游离和脂质体阿霉素治疗腹腔内结肠肿瘤:治疗和药理学研究。

E Mayhew, M Cimino, J Klemperer, R Lazo, J Wiernikowski, S Arbuck
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引用次数: 16

摘要

腹腔内化疗(i.p.)正在被研究作为手术的辅助手段,以杀死残留的癌细胞,抑制癌细胞的播散,局部复发和卵巢癌、胃癌和结肠癌的转移。本文比较了阿霉素(Dox)和脂质体包裹的阿霉素(Dox- lip)对小鼠结肠26 (C26)肿瘤的治疗效果。在非荷瘤动物中,经腹腔注射后发现Dox- lip的毒性低于Dox。在肿瘤细胞接种后第1天,I.P. Dox和Dox- lip可显著抑制C26肿瘤的生长,但两种给药方式对已建立的肿瘤(8天)无效。多次给药并没有改善治疗反应。Dox- lip在等剂量或近似等毒性剂量下的治疗效果并不优于Dox。此外,我们还研究了Dox和Dox- lip在腹腔内的相对滞留和血浆药代动力学。结果发现,口服Dox- lip后,腹腔内Dox水平维持时间较长。然而,结果表明,维持腹腔内药物水平升高并不一定会增加治疗效果。
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Free and liposomal doxorubicin treatment of intraperitoneal colon 26 tumor: therapeutic and pharmacologic studies.

Intraperitoneal (i.p.) chemotherapy is being investigated as an adjunct to surgery to kill residual cancer cells, inhibit cancer cell seeding, local recurrence, and metastases for ovarian, gastric, and colon cancers. In this report, the therapeutic effects of Doxorubicin (Dox) and liposome-entrapped Dox (Dox-Lip) against i.p. mouse colon 26 (C26) tumor were compared. It was found that Dox-Lip was less toxic than Dox after i.p. administration in non-tumor bearing animals. I.P. Dox and Dox-Lip significantly inhibited the growth of C26 tumor when the treatment was initiated 1 day after tumor cell inoculation, but both administration forms were ineffective against well-established (8-day) tumors. Multiple dose schedules did not improve the therapeutic response. Dox-Lip was not therapeutically superior to Dox at equal doses or at approximately equi-toxic doses. In addition, the relative retention of Dox and Dox-Lip in the peritoneal cavity and their plasma pharmacokinetics were investigated. It was found that Dox levels in the peritoneal cavity were maintained for longer periods after i.p. Dox-Lip was administered. However, the results show that maintenance of elevated drug levels in the peritoneal cavity does not necessarily lead to increased therapeutic effects.

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