Role of Immature Red Blood Cells in Neonatal Immunity

Alberta Academic Review Pub Date : 2019-09-10 DOI:10.29173/aar43

Brandi S. Goddard, J. Grewal, Lai Xu, G. Dunsmore, S. Elahi

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Abstract

Newborns are highly susceptible to diseases. Infections such as Bordetella Pertussis (i.e. whooping cough) and Listeria (i.e. food poisoning) can result in the death of neonates while causing little harm to older children and adults. Although previously attributed to an underdeveloped immune system, recent research has shown that this susceptibility is due to the high presence of immature red blood cells or CD71+ cells. These cells possess immunosuppressive properties. By interfering with the function of other immune cells, they can prevent an effective pathogenic immune response. In this study, the changes in the amount of CD71+ cells were observed throughout the different age points of mice as well as in mice infected with Bordetella pertussis and Listeria. This study aimed to gain a better understanding of the development of the immune system as to better aid neonates in fighting infection. Flow cytometry was used to determine the amount of CD71+ cells in the spleens of mice at different age points. The results showed that overall the amount of CD71+ cells decreased as the age of the mouse increased, paralleling the decrease in susceptibility of the immune system. Furthermore, the change in CD71+ cells was also observed in the spleens of mice infected with Bordetella pertussis and mice infected with Listeria. There was no significant change for the Listeria infected mice, as CD71+ cells play no immunological role in fighting Listeria, an intracellular bacteria. However, there was a significant increase in CD71+ cells in Bordetella Pertussis infected mice since this infection was extracellular. These results show that CD71+ cells react differently to different infections and play a different immunological role in the presence of different pathogens. Furthermore, the results shows a direct correlation between age and the amount of CD71+ cells present in the spleen. The changes in the amount of CD71+ cells was most likely due to different pathological conditions and requirements at different ages.

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未成熟红细胞在新生儿免疫中的作用

新生儿极易感染疾病。百日咳博德特氏菌(即百日咳)和李斯特菌(即食物中毒)等感染可导致新生儿死亡，而对年龄较大的儿童和成人几乎没有伤害。虽然以前认为是由于不发达的免疫系统，但最近的研究表明，这种易感性是由于未成熟红细胞或CD71+细胞的大量存在。这些细胞具有免疫抑制特性。通过干扰其他免疫细胞的功能，它们可以阻止有效的致病性免疫反应。在本研究中，CD71+细胞数量的变化在小鼠的不同年龄点以及感染百日咳博德泰拉和李斯特菌的小鼠中被观察到。这项研究旨在更好地了解免疫系统的发育，以便更好地帮助新生儿对抗感染。采用流式细胞术检测不同年龄小鼠脾脏中CD71+细胞的数量。结果显示，随着小鼠年龄的增长，CD71+细胞的总体数量减少，与免疫系统易感性的下降平行。此外，在感染百日咳博德泰拉和李斯特菌小鼠的脾脏中也观察到CD71+细胞的变化。感染李斯特菌的小鼠没有明显的变化，因为CD71+细胞在对抗李斯特菌(一种细胞内细菌)时没有免疫作用。然而，在感染百日咳博德泰拉的小鼠中，CD71+细胞显著增加，因为这种感染是细胞外的。这些结果表明，CD71+细胞对不同感染的反应不同，在不同病原体存在下发挥不同的免疫作用。此外，结果显示年龄与脾脏中CD71+细胞的数量直接相关。CD71+细胞数量的变化很可能是由于不同年龄的病理条件和需求不同所致。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Alberta Academic Review

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