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亚慢性暴露于甲醛的F344大鼠鼻腔特定部位的DNA-蛋白质交联与细胞复制

DNA-protein cross-links and cell replication at specific sites in the nose of F344 rats exposed subchronically to formaldehyde.

作者信息

Casanova M, Morgan K T, Gross E A, Moss O R, Heck H A

机构信息

Chemical Industry Institute of Toxicology, Research Triangle Park, North Carolina 27709.

出版信息

Fundam Appl Toxicol. 1994 Nov;23(4):525-36. doi: 10.1006/faat.1994.1137.

Abstract

Chronic exposures to high concentrations (> or = 6 ppm) of formaldehyde (HCHO) induce cell proliferation, squamous metaplasia, and squamous cell carcinomas in F344 rats. To assess the cancer risk associated with HCHO exposure, DNA-protein cross-links (DPX) formed in a single exposure of naive (previously unexposed) rats and monkeys have been used as a surrogate for the internal dose. Since the quantity of DPX may differ in subchronically exposed animals, the effects of preexposure to HCHO on the acute DPX yield (concentration of DPX following a single exposure) and the cumulative DPX yield (concentration of DPX following repeated exposures) were determined. Male F344 rats were preexposed (PE) to 0.7, 2, 6, or 15 ppm of HCHO (6 hr/day, 5 days/week, 11 weeks + 4 days). Naive (N) rats were exposed to room air. On the 5th day of the 12th week, PE and N rats were simultaneously exposed (3 hr) to H14CHO at the same concentrations used for preexposure. Acute DPX yields and cell replication (incorporation of 14C into DNA) were determined in the mucosal lining of the nasal lateral meatus (LM) (high tumor site in HCHO bioassay) and the medial and posterior meatuses (M:PM) (low tumor site in bioassay). DPX yields in the LM were approximately sixfold higher than in the M:PM. At 0.7 and 2 ppm, no differences between PE and N rats were detected in either tissue. At 6 and 15 ppm, acute DPX yields in the LM of PE rats were approximately half those of N rats, but no differences were detected in the M:PM. Cell proliferation was induced in PE rats at 6 ppm (LM only) and especially at 15 ppm (LM and M:PM). Cumulative DPX yields were measured indirectly by determining the decrease in extractability of DNA from proteins. PE rats were preexposed to 6 or 10 ppm as above, while N rats were exposed to room air. Both groups (PE and N) were then exposed (3 hr) to the same concentration of unlabeled HCHO. DPX yields increased in a concentration-dependent manner in both groups, but the yields were smaller in PE than N rats, suggesting that no accumulation of DPX occurred in PE rats. The results demonstrate that at concentrations < or = 2 ppm, N and PE rats are equivalent with respect to the formation of DPX.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

长期暴露于高浓度(≥6 ppm)甲醛(HCHO)会在F344大鼠中诱导细胞增殖、鳞状化生和鳞状细胞癌。为评估与HCHO暴露相关的癌症风险,在初次(先前未暴露)的大鼠和猴子单次暴露后形成的DNA-蛋白质交联(DPX)已被用作内剂量的替代指标。由于亚慢性暴露动物体内的DPX数量可能不同,因此确定了预先暴露于HCHO对急性DPX产量(单次暴露后的DPX浓度)和累积DPX产量(重复暴露后的DPX浓度)的影响。雄性F344大鼠预先暴露于0.7、2、6或15 ppm的HCHO(每天6小时,每周5天,共11周+4天)。初次(N)大鼠暴露于室内空气。在第12周的第5天,预先暴露组和初次暴露组的大鼠同时暴露(3小时)于与预先暴露相同浓度的H14CHO。测定了鼻外侧道(LM)(HCHO生物测定中的高肿瘤部位)以及中道和后道(M:PM)(生物测定中的低肿瘤部位)黏膜衬里中的急性DPX产量和细胞复制(14C掺入DNA的情况)。LM中的DPX产量比M:PM中的高约六倍。在0.7和2 ppm时,预先暴露组和初次暴露组大鼠在这两个组织中均未检测到差异。在6和15 ppm时,预先暴露组大鼠LM中的急性DPX产量约为初次暴露组大鼠的一半,但在M:PM中未检测到差异。在6 ppm(仅在LM)尤其是15 ppm(在LM和M:PM)时,预先暴露组大鼠诱导了细胞增殖。通过测定DNA与蛋白质的可提取性降低间接测量累积DPX产量。预先暴露组大鼠如上述预先暴露于6或10 ppm,而初次暴露组大鼠暴露于室内空气。然后两组(预先暴露组和初次暴露组)均暴露(3小时)于相同浓度的未标记HCHO。两组中的DPX产量均以浓度依赖性方式增加,但预先暴露组大鼠的产量低于初次暴露组大鼠,这表明预先暴露组大鼠中未发生DPX的积累。结果表明,在浓度≤2 ppm时,初次暴露组和预先暴露组大鼠在DPX形成方面是等效的。(摘要截短于400字)

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