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环磷酰胺与嘧啶酮联合用于B16黑色素瘤和P388白血病的化学免疫疗法。

Chemoimmunotherapy of B 16 melanoma and P388 leukemia with cyclophosphamide and pyrimidinones.

作者信息

Li L H, Johnson M A, Moeller R B, Wallace T L

出版信息

Cancer Res. 1984 Jul;44(7):2841-7.

PMID:6722813
Abstract

Since increasing evidence indicates that combination modality of cancer treatment is preferable, and a series of 5-halo-6- phenylpyrimidinones has been found to induce interferon production and to stimulate a variety of immune responses, several were tested alone or in combination with cyclophosphamide (CY) against B 16 melanoma and P388 leukemia. Thus far, 2-amino-5-bromo-6-(3-fluorophenyl)-4(3H)pyrimidinone ( ABMFPP ) and its sister compound 2-amino-5-bromo-6-(2-fluorophenyl)-4(3H)pyrimidinone ( ABOFPP ) were found to be superior to other pyrimidinones including 2-amino-5-bromo-6-(6-phenyl)-4-pyrimidinone which is currently under clinical investigation. Neither ABMFPP nor ABOFPP alone had any significant activity against P388 leukemia. However, a marked synergistic effect was observed when a single i.p. injection of CY at 24 hr after tumor inoculation (10(6) cells/mouse) was followed by multiple i.p. injections of either ABMFPP or ABOFPP . For instance, the increase of life span was about 180% when animals received both CY (150 mg/kg) and ABMFPP (125 mg/kg/injection) as compared to 100% increased life span when animals received CY alone, and 0% increased life span when animals received ABMFPP alone. Also, 80% of the animals were long-term survivors (greater than 30 days) when animals received the combination therapy as compared to 20% survivors when animals received CY alone. The synergistic effect exhibited by ABMFPP or ABOFPP correlated positively to the initial reduction of tumor burden by CY. The optimal gap between CY and pyrimidinone administration was one day. The best therapeutic response was observed when pyrimidinone was given every 4 days for a total of 7 injections; however, other schedules and dosing frequencies also gave significant responses. The synergistic effect was also observed with B 16 melanoma when animals received the combination therapy. The significance of these findings, in terms of theoretical consideration as well as drug development, is discussed.

摘要

由于越来越多的证据表明癌症联合治疗方式更为可取,并且已发现一系列5-卤代-6-苯基嘧啶酮可诱导干扰素产生并刺激多种免疫反应,因此对其中几种进行了单独测试,或与环磷酰胺(CY)联合用于对抗B16黑色素瘤和P388白血病。到目前为止,发现2-氨基-5-溴-6-(3-氟苯基)-4(3H)嘧啶酮(ABMFPP)及其同类化合物2-氨基-5-溴-6-(2-氟苯基)-4(3H)嘧啶酮(ABOFPP)优于其他嘧啶酮,包括目前正在进行临床研究的2-氨基-5-溴-6-(6-苯基)-4-嘧啶酮。ABMFPP和ABOFPP单独使用时对P388白血病均无明显活性。然而,在肿瘤接种(10^6个细胞/小鼠)后24小时单次腹腔注射CY,随后多次腹腔注射ABMFPP或ABOFPP时,观察到明显的协同效应。例如,与单独接受CY时寿命延长100%以及单独接受ABMFPP时寿命延长0%相比,动物同时接受CY(150mg/kg)和ABMFPP(125mg/kg/注射)时寿命延长约180%。此外,接受联合治疗的动物中有80%为长期存活者(超过30天),而单独接受CY治疗的动物中这一比例为20%。ABMFPP或ABOFPP表现出的协同效应与CY对肿瘤负荷的初始降低呈正相关。CY与嘧啶酮给药之间的最佳间隔为一天。当嘧啶酮每4天给药一次,共注射7次时观察到最佳治疗反应;然而,其他给药方案和给药频率也产生了显著反应。当动物接受联合治疗时,B16黑色素瘤也观察到了协同效应。本文讨论了这些发现从理论考虑以及药物开发角度的意义。

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