3,3′-亚胺比斯-1-丙醇二甲磺酸酯盐酸盐(IPD)可能致癌性的生物测定。

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引用次数: 0

摘要

通过对Sprague-Dawley大鼠和B6C3F1小鼠腹腔注射3,3′-亚胺比斯-1-丙醇二甲基磺酸酯盐酸盐[IPD]进行生物测定,以确定其致癌性。IPD每周注射三次,每组35只动物,大鼠的剂量为12、24或48 mg/kg,小鼠的剂量为20或40 mg/kg。大鼠按12 mg/kg剂量给药52周。由于该化学物质的毒性,接受24 mg/kg IPD的组在第34周停止给药。剂量为48 mg/kg的大鼠在第23周(雄性)和第27周(雌性)均死亡。两组小鼠均治疗52周。所有幸存者都是在行政管理结束后被杀害的,这一时期因群体而异。对于大鼠,未处理组和车辆对照组,每组10只雄性和10只雌性,从高剂量组和中剂量组开始,另外相同大小的未处理组和车辆对照组从低剂量组开始。对于小鼠,未治疗组和车辆对照组各有15只雄性和15只雌性。IPD的毒性与大鼠和小鼠较低的平均体重和较低的存活率有关。寿命的缩短,尤其是老鼠的寿命缩短,降低了患肿瘤的可能性。在大鼠中,在大多数处理过的大鼠尸检中观察到腹膜炎和纤维粘连,可能是由试验化学物质直接刺激引起的。腹膜肉瘤、纤维瘤或纤维肉瘤发生在两只低剂量雄性大鼠、一只中等剂量雄性大鼠和一只中等剂量雌性大鼠中,但没有发生在任何对照动物中。由于这种低发病率,并且由于试验化学物质的刺激参与了发病机制,这些肿瘤可能是由于化学物质的局部作用。在小鼠中,观察到的淋巴瘤发生率如下(雄性:对照组0/14,低剂量0/26,高剂量3/21;女性:对照组1/15,低剂量2/29,高剂量6/27)。无淋巴瘤生存概率的生命表分析的Tarone试验表明,淋巴瘤的显著正剂量相关增加,雄性小鼠的概率水平为0.011,雌性小鼠为0.003。小鼠鳞状细胞癌(低剂量雄性6/26,高剂量雌性2/27)。其中7例肿瘤位于靠近注射部位的腹股沟区皮下组织。虽然没有统计学意义,但这种肿瘤可能与IPD的使用有关。大鼠腹膜的肿瘤和小鼠皮下组织的肿瘤可能是由于与施用试验化学品有关的局部效应。小鼠的淋巴瘤,虽然轻微显著,但数量太少,不能明确地与剂量有关。这项研究的结论受到早期死亡和毒性的限制,但大鼠和小鼠注射部位附近腹膜肿瘤的出现表明IPD的致癌潜力。
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Bioassay of 3,3'-iminobis-1-propanol dimethanesulfonate (ester) hydrochloride (IPD) for possible carcinogenicity.

A bioassay of 3,3'-iminobis-1-propanol dimethanesulfonate (ester) hydrochloride [IPD] for possible carcinogenicity was conducted by administering the test chemical intraperitoneally to Sprague-Dawley rats and B6C3F1 mice. The IPD was injected three times per week to groups of 35 animals, using doses of 12, 24, or 48 mg/kg for the rats, and 20 or 40 mg/kg for the mice. Rats at 12 mg/kg were treated for 52 weeks. Because of the toxicity of the chemical, administration of IPD for the group receiving 24 mg/kg was discontinued at week 34. Rats receiving 48 mg/kg were treated until all had died at week 23 (males) and week 27 (females). Both groups of mice were treated for 52 weeks. All survivors were killed after post-administration periods that varied among groups. With rats, untreated and vehicle-control groups, each consisting of 10 males and 10 females, were started with the high- and mid-dose groups and additional untreated and vehicle-control groups of the same size were started with the low-dose groups. With mice, untreated and vehicle-control groups each consisted of 15 males and 15 females. The toxicity of IPD was associated with lower mean body weights and lower rates of survival of both the rats and mice. The shortened life spans, particularly in the rats, reduced the likelihood of the development of tumors. In rats, peritonitis and fibrous adhesions, possibly, from direct irritation by the test chemical were observed in most treated rats at necropsy. Sarcoma, fibroma, or fibrosarcoma of the peritoneum occurred in two low-dose male, one mid-dose male, and one mid-dose female rats, but not in any control animals. Because of this low incidence, and because irritation by the test chemical have been involved in the pathogenesis, these tumors may have been due to local effects of the chemical. In mice, lymphomas were observed at the following incidences (males: controls 0/14, low-dose 0/26, high-dose 3/21; females: controls 1/15, low-dose 2/29, high-dose, 6/27). The Tarone test for life-table analysis of the probability of survival without lymphoma indicated a significant positive dose-related increase of lymphomas with a probability level of 0.011 for male mice and 0.003 for female mice. Squamous-cell carcinoma was noted in the mice (low-dose males 6/26, high-dose females 2/27). Seven of these tumors were observed in subcutaneous tissue in the inguinal region near the sites of injection. Although not statistically significant, this tumor may be associated with administration of IPD. Tumors of the peritoneum in rats and tumors in the subcutaneous tissue in mice may have been due to local effects related to administration of the test chemical. The lymphomas in mice, although marginally significant, were too few in number to clearly be related to dosing. Conclusions from this study are limited by early deaths and toxicity, but the appearance of tumors in the peritoneum near the injection sites in both rats and mice indicate the carcinogenic potential of IPD.

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