Lysozymes are key antimicrobial peptides in the host innate immune system that protect against pathogen infection. In this study, the full-length cDNAs of two c-type lysozymes (gfLyz-C1 and gfLyz-C2) were cloned from goldfish (). The structural domains, three-dimensional structures, and amino acid sequences of gfLyz-C1 and gfLyz-C2 were highly comparable, as the two proteins shared 89.7% sequence identity. The gfLyz-C1 and gfLyz-C2 recombinant proteins were generated in the insoluble fractions of an system. Based on the results of lysoplate and turbidimetric assays, gfLyz-C1 and gfLyz-C2 showed broad-spectrum antimicrobial properties with high levels of activity against , , and , and relatively low activity against . Both and mRNAs were mainly expressed in the trunk kidney and head kidney, and was expressed at much higher levels than in the corresponding tissues. The expression of the and transcripts in the trunk kidney and head kidney was induced in these tissues by challenge with heat-inactivated and lipopolysaccharides (LPS), and the transcriptional responses of were more intense. In goldfish primary trunk kidney cells, the levels of the and transcripts were upregulated by heat-inactivated , , and , as well as LPS, and downregulated by treatment with dexamethasone and leptins. Overall, this study may provide new insights that will improve our understanding of the roles of c-type lysozymes in the innate immunity of cyprinid fish, including the structural and phylogenetic characteristics, antimicrobial effects, and regulatory mechanism.
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http://dx.doi.org/10.3390/ijms21020501 | DOI Listing |
Int J Mol Sci
January 2020
School of Stomatology and Medicine, School of Life Science and Engineering, Foshan University, Foshan 528000, China.
Lysozymes are key antimicrobial peptides in the host innate immune system that protect against pathogen infection. In this study, the full-length cDNAs of two c-type lysozymes (gfLyz-C1 and gfLyz-C2) were cloned from goldfish (). The structural domains, three-dimensional structures, and amino acid sequences of gfLyz-C1 and gfLyz-C2 were highly comparable, as the two proteins shared 89.
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