Issue 9, 2024

Breaking barriers: How modified citrus pectin inhibits galectin-8

Abstract

Inhibition of galectin-3-mediated interactions by modified citrus pectin (MCP) could affect several rate-limiting steps in cancer metastasis, but the ability of MCP to antagonize galectin-8 function remains unknown. We hypothesized that MCP could bind to galectin-8 in addition to galectin-3. In this study, a combination of gradual ethanol precipitation and DEAE-Sepharose Fast Flow chromatography was used to isolate several fractions from MCP. The ability of these fractions to antagonize galectin-8 function was studied as well as the primary structure and initial structure–function relationship of the major active component MCP-30–3. The results showed that MCP-30–3 (168 kDa) was composed of Gal (13.8%), GalA (63.1%), GlcA (13.0%), and Glc (10.1%). MCP-30–3 could specifically bind to galectin-8, with an MIC value of 0.04 mg mL−1. After MCP-30–3 was hydrolyzed by β-galactosidase or pectinase, its binding activity was significantly reduced. These results provide new insights into the interaction between MCP structure and galectin function, as well as the potential utility in the development of functional foods.

Graphical abstract: Breaking barriers: How modified citrus pectin inhibits galectin-8

Article information

Article type
Paper
Submitted
17 Jan 2024
Accepted
05 Apr 2024
First published
08 Apr 2024

Food Funct., 2024,15, 4887-4893

Breaking barriers: How modified citrus pectin inhibits galectin-8

M. Shuai, Y. Li, F. Guan, G. Fu, C. Sun, Q. Ren, L. Wang and T. Zhang, Food Funct., 2024, 15, 4887 DOI: 10.1039/D4FO00285G

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