Structure-based design of UDP-GlcNAc analogs as candidate GnT-V inhibitors

基于结构的设计UDP-GlcNAc类似物作为GnT-V抑制剂候选物

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作者：Amol M Vibhute, Hide-Nori Tanaka, Sushil K Mishra, Reina F Osuka, Masamichi Nagae, Chizuko Yonekawa, Hiroaki Korekane, Robert J Doerksen, Hiromune Ando, Yasuhiko Kizuka

期刊：

Biochimica et Biophysica Acta-General Subjects

影响因子：

2.800

时间：

2022

起止号：

2022 Jun;1866(6):130118.

doi：

10.1016/j.bbagen.2022.130118

Background

N-Glycan branching regulates various functions of glycoproteins. N-Acetylglucosaminyltransferase V (GnT-V) is a GlcNAc transferase that acts on N-glycans and the GnT-V-producing branch is highly related to cancer progression. This indicates that specific GnT-V inhibitors may be drug candidates for cancer treatment. To design novel GnT-V inhibitors, we focused on the unique and weak recognition of the donor substrate UDP-GlcNAc by GnT-V. On the basis of the catalytic pocket structure, we hypothesized that UDP-GlcNAc analogs with increasing hydrophobicity may be GnT-V inhibitors.

Conclusions

Chemical modification of the donor substrate may be a promising strategy to develop selective inhibitors of GnT-V. General significance: Our findings provide new insights into the design of GnT inhibitors and how GnTs recognize the donor substrate.

Methods

We chemically synthesized 10 UDP-GlcNAc analogs in which one or two phosphate groups were replaced with hydrophobic groups. To test these compounds, we set up an HPLC-based enzyme assay system for all N-glycan-branching GlcNAc transferases in which GnT-I-V activity was measured using purified truncated enzymes. Using this system, we assessed the inhibitory effects of the synthesized compounds on GnT-V and their specificity.

Results

Several UDP-GlcNAc analogs inhibited GnT-V activity, although the inhibition potency was modest. Compared with other GnTs, these compounds showed a preference for GnT-V, which suggested that GnT-V was relatively tolerant of hydrophobicity in the donor substrate. Docking models of the inhibitory compounds with GnT-V suggested the mechanisms of how these compounds interacted with GnT-V and inhibited its action. Conclusions: Chemical modification of the donor substrate may be a promising strategy to develop selective inhibitors of GnT-V. General significance: Our findings provide new insights into the design of GnT inhibitors and how GnTs recognize the donor substrate.

Significance

Our findings provide new insights into the design of GnT inhibitors and how GnTs recognize the donor substrate.