Small Molecules as Structural and Functional Mimics of Sialyl Lewis X Tetrasaccharide in Selectin Inhibition:  A Remarkable Enhancement of Inhibition by Additional Negative Charge and/or Hydrophobic Group

Wong, Chi‐Huey; Morís-Varas, Francisco; Hung, Shang‐Cheng; Marron, Thomas G.; Lin, Chun-Cheng; Gong, KeWei; Weitz‐Schmidt, Gabriele

doi:10.1021/ja970920q

Cited by 96 publications

(50 citation statements)

References 8 publications

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“…In this case, it would be necessary for the PLD to recognize more than four sugar residues to distinguish between HNK-1-reactive glycolipids and glycoproteins. This seems unlikely, because functional groups of carbohydrate determinants interacting with selectins are restricted to the three terminal sugar residues (39,40 (43)(44)(45)(46). On the other hand, neural glycoproteins that carry HNK-1 carbohydrates are not mucin-type glycoproteins, and therefore presumably are incapable of sustaining high affinity interactions.…”

Section: Discussionmentioning

confidence: 99%

The Proteoglycan Lectin Domain Binds Sulfated Cell Surface Glycolipids and Promotes Cell Adhesion

Miura

Aspberg

Ethell

et al. 1999

Journal of Biological Chemistry

107

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The lecticans are a group of chondroitin sulfate proteoglycans characterized by the presence of C-type lectin domains. Despite the suggestion that their lectin domains interact with carbohydrate ligands, the identity of such ligands has not been elucidated. We previously showed that brevican, a nervous system-specific lectican, binds the surface of B28 glial cells (Yamada, H., Fredette, B., Shitara, K., Hagihara, K., Miura, R., Ranscht, B., Stallcup, W. B., and Yamaguchi, Y. (1997) J. Neurosci. 17, 7784 -7795). In this paper, we demonstrate that two classes of sulfated glycolipids, sulfatides and HNK-1-reactive sulfoglucuronylglycolipids (SGGLs), act as cell surface receptors for brevican. The lectin domain of brevican binds sulfatides and SGGLs in a calcium-dependent manner as expected of a C-type lectin domain. Intact, full-length brevican also binds both sulfatides and SGGLs. The lectin domain immobilized as a substrate supports adhesion of cells expressing SGGLs or sulfatides, which was inhibited by monoclonal antibodies against these glycolipids or by treatment of the substrate with SGGLs or sulfatides. Our findings demonstrate that the interaction between the lectin domains of lecticans and sulfated glycolipids comprises a novel cell substrate recognition system, and suggest that lecticans in extracellular matrices serve as substrate for adhesion and migration of cells expressing these glycolipids in vivo.The lecticans are a family of chondroitin sulfate proteoglycans (CSPGs) 1 characterized by the presence of a C-type lectin domain in their core proteins (1, 2). The C-terminal globular domains of lecticans, or "proteoglycan lectin domain" (PLD), consist of one or two epidermal growth factor (EGF)-like domains, a C-type lectin domain, and a complement regulatory protein (CRP) domain. This arrangement of domains is similar to that of selectins, suggesting that lecticans are also involved in the recognition of carbohydrate ligands.Lecticans are the most abundantly expressed family of proteoglycans in the nervous system. The lectican family includes aggrecan (3), versican (4), neurocan (5), and brevican (6), all of which are expressed in the nervous system at certain stages of development (1, 7). Although aggrecan and versican were initially characterized as connective tissue proteoglycans, their expression in the nervous system has been demonstrated in a number of reports (8 -12). Brevican and neurocan are specifically expressed in the nervous system (6, 13-15). Structural similarities with selectins and the abundant expression in the nervous system suggest that lecticans play major roles in carbohydrate recognition in the nervous system.The identity of the ligand to PLDs has been a focus of our interest. We previously showed that the PLD of versican binds tenascin-R, an extracellular matrix (ECM) protein predominantly expressed in the nervous system (16). More recently, we demonstrated that the PLDs of all lecticans bind tenascin-R, and that brevican and tenascin-R indeed form a complex in adult rat brain e...

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Section: Discussionmentioning

confidence: 99%

The Proteoglycan Lectin Domain Binds Sulfated Cell Surface Glycolipids and Promotes Cell Adhesion

Miura

Aspberg

Ethell

et al. 1999

Journal of Biological Chemistry

107

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“…Glycosyl donor 9 was also synthesized from phenyl 1-thio--D-galactopyranoside (7). 10) After the C4 and C6 alcohols in 7 had been simultaneously protected in the form of p-methoxyphenylmethylidene acetal, 11) the remaining C2 and C3 alcohols were transformed into MPM ethers with MPMBr/NaH to afford 8 in 69% yield in two steps. Treatment of 8 with NBS under the aqueous condition hydrolyzed the phenylthio acetal to provide the corresponding hemiacetal, which was further converted into -trichloroacetimidate 9 according to Schmidt's protocol.…”

Section: Resultsmentioning

confidence: 99%

Synthesis ofD-Trigalacturonic Acid Methylglycoside and Conformational Comparison with Its Sulfur Analogue

Yamamoto

Sato

Ishimori

et al. 2008

Bioscience, Biotechnology, and Biochemistry

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“…The tetrasaccharide did not block the sLe a -polymer/P-selectin and the HL-60 cell/P-selectin interaction up to 3 mM. Investigation of sLe x -related compounds including mannose-based derivatives (9,11) and fucopeptides (10,12) further proved that the sLe a -polymer-based E-, P-, and L-selectin assays are suitable for the rapid determination of the selectivity profile of selectin antagonists.…”

Section: Fig 4 Structures Of Slementioning

confidence: 97%

“…Inhibitors with IC 50 values in the low micromolar and high nanomolar range were identified (9,10). The activity profile of FM233 (Fig.…”

Section: Identification Of P-selectin Inhibitorsmentioning

confidence: 99%

“…Analogous to the E-selectin assay we have developed two ELISA-type assays which quantify the binding of sLe a -polymer to immobilized P-and Lselectin. The P-selectin assay was successfully applied to identify novel P-selectin antagonists (9,10). The E-, P-, and L-selectin assays were utilized to determine the selectivity profile of sLe x and other sLe x -related compounds (9 -12).…”

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confidence: 99%

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Selectin/Glycoconjugate Binding Assays for the Identification and Optimization of Selectin Antagonists

Weitz‐Schmidt

Gong

Wong

1999

Analytical Biochemistry

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Small Molecules as Structural and Functional Mimics of Sialyl Lewis X Tetrasaccharide in Selectin Inhibition: A Remarkable Enhancement of Inhibition by Additional Negative Charge and/or Hydrophobic Group

Cited by 96 publications

References 8 publications

The Proteoglycan Lectin Domain Binds Sulfated Cell Surface Glycolipids and Promotes Cell Adhesion

The Proteoglycan Lectin Domain Binds Sulfated Cell Surface Glycolipids and Promotes Cell Adhesion

Synthesis ofD-Trigalacturonic Acid Methylglycoside and Conformational Comparison with Its Sulfur Analogue

Selectin/Glycoconjugate Binding Assays for the Identification and Optimization of Selectin Antagonists

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