Undersulfated and Glycol-Split Heparins Endowed with Antiangiogenic Activity

Casu, Benito; Guerrini, Marco; Guglieri, Sara; Naggi, Annamaria; Perez, Marta; Torri, Giangiacomo; Cassinelli, Giuseppe; Ribatti, Doménico; Carminati, Paolo; Giannini, Giuseppe; Penco, Sergio; Pisano, Claudio; Belleri, Mirella; Rusnati, Marco; Presta, Marco

doi:10.1021/jm030893g

Cited by 78 publications

(96 citation statements)

References 47 publications

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“…When framing heparin sequences that bind FGF-2, glycol-split residues were shown not to impair the binding to FGF-2. However, they prevented activation of FGF-2 and FGF-2-induced angiogenic activity (37,38). The present study shows that glycol splitting enhances the heparanase-inhibiting activity of heparin.…”

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confidence: 50%

“…In the present study, relationships between structure and heparanase-inhibiting activity of heparin were studied using a larger number of heparins and heparin derivatives, including some with various degrees of 6-O-sulfation of GlcN and 2-O-sulfation of IdoA residues as well as "glycol-split" derivatives obtained by controlled periodate oxidation/borohydride reduction of natural (36) or partially 2-O-desulfated heparins (37,38). Glycol splitting of C-2-C-3 bonds of nonsulfated uronic acid residues was suggested to interfere with the biological interactions of heparin by providing flexible joints between protein binding sequences (37)(38)(39). When framing heparin sequences that bind FGF-2, glycol-split residues were shown not to impair the binding to FGF-2.…”

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confidence: 99%

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Modulation of the Heparanase-inhibiting Activity of Heparin through Selective Desulfation, Graded N-Acetylation, and Glycol Splitting

Naggi

Casu

Perez

et al. 2005

Journal of Biological Chemistry

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203

141

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Heparanase is an endo-␤-glucuronidase that cleaves heparan sulfate (HS) chains of heparan sulfate proteoglycans on cell surfaces and in the extracellular matrix (ECM). Heparanase, overexpressed by most cancer cells, facilitates extravasation of blood-borne tumor cells and causes release of growth factors sequestered by HS chains, thus accelerating tumor growth and metastasis. Inhibition of heparanase with HS mimics is a promising target for a novel strategy in cancer therapy. In this study, in vitro inhibition of recombinant heparanase was determined for heparin derivatives differing in degrees of 2-O-and 6-O-sulfation, N-acetylation, and glycol splitting of nonsulfated uronic acid residues. The contemporaneous presence of sulfate groups at O-2 of IdoA and at O-6 of GlcN was found to be non-essential for effective inhibition of heparanase activity provided that one of the two positions retains a high degree of sulfation. N-Desulfation/ N-acetylation involved a marked decrease in the inhibitory activity for degrees of N-acetylation higher than 50%, suggesting that at least one NSO 3 group per disaccharide unit is involved in interaction with the enzyme. On the other hand, glycol splitting of preexisting or of both preexisting and chemically generated nonsulfated uronic acids dramatically increased the heparanase-inhibiting activity irrespective of the degree of N-acetylation. Indeed N-acetylated heparins in their glycol-split forms inhibited heparanase as effectively as the corresponding N-sulfated derivatives. Whereas heparin and N-acetylheparins containing unmodified D-glucuronic acid residues inhibited heparanase by acting, at least in part, as substrates, their glycol-split derivatives were no more susceptible to cleavage by heparanase. Glycol-split N-acetylheparins did not release basic fibroblast growth factor from ECM and failed to stimulate its mitogenic activity. The combination of high inhibition of heparanase and low release/potentiation of ECM-bound growth factor indicates that N-acetylated, glycol-split heparins are potential antiangiogenic and antimetastatic agents that are more effective than their counterparts with unmodified backbones.

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confidence: 99%

Modulation of the Heparanase-inhibiting Activity of Heparin through Selective Desulfation, Graded N-Acetylation, and Glycol Splitting

Naggi

Casu

Perez

et al. 2005

Journal of Biological Chemistry

Self Cite

203

141

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“…Attempts to inhibit heparanase were initiated in parallel with the emergence clinical relevance of this activity, focusing on heparin and heparin mimetics, which bind heparanase with high affinity but serve as poor substrates (9,32). Two types of endogenous inhibitors of heparanase have so far been reported, namely disaccharide end products of HS cleavage (33) and highly basic proteins such as eosinophil major basic protein (34).…”

Section: Discussionmentioning

confidence: 99%

Heparanase 2 Interacts with Heparan Sulfate with High Affinity and Inhibits Heparanase Activity

Levy-Adam

Feld

Cohen-Kaplan

et al. 2010

Journal of Biological Chemistry

119

234

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Heparanase activity is highly implicated in cell dissemination associated with tumor metastasis, angiogenesis, and inflammation. Heparanase expression is induced in many hematological and solid tumors, associated with poor prognosis. Heparanase homolog, termed heparanase 2 (Hpa2), was cloned based on sequence homology. Detailed characterization of Hpa2 at the biochemical, cellular, and clinical levels has not been so far reported, and its role in normal physiology and pathological disorders is obscure. We provide evidence that unlike heparanase, Hpa2 is not subjected to proteolytic processing and exhibits no enzymatic activity typical of heparanase. Notably, the fulllength Hpa2c protein inhibits heparanase enzymatic activity, likely due to its high affinity to heparin and heparan sulfate and its ability to associate physically with heparanase. Hpa2 expression was markedly elevated in head and neck carcinoma patients, correlating with prolonged time to disease recurrence (follow-up to failure; p ‫؍‬ 0.006) and inversely correlating with tumor cell dissemination to regional lymph nodes (N-stage; p ‫؍‬ 0.03). Hpa2 appears to restrain tumor metastasis, likely by attenuating heparanase enzymatic activity, conferring a favorable outcome of head and neck cancer patients.

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“…[99] Astenose Adjuvant in cardiovascular intervention c [113] ROH Heparanase antiangiogenesis inhibitor b [114] ROH P selectin inhibitor [115] LAC-HP antimetastatic b [116] ROH Integrin-melanoma cell binding inhibitor a [117] ROH Antianemic as hepicdine inhibitor b [118] ROH Antinflammation-human elastase inhibitors a [118] gs-LMWH ORG 31733 HIV-1 and HIV-2 inhibitor a [120] SR 80258 Allergic airway response inhibitor b [121] Vasoflux Anticoagulant independent from AT activity, coadjuvant in myocardial infarction therapy d [108,109] NAC from Tinzaparin Antimetastatic b [122] gs-LMWH antimalarial, parasite adhesion, inhibitor b [44] DF01 -Tafoxiparin Labor pain attenuation d [111] M-402 Nocuparanib Metastasis and multiple pathway inhibitor d [110] DFX 232-Sevuparin Antimalarial, distrupting "Plasmodium falciparium" rosettes d [112]]-Preventive activity of vasoocclusion in sickle severe hereditary anemia d S-NACH Anticancer increasing tumor chemo-responsiveness c [35] gs-ULMWH RO-Fondaparinux Antinflammation b [123] Undersulfated RO ST1514" Antinflammatory -heparanase inhibitor b [124] Antiangiogenic, as FGF-2 and VEGF inhibitors b [125,126] N-acylated gs-heparins …”

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confidence: 99%