首页> 外文期刊>Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems >Effects of aging on resistance to Trichinella spiralis infection in rodents exposed to 2,3,7,8-tetrachlorodibenzo-p-dioxin.
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Effects of aging on resistance to Trichinella spiralis infection in rodents exposed to 2,3,7,8-tetrachlorodibenzo-p-dioxin.

机译:老化对暴露于2,3,7,8-四氯二苯并-p-二恶英的啮齿类动物对旋毛虫感染的抵抗力的影响。

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摘要

Immune function, including resistance to infection, decreases as humans and rodents age. We have shown that preinfection exposure of young (9-11 weeks) mice or rats to TCDD decreased resistance to Trichinella spiralis (Ts) infection, expressed as delayed onset or completion of parasite elimination and as increased muscle burdens of larvae. It has also been shown that aged mice express lower constitutive levels of resistance to Ts infection, compared to young adult animals. This study tested the hypothesis that the age-related decrease in constitutive levels of resistance to Ts infection exacerbates the decreased resistance to infection that follows TCDD exposure. This hypothesis addresses the concern that TCDD may pose a greater threat to the elderly than to the population at large. Animals were given a single oral dose of 1, 10, or 30 microg TCDD/kg, 7 days before infection. Eleven days later, young (approximately 10 weeks) control rodents had eliminated a greater proportion of the original parasite burden from the intestine than aged control animals. Nevertheless, parasite elimination was decreased by TCDD exposure only in young rodents. The effect of TCDD exposure on numbers of encysted larvae was evaluated only in rats. Increased larvae burdens occurred in young rats at 30 microg TCDD/kg and at 10 or 30 microg TCDD/kg in aged rats. Parasite-specific splenocyte and lymph node cell proliferation was suppressed following dioxin exposure in young mice; cells from aged mice were markedly less responsive to stimulation, yet less sensitive to TCDD exposure. The response to parasite antigens was not affected in aged rats exposed to TCDD, although elevated mitogen-driven B-cell proliferation was observed. These results indicate that age-related constitutive immunosuppression did not exacerbate TCDD-induced suppression of T-cell mediated adult parasite expulsion; rather, advanced age provided some degree of protection. On the other hand, a lower dose of TCDD was required in aged rats to suppress the combined humoral and cellular responses that limit the burden of encysted larvae, compared to young rats. These model-dependent results preclude acceptance or rejection of the tested hypothesis.
机译:免疫功能,包括对感染的抵抗力,随着人类和啮齿动物的衰老而降低。我们已经表明,年轻的(9-11周)小鼠或大鼠在TCDD感染前的暴露降低了对旋毛虫(Ts)感染的抵抗力,表现为延迟发作或完成了寄生虫消除,并且表现为幼虫的肌肉负担增加。还已经表明,与成年幼鼠相比,成年小鼠对Ts感染的抵抗力较低。这项研究检验了以下假设:与年龄相关的对Ts感染的抵抗力构成水平的下降会加剧TCDD暴露后对感染的抵抗力的下降。该假设解决了以下问题:TCDD对老年人的威胁可能大于对整个人口的威胁。在感染前7天给动物口服1、10或30微克TCDD / kg的单次口服剂量。 11天后,年轻(约10周)的对照啮齿动物与年长的对照动物相比,消除了肠道中较大比例的原始寄生虫负担。然而,仅在年轻的啮齿动物中,TCDD暴露可减少寄生虫的消除。仅在大鼠中评估了TCDD暴露对入幼虫数量的影响。在幼鼠中幼虫的负担增加,为30微克TCDD / kg,在老年鼠中为10或30微克TCDD / kg。幼鼠暴露于二恶英后,寄生虫特异性脾细胞和淋巴结细胞增殖受到抑制;来自衰老小鼠的细胞对刺激的反应明显较弱,但对TCDD暴露的敏感性较弱。尽管观察到丝裂原驱动的B细胞增殖升高,但在暴露于TCDD的老年大鼠中对寄生虫抗原的反应没有受到影响。这些结果表明,与年龄相关的组成型免疫抑制并没有加剧TCDD诱导的T细胞介导的成人寄生虫驱逐的抑制。相反,高龄提供了一定程度的保护。另一方面,与年轻大鼠相比,老年大鼠需要较低剂量的TCDD来抑制体液和细胞反应,从而限制了幼虫的负担。这些与模型相关的结果排除了接受或拒绝测试假设的可能性。

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