日本口腔診断学会雑誌
Online ISSN : 2188-2843
Print ISSN : 0914-9694
ISSN-L : 0914-9694
総説
Alarmin Interleukin-1αの機能について
浅野 正岳
著者情報
ジャーナル フリー

2020 年 33 巻 3 号 p. 189-194

詳細
抄録
Alarmins, also called danger-associated molecular patterns (DAMPs), are molecules that are rapidly released from necrotic cells. They serve as early warning signals for the surrounding cells and tissues and cause inflammatory reactions by accumulating immune cells, such as neutrophils and macrophages. This type of inflammation is called “sterile inflammation” and is not accompanied by infection with pathogenic organisms. Interleukin-1α (IL-1α) is a typical alarmin. Its precursor (pIL-1α) is synthesized inside the cell and enzymatically cleaved to generate N-terminal propiece IL-1α (ppIL-1α) and C-terminal mature IL-1α (mIL-1α). pIL-1α and ppIL-1α are preferentially localized in the nucleus due to the presence of nuclear localizing sequence (NLS). pIL-1α is cleaved by proteases such as calpain and secreted outside the cells where it functions as a cytokine by binding to IL-1 receptor type 1 (IL-1R1). Interestingly, pIL-1α is also released from damaged cells and binds to the same receptor. On the other hand, both pIL-1α and ppIL-1α contribute to the transcriptional regulation of some genes in the nucleus. Hence, based on these properties, IL-1α is recognized as a dual-functional cytokine. This review summarizes recent knowledge on the role of IL-1α as an alarmin.
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