Potent Angiogenesis Inhibition by the Particulate Form of Fullerene Derivatives

Meng, Huan; Xing, Gengmei; Sun, Baoyun; Zhao, Feng; Lei, Hao; Li, Wei; Song, Yan; Chen, Zhe; Yuan, Hui; Wang, Xuxia; Long, Jing; Chen, Chunying; Liang, Xing‐Jie; Zhang, Ning; Chai, Zhifang; Zhao, Yuliang

doi:10.1021/nn100448z

Cited by 152 publications

(144 citation statements)

References 38 publications

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“…Contrary to the traditional "molecular" form (one drug molecule only), the clustered binding to MMP-9 imposes the significance of the so-called "particulate" form (multiple molecules [Gd@C 82 (OH) 22 ] n ). A large surface area of the aggregate was proposed to attribute a wide range of inhibition of angiogenic factors [i.e., MMP-2/-9, VEGF, CXC chemokine ligand (Cxcl)1, and FGF6] at the mRNA level (16), as well as a more efficient blockage of tumor blood vessels of chaotic and disordered structures rather than the normal blood vessels under tight regulatory control (6).…”

Section: Resultsmentioning

confidence: 99%

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine

Kang

Zhou

Yang

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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203

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Pancreatic adenocarcinoma is the most lethal of the solid tumors and the fourth-leading cause of cancer-related death in North America. Matrix metalloproteinases (MMPs) have long been targeted as a potential anticancer therapy because of their seminal role in angiogenesis and extracellular matrix (ECM) degradation of tumor survival and invasion. However, the inhibition specificity to MMPs and the molecular-level understanding of the inhibition mechanism remain largely unresolved. Here, we found that endohedral metallofullerenol Gd@C 82 (OH) 22 can successfully inhibit the neoplastic activity with experiments at animal, tissue, and cellular levels. Gd@C 82 (OH) 22 effectively blocks tumor growth in human pancreatic cancer xenografts in a nude mouse model. Enzyme activity assays also show Gd@C 82 (OH) 22 not only suppresses the expression of MMPs but also significantly reduces their activities. We then applied large-scale molecular-dynamics simulations to illustrate the molecular mechanism by studying the Gd@C 82 (OH) 22 -MMP-9 interactions in atomic detail. Our data demonstrated that Gd@C 82 (OH) 22 inhibits MMP-9 mainly via an exocite interaction, whereas the wellknown zinc catalytic site only plays a minimal role. Steered by nonspecific electrostatic, hydrophobic, and specific hydrogen-bonding interactions, Gd@C 82 (OH) 22 exhibits specific binding modes near the ligand-specificity loop S1′, thereby inhibiting MMP-9 activity. Both the suppression of MMP expression and specific binding mode make Gd@C 82 (OH) 22 a potentially more effective nanomedicine for pancreatic cancer than traditional medicines, which usually target the proteolytic sites directly but fail in selective inhibition. Our findings provide insights for de novo design of nanomedicines for fatal diseases such as pancreatic cancer.indirect inhibition mode | tumor metastasis | antiangiogenesis |

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Section: Resultsmentioning

confidence: 99%

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine

Kang

Zhou

Yang

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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203

183

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“…In particular, Gadolinium (Gd) based metallofullerenes are developed as innovative contrast agents, and may also act as anti-cancer agents. Meng et al (56) found that Gd@C 82 (OH) 22 downregulated multiple angiogenic factors and in vivo studies using a MCF-7 human breast cancer xenograft model demonstrated that the metallofullerenol nanoparticles displayed anti-cancer efficacy comparable to the chemotherapeutic drug paclitaxel. In a subsequent study, the same nanoparticles were shown to inhibit cancer metastasis through matrix metalloproteinase (MMP) inhibition (57).…”

