The Role of BPIFB4 in Immune System and Cardiovascular Disease: The Lesson from Centenarians.

IF 1.1 Q4 MEDICINE, RESEARCH & EXPERIMENTAL Translational Medicine at UniSa Pub Date : 2021-12-23 eCollection Date: 2021-01-01 DOI:10.37825/2239-9754.1029
Francesco Montella, Valentina Lopardo, Monica Cattaneo, Albino Carrizzo, Carmine Vecchione, Elena Ciaglia, Annibale Alessandro Puca
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引用次数: 2

Abstract

Recent discoveries have shed light on the participation of the immune system in the physio pathology of the cardiovascular system underpinning the importance of keeping the balance of the first to preserve the latter. Aging, along with other risk factors, can challenge such balance triggering the onset of cardiovascular diseases. Among several mediators ensuring the proper cross-talk between the two systems, bactericidal/permeability-increasing fold-containing family B member 4 (BPIFB4) has been shown to have a pivotal role, also by sustaining important signals such as eNOS and PKC-alpha. In addition, the Longevity-associated variant (LAV), which is an haplotype allele in BPIFB4 characterized by 4 missense polymorphisms, enriched in homozygosity in Long Living Individuals (LLIs), has been shown to be efficient, if administered systemically through gene therapy, in improving many aspects of cardiovascular diseases (CVDs). This occurs mainly through a fine immune system remodeling across: 1) a M2 macrophage polarizing effect, 2) a favorable redistribution of the circulating monocyte cell subsets and 3) the reduction of T-cell activation. Furthermore, LAV-BPIFB4 treatment induced a desirable recovery of the inflammatory balance by mitigating the pro-inflammatory factor levels and enhancing the anti-inflammatory boost through a mechanism that is partially dependent on SDF-1/CXCR4 axis. Importantly, the remarkable effects of LAV-BPIFB4 treatment, which translates in increased BPIFB4 circulating levels, mirror what occurs in long-living individuals (LLIs) in whom the high circulating levels of BPIFB4 are protective from age-related and CVDs and emphasize the reason why LLIs are considered a model of successful aging. Here, we review the mechanisms by which LAV-BPIFB4 exerts its immunomodulatory activity in improving the cardiovascular-immune system dialogue that might strengthen its role as a key mediator in CVDs.

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BPIFB4在免疫系统和心血管疾病中的作用:来自百岁老人的教训。
最近的发现揭示了免疫系统在心血管系统的生理病理中的参与,支持了保持前者的平衡以保护后者的重要性。衰老和其他风险因素会挑战这种平衡,引发心血管疾病的发作。在确保两个系统之间适当的串扰的几种介质中,杀菌/增加透性的含折叠家族成员4 (BPIFB4)已被证明具有关键作用,也通过维持重要信号如eNOS和pkc - α。此外,长寿相关变异(LAV)是BPIFB4的一个单倍型等位基因,具有4个错义多态性,在长寿个体(LLIs)中富集纯合子,如果通过基因治疗系统地给予,已被证明在改善心血管疾病(cvd)的许多方面是有效的。这主要是通过精细的免疫系统重塑发生的:1)M2巨噬细胞极化效应,2)循环单核细胞亚群的有利重新分配,3)t细胞活化的减少。此外,LAV-BPIFB4治疗通过部分依赖于SDF-1/CXCR4轴的机制,通过减轻促炎因子水平和增强抗炎促进作用,诱导炎症平衡的理想恢复。重要的是,LAV-BPIFB4治疗的显著效果,转化为BPIFB4循环水平的增加,反映了长寿个体(LLIs)的情况,在LLIs中,高循环水平的BPIFB4可以预防与年龄相关的心血管疾病,并强调了LLIs被认为是成功衰老模型的原因。在这里,我们回顾了LAV-BPIFB4在改善心血管-免疫系统对话中发挥其免疫调节活性的机制,这可能加强其作为心血管疾病关键介质的作用。
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Translational Medicine at UniSa
Translational Medicine at UniSa MEDICINE, RESEARCH & EXPERIMENTAL-
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