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雄性转基因TGFα小鼠的行为、类固醇激素和自然杀伤细胞活性的改变

Alterations in behavior, steroid hormones and natural killer cell activity in male transgenic TGF alpha mice.

作者信息

Hilakivi-Clarke L A, Arora P K, Sabol M B, Clarke R, Dickson R B, Lippman M E

机构信息

Vincent T. Lombardi Cancer Research Center, Georgetown University Medical School, Washington, DC 20007.

出版信息

Brain Res. 1992 Aug 14;588(1):97-103. doi: 10.1016/0006-8993(92)91348-i.

Abstract

The expression of transforming growth factor alpha (TGF alpha) is widely distributed throughout many normal and neoplastic tissues, but its physiological significance remains unclear. We have utilized male transgenic mice overexpressing the gene encoding human TGF alpha in multiple tissues to further identify those functions which are influenced by this protein. Male TGF alpha mice develop hepatocellular carcinoma at the age of 10-15 months. At the age of 2-3 months these mice, compared to age matched CD-1 controls, spent significantly longer times immobile in Porsolt's swim test, a model of stress and depressive behavior, and exhibiting aggressive behavior in the resident-intruder test. In contrast, the transgenic TGF alpha mice did not differ from the controls in either the plusmaze test of anxiety, or in their voluntary alcohol intake. Significantly, the TGF alpha mice exhibited a 25% lower Natural Killer (NK) cell activity and a four-fold increase in the plasma levels of 17-beta-estradiol (E2) than the controls. No significant changes in plasma testosterone or corticosterone levels were noted. The results indicate that transgenic male mice overexpressing TGF alpha exhibit behaviors characteristic of both an impaired ability to cope with stress and an increased aggressivity. The TGF alpha mice also show reduced NK cell activity and increased plasma estradiol concentrations. The present data suggest that TGF alpha may be important in influencing behavioral, immunological and hormonal systems prior to the onset of tumors. It remains to be determined whether hepatocarcinoma is associated with the direct proliferative and transforming effects of TGF alpha and/or indirect effects mediated through immune, hormonal and behavioral mechanisms.

摘要

转化生长因子α(TGFα)的表达广泛分布于许多正常组织和肿瘤组织中,但其生理意义仍不清楚。我们利用在多个组织中过表达编码人TGFα基因的雄性转基因小鼠,进一步确定受该蛋白影响的那些功能。雄性TGFα小鼠在10至15个月大时会发生肝细胞癌。在2至3个月大时,与年龄匹配的CD-1对照小鼠相比,这些小鼠在波索尔特游泳试验(一种应激和抑郁行为模型)中静止不动的时间明显更长,并且在定居者-入侵者试验中表现出攻击行为。相比之下,转基因TGFα小鼠在焦虑的十字迷宫试验或自愿饮酒量方面与对照小鼠没有差异。值得注意的是,TGFα小鼠的自然杀伤(NK)细胞活性比对照小鼠低25%,血浆17-β-雌二醇(E2)水平增加了四倍。血浆睾酮或皮质酮水平没有明显变化。结果表明,过表达TGFα的转基因雄性小鼠表现出应对压力能力受损和攻击性增加的行为特征。TGFα小鼠还表现出NK细胞活性降低和血浆雌二醇浓度升高。目前的数据表明,TGFα在肿瘤发生之前可能对影响行为、免疫和激素系统很重要。肝细胞癌是否与TGFα的直接增殖和转化作用和/或通过免疫、激素和行为机制介导的间接作用有关,仍有待确定。

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