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Developing a solid-phase method for the enzymatic synthesis of heparan sulfate and chondroitin sulfate backbones

https://doi.org/10.1093/glycob/cwad093

Stancanelli, Eduardo; Liu, Wei; Su, Guowei; Padagala, Vijay; Liu, Jian (February 2024, Glycobiology)

Abstract Despite the recent progress on the solution-phase enzymatic synthesis of heparan sulfate (HS) and chondroitin sulfate (CS), solid-phase enzymatic synthesis has not been fully investigated. Here, we describe the solid-phase enzymatic synthesis of HS and CS backbone oligosaccharides using specialized linkers. We demonstrate the use of immobilized HS linker to synthesize CS, and the use of immobilized CS linker to synthesize HS. The linkers were then digested with chondroitin ABCase and heparin lyases, respectively, to obtain the products. Our findings uncover a potential approach for accelerating the synthesis of structurally homogeneous HS and CS oligosaccharides.
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Host heparan sulfate promotes ACE2 super-cluster assembly and enhances SARS-CoV-2-associated syncytium formation

https://doi.org/10.1038/s41467-023-41453-w

Zhang, Qi; Tang, Weichun; Stancanelli, Eduardo; Jung, Eunkyung; Syed, Zulfeqhar; Pagadala, Vijayakanth; Saidi, Layla; Chen, Catherine Z.; Gao, Peng; Xu, Miao; et al (December 2023, Nature Communications)

Abstract SARS-CoV-2 infection causes spike-dependent fusion of infected cells with ACE2 positive neighboring cells, generating multi-nuclear syncytia that are often associated with severe COVID. To better elucidate the mechanism of spike-induced syncytium formation, we combine chemical genetics with 4D confocal imaging to establish the cell surface heparan sulfate (HS) as a critical stimulator for spike-induced cell-cell fusion. We show that HS binds spike and promotes spike-induced ACE2 clustering, forming synapse-like cell-cell contacts that facilitate fusion pore formation between ACE2-expresing and spike-transfected human cells. Chemical or genetic inhibition of HS mitigates ACE2 clustering, and thus, syncytium formation, whereas in a cell-free system comprising purified HS and lipid-anchored ACE2, HS stimulates ACE2 clustering directly in the presence of spike. Furthermore, HS-stimulated syncytium formation and receptor clustering require a conserved ACE2 linker distal from the spike-binding site. Importantly, the cell fusion-boosting function of HS can be targeted by an investigational HS-binding drug, which reduces syncytium formation in vitro and viral infection in mice. Thus, HS, as a host factor exploited by SARS-CoV-2 to facilitate receptor clustering and a stimulator of infection-associated syncytium formation, may be a promising therapeutic target for severe COVID.
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Chemoenzymatic Synthesis of Homogeneous Heparan Sulfate and Chondroitin Sulfate Chimeras

https://doi.org/10.1021/acschembio.2c00146

Stancanelli, Eduardo; Liu, Wei; Wander, Rylee; Li, Jine; Wang, Zhangjie; Arnold, Katelyn; Su, Guowei; Kanack, Adam; Pham, Truong Quang; Pagadala, Vijayakanth; et al (May 2022, ACS Chemical Biology)

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Structural and Substrate Specificity Analysis of 3- O -Sulfotransferase Isoform 5 to Synthesize Heparan Sulfate

https://doi.org/10.1021/acscatal.1c04520

Wander, Rylee; Kaminski, Andrea M.; Wang, Zhangjie; Stancanelli, Eduardo; Xu, Yongmei; Pagadala, Vijayakanth; Li, Jine; Krahn, Juno M.; Pham, Truong Quang; Liu, Jian; et al (December 2021, ACS Catalysis)

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