α4β7/α4β1Dual Integrin Antagonists Block α4β7-Dependent Adhesion under Shear Flow

Egger, Linda A.; Kidambi, Usha; Cao, Jun; Riper, Gail Van; McCauley, Ermengilda; Mumford, Richard A.; Amo, Suzanne; Lingham, Russell B.; Lanza, Thomas J.; Lin, Linus S.; Laszlo, Stephen E. de; Young, Darrin J.; Kopka, Ihor E.; Tong, Sharon; Pikounis, Bill; Benson, Evelyn E.; Warwood, S.J.; Bargatze, Robert F.; Schmidt, John A.; Detmers, Patricia A.

doi:10.1124/jpet.302.1.153

Cited by 9 publications

(9 citation statements)

References 31 publications

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“…Mouse anti-human CD29, HUTS-21(PE), isotype control (mouse IgG2a κ PE) clone G155-178 were purchased from BD Biosciences (San Jose, CA) and used according to manufacturer's instructions. 16 was synthesized by Dr. Wei Wang (Department of Chemistry, University of New Mexico). Two recently identifi ed VLA-4 ligands 3-(adamantane-1-carbonylamino)-3-(4-ethoxyphenyl) propanoic acid and 3-(adamantane-1-carbonylamino)-3-(4-propoxyphenyl) propanoic acid (SID: 14732971, CID: 5197400; and SID: 14732972, CID: 4329131) were from NIH molecular libraries small molecule repository (NIH MLSMR) (http://pubchem.ncbi.nlm.nih.gov/) curated by BioFocus/ DPI (South San Francisco, CA).…”

Section: Methodsmentioning

confidence: 99%

“…2C) is described in the literature as a potent ligand that blocks VLA-4 binding to vascular cell adhesion molecule 1 (VCAM-1). 11,16,24 Compounds D and E ( Fig. 2D and 2E) are two novel VLA-4 ligands discovered in a high-throughput screen at the University of New Mexico Center for Molecular Discovery (http://pubchem.ncbi.nlm.nih.gov, AID: 529, 702).…”

Section: Homology Modeling and Dockingmentioning

confidence: 99%

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Conformational mAb as a Tool for Integrin Ligand Discovery

Njus

Chigaev

Waller

et al. 2009

ASSAY and Drug Development Technologies

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alpha(4)beta(1)-Integrin (very late antigen-4 (VLA-4)) mediates cell adhesion to cell surface ligands (VCAM-1). Binding of VLA-4 to VCAM-1 initiates rolling and firm adhesion of leukocytes to vascular endothelium followed by the extravasation into the tissue. VLA-4-dependent adhesion plays a key role in controlling leukocyte adhesive events. Small molecules that bind to the integrin ligand-binding site and block its interaction with natural ligands represent promising candidates for treatment of several diseases. Following a flow cytometric screen for small molecule discovery, we took advantage of a conformationally sensitive anti-beta(1)-integrin antibody (HUTS-21) and a small LDV-containing ligand (LDV-FITC) with known affinity to study binding affinities of several known and recently discovered integrin ligands. We found that binding of the LDV-containing small molecule induced exposure of HUTS-21 epitope and that the EC(50) for antibody binding was equal to previously reported K(d) for fluorescent LDV (LDV-FITC). Thus, binding of HUTS-21 can be used to report ligand-binding site occupancy. We studied binding of two known integrin ligands (YLDV and TR14035), as well as of two novel compounds. EC(50) values for HUTS-21 binding showed good correlation with K(i)s determined in the competition assay with LDV-FITC for all ligands. A docking model suggests a common mode of binding for the small molecule VLA-4 ligands. This novel approach described here can be used to determine ligand-binding affinities for unlabeled integrin ligands, and can be adapted to a high-throughput screening format for identification of unknown integrin ligands.

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Section: Methodsmentioning

confidence: 99%

Section: Homology Modeling and Dockingmentioning

confidence: 99%

Conformational mAb as a Tool for Integrin Ligand Discovery

Njus

Chigaev

Waller

et al. 2009

ASSAY and Drug Development Technologies

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“…TR14035 (Fig. 1) has been reported to potently inhibit both ␣ 4 ␤ 1 and ␣ 4 ␤ 7 Sircar et al, 1999a,b;Egger et al, 2002), and this was confirmed (Table 1).…”

Section: Downloaded Frommentioning

confidence: 55%

“…Compound 2, a recently described ␣ 4 ␤ 1 antagonist (Hagmann et al, 2001), and compound 3, a structurally related analog, inhibited binding to both ␣ 4 ␤ 1 and ␣ 4 ␤ 7 (Table 1). An inactive analog, compound 4 (Hagmann et al, 2001;Egger et al, 2002), did not inhibit binding when tested at concentrations up to 100 M, demonstrating the importance of specific structural features to the activities of compounds 1, 2, and 3 (Kopka et al, 2002; Table 1). TR14035 (Fig.…”

Section: Downloaded Frommentioning

confidence: 99%

“…Small molecule antagonists of ␣ 4 ␤ 7 that mimic the LDT motif have been described that block the binding of ␣ 4 ␤ 7 -expressing cells to MAdCAM-Ig in the presence of Mn 2ϩ (Carson et al, 1997;Shroff et al, 1998;Martin et al, 1999;Harriman et al, 2000;Egger et al, 2002). Similarly, antagonists of ␣ 4 ␤ 1 have been reported to block binding of Mn 2ϩ -activated (Jackson et al, 1997;Vanderslice et al, 1997;Lin et al, 1998;Hagmann et al, 2001;Muller et al, 2001) and unactivated ␣ 4 ␤ 1 (Chen et al, 1999) to ligand in vitro.…”

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confidence: 99%

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