Fields Gregg B
Florida Atlantic University, Department of Chemistry & Biochemistry, 5353 Parkside Drive, Building MC17, Jupiter, FL 33458, United States; The Scripps Research Institute/Scripps Florida, Department of Chemistry, 130 Scripps Way, Jupiter, FL 33458, United States; Torrey Pines Institute for Molecular Studies, Department of Chemistry, 11350 SW Village Parkway, Port St. Lucie, FL 34987, United States; Torrey Pines Institute for Molecular Studies, Department of Biology, 11350 SW Village Parkway, Port St. Lucie, FL 34987, United States.
Matrix Biol. 2015 May-Jul;44-46:239-46. doi: 10.1016/j.matbio.2015.01.002. Epub 2015 Jan 14.
The development of matrix metalloproteinase (MMP) inhibitors has often been frustrated by a lack of specificity and subsequent off-target effects. More recently, inhibitor design has considered secondary binding sites (exosites) to improve specificity. Small molecules and peptides have been developed that bind exosites in the catalytic (CAT) domain of MMP-13, the CAT or hemopexin-like (HPX) domain of MT1-MMP, and the collagen binding domain (CBD) of MMP-2 and MMP-9. Antibody-based approaches have resulted in selective inhibitors for MMP-9 and MT1-MMP that target CAT domain exosites. Triple-helical "mini-proteins" have taken advantage of collagen binding exosites, producing a family of novel probes. A variety of non-traditional approaches that incorporate exosite binding into the design process has yielded inhibitors with desirable selectivities within the MMP family.
基质金属蛋白酶(MMP)抑制剂的研发常常因缺乏特异性及随之产生的脱靶效应而受阻。最近,抑制剂设计开始考虑二级结合位点(别构位点)以提高特异性。已开发出能结合MMP - 13催化(CAT)结构域、MT1 - MMP的CAT或血色素结合蛋白样(HPX)结构域以及MMP - 2和MMP - 9的胶原结合结构域(CBD)中别构位点的小分子和肽。基于抗体的方法已产生针对CAT结构域别构位点的MMP - 9和MT1 - MMP选择性抑制剂。三螺旋“微型蛋白”利用了胶原结合别构位点,产生了一系列新型探针。多种将别构位点结合纳入设计过程的非传统方法已产生在MMP家族中具有理想选择性的抑制剂。
Zotero 插件