Section: The Other Side Of the Coin: Nanomedicinementioning

confidence: 99%

Keeping it small: towards a molecular definition of nanotoxicology

Gallud

Fadeel

2015

European Journal of Nanomedicine

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Abstract:In this essay, we offer the opinion that engineered nanomaterials are, by definition, materials that can interact with biological systems at the nanoscale, and that this very fact underlies both the promise and the peril of this multifaceted class of materials. Furthermore, nanomaterials are cloaked in host-derived proteins, lipids, or other biomolecules as they enter into a living organism and this so-called bio-corona may impact on subsequent interactions with biological structures. We will explore some examples of nanoscale effects of engineered nanomaterials, and discuss how such interactions may underpin toxicity, and, conversely, how nanoscale interactions may be harnessed for clinical applications, including the use of nanoparticles as drugs per se.Keywords: biological mimicry; cellular nanomachineries; engineered nanomaterials; molecular dynamics simulations; nanomedicine; nanotopographies; nanotoxicology. Life is a nanoscale phenomenonIn their seminal paper published one decade ago, Donaldson et al. (1) proposed that a new subcategory of toxicology -namely nanotoxicology -be defined to specifically address "the special problems likely to be caused by nanoparticles", and the authors suggested that nanotoxicology be considered "a new frontier in particle toxicology". However, one may argue, instead, that nanotoxicology represents a departure from the traditional toxicology of fine and ultrafine particles and fibers. In fact, nanotoxicology may be understood in light of "the interference of engineered nanomaterials with the functions of cellular and extracellular nanomachineries" (2). This view places emphasis on the fact that life (biology) is "a nanoscale phenomenon" (3). Indeed, living organisms are host to a range of dedicated intra-and extracellular nanoscale machines (4) and this, therefore, suggests that specific, size-dependent toxicities may ensue as a result of exposure to engineered nanomaterials. This does not, however, mean that all nanomaterials are inherently toxic (5), or that a nanospecific effect is necessarily detrimental to the host; in fact, the controlled manipulation of biological systems at the nanoscale may very well open up for novel therapeutic approaches. In this essay, we will explore both sides of the coin. The right size in nanotoxicologyIn his review on "the 'right' size in nanobiotechnology", Whitesides argued that "small" -both nano and micromust be a part of the future of biotechnology; which size is most important depends on what question one is asking (6). Surprisingly, in the field of nanotoxicology, the question of size, and more specifically, how one should define a nanomaterial (indeed, whether or not one should define nanomaterials in the first place) remains a matter of debate. Hence, while some have argued that we should not define nanomaterials, or to be more precise, that a 'one-size-fitsall' definition of nanomaterials will fail to capture what is important for addressing risk (7), others have stated that a definition of nanomaterials for regulatory ...

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“…This observation is consistent with the results from experiments with mice, which showed that the other form of carbon (endohedral fullerenes with encapsulated gadolinium) downregulates the expression of genes encoding the fibroblast growth factor family (FGF1, FGF3, and FGF6). 39 Furthermore, a decrease in bFGF expression after treatment with carbon nanotubes, fullerenes, or graphite has been reported in previous studies. 11 Observed results are also consistent with our previous study that showed that ND and GR cause a reduction in the concentration of bFGF in glioblastoma cultures in ovo.…”

mentioning

confidence: 56%

Carbon nanoparticles downregulate expression of basic fibroblast growth factor in the heart during embryogenesis

Wierzbicki¹,

Sawosz²,

Grodzik³

et al. 2013

IJN

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Potent Angiogenesis Inhibition by the Particulate Form of Fullerene Derivatives

Cited by 152 publications

References 38 publications

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine

Keeping it small: towards a molecular definition of nanotoxicology

Carbon nanoparticles downregulate expression of basic fibroblast growth factor in the heart during embryogenesis

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Potent Angiogenesis Inhibition by the Particulate Form of Fullerene Derivatives

Cited by 152 publications

References 38 publications

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C 82 (OH) 22 and its implication for de novo design of nanomedicine

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C 82 (OH) 22 and its implication for de novo design of nanomedicine

Keeping it small: towards a molecular definition of nanotoxicology

Carbon nanoparticles downregulate expression of basic fibroblast growth factor in the heart during embryogenesis

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Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine

Molecular mechanism of pancreatic tumor metastasis inhibition by Gd@C ₈₂ (OH) ₂₂ and its implication for de novo design of nanomedicine