Critical Role of Flanking Residues in NGR-to-isoDGR Transition and CD13/Integrin Receptor Switching

Curnis, Flavio; Cattaneo, Angela; Longhi, Renato; Sacchi, Angela; Gasparri, Anna Maria; Pastorino, Fabio; Matteo, P. Di; Traversari, Catia; Bachi, Ángela; Ponzoni, Mirco; Rizzardi, Gian Paolo; Corti, Angelo

doi:10.1074/jbc.m109.044297

Cited by 79 publications

(112 citation statements)

References 37 publications

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“…3B). Competitive binding experiments, performed either with the isoDGR peptide capable to bind the RGD binding pocket of integrins (12) or with the control ARA peptide, showed that the isoDGR peptide could abolish the binding of oxidized-aged Cp to the ␣v␤6 integrin (Student's t test, p Ͻ 0.0001) (Fig. 3C), supporting the role of Cp NGR deamidation in the acquisition of binding activity after aging.…”

Section: Accelerated Aging Of Cp Under Oxidative Conditions Causesmentioning

confidence: 81%

Oxidation-induced Structural Changes of Ceruloplasmin Foster NGR Motif Deamidation That Promotes Integrin Binding and Signaling

Barbariga

Curnis

Spitaleri

et al. 2014

Journal of Biological Chemistry

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Background: Asparagine deamidation at Asn-Gly-Arg (NGR) sites leads to the isoAsp-Gly-Arg (isoDGR) integrin-binding motif formation. Results: Ceruloplasmin (Cp), which contains two NGR sites and is oxidized in cerebrospinal fluid (CSF) in neurodegenerative diseases, can, undergo oxidation-induced structural changes fostering NGR deamidation with gain of integrin binding and signaling properties, in vitro and ex vivo in pathological CSF. Conclusion: Cp NGR motifs can deamidate acquiring integrin-binding functions. Significance: Cp structural changes favor NGR deamidation.

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Section: Accelerated Aging Of Cp Under Oxidative Conditions Causesmentioning

confidence: 81%

Oxidation-induced Structural Changes of Ceruloplasmin Foster NGR Motif Deamidation That Promotes Integrin Binding and Signaling

Barbariga

Curnis

Spitaleri

et al. 2014

Journal of Biological Chemistry

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“…Cyclic peptides of different ring sizes (15 < n < 18 atoms) were designed based on previous studies. 13,19,20 The smallest ring size (n=15) is that of 3, (2)) were prepared that were successfully applied previously for drug targeting. 33,34 An alternative synthetic route for 1 is proposed here.…”

Section: Discussionmentioning

confidence: 99%

“…43 However, the receptor recognition of isoDGR peptides highly depends on their structure. 13,44 Our objective was to evaluate the 3D structure, the chemo-stability as well as the in vitro interaction of these peptide models. For such study, cell adhesion was monitored as one of the most…”

Section: Cyclic Ngr-peptides Effect On Cell Adhesionmentioning

confidence: 99%

“…30,31 By comparing c [CNGRC] and GNGRG, a cyclic and a linear peptide, not only the higher CD13 binding affinity of cyclic variant was detected but also its increased stability in PBS solution (half-lives were [6][7][8] h and 3-4 h, respectively at pH 7.3, 37°C) and in serum (5 h and 3 h, respectively) was measured. 13 However, chemo-stability of NGR-peptides under relevant biological conditions is not studied.…”

Section: Introductionmentioning

confidence: 99%

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Development of Cyclic NGR Peptides with Thioether Linkage: Structure and Dynamics Determining Deamidation and Bioactivity

