Inflammasomes as a Prognostic Marker and Possible Therapeutic Target in Multiple Sclerosis: A Rapid Review of the Literature

Nury Tatiana Rincón Cuenca, Daniela Pereira Lamas, Rosa Fernández Hawa, Ketty Quezada, L. Garcia, Pamela Baez, Assma A. Althobaity, N. Dim
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Abstract

Introduction: Inflammasomes are multiprotein complexes innate to the immune system that, upon activation, initiate a chain reaction culminating in the production of cytokines IL-1 and IL-18. Recent studies have suggested a connection between inflammasome activation and neurological diseases such as multiple sclerosis (MS). In this review, we aimed to evaluate the role of inflammasomes as potential therapeutic agents and prognostic markers of MS. Methods: Through a database search, 156 articles were identified. Of these, we selected articles focusing on observational and interventional studies that either directly measured the expression of inflammasomes or the levels of cytokines or interleukin as outcomes. After applying a snowball sampling strategy, this review ultimately included nine studies. Results: Our search yielded nine studies published between 2010 and 2022—9 observational studies included case-control and cohort designs. All studies comprised adult populations, 20–72 years of age. All studies incorporated a control group. We selected studies that utilized surrogate measures to evaluate outcomes such as inflammasome expression of NLRP3 or similar genes and assess cytokine levels such as IL-1β, IL-18, IL-23, and TNF. Discussion: Overall, the revised studies suggest a possible role for inflammasomes components, including ASC and caspase-1, which have been evaluated as potential prognostic markers in MS. Therapeutic strategies have focused on the inhibition of NLRP3, which is one of the most prominent and studied inflammasomes, by IFN-β.
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炎症小体作为多发性硬化症的预后标志物和可能的治疗靶点:文献综述
炎性小体是免疫系统固有的多蛋白复合物,一旦激活,就会引发连锁反应,最终产生细胞因子IL-1和IL-18。最近的研究表明,炎症小体激活与多发性硬化症(MS)等神经系统疾病之间存在联系。在这篇综述中,我们旨在评估炎症小体作为多发性硬化症潜在治疗剂和预后标志物的作用。方法:通过数据库检索,确定了156篇文章。其中,我们选择了关注观察性和干预性研究的文章,这些研究要么直接测量炎症小体的表达,要么测量细胞因子或白细胞介素的水平。在采用滚雪球抽样策略后,本综述最终纳入了9项研究。结果:我们检索了2010年至2022年间发表的9项研究,其中9项观察性研究包括病例对照和队列设计。所有的研究对象都是20-72岁的成年人。所有的研究都纳入了一个对照组。我们选择了使用替代方法来评估结果的研究,如炎性体NLRP3或类似基因的表达,并评估细胞因子水平,如IL-1β、IL-18、IL-23和TNF。讨论:总体而言,修订后的研究表明炎症小体成分(包括ASC和caspase-1)可能发挥作用,这些成分已被评估为ms的潜在预后标志物。治疗策略侧重于IFN-β抑制NLRP3,这是最突出的研究炎症小体之一。
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