Increased lethality of respiratory infection by Streptococcus pneumoniae in the Dp16 mouse model of Down syndrome

IF 2.5 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Kelley L. Colvin, Robert J. Elliott, Desiree M. Goodman, Julie Harral, Edward G. Barrett, Michael E. Yeager
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Abstract

Objectives

We sought to investigate whether the Dp16 mouse model of Down syndrome (DS) is more susceptible to severe and lethal respiratory tract infection by Streptococcus pneumoniae.

Study Design

We infected controls and Dp16 mice with Streptococcus pneumoniae and measured survival rates. We compared cytokine production by primary lung cell cultures exposed to Streptococcus pneumoniae. We examined lung protein expression for interferon signaling related pathways. We characterized the histopathology and quantified the extent of bronchus-associated lymphoid tissue. Finally, we examined mouse tissues for the presence of oligomeric tau protein.

Results

We found that the Dp16 mouse model of DS displayed significantly higher susceptibility to lethal respiratory infection with Streptococcus pneumoniae compared to control mice. Lung cells cultured from Dp16 mice displayed unique secreted cytokine profiles compared to control mice. The Dp16 mouse lungs were characterized by profound lobar pneumonia with massive diffuse consolidation involving nearly the entire lobe. Marked red hepatization was noted, and Dp16 mice lungs contained numerous bronchus-associated lymphoid tissues that were highly follicularized. Compared to uninfected mice, both control mice and Dp16 mice infected with Streptococcus pneumoniae showed evidence of oligomeric tau aggregates.

Conclusions

Increased susceptibility to severe respiratory tract infection with Streptococcus pneumoniae in Dp16 mice closely phenocopies infection in individuals with DS. The increase does not appear to be linked to overexpression of mouse interferon genes syntenic to human chromosome 21.

Abstract Image

唐氏综合征 Dp16 小鼠模型中肺炎链球菌呼吸道感染的致死率增加
目的 我们试图研究唐氏综合症(DS)的 Dp16 小鼠模型是否更容易受到肺炎链球菌的严重致命性呼吸道感染。 研究设计 我们用肺炎链球菌感染对照组和 Dp16 小鼠,并测量存活率。我们比较了暴露于肺炎链球菌的原代肺细胞培养物产生的细胞因子。我们检测了干扰素信号相关通路的肺蛋白表达。我们对组织病理学进行了描述,并对支气管相关淋巴组织的范围进行了量化。最后,我们检测了小鼠组织中是否存在低聚 tau 蛋白。 结果 我们发现,与对照小鼠相比,Dp16 DS 小鼠对肺炎链球菌致命性呼吸道感染的易感性明显更高。与对照小鼠相比,从 Dp16 小鼠培养的肺细胞显示出独特的分泌细胞因子谱。Dp16 小鼠肺部的特征是严重的大叶性肺炎,大面积弥漫性固缩几乎涉及整个肺叶。Dp16小鼠肺部出现明显的红色肝化,并含有大量高度滤泡化的支气管相关淋巴组织。与未感染的小鼠相比,对照组小鼠和感染肺炎链球菌的 Dp16 小鼠均显示出低聚 tau 聚合体的证据。 结论 Dp16 小鼠对肺炎链球菌严重呼吸道感染的易感性增加与 DS 患者的感染表型相似。这种增加似乎与与人类 21 号染色体同源的小鼠干扰素基因的过度表达无关。
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来源期刊
FASEB bioAdvances
FASEB bioAdvances Multiple-
CiteScore
5.40
自引率
3.70%
发文量
56
审稿时长
10 weeks
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