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自噬之外的P62/SQSTM1:在实验动物和家畜中的生理作用及治疗应用

P62/SQSTM1 beyond Autophagy: Physiological Role and Therapeutic Applications in Laboratory and Domestic Animals.

作者信息

Sabbieti Maria Giovanna, Marchegiani Andrea, Sufianov Albert A, Gabai Vladimir L, Shneider Alexander, Agas Dimitrios

机构信息

School of Biosciences and Veterinary Medicine, University of Camerino, 62032 Camerino, Italy.

Federal Center of Neurosurgery, 625032 Tyumen, Russia.

出版信息

Life (Basel). 2022 Apr 6;12(4):539. doi: 10.3390/life12040539.

Abstract

Inflammation is the preceding condition for the development of mild and severe pathological conditions, including various forms of osteopenia, cancer, metabolic syndromes, neurological disorders, atherosclerosis, cardiovascular, lung diseases, etc., in human and animals. The inflammatory status is induced by multifarious intracellular signaling cascades, where cytokines, chemokines, arachidonic acid metabolites, adhesion molecules, immune cells and other components foster a "slow burn" at a local or systemic level. Assuming that countering inflammation limits the development of inflammation-based diseases, a series of new side-effects-free therapies was assessed in experimental and domestic animals. Within the targets of the drug candidates for quenching inflammation, an archetypal autophagic gear, the p62/sqstm1 protein, has currently earned attention from researchers. Intracellular p62 has been recently coined as a multi-task tool associated with autophagy, bone remodeling, bone marrow integrity, cancer progression, and the maintenance of systemic homeostasis. Accordingly, p62 can act as an effective suppressor of inflamm-aging, reducing oxidative stress and proinflammatory signals. Such an operational schedule renders this protein an effective watchdog for degenerative diseases and cancer development in laboratory and pet animals. This review summarizes the current findings concerning p62 activities as a molecular hub for cell and tissues metabolism and in a variety of inflammatory diseases and other pathological conditions. It also specifically addresses the applications of exogenous p62 (DNA plasmid) as an anti-inflammatory and homeostatic regulator in the treatment of osteoporosis, metabolic syndrome, age-related macular degeneration and cancer in animals, and the possible application of p62 plasmid in other inflammation-associated diseases.

摘要

炎症是人类和动物发生轻度和重度病理状况的前提条件,这些病理状况包括各种形式的骨质减少、癌症、代谢综合征、神经紊乱、动脉粥样硬化、心血管疾病、肺部疾病等。炎症状态是由多种细胞内信号级联反应诱导的,其中细胞因子、趋化因子、花生四烯酸代谢产物、黏附分子、免疫细胞和其他成分在局部或全身水平引发“缓慢燃烧”。假设对抗炎症可限制炎症性疾病的发展,人们在实验动物和家畜中评估了一系列无新副作用的疗法。在用于消除炎症的候选药物靶点中,一种典型的自噬机制——p62/sqstm1蛋白,目前已引起研究人员的关注。细胞内的p62最近被视为一种与自噬、骨重塑、骨髓完整性、癌症进展以及全身稳态维持相关的多功能工具。因此,p62可作为炎症衰老的有效抑制剂,减少氧化应激和促炎信号。这样的作用机制使该蛋白成为实验室动物和宠物中退行性疾病和癌症发展的有效监测指标。本综述总结了目前关于p62作为细胞和组织代谢的分子枢纽以及在各种炎症性疾病和其他病理状况中的活性研究结果。它还特别探讨了外源性p62(DNA质粒)作为抗炎和稳态调节剂在治疗动物骨质疏松症、代谢综合征以及年龄相关性黄斑变性和癌症方面的应用,以及p62质粒在其他炎症相关疾病中的可能应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/61ef/9025487/f10a8fcff6d2/life-12-00539-g001.jpg

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