Elastin-Derived Peptides: Matrikines Critical for Glioblastoma Cell Aggressiveness in a 3-D System

被引:49
作者
Coquerel, Berenice [1 ]
Poyer, Florent [1 ]
Torossian, Frederic [1 ]
Dulong, Virginie [2 ]
Bellon, Georges [3 ]
Dubus, Isabelle [1 ]
Reber, Annie [1 ]
Vannier, Jean-Pierre [1 ]
机构
[1] Univ Rouen, Fac Med & Pharm, Grp Rech Microenvironm & Renouvellement Cellulair, MERCI UPRES EA3829, F-76183 Rouen, France
[2] Univ Rouen, CNRS, Lab PBM, UMR 6522, F-76821 Mont St Aignan, France
[3] Univ Reims, Fac Med, CNRS, Lab Biochim & Biol Mol,CHU Reims,UMR 6237, F-51095 Reims, France
关键词
glioma aggressiveness; elastin-derived peptide; 3-D culture system; EXTRACELLULAR-MATRIX; BETA-GALACTOSIDASE; SPLICED VARIANT; GLIOMA INVASION; BINDING PROTEIN; GROWTH; MODEL; PROLIFERATION; DEGRADATION; MECHANISMS;
D O I
10.1002/glia.20884
中图分类号
Q189 [神经科学];
学科分类号
071006 [神经生物学];
摘要
In the most common primary brain tumors, malignant glioma cells invade the extracellular matrix (ECM) and proliferate rapidly in the cerebral tissue, which is mainly composed of hyaluronan (HA) along with the elastin present in the basement membrane of blood vessels. To determine the role of ECM components in the invasive capacity of glioma cell lines, we developed a 3-D cell-culture system, based on a hydrogel in which HA can be coreticulated with kappa-elastin (HA-kappa E). Using this system, the invasiveness of cells from four glioma cell lines was dramatically increased by the presence of kappa E and a related, specific peptide (VGVAPG)(3). In addition, MMP-2 secretion increased and MMP-12 synthesis occurred. Extracellular injections of kappa E or (VGVAPG)(3) provoked a pronounced and dose-dependent increase in [Ca2+](i). kappa E significantly enhanced the expression of the genes encoding elastin-receptor and tropoelastin. We propose the existence of a positive feedback loop in which degradation of elastin generates fragments that stimulate synthesis of tropoelastin followed by further degradation as well as migration and proliferation of the very cells responsible for degradation. All steps in this ECM-based loop could be blocked by the addition of either of the EBP antagonists, lactose, and V-14 peptide, suggesting that the loop itself should be considered as a new therapeutic target. (C) 2009 Wiley-Liss, Inc.
引用
收藏
页码:1716 / 1726
页数:11
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