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冲击波在小鼠模型中导致免疫系统功能障碍和短暂性骨髓衰竭。

Blast Waves Cause Immune System Dysfunction and Transient Bone Marrow Failure in a Mouse Model.

作者信息

Bergmann-Leitner Elke S, Bobrov Alexander G, Bolton Jessica S, Rouse Michael D, Heyburn Lanier, Pavlovic Radmila, Garry Brittany I, Alamneh Yonas, Long Joseph, Swierczewski Brett, Tyner Stuart, Getnet Derese, Sajja Venkatasivasai S, Antonic Vlado

机构信息

Biologics Research and Development, Walter Reed Army Institute of Research, Silver Spring, MD, United States.

Wound Infections Department, Walter Reed Army Institute of Research, Silver Spring, MD, United States.

出版信息

Front Bioeng Biotechnol. 2022 Mar 22;10:821169. doi: 10.3389/fbioe.2022.821169. eCollection 2022.

Abstract

Explosive devices, either conventional or improvised, are common sources of injuries during combat, civil unrest, and terror attacks, resulting in trauma from exposure to blast. A blast wave (BW), a near-instantaneous rise in pressure followed by a negative pressure, propagates through the body in milliseconds and can affect physiology for days/months after exposure. Epidemiological data show that blast-related casualties result in significantly higher susceptibility to wound infections, suggesting long-lasting immune modulatory effects from blast exposure. The mechanisms involved in BW-induced immune changes are poorly understood. We evaluated the effects of BW on the immune system using an established murine model. Animals were exposed to BWs (using an Advanced Blast Simulator), followed by longitudinally sampling for 14 days. Blood, bone marrow, and spleen were analyzed for changes in the 1) complete blood count (CBC), and 2) composition of bone marrow cells (BMC) and splenocytes, and 3) concentrations of systemic cytokines/chemokines. Our data demonstrate that BW results in transient bone marrow failure and long-term changes in the frequency and profile of progenitor cell populations. Viability progressively decreased in hematopoietic stem cells and pluripotent progenitor cells. Significant decrease of CD4 T cells in the spleen indicates reduced functionality of adaptive immune system. Dynamic changes in the concentrations of several cytokines and chemokines such as IL-1α and IL-17 occurred potentially contributing to dysregulation of immune response after trauma. This work lays the foundation for identifying the potential mechanisms behind BW's immunosuppressive effects to inform the recognition of this compromised status is crucial for the development of therapeutic interventions for infections to reduce recovery time of wounded patients injured by explosive devices.

摘要

无论是传统的还是简易的爆炸装置,都是战斗、内乱和恐怖袭击期间常见的致伤源,会导致因接触爆炸冲击波而造成创伤。爆炸冲击波(BW)是一种压力近乎瞬间升高随后又出现负压的情况,会在数毫秒内传遍全身,并且在接触后的数天/数月内都可能影响生理机能。流行病学数据表明,与爆炸相关的伤亡会导致伤口感染的易感性显著增加,这表明爆炸暴露会产生持久的免疫调节作用。人们对爆炸冲击波引起免疫变化的机制了解甚少。我们使用已建立的小鼠模型评估了爆炸冲击波对免疫系统的影响。让动物暴露于爆炸冲击波(使用先进的爆炸模拟器),然后纵向采样14天。分析血液、骨髓和脾脏在以下方面的变化:1)全血细胞计数(CBC);2)骨髓细胞(BMC)和脾细胞的组成;3)全身细胞因子/趋化因子的浓度。我们的数据表明,爆炸冲击波会导致短暂的骨髓衰竭以及祖细胞群体的频率和特征发生长期变化。造血干细胞和多能祖细胞的活力逐渐下降。脾脏中CD4 T细胞的显著减少表明适应性免疫系统的功能降低。几种细胞因子和趋化因子(如IL-1α和IL-17)浓度的动态变化可能导致创伤后免疫反应失调。这项工作为确定爆炸冲击波免疫抑制作用背后的潜在机制奠定了基础,认识到这种受损状态对于开发针对感染的治疗干预措施以减少爆炸装置受伤患者的恢复时间至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b711/8980552/4bbfed469b6c/fbioe-10-821169-g001.jpg

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