965
container_issue 35
container_start_page 5958
container_title Biomaterials
container_volume 27
creator Ye, Haifeng
Jin, Li
Hu, Rongzhang
Yi, Zhengfang
Li, Jing
Wu, Yelin
Xi, Xuguang
Wu, Zirong
description An easily administered cis-dichlorodiammineplatinum (II) (CDDP) formulation with less toxicity and greater antitumor effect would be extremely valuable. We describe PGA–CDDP, a water-soluble CDDP derivative. The hydrolyzed γ-PGA has a molecular weight between 45 and 60 kDa, and is a water-soluble, biodegradable, and nontoxic polymer produced by microbial fermentation. CDDP can be released from the resulting conjugate in PBS: there was initially a burst release during the first 6 h, followed by sustained release. In vitro, PGA–CDDP was less potent than free CDDP at inhibiting cell growth in the Bcap-37 cell line. PGA–CDDP was given as 3 doses at an equivalent CDDP dose of 4 or 12 mg/kg with 2-day intervals between injections to Bcap-37-grafted mice. This treatment showed stronger antitumor activity and was less toxic than CDDP in vivo. Antitumor activity assays demonstrated that the PGA–CDDP conjugate treatment had significantly higher antitumor activity than control PBS treatment ( P < 0.01 ). PGA–CDDP also increased the survival of mice bearing Bcap-37 cells with reference to PBS treatment or free CDDP treatment. Furthermore, mice treated with PGA–CDDP (4 mg/kg, administered on day 0 and 5) showed no body weight loss ( P > 0.05 with respect to PBS treatment), whereas free CDDP treatment at the same dose caused a body weight loss of 20–30% ( P < 0.001 ). These findings suggest that PGA produced by microbial fermentation may be used as an effective drug carrier for CDDP and that PGA–CDDP may have potential applications in the treatment of human breast cancer.
doi_str_mv 10.1016/j.biomaterials.2006.08.016
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Furthermore, mice treated with PGA–CDDP (4 mg/kg, administered on day 0 and 5) showed no body weight loss ( P &gt; 0.05 with respect to PBS treatment), whereas free CDDP treatment at the same dose caused a body weight loss of 20–30% ( P &lt; 0.001 ). 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subjects Animals
Antineoplastic Agents - pharmacology
Antitumor efficacy
Breast Neoplasms - pathology
Cis-dichlorodiammineplatinum(II)
Cisplatin - chemistry
Drug carriers
Humans
Mice
Mice, Nude
Neoplasm Transplantation
Poly( γ-glutamic acid)
Polyglutamic Acid - chemistry
title Poly( γ, l-glutamic acid)–cisplatin conjugate effectively inhibits human breast tumor xenografted in nude mice
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