针对慢性破坏性tnf驱动的关节病理衰老和炎症

IF 5.3 3区 医学 Q2 CELL BIOLOGY Mechanisms of Ageing and Development Pub Date : 2023-09-01 DOI:10.1016/j.mad.2023.111856
Nikolaos I. Vlachogiannis , Konstantinos Evangelou , Lydia Ntari , Christoforos Nikolaou , Maria C. Denis , Niki Karagianni , Dimitris Veroutis , Vassilis Gorgoulis , George Kollias , Petros P. Sfikakis
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引用次数: 0

摘要

我们已经证明,当与亚治疗剂量的抗TNF单抗英夫利昔单抗(1mg /kg)联合给药时,抗衰老的达沙替尼可以消除慢性破坏性关节炎的人TNF转基因小鼠模型中的关节炎。在此,我们发现,虽然根据指南算法方法评估的衰老软骨细胞数量(GL13+/Ki67-)不受达沙替尼或亚治疗性英夫利昔单抗单一疗法的影响,但它们的联合治疗使衰老软骨细胞减少了50%,这与治疗性英夫利昔单抗单一疗法(10 mg/kg)观察到的水平相当。这种联合治疗也减少了关节炎关节中与衰老相关的分泌表型的多种因素的表达。研究阐明炎症和衰老的相互作用可能有助于优化治疗策略,也有助于以慢性低度关节炎症为特征的年龄相关病理。
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Targeting senescence and inflammation in chronic destructive TNF-driven joint pathology

We had shown that administration of the senolytic Dasatinib abolishes arthritis in the human TNF transgenic mouse model of chronic destructive arthritis when given in combination with a sub-therapeutic dose of the anti-TNF mAb Infliximab (1 mg/kg). Herein, we found that while the number of senescent chondrocytes (GL13+/Ki67-), assessed according to guideline algorithmic approaches, was not affected by either Dasatinib or sub-therapeutic Infliximab monotherapies, their combination reduced senescent chondrocytes by 50 %, which was comparable to levels observed with therapeutic Infliximab monotherapy (10 mg/kg). This combination therapy also reduced the expression of multiple factors of senescence-associated secretory phenotype in arthritic joints. Studies to elucidate the interplay of inflammation and senescence may help in optimizing treatment strategies also for age-related pathologies characterized by chronic low-grade joint inflammation.

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来源期刊
CiteScore
11.10
自引率
1.90%
发文量
79
审稿时长
32 days
期刊介绍: Mechanisms of Ageing and Development is a multidisciplinary journal aimed at revealing the molecular, biochemical and biological mechanisms that underlie the processes of aging and development in various species as well as of age-associated diseases. Emphasis is placed on investigations that delineate the contribution of macromolecular damage and cytotoxicity, genetic programs, epigenetics and genetic instability, mitochondrial function, alterations of metabolism and innovative anti-aging approaches. For all of the mentioned studies it is necessary to address the underlying mechanisms. Mechanisms of Ageing and Development publishes original research, review and mini-review articles. The journal also publishes Special Issues that focus on emerging research areas. Special issues may include all types of articles following peered review. Proposals should be sent directly to the Editor-in-Chief.
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