Ledderose Carola, Valsami Eleftheria-Angeliki, Elevado Mark, Liu Qing, Giva Brennan, Curatolo Julian, Delfin Joshua, Abutabikh Reem, Junger Wolfgang G
Department of Surgery, University of California, San Diego Health, 9452 Medical Ctr Dr, La Jolla, San Diego, CA, 92037, USA.
Department of Surgery, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA, USA.
Immun Ageing. 2024 Jul 3;21(1):45. doi: 10.1186/s12979-024-00441-4.
The function of polymorphonuclear neutrophils (PMNs) decreases with age, which results in infectious and inflammatory complications in older individuals. The underlying causes are not fully understood. ATP release and autocrine stimulation of purinergic receptors help PMNs combat microbial invaders. Excessive extracellular ATP interferes with these mechanisms and promotes inflammatory PMN responses. Here, we studied whether dysregulated purinergic signaling in PMNs contributes to their dysfunction in older individuals.
Bacterial infection of C57BL/6 mice resulted in exaggerated PMN activation that was significantly greater in old mice (64 weeks) than in young animals (10 weeks). In contrast to young animals, old mice were unable to prevent the systemic spread of bacteria, resulting in lethal sepsis and significantly greater mortality in old mice than in their younger counterparts. We found that the ATP levels in the plasma of mice increased with age and that, along with the extracellular accumulation of ATP, the PMNs of old mice became increasingly primed. Stimulation of the formyl peptide receptors of those primed PMNs triggered inflammatory responses that were significantly more pronounced in old mice than in young animals. However, bacterial phagocytosis and killing by PMNs of old mice were significantly lower than that of young mice. These age-dependent PMN dysfunctions correlated with a decrease in the enzymatic activity of plasma ATPases that convert extracellular ATP to adenosine. ATPases depend on divalent metal ions, including Ca, Mg, and Zn, and we found that depletion of these ions blocked the hydrolysis of ATP and the formation of adenosine in human blood, resulting in ATP accumulation and dysregulation of PMN functions equivalent to those observed in response to aging.
Our findings suggest that impaired hydrolysis of plasma ATP dysregulates PMN function in older individuals. We conclude that strategies aimed at restoring plasma ATPase activity may offer novel therapeutic opportunities to reduce immune dysfunction, inflammation, and infectious complications in older patients.
多形核中性粒细胞(PMN)的功能随年龄增长而下降,这导致老年个体出现感染性和炎症性并发症。其潜在原因尚未完全明确。ATP释放以及嘌呤能受体的自分泌刺激有助于PMN对抗微生物入侵者。过多的细胞外ATP会干扰这些机制并促进PMN的炎症反应。在此,我们研究了PMN中嘌呤能信号失调是否导致老年个体中PMN功能障碍。
C57BL/6小鼠的细菌感染导致PMN活化加剧,老年小鼠(64周)的这种活化程度明显高于年轻动物(10周)。与年轻动物不同,老年小鼠无法阻止细菌的全身扩散,导致致命性败血症,且老年小鼠的死亡率明显高于年轻小鼠。我们发现小鼠血浆中的ATP水平随年龄增长而升高,并且随着ATP在细胞外的积累,老年小鼠的PMN变得越来越易被激活。刺激那些已被激活的PMN的甲酰肽受体引发的炎症反应在老年小鼠中比在年轻动物中明显更显著。然而,老年小鼠的PMN对细菌的吞噬和杀伤能力明显低于年轻小鼠。这些与年龄相关的PMN功能障碍与将细胞外ATP转化为腺苷的血浆ATP酶的酶活性降低有关。ATP酶依赖于二价金属离子,包括钙、镁和锌,我们发现这些离子的耗竭会阻断人血液中ATP的水解和腺苷的形成,导致ATP积累以及PMN功能失调,这与衰老时观察到的情况相当。
我们的研究结果表明,血浆ATP水解受损会导致老年个体中PMN功能失调。我们得出结论,旨在恢复血浆ATP酶活性的策略可能为减少老年患者的免疫功能障碍、炎症和感染性并发症提供新的治疗机会。
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