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控制感染刚果锥虫小鼠贫血的机制。

Mechanisms controlling anaemia in Trypanosoma congolense infected mice.

作者信息

Noyes Harry A, Alimohammadian Mohammad H, Agaba Morris, Brass Andy, Fuchs Helmut, Gailus-Durner Valerie, Hulme Helen, Iraqi Fuad, Kemp Stephen, Rathkolb Birgit, Wolf Eckard, de Angelis Martin Hrabé, Roshandel Delnaz, Naessens Jan

机构信息

School of Biological Sciences, University of Liverpool, Liverpool, United Kingdom.

出版信息

PLoS One. 2009;4(4):e5170. doi: 10.1371/journal.pone.0005170. Epub 2009 Apr 13.

Abstract

BACKGROUND

Trypanosoma congolense are extracellular protozoan parasites of the blood stream of artiodactyls and are one of the main constraints on cattle production in Africa. In cattle, anaemia is the key feature of disease and persists after parasitaemia has declined to low or undetectable levels, but treatment to clear the parasites usually resolves the anaemia.

METHODOLOGY/PRINCIPAL FINDINGS: The progress of anaemia after Trypanosoma congolense infection was followed in three mouse strains. Anaemia developed rapidly in all three strains until the peak of the first wave of parasitaemia. This was followed by a second phase, characterized by slower progress to severe anaemia in C57BL/6, by slow recovery in surviving A/J and a rapid recovery in BALB/c. There was no association between parasitaemia and severity of anaemia. Furthermore, functional T lymphocytes are not required for the induction of anaemia, since suppression of T cell activity with Cyclosporin A had neither an effect on the course of infection nor on anaemia. Expression of genes involved in erythropoiesis and iron metabolism was followed in spleen, liver and kidney tissues in the three strains of mice using microarrays. There was no evidence for a response to erythropoietin, consistent with anaemia of chronic disease, which is erythropoietin insensitive. However, the expression of transcription factors and genes involved in erythropoiesis and haemolysis did correlate with the expression of the inflammatory cytokines Il6 and Ifng.

CONCLUSIONS/SIGNIFICANCE: The innate immune response appears to be the major contributor to the inflammation associated with anaemia since suppression of T cells with CsA had no observable effect. Several transcription factors regulating haematopoiesis, Tal1, Gata1, Zfpm1 and Klf1 were expressed at consistently lower levels in C57BL/6 mice suggesting that these mice have a lower haematopoietic capacity and therefore less ability to recover from haemolysis induced anaemia after infection.

摘要

背景

刚果锥虫是偶蹄动物血流中的细胞外原生动物寄生虫,是非洲养牛业的主要制约因素之一。在牛身上,贫血是疾病的关键特征,在寄生虫血症降至低水平或无法检测到的水平后仍会持续,但清除寄生虫的治疗通常能解决贫血问题。

方法/主要发现:在三种小鼠品系中追踪了刚果锥虫感染后贫血的进展情况。在所有三个品系中,贫血迅速发展,直至第一波寄生虫血症达到峰值。随后进入第二阶段,其特征是C57BL/6小鼠进展为严重贫血的速度较慢,存活的A/J小鼠恢复缓慢,而BALB/c小鼠则迅速恢复。寄生虫血症与贫血严重程度之间没有关联。此外,贫血的诱导不需要功能性T淋巴细胞,因为用环孢菌素A抑制T细胞活性对感染进程和贫血均无影响。使用微阵列技术追踪了三种小鼠品系的脾脏、肝脏和肾脏组织中参与红细胞生成和铁代谢的基因表达。没有证据表明对促红细胞生成素有反应,这与慢性病贫血一致,即对促红细胞生成素不敏感。然而,转录因子以及参与红细胞生成和溶血的基因表达确实与炎性细胞因子Il6和Ifng的表达相关。

结论/意义:由于用环孢菌素A抑制T细胞没有可观察到的影响,先天免疫反应似乎是与贫血相关炎症的主要促成因素。几种调节造血的转录因子Tal1、Gata1、Zfpm1和Klf1在C57BL/6小鼠中的表达水平始终较低,这表明这些小鼠的造血能力较低,因此感染后从溶血诱导的贫血中恢复的能力也较低。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3063/2664899/2ab7909fbfe2/pone.0005170.g001.jpg

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