Enyedi¹,

Czajlik

Knapp³

et al. 2015

J. Med. Chem.

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Abstract AbstractIn drug targeting NGR-peptides recognized by CD13 receptors on tumor neovasculature have got improved interest. Here we present the synthesis and structure analysis of novel thioether linked cyclic NGR-peptides. We found that chemo-stability (resistance against spontaneous decomposition forming isoAsp and Asp derivatives) strongly depends both on sample handling conditions and structural properties. Significant correlation was found between chemo-stability and structural measures: e.g. NH Gly …CO Asn-sc distances. Side chain orientation of Asn is the key determining factor, if turned away from HN Gly chemo-stability increases. Structure stabilizing factors (e.g. H-bond(s)) lower their internal dynamics and thus macromolecules become even more resistant against spontaneous decomposition. Effect of cyclic NGR-peptides on cell adhesion was examined on A2058 melanoma cell lines. It was found that some of them gradually increased the cell adhesion with long term characteristics indicating the time-dependent formation of integrin binding isoAsp derivatives, responsible for the adhesion inducing effect.

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“…This pattern of expression may due to the fact that during tumor progression endothelial cells and pericytes are differently exposed or susceptible to the angiogenic factors known to regulate CD13. 23 To investigate the interaction between the CNGRCG peptide and CD13 in vivo, the CNGRCGVRSSSRTPSDKY peptide, corresponding to the 17 N-terminal amino acids of the NGR-TNF, was conjugated to quantum dots (hereafter reported as NGR-Qd) 24 and injected in 9 weeks old RIP1-Tag2 mice, during the angiogenic switch stage. Specimens of fresh pancreas were then analyzed by ex vivo whole mount histology.…”

Section: Identification and Localization Of Cd13mentioning

confidence: 99%

The tumor vessel targeting agent NGR-TNF controls the different stages of the tumorigenic process in transgenic mice by distinct mechanisms

et al. 2015

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NGR-TNF is a vascular targeting agent in advanced clinical development, coupling tumor necrosis factor-a (TNF) with the CNGRCG peptide, which targets a CD13 isoform specifically expressed by angiogenic vessels. Antitumor efficacy of NGR-TNF has been described in different transplantation tumor models. Nevertheless, the mechanism underlying its activity is not fully understood. In the wild type and in the immunodeficient (RAG ¡/¡ ) RIP1-Tag2 models of multistage pancreatic carcinogenesis, we demonstrate that CD13 is highly expressed on endothelial cells of hyperplastic and angiogenic islets, whereas its expression is down regulated in tumors where it partially colocalize with pericytes. In vivo CNGRCG peptides coupled to fluorescent nanoparticles (quantum dots) bind to CD13 and colocalize with anti-CD31, in pancreatic islets. At early stage, low doses of NGR-murine (m)TNF have a direct cytotoxic effect inducing endothelial cell apoptosis, reducing vessel density and eventually inhibiting the development of angiogenic islets. At a later stage, NGRmTNF is able to reduce tumor growth inducing vascular normalization, exclusively when treatment is carried out in the immunocompetent mice. Interestingly, NGR-mTNF-treated tumors from these mice are characterized by CD8 C T cell infiltration. At molecular level, overexpression of genes involved in vessels normalization was detected only in NGRmTNF-treated tumors from immunocompetent mice.These findings identified a new mechanism of action of NGR-mTNF, providing support for the development of new therapeutic strategies combining chemotherapy or active/adoptive immunotherapies to low dose NGR-TNF treatment.

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Critical Role of Flanking Residues in NGR-to-isoDGR Transition and CD13/Integrin Receptor Switching

Cited by 79 publications

References 37 publications

Oxidation-induced Structural Changes of Ceruloplasmin Foster NGR Motif Deamidation That Promotes Integrin Binding and Signaling

Oxidation-induced Structural Changes of Ceruloplasmin Foster NGR Motif Deamidation That Promotes Integrin Binding and Signaling

Development of Cyclic NGR Peptides with Thioether Linkage: Structure and Dynamics Determining Deamidation and Bioactivity

The tumor vessel targeting agent NGR-TNF controls the different stages of the tumorigenic process in transgenic mice by distinct mechanisms

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