Agnihotri R, Crawford H C, Haro H, Matrisian L M, Havrda M C, Liaw L
Center for Molecular Medicine, Maine Medical Center Research Institute, Scarborough, Maine 04074, USA.
J Biol Chem. 2001 Jul 27;276(30):28261-7. doi: 10.1074/jbc.M103608200. Epub 2001 May 25.
Osteopontin (OPN) is a secreted phosphoprotein shown to function in wound healing, inflammation, and tumor progression. Expression of OPN is often co-localized with members of the matrix metalloproteinase (MMP) family. We report that OPN is a novel substrate for two MMPs, MMP-3 (stromelysin-1) and MMP-7 (matrilysin). Three cleavage sites were identified for MMP-3 in human OPN, and two of those sites were also cleaved by MMP-7. These include hydrolysis of the human Gly166-Leu167, Ala201-Tyr202 (MMP-3 only), and Asp210-Leu211 peptide bonds. Only the N-terminal Gly-Leu cleavage site is conserved in rat OPN (Gly151-Leu152). These sites are distinct from previously reported cleavage sites in OPN for the proteases thrombin or enterokinase. We found evidence for the predicted MMP cleavage fragments of OPN in vitro in tumor cell lines, and in vivo in remodeling tissues such as the postpartum uterus, where OPN and MMPs are co-expressed. Furthermore, cleavage of OPN by MMP-3 or MMP-7 potentiated the function of OPN as an adhesive and migratory stimulus in vitro through cell surface integrins. We predict that interaction of MMPs with OPN at tumor and wound healing sites in vivo may be a mechanism of regulation of OPN bioactivity.
骨桥蛋白(OPN)是一种分泌型磷蛋白,在伤口愈合、炎症和肿瘤进展中发挥作用。OPN的表达常与基质金属蛋白酶(MMP)家族成员共定位。我们报告OPN是两种MMP(MMP-3(基质溶解素-1)和MMP-7(基质溶素))的新型底物。在人OPN中鉴定出MMP-3的三个切割位点,其中两个位点也被MMP-7切割。这些切割包括人Gly166-Leu167、Ala201-Tyr202(仅MMP-3)和Asp210-Leu211肽键的水解。在大鼠OPN中仅N端Gly-Leu切割位点保守(Gly151-Leu152)。这些位点与先前报道的OPN中凝血酶或肠激酶蛋白酶的切割位点不同。我们在体外肿瘤细胞系以及体内如产后子宫等重塑组织中发现了OPN预测的MMP切割片段的证据,在这些组织中OPN和MMP共表达。此外,MMP-3或MMP-7对OPN的切割通过细胞表面整合素增强了OPN在体外作为黏附及迁移刺激因子的功能。我们预测体内肿瘤和伤口愈合部位MMP与OPN的相互作用可能是调节OPN生物活性的一种机制。
