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奥替普拉单独及联合4-羟基苯维甲酸和二氟甲基鸟氨酸对OH-BBN诱导的小鼠膀胱癌的化学预防作用

Chemoprevention of OH-BBN-induced bladder cancer in mice by oltipraz, alone and in combination with 4-HPR and DFMO.

作者信息

Moon R C, Kelloff G J, Detrisac C J, Steele V E, Thomas C F, Sigman C C

机构信息

IIT Research Institute, Chicago, IL 60616.

出版信息

Anticancer Res. 1994 Jan-Feb;14(1A):5-11.

PMID:8166455
Abstract

The chemopreventive efficacy of the schistosomicidal drug oltipraz (5-(2-pyrazinyl)-4-methyl-1,2-dithiol-3-thione) was evaluated against urinary bladder transitional cell carcinoma (TCC) induced in male C57BL/6 x DBA/2FI (BDF) mice by N-butyl-N(4-hydroxybutyl)nitrosamine (OH-BBN). Oltipraz was fed in the diet from one week prior to OH-BBN dosing until sacrifice, six months later. The agent at 250 mg/kg diet significantly reduced the incidence of TCC compared with that in carcinogen controls. Oltipraz also significantly reduced TCC incidence when fed at 500 mg/kg diet for 76 days, then at 125 mg/kg diet until the end of the test period. Treatment with this higher dose level of oltipraz also appeared to decreases the depth of tumor invasion. At lower dose levels of 100 and 200 mg/kg diet, oltipraz alone had no effect on tumor incidence. It also was tested at these dose levels in combinations with 2-difluoromethylornithine (DFMO) and with all-trans-N-(4-hydroxyphenyl)retinamide (4-HPR). Treatment with the combination of 640 mg DFMO/kg and 100 mg oltipraz/kg diet was efficacious, although DFMO alone at 640 mg/kg diet was inactive. The combination of 1280 mg DFMO/kg and 200 mg oltipraz/kg diet reduced TCC incidence significantly compared with carcinogen controls, but the effect was no greater than that of DFMO alone at 1280 mg/kg, and weight gain was suppressed compared with carcinogen controls. The depth of tumor invasion was decreased with this combination treatment. Combinations of oltipraz at 100 and 200 mg/kg diet, 4-HPR at 156 and 313 mg/kg diet, and DFMO at 640 and 1280 mg/kg diet were efficacious and without apparent toxicity. Nonetheless, the three agent combinations cannot be considered more effective than DFMO alone at 1280 mg/kg diet or the lower dose combination of oltipraz and DFMO.

摘要

对用N-丁基-N(4-羟丁基)亚硝胺(OH-BBN)诱导雄性C57BL/6xDBA/2FI(BDF)小鼠发生的膀胱移行细胞癌(TCC),评估了杀血吸虫药物奥替普拉(5-(2-吡嗪基)-4-甲基-1,2-二硫醇-3-硫酮)的化学预防效果。在给予OH-BBN前一周开始直至6个月后处死,在饮食中添加奥替普拉。与致癌物对照组相比,饮食中含250mg/kg奥替普拉可显著降低TCC的发生率。当饮食中含500mg/kg奥替普拉喂养76天,然后含125mg/kg奥替普拉直至试验期结束时,奥替普拉也显著降低了TCC的发生率。用这种较高剂量水平的奥替普拉治疗似乎也降低了肿瘤浸润深度。在饮食中含100和200mg/kg较低剂量水平时,单独使用奥替普拉对肿瘤发生率没有影响。还在这些剂量水平下将其与2-二氟甲基鸟氨酸(DFMO)以及全反式-N-(4-羟苯基)视黄酰胺(4-HPR)联合进行了试验。用640mg DFMO/kg与100mg奥替普拉/kg饮食联合治疗是有效的,尽管单独使用640mg/kg饮食的DFMO没有活性。与致癌物对照组相比,1280mg DFMO/kg与200mg奥替普拉/kg饮食联合可显著降低TCC发生率,但效果不大于单独使用1280mg/kg的DFMO,并且与致癌物对照组相比体重增加受到抑制。这种联合治疗降低了肿瘤浸润深度。饮食中含100和200mg/kg的奥替普拉、156和313mg/kg的4-HPR以及640和1280mg/kg的DFMO联合是有效的且无明显毒性。尽管如此,三种药物联合不能被认为比单独使用1280mg/kg饮食的DFMO或奥替普拉与DFMO的低剂量联合更有效。

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