A novel role for β2-microglobulin: a precursor of antibacterial chemokine in respiratory epithelial cells

β2-微球蛋白的新作用:呼吸道上皮细胞中抗菌趋化因子的前体

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作者:Shean-Jaw Chiou, Chan-Chi Wang, Yan-Shen Tseng, Yen-Jung Lee, Shih-Chieh Chen, Chi-Hsien Chou, Lea-Yea Chuang, Yi-Ren Hong, Chi-Yu Lu, Chien-Chih Chiu, Michel Chignard

Abstract

We analyzed a panel of cationic molecules secreted in the culture medium of human respiratory epithelial cells (REC) upon activation by IL-1β and different pathogen-associated molecular patterns. A 9 kDa fragment derived from β2-microglobulin (B2M) was identified and named shed 9 kDa B2M (sB2M-9). The primary structure of sB2M-9 was revealed to increase its pI value that potentially could play an important role in innate defense. sB2M-9 exhibits antibacterial activity against Gram positive Staphylococcus aureus (SA) but not against Gram negative Klebsiella pneumonia (KP). Upon its binding to SA, sB2M-9 induces clumps, a phenomenon not observed with B2M. Migration of THP-1 monocytes exposed to SA clumps was significantly greater than that to SA without clumps. sB2M-9 binds to SA, more likely as a chemokine, to facilitate THP-1 migration. As a whole, we demonstrated that REC release a novel chemokine with antibacterial activity that is shed from B2M to facilitate THP-1 migration.

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