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 well-known 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.
Source: Molecular mechanism of
pancreatic tumor metastasis inhibition by Gd@C82(OH)22 and its implication for
de novo design of nanomedicine. Kang SG, Zhou G, Yang P, Liu Y, Sun B, Huynh T,
Meng H, Zhao L, Xing G, Chen C, Zhao Y, Zhou R. Proc Natl Acad Sci U S A. 2012
Sep 4
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