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新生大鼠接受γ射线和二乙基亚硝胺单独及联合处理对诱导肝细胞灶性改变和肝肿瘤的影响。

Effects of separate and combined treatments with gamma radiation and diethylnitrosamine in neonatal rats on the induction of altered hepatocyte foci and hepatic tumors.

作者信息

Peraino C, Grdina D J, Staffeldt E F, Russell J J, Prapuolenis A, Carnes B A

出版信息

Carcinogenesis. 1987 Apr;8(4):599-600. doi: 10.1093/carcin/8.4.599.

Abstract

To characterize the effects of combined treatments with gamma radiation and diethylnitrosamine (DEN) on the induction of histochemically detectable altered hepatocyte foci and hepatic tumors, we assessed the yields of these lesions in the livers of 150-day-old rats that had been treated neonatally with a single dose of gamma radiation (75 rad, whole body) and i.p.-injected DEN (0.15 mumol/g body wt), either separately or in combination. The combined treatments involved the administration of the two stimuli in both possible sequences, with the interval between treatments set at 1 h. The focus population was examined for two histochemical markers (elevated gamma-glutamyl transpeptidase [GGT(+)] and iron exclusion [FE(-)], giving rise to three detectable focus phenotypes, i.e. GGT(+) foci, FE(-) foci, and GGT(+), FE(-) foci. Frequencies of the three phenotypes were quantitated through the use of serial frozen sectioning techniques and computer-assisted image analysis. GGT(+) focus induction was synergistically enhanced by the combined treatment irrespective of the order in which the two stimuli were administered; the remaining two phenotypes did not show such enhancement. The magnitude of the GGT(+) focus response was significantly greater when the treatment sequence was gamma----DEN as opposed to DEN----gamma. Tumor yields in rats receiving combined gamma--DEN treatment were similar to those in rats receiving the DEN alone, irrespective of the gamma--DEN treatment sequence. These results suggest that phenotypically distinguishable lesions, including foci with different histochemical marker patterns and tumors, originate from specific types of damage at different genetic loci and are developmentally independent; and the expression of the GGT(+) marker per se in altered hepatocyte foci is not a reliable index of incipient hepatic neoplasia.

摘要

为了描述γ射线辐射与二乙基亚硝胺(DEN)联合处理对诱导组织化学可检测到的肝细胞灶改变和肝肿瘤的影响,我们评估了150日龄大鼠肝脏中这些病变的发生率。这些大鼠在新生期接受了单次γ射线辐射(全身75拉德)和腹腔注射DEN(0.15微摩尔/克体重),处理方式包括单独处理或联合处理。联合处理涉及以两种可能的顺序给予两种刺激,处理间隔设定为1小时。对灶性群体检测了两种组织化学标记物(γ-谷氨酰转肽酶升高[GGT(+)]和铁排除[FE(-)]),从而产生三种可检测到的灶性表型,即GGT(+)灶、FE(-)灶和GGT(+)、FE(-)灶。通过使用连续冰冻切片技术和计算机辅助图像分析对这三种表型的频率进行了定量。无论两种刺激的给药顺序如何,联合处理均协同增强了GGT(+)灶的诱导;其余两种表型未显示出这种增强。当处理顺序为γ射线→DEN时,GGT(+)灶反应的幅度明显大于DEN→γ射线时。接受γ射线-DEN联合处理的大鼠的肿瘤发生率与仅接受DEN处理的大鼠相似,与γ射线-DEN处理顺序无关。这些结果表明,表型可区分的病变,包括具有不同组织化学标记模式的灶和肿瘤,起源于不同基因位点的特定类型损伤,并且在发育上是独立的;并且在改变的肝细胞灶中GGT(+)标记物本身的表达不是早期肝肿瘤形成的可靠指标。

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