Inhibition of chemically-induced neoplastic transformation by a novel tetrasodium diphosphate astaxanthin derivative

被引:32
作者
Hix, LM
Frey, DA
McLaws, MD
Osterlie, M
Lockwood, SF
Bertram, JS
机构
[1] Univ Hawaii Manoa, Dept Cell & Mol Biol, Honolulu, HI 96822 USA
[2] Hawaii Biotech Inc, Aiea, HI 96701 USA
[3] Albany Mol Res Inc, Chem Dev & Analyt Qual Serv, Albany, NY 12212 USA
[4] HIST, Dept Food Sci, N-7004 Trondheim, Norway
[5] Univ Hawaii Manoa, Canc Res Ctr Hawaii, Honolulu, HI 96813 USA
关键词
D O I
10.1093/carcin/bgi121
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Carotenoids have been implicated in numerous epidemiological studies as being protective against cancer at many sites, and their chemopreventive properties have been confirmed in laboratory studies. Astaxanthin (AST), primarily a carotenoid of marine origin, responsible for the pink coloration of salmon, shrimp and lobster, has received relatively little attention. As with other carotenoids, its highly lipophilic properties complicate delivery to model systems. To overcome this issue we have synthesized a novel tetrasodium diphosphate astaxanthin (pAST) derivative with aqueous dispersibility of 25.21 mg/ml. pAST was delivered to C3H/10T1/2 cells in an aqueous/ethanol solution and compared with non-esterified AST dissolved in tetrahydrofuran. We show pAST to (i) upregulate connexin 43 (Cx43) protein expression; (ii) increase the formation of Cx43 immunoreactive plaques; (iii) upregulate gap junctional intercellular communication (GJIC); and (iv) cause 100% inhibition of methylcholanthrene-induced neoplastic transformation at 10(-6) M. In all these assays, pAST was superior to non-esterified AST itself; in fact, pAST exceeded the potency of all other previously tested carotenoids in this model system. Cleavage of pAST to non-esterified (free) AST and uptake into cells was also verified by HPLC; however, levels of free AST were similar to 100-fold lower than in cells treated with AST itself, suggesting that pAST possesses intrinsic activity. The dual properties of water dispersibility (enabling parenteral administration in vivo) and increased potency should prove extremely useful in the future development of cancer chemopreventive agents.
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页码:1634 / 1641
页数:8
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