Peptide ligands for a sugar-binding protein isolated from a random peptide library.

Oldenburg, Kevin R.; Loganathan, Duraikkannu; Goldstein, Irwin J.; Schultz, Peter G.; Gallop, Mark A.

doi:10.1073/pnas.89.12.5393

Cited by 249 publications

(124 citation statements)

References 42 publications

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“…The fact that peptides can mimic carbohydrates in their binding to target proteins has been first demonstrated by Oldenburg and colleagues (43). Given the diverse potential applications of such peptides, a significant number of mimetics have been described since.…”

Section: Discussionmentioning

confidence: 99%

Structural Basis of GD2 Ganglioside and Mimetic Peptide Recognition by 14G2a Antibody

Horwacik

Golik

Grudnik

et al. 2015

Molecular & Cellular Proteomics

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Monoclonal antibodies targeting GD2 ganglioside (GD2)have recently been approved for the treatment of high risk neuroblastoma and are extensively evaluated in clinics in other indications. This study illustrates how a therapeutic antibody distinguishes between different types of gangliosides present on normal and cancer cells and informs how synthetic peptides can imitate ganglioside in its binding to the antibody. Using high resolution crystal structures we demonstrate that the ganglioside recognition by a model antibody (14G2a) is based primarily on an extended network of direct and water molecule mediated hydrogen bonds. Comparison of the GD2-Fab structure with that of a ligand free antibody reveals an induced fit mechanism of ligand binding. These conclusions are validated by directed mutagenesis and allowed structure guided generation of antibody variant with improved affinity toward GD2. Contrary to the carbohydrate, both evaluated mimetic peptides utilize a "key and lock" interaction mechanism complementing the surface of the antibody binding groove exactly as found in the empty structure. The interaction of both peptides with the Fab relies considerably on hydrophobic contacts however, the detailed connections differ significantly between the peptides. As such, the evaluated peptide carbohydrate mimicry is defined primarily in a functional and not in structural manner. Molecular & Cellular

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Section: Discussionmentioning

confidence: 99%

Structural Basis of GD2 Ganglioside and Mimetic Peptide Recognition by 14G2a Antibody

Horwacik

Golik

Grudnik

et al. 2015

Molecular & Cellular Proteomics

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“…It is a technique to define peptides mimicking natural epitopes, including carbohydrate structures [34][35][36]. Phage display peptide libraries consist of filamentous phage particles displaying random peptides of defined length on their surface.…”

Section: Discussionmentioning

confidence: 99%

Induction of IgG antibodies against the GD2 carbohydrate tumor antigen by vaccination with peptide mimotopes

et al. 2006

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The disialoganglioside GD2, a carbohydrate antigen, is expressed on all tumors of neuroectodermal origin, including melanoma, neuroblastoma, sarcoma and small cell lung cancer. Due to its specific expression on tumor surfaces, GD2 is an attractive target for immunotherapies. The mouse/human chimeric anti-GD2 mAb ch14.18 is already applied in melanoma and neuroblastoma trials as a passive immunotherapy. To establish an active immunotherapy alternative, we aimed to replace the poorly immunogenic ganglioside with immunogenic peptides. Previously, we used the ch14.18 antibody to select GD2 peptide mimics from a phage display library. In the present study, two mimics of the ch14.18 epitope were coupled to keyhole limpet hemocyanin and used for immunizing BALB/c mice. Induction of a specific humoral immune response towards the original antigen GD2, both purified and expressed on neuroblastoma and melanoma cells, could be demonstrated in ELISA, Western blot, and immunofluorohistochemistry. As the elicited antibodies were of the IgG isotype, the mimotope conjugates were capable of recruiting T cell help and inducing memory phenomena. In conclusion, we show that an epitope of the carbohydrate antigen GD2 can successfully be translated into immunogenic peptide mimotopes. Our immunization experiments indicate that GD2 mimotopes are suitable for active immunotherapy of GD2-expressing tumors.

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“…Methyl a-D-mannopyranoside and a dodecapeptide (DVFYPY-PYASGS) known to bind Con A with comparable affinities have been studied extensively as a model system to address molecular mimicry in the humoral immune response (17)(18)(19). Polyclonal sera generated against methyl a-D-mannopyranoside cross-recognize the dodecapeptide, and correspondingly antipeptide sera cross-react with the mannopyranoside (20).…”

mentioning

confidence: 99%

Structural Evaluation of a Mimicry-Recognizing Paratope: Plasticity in Antigen–Antibody Interactions Manifests in Molecular Mimicry

Tapryal

Gaur

Kaur

et al. 2013

The Journal of Immunology

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Molecular mimicry manifests antagonistically with respect to the specificity of immune recognition. However, it often occurs because different Ags share surface topologies in terms of shape or chemical nature. It also occurs when a flexible paratope accommodates dissimilar Ags by adjusting structural features according to the antigenic epitopes or differential positioning in the Ag combining site. Toward deciphering the structural basis of molecular mimicry, mAb 2D10 was isolated from a maturing immune response elicited against methyl α-d-mannopyranoside and also bound equivalently to a dodecapeptide. The physicochemical evidence of this carbohydrate–peptide mimicry in the case of mAb 2D10 had been established earlier. These studies had strongly suggested direct involvement of a flexible paratope in the observed mimicry. Surprisingly, comparison of the Ag-free structure of single-chain variable fragment 2D10 with those bound to sugar and peptide Ags revealed a conformationally invariant state of the Ab while binding to chemically and structurally disparate Ags. This equivalent binding of the two dissimilar Ags was through mutually independent interactions, demonstrating functional equivalence in the absence of structural correlation. Thus, existence of a multispecific, mature Ab in the secondary immune response was evident, as was the plasticity in the interactions while accommodating topologically diverse Ags. Although our data highlight the structural basis of receptor multispecificity, they also illustrate mechanisms adopted by the immune system to neutralize the escape mutants generated during pathogenic insult.

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Peptide ligands for a sugar-binding protein isolated from a random peptide library.

Cited by 249 publications

References 42 publications

Structural Basis of GD2 Ganglioside and Mimetic Peptide Recognition by 14G2a Antibody

Structural Basis of GD2 Ganglioside and Mimetic Peptide Recognition by 14G2a Antibody

Induction of IgG antibodies against the GD2 carbohydrate tumor antigen by vaccination with peptide mimotopes

Structural Evaluation of a Mimicry-Recognizing Paratope: Plasticity in Antigen–Antibody Interactions Manifests in Molecular Mimicry

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