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随着衰老,Vγ4 T细胞的积累与小鼠经食源性单核细胞增生李斯特菌感染后适应性Vγ4 T细胞反应增强有关。

The accumulation of Vγ4 T cells with aging is associated with an increased adaptive Vγ4 T cell response after foodborne Listeria monocytogenes infection of mice.

作者信息

Khairallah Camille, Chu Timothy H, Qiu Zhijuan, Imperato Jessica N, Yang Daniella, Sheridan Brian S

机构信息

Department of Microbiology and Immunology, Center for Infectious Diseases, Renaissance School of Medicine, Stony Brook University, 246 Centers for Molecular Medicine, Stony Brook, 11794, NY, USA.

出版信息

Immun Ageing. 2022 May 3;19(1):19. doi: 10.1186/s12979-022-00275-y.

Abstract

BACKGROUND

It is generally accepted that aging has detrimental effects on conventional T cell responses to systemic infections. However, most pathogens naturally invade the body through mucosal barriers. Although mucosal sites are highly enriched in unconventional immune sentinels like γδ T cells, little is currently known about the impact of aging on unconventional mucosal T cell responses. We previously established that foodborne infection with a mouse-adapted internalin A mutant Listeria monocytogenes (Lm) generates an adaptive intestinal memory CD44 CD27 Vγ4 T cells capable of co-producing IL-17A and IFNγ. Therefore, we used this model to evaluate the impact of aging on adaptive Vγ4 T cell responses elicited by foodborne infection.

RESULTS

Foodborne Lm infection of female Balb/c and C57BL/6 mice led to an increased adaptive CD44 CD27 Vγ4 T cell response associated with aging. Moreover, Lm-elicited CD44 CD27 Vγ4 T cells maintained diverse functional subsets despite some alterations favoring IL-17A production as mice aged. In contrast to the documented susceptibility of aged mice to intravenous Lm infection, mice contained bacteria after foodborne Lm infection suggesting that elevated bacterial burden was not a major factor driving the increased adaptive CD44 CD27 Vγ4 T cell response associated with mouse age. However, CD44 CD27 Vγ4 T cells accumulated in naïve mice as they aged suggesting that an increased precursor frequency contributes to the robust Lm-elicited mucosal response observed. Body mass did not appear to have a strong positive association with CD44 CD27 Vγ4 T cells within age groups. Although an increased adaptive CD44 CD27 Vγ4 T cell response may contribute to foodborne Lm resistance of C57BL/6 mice aged 19 or more months, neither anti-TCRδ or anti-IL-17A treatment impacted Lm colonization after primary infection. These results suggest that γδTCR signaling and IL-17A are dispensable for protection after primary foodborne Lm infection consistent with the role of conventional T cells during the early innate immune response to Lm.

CONCLUSIONS

Lm-elicited adaptive Vγ4 T cells appear resistant to immunosenescence and memory Vγ4 T cells could be utilized to provide protective immune functions during enteric infection of aged hosts. As such, oral immunization might offer an efficient therapeutic approach to generate unconventional memory T cells in the elderly.

摘要

背景

人们普遍认为衰老会对传统T细胞对全身感染的反应产生不利影响。然而,大多数病原体通过黏膜屏障自然侵入人体。尽管黏膜部位富含γδT细胞等非传统免疫哨兵,但目前对于衰老对非传统黏膜T细胞反应的影响知之甚少。我们之前证实,用适应小鼠的内化素A突变单核细胞增生李斯特菌(Lm)进行食源性感染可产生能够共同产生IL-17A和IFNγ的适应性肠道记忆CD44 CD27 Vγ4 T细胞。因此,我们使用该模型来评估衰老对食源性感染引发的适应性Vγ4 T细胞反应的影响。

结果

雌性Balb/c和C57BL/6小鼠的食源性Lm感染导致与衰老相关的适应性CD44 CD27 Vγ4 T细胞反应增加。此外,尽管随着小鼠年龄增长,Lm诱导的CD44 CD27 Vγ4 T细胞存在一些有利于IL-17A产生的改变,但仍维持了不同的功能亚群。与已记录的老年小鼠对静脉注射Lm感染的易感性相反,食源性Lm感染后的小鼠体内含有细菌,这表明细菌负荷增加并非驱动与小鼠年龄相关的适应性CD44 CD27 Vγ4 T细胞反应增加的主要因素。然而,随着幼稚小鼠年龄增长,CD44 CD27 Vγ4 T细胞会积累,这表明前体频率增加有助于观察到的对Lm引发的强大黏膜反应。在各年龄组中,体重似乎与CD44 CD27 Vγ4 T细胞没有强烈的正相关。尽管适应性CD44 CD27 Vγ4 T细胞反应增加可能有助于19个月及以上的C57BL/6老年小鼠抵抗食源性Lm感染,但抗TCRδ或抗IL-17A治疗在初次感染后均未影响Lm定植。这些结果表明,γδTCR信号传导和IL-17A在初次食源性Lm感染后的保护中并非必需,这与传统T细胞在对Lm的早期固有免疫反应中的作用一致。

结论

Lm诱导的适应性Vγ4 T细胞似乎对免疫衰老具有抗性,记忆Vγ4 T细胞可用于在老年宿主肠道感染期间提供保护性免疫功能。因此,口服免疫可能为在老年人中产生非传统记忆T细胞提供一种有效的治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8eff/9063344/b7b03bc61bf7/12979_2022_275_Fig1_HTML.jpg

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