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利用鼠伤寒沙门氏菌突变株检测人尿液中的诱变活性。

Detection of mutagenic activity in human urine using mutant strains of Salmonella typhimurium.

作者信息

Minnich V, Smith M E, Thompson D, Kornfeld S

出版信息

Cancer. 1976 Sep;38(3):1253-8. doi: 10.1002/1097-0142(197609)38:3<1253::aid-cncr2820380327>3.0.co;2-6.

Abstract

Histidine-requiring mutants of Salmonella typhimurium that can be reverted to prototrophy by a variety of mutagens were used mutagenic activity in the urine of patients receiving chemotherapeutic agents. Patients given cyclophosphamide and BCNU had detectable urinary mutagenic activity over a 24-hour period, with maximal levels occurring 12 to 21 hours after drug injection. Whereas native cyclophosphamide required the presence of a rat liver extract to be mutagenic in the test system, the cyclophosphamide metabolites in the urine were fully active in the absence of added liver extract. Mutagenic activity was detected in only the first voided urine specimen of patients receiving fluorouracil. Patients receiving Adriamycin, methotrexate, Mitomycin C, and low doses or oral melphalan did not have detectable mutagenic activity in their urines. One thousand and ten random urine speciments were screened for mutagenic activity. Only eight had greater than 26 revertant colonies per plate. Four of the eight had received metronidazole (Flagyl) for vaginitis while two others had received chemotherapeutic drugs. We were unable to detect increased mutagenic metabolites in the urine of 43 patients with known malignancies, using the standard assay conditions.

摘要

利用鼠伤寒沙门氏菌的组氨酸需求型突变体,这些突变体可被多种诱变剂回复为原养型,来检测接受化疗药物治疗的患者尿液中的诱变活性。接受环磷酰胺和卡氮芥治疗的患者在24小时内可检测到尿液诱变活性,在药物注射后12至21小时出现最高水平。虽然天然环磷酰胺在测试系统中需要大鼠肝提取物的存在才具有诱变活性,但尿液中的环磷酰胺代谢物在不添加肝提取物的情况下也具有充分活性。仅在接受氟尿嘧啶治疗的患者的首次晨尿标本中检测到诱变活性。接受阿霉素、甲氨蝶呤、丝裂霉素C以及低剂量或口服美法仑治疗的患者尿液中未检测到诱变活性。对1010份随机尿液标本进行了诱变活性筛查。每平板只有8份标本有超过26个回复菌落。这8份标本中有4份因阴道炎接受了甲硝唑(灭滴灵)治疗,另外2份接受了化疗药物治疗。在标准检测条件下,我们未能在43名已知患有恶性肿瘤的患者尿液中检测到诱变代谢物增加。

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