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I 型胶原α2 链的柔韧性对胶原酶切割的影响。

Effects of flexibility of the α2 chain of type I collagen on collagenase cleavage.

机构信息

Department of Chemistry, Tufts University, Medford, MA, USA.

Department of Biomedical Engineering, Tufts University, Medford, MA, USA.

出版信息

J Struct Biol. 2018 Sep;203(3):247-254. doi: 10.1016/j.jsb.2018.05.002. Epub 2018 May 12.

Abstract

Cleavage of collagen by collagenases such as matrix metalloproteinase 1 (MMP-1) is a key step in development, tissue remodeling, and tumor proliferation. The abundant heterotrimeric type I collagen composed of two α1(I) chains and one α2(I) chain is efficiently cleaved by MMP-1 at a unique site in the triple helix, a process which may be initiated by local unfolding within the peptide chains. Atypical homotrimers of the α1(I) chain, found in embryonic and cancer tissues, are very resistant to MMP cleavage. To investigate MMP-1 cleavage, recombinant homotrimers were constructed with sequences from the MMP cleavage regions of human collagen chains inserted into a host bacterial collagen protein system. All triple-helical constructs were cleaved by MMP-1, with α2(I) homotrimers cleaved efficiently at a rate similar to that seen for α1(II) and α1(III) homotrimers, while α1(I) homotrimers were cleaved at a much slower rate. The introduction of destabilizing Gly to Ser mutations within the human collagenase susceptible region of the α2(I) chain did not interfere with MMP-1 cleavage. Molecular dynamics simulations indicated a greater degree of transient hydrogen bond breaking in α2(I) homotrimers compared with α1(I) homotrimers at the MMP-1 cleavage site, and showed an extensive disruption of hydrogen bonding in the presence of a Gly to Ser mutation, consistent with chymotrypsin digestion results. This study indicates that α2(I) homotrimers are susceptible to MMP-1, proves that the presence of an α1(I) chain is not a requirement for α2(I) cleavage, and supports the importance of local unfolding of α2(I) in collagenase cleavage.

摘要

胶原酶(如基质金属蛋白酶 1 [MMP-1])对胶原的裂解是发育、组织重塑和肿瘤增殖的关键步骤。富含的三聚体 I 型胶原由两条 α1(I)链和一条 α2(I)链组成,可被 MMP-1 在三螺旋的独特位点有效裂解,这一过程可能是由肽链内的局部展开引发的。在胚胎组织和癌组织中发现的 α1(I)链的非典型三聚体对 MMP 裂解非常具有抗性。为了研究 MMP-1 裂解,将来自人胶原链 MMP 裂解区的序列插入宿主细菌胶原蛋白系统中,构建了重组的同源三聚体。所有三螺旋结构均被 MMP-1 裂解,α2(I)三聚体的裂解效率很高,与 α1(II)和 α1(III)三聚体的裂解速率相似,而 α1(I)三聚体的裂解速率则慢得多。在人胶原酶敏感区的 α2(I)链中引入不稳定的 Gly 到 Ser 突变,不会干扰 MMP-1 裂解。分子动力学模拟表明,在 MMP-1 裂解位点,α2(I)三聚体比 α1(I)三聚体的瞬时氢键断裂程度更大,并且在存在 Gly 到 Ser 突变时氢键的破坏非常广泛,与糜蛋白酶消化结果一致。这项研究表明,α2(I)三聚体易受 MMP-1 的影响,证明 α1(I)链的存在不是 α2(I)裂解的必要条件,并支持 α2(I)在胶原酶裂解中局部展开的重要性。

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