Suppression of Tumor Growth and Angiogenesis by a Specific Antagonist of the Cell-Surface Expressed Nucleolin

Destouches, Damien; Khoury, Diala El; Hamma-Kourbali, Yamina; Krust, Bernard; Albanese, Patricia; Katsoris, Panagiotis; Guichard, Gilles; Briand, Jean Paul; Courty, José; Hovanessian, Ara G.

doi:10.1371/journal.pone.0002518

Cited by 129 publications

(197 citation statements)

References 47 publications

(100 reference statements)

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“…A direct interaction between this acidic domain and ADAMTS-2 would not be surprising considering that ADAMTS-2 has affinity for the negatively charged heparin and HSPG and that the heparin-binding domain of endostatin is required for its efficient binding on the acidic domain of nucleolin. Moreover, a specific antagonist of cell-surface nucleolin reduces the phosphorylation of Erk1/2 within a few minutes and suppresses tumor growth and angiogenesis [45], two features also observed here for ADAMTS-2. The hypothesis that nucleolin is a receptor mediating the proapoptotic effect of ADAMTS-2 may seemed challenged by the observation that HEK 293-EBNA cells are not affected by ADAMTS-2 although they express nucleolin at their surface (not shown).…”

Section: Discussionsupporting

confidence: 73%

ADAMTS-2 functions as anti-angiogenic and anti-tumoral molecule independently of its catalytic activity

Dubail¹,

Kesteloot²,

Deroanne³

et al. 2010

Cell. Mol. Life Sci.

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ADAMTS-2 is a metalloproteinase that plays a key role in the processing of fibrillar procollagen precursors into mature collagen molecules by excising the amino-propeptide. We demonstrate that recombinant ADAMTS-2 is also able to reduce proliferation of endothelial cells, and to induce their retraction and detachment from the substrate resulting in apoptosis. Dephosphorylation of Erk1/2 and MLC largely precedes the ADAMTS-2 induced morphological alterations. In 3-D culture models, ADAMTS-2 strongly reduced branching of capillarylike structures formed by endothelial cells and their long-term maintenance and inhibited vessels formation in embryoid bodies (EB). Growth and vascularization of tumors formed in nude mice by HEK 293-EBNA cells expressing ADAMTS-2 were drastically reduced. A similar anti-tumoral activity was observed when using cells expressing recombinant deleted forms of ADAMTS-2, including catalytically inactive enzyme. Nucleolin, a nuclear protein also found to be associated with the cell membrane, was identified as a potential receptor mediating the antiangiogenic properties of ADAMTS-2.

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Section: Discussionsupporting

confidence: 73%

ADAMTS-2 functions as anti-angiogenic and anti-tumoral molecule independently of its catalytic activity

Dubail¹,

Kesteloot²,

Deroanne³

et al. 2010

Cell. Mol. Life Sci.

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“…This result appears consistent with our previous reports that gelonin is quite stable in fusions due to its structure [26,32] , which consequently contributes to the retention of its activity even after fusion with F3 peptide. To elucidate any anti-cancer targeting effects of F3-Gel or gelonin alone, for the in vitro cell experiments, we used HeLa, LnCaP, 9L, and U87 MG cancer cells because these cell lines were fully examined in other previous studies related to the F3 peptide [18,33] . In contrast to the equipotent intrinsic activity compared with unmodified gelonin in the cell-free conditions (Figure 2), in the U87 MG cell lines, F3-Gel exhibited a significantly greater ability to reduce the protein level to less than 50% than that of the gelonin ( Figure 5).…”

Section: Discussionmentioning

confidence: 99%

“…Nucleolin is known as a multifunctional DNA/RNA binding protein involved in regulation of gene transcription, chromatin remodeling, RNA metabolism, and ribosomal RNA synthesis [19] . Tumor cells with high proliferation rates are known to overexpress surface-associated nucleolins in addition to cytoplasmic and nuclear nucleolins, whereas normal cells express nucleolins in the cytoplasm and nuclear membrane [18] . Thus, surface nucleolins make tumor cells the preferential targets.…”

Section: Discussionmentioning

confidence: 99%

“…F3 is a 30-34-amino acid fragment of a high mobility group protein, HMG2N. Nucleolin is known to be highly expressed on the surface of tumor cells, whereas it is primarily expressed in the cytoplasm and nuclear membrane in normal cells, which might help to achieve selective drug targeting into the tumor site [18] . These receptor molecules expressed on the tumor cell surface are known to play an important role in facilitating the internalization of F3 peptide into tumor cells and transport into the cell nucleus.…”

Section: Introductionmentioning

confidence: 99%

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Molecular tumor targeting of gelonin by fusion with F3 peptide

2017

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Therapeutically potent macromolecular drugs have shown great promise for overcoming the limitations of small-molecule anti-cancer drugs. But tumor cell-selective intracellular delivery of the macromolecules remains a major hurdle for their successful clinical application. To overcome this challenge, we engineered a novel genetic fusion protein (F3-Gel) that composed of F3 peptide, a tumorhoming peptide, and gelonin, a plant-derived ribosome-inactivating protein (RIP), and then evaluated its anti-cancer activity in vitro and in vivo. The F3-Gel-encoding gene was synthesized by genetic recombination, and F3-Gel was successfully expressed in E coli. The anti-cancer activity of the produced F3-Gel was evaluated by various in vitro assays, which revealed that F3-Gel maintained equipotent protein synthesis inhibition activity (IC 50 =11 pmol/L) as unmodified gelonin (IC 50 =10 pmol/L). Furthermore, F3-Gel displayed enhanced cellular uptake into cancer cells (U87 MG, HeLa, LnCaP and 9L) than noncancerous cells (293 HEK and SVGp12). Compared with gelonin, F3-Gel exerted significantly higher cytotoxicity against these cancer cells. F3-Gel displayed significantly greater inhibition of protein translation in U87 MG cells: F3-Gel (0.5 μmol/L) was able to reduce the protein level to less than 50%, while gelonin (1 μmol/L) did not affect the intracellular protein level. In a U87 MG xenograft tumor-bearing mouse model, F3-Gel was accumulated in the tumor site at much higher levels and maintained for a prolonged time compared with gelonin. Administration of F3-Gel (0.5, 0.75 mol/kg, iv) caused 36% and 66%, respectively, inhibition of tumor growth in U87 MG xenograft mice, suggesting that it is a promising candidate drug for cancer treatment. Furthermore, this study demonstrates that fusion of F3 peptide to a potent macromolecule could provides an effective method for targeting tumors and eventually could improve their druggability.

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“…As explained above, the synthetic peptide HB-19 specifically antagonizes the C-terminal RGG domain of nucleolin and inhibits cell membrane-associated nucleolin function, thereby preventing the growth, angiogenesis and tumorigenicity of numerous cancer cells using different assays. 139,140 The V3 loop-mimicking pseudopeptide 5[Kpsi(CH2N)PR]-TASP binds to the cell-surface nucleolin in monocyte-derived macrophages and synergizes with the inhibitory effects of β-chemokines on HIV infection. 141 Another synthetic ligand targeting cell-surface nucleolin, N6L, also displays potent anti-tumor activities, enhances apoptosis, blocks angiogenesis and prevents tumor growth.…”

Section: Targeting Nucleolin For Therapymentioning

confidence: 99%