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合成视黄酸芬维A胺用于人类癌症化学预防的前景

Prospects of chemoprevention of human cancers with the synthetic retinoid fenretinide.

作者信息

Costa A, Formelli F, Chiesa F, Decensi A, De Palo G, Veronesi U

机构信息

Istituto Nazinale Tumori, Milan, Italy.

出版信息

Cancer Res. 1994 Apr 1;54(7 Suppl):2032s-2037s.

PMID:8137334
Abstract

Fenretinide or N-(4-hydroxyphenyl)retinamide is a vitamin A analogue synthesized in the United States in the late 1960s. This retinoid shows a preferential accumulation in breast instead of liver, is effective in the inhibition of chemically induced mammary carcinoma in rats, and has proved to be less toxic than many other vitamin A analogues. The Milan Cancer Institute has put a particular effort in this molecule in both the experimental and clinical fields. We have demonstrated, in animals and humans, that fenretinide induces a rapid reduction of retinol plasma concentration, that its blood levels remain constant during administration for as long as 5 years, and that the drug is able to accumulate in the human breast. To date, 2969 stage I breast cancer patients have been randomized to evaluate the efficacy of this retinoid to prevent contralateral new primaries, 709 subjects have been accrued in a prevention trial of basal cell carcinoma of the head and neck, and 153 patients entered a study the preliminary results of which already show the capability of fenretinide to prevent recurrences and new localizations of oral leukoplakia. Further studies on fenretinide will be aimed at evaluating its preventive efficacy in superficial bladder and prostate cancers and at exploring possible synergism with tamoxifen and interferons in breast cancer and skin cancer, respectively.

摘要

芬维A胺或N-(4-羟基苯基)视黄酰胺是一种维生素A类似物,于20世纪60年代末在美国合成。这种类视黄醇在乳腺而非肝脏中优先蓄积,对抑制大鼠化学诱导的乳腺癌有效,且已证明其毒性低于许多其他维生素A类似物。米兰癌症研究所在该分子的实验和临床领域都付出了特别的努力。我们已经在动物和人类身上证明,芬维A胺能迅速降低血浆视黄醇浓度,在长达5年的给药过程中其血药浓度保持恒定,且该药物能够在人类乳腺中蓄积。迄今为止,2969例I期乳腺癌患者已被随机分组,以评估这种类视黄醇预防对侧新发原发性肿瘤的疗效,709名受试者已纳入头颈基底细胞癌预防试验,153例患者进入一项研究,其初步结果已显示芬维A胺预防口腔白斑复发和新发病灶的能力。对芬维A胺的进一步研究将旨在评估其对浅表膀胱癌和前列腺癌的预防疗效,并分别探索其与他莫昔芬和干扰素在乳腺癌和皮肤癌中可能的协同作用。

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