Abstract
Complex dietary carbohydrate structures including β(1–4) galacto-oligosaccharides (GOS) are resistant to digestion in the upper gastrointestinal (GI) tract and arrive intact to the colon where they benefit the host by selectively stimulating microbial growth. Studies have reported the beneficial impact of GOS (alone or in combination with other prebiotics) by serving as metabolic substrates for modulating the assembly of the infant gut microbiome while reducing GI infections. N-Acetyl-D-lactosamine (LacNAc, Galβ1,4GlcNAc) is found in breast milk as a free disaccharide. This compound is also found as a component of human milk oligosaccharides (HMOs), which have repeating and variably branched lactose and/or LacNAc units, often attached to sialic acid and fucose monosaccharides. Human glycosyl-hydrolases do not degrade most HMOs, indicating that these structures have evolved as natural prebiotics to drive the proper assembly of the infant healthy gut microbiota. Here, we sought to develop a novel enzymatic method for generating LacNAc-enriched GOS, which we refer to as humanized GOS (hGOS). We showed that the membrane-bound β-hexosyl transferase (rBHT) from Hamamotoa (Sporobolomyces) singularis was able to generate GOS and hGOS from lactose and N-Acetyl-glucosamine (GlcNAc). The enzyme catalyzed the regio-selective, repeated addition of galactose from lactose to GlcNAc forming the β-galactosyl linkage at the 4-position of the GlcNAc and at the 1-position of D-galactose generating, in addition to GOS, LacNAc, and Galactosyl-LacNAc trisaccharides which were produced by two sequential transgalactosylations. Humanized GOS is chemically distinct from HMOs, and its effects in vivo have yet to be determined. Thus, we evaluated its safety and demonstrated the prebiotic's ability to modulate the gut microbiome in 6-week-old C57BL/6J mice. Longitudinal analysis of gut microbiome composition of stool samples collected from mice fed a diet containing hGOS for 5 weeks showed a transient reduction in alpha diversity. Differences in microbiome community composition mostly within the Firmicutes phylum were observed between hGOS and GOS, compared to control-fed animals. In sum, our study demonstrated the biological synthesis of hGOS, and signaled its safety and ability to modulate the gut microbiome in vivo, promoting the growth of beneficial microorganisms, including Bifidobacterium and Akkermansia.
Highlights
Gut microbial communities play a critical role in the maintenance of host health [1, 2]
Prebiotics, including GOS, are selectively fermented by gut microorganisms and promote the growth of beneficial microorganisms when consumed in adequate amounts [16, 17]
We report the biological synthesis of hGOS enriched in LacNAc and determined its lack of adverse effects by determining the impact of feeding on the gut microbiome of healthy 6-week-old C57BL/6J mice in comparison with defined control and GOS-containing diets
Summary
Gut microbial communities play a critical role in the maintenance of host health [1, 2]. In previous studies we evaluated highly pure β(1–4) galactooligosaccharides (GOS) formulations produced by the optimized version of the hexosyl-transferase gene from Hamamotoa (Sporobolomyces) singularis heterologously expressed in Komagataella (Pichia) pastoris [13, 14]. This enzyme is one of the most promising catalysts in the field of glycobiology due to its high stability, highly desirable enzymatic properties, and the metabolism of its reaction products (GOS) by specific members of the gut microbial community, impacting its composition and function [15, 16]. Short-chain fatty acids (SCFAs) generated as the result of GOS assimilation include acetate and lactate [17], which community members, including Roseburia and Faecalibacterium, can transform into butyrate [6, 19]
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