Department of Surgery, Children's Hospital Boston, Boston, MA 02115, USA.
Front Biosci (Landmark Ed). 2011 Jan 1;16(4):1574-88. doi: 10.2741/3806.
The anthrax toxin receptors tumor endothelial marker-8 (TEM-8) and capillary morphogenesis gene-2 (CMG-2) are responsible for allowing entry of anthrax toxin into host cells. These receptors were first discovered due to their enhanced expression on endothelial cells undergoing blood vessel growth or angiogenesis in model systems. Inhibition of angiogenesis is an important strategy for current anti-cancer therapies and treatment of retinal diseases. Functional roles for TEM-8 and CMG-2 in angiogenesis have recently emerged. TEM-8 appears to regulate endothelial cell migration and tubule formation whereas a role for CMG-2 in endothelial proliferation has been documented. TEM-8 and CMG-2 bind differentially to extracellular matrix proteins including collagen I, collagen IV and laminin and these properties may be responsible for their apparent roles in regulating endothelial cell behavior during angiogenesis. TEM-8-binding moieties have also been suggested to be useful in selectively targeting anti-angiogenic and anti-tumorigenic therapies to tumor endothelium. Additionally, studies of modified forms of lethal toxin (LeTx) have demonstrated that targeted inhibition of MAPKs within tumor vessels may represent an efficacious anti-angiogenic strategy.
炭疽毒素受体肿瘤内皮标志物-8(TEM-8)和毛细血管形态发生基因-2(CMG-2)负责允许炭疽毒素进入宿主细胞。这些受体最初是由于它们在模型系统中血管生长或血管生成过程中内皮细胞的表达增强而被发现的。抑制血管生成是当前抗癌疗法和治疗视网膜疾病的重要策略。TEM-8 和 CMG-2 在血管生成中的功能作用最近已经出现。TEM-8 似乎调节内皮细胞迁移和小管形成,而 CMG-2 在内皮细胞增殖中的作用已被记录在案。TEM-8 和 CMG-2 以不同的方式结合细胞外基质蛋白,包括胶原蛋白 I、胶原蛋白 IV 和层粘连蛋白,这些特性可能是它们在调节血管生成过程中内皮细胞行为方面的明显作用的原因。TEM-8 结合部分也被认为可用于将抗血管生成和抗肿瘤治疗选择性靶向肿瘤内皮细胞。此外,对修饰形式的致死毒素(LeTx)的研究表明,靶向抑制肿瘤血管内的 MAPKs 可能代表一种有效的抗血管生成策略。
