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Amelogenin processing by MMP-20 prevents protein occlusion inside calcite crystals

机译:MMP-20的Amelogenin加工可防止蛋白质闭塞在方解石晶体中

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摘要

Calcite crystals were grown in the presence of full-length amelogenin and during its proteolysis by recombinant human matrix metalloproteinase 20 (rhMMP-20). Recombinant porcine amelogenin (rP172) altered the shape of calcite crystals by inhibiting the growth of steps on the {104} faces and became occluded inside the crystals. Upon co-addition of rhMMP-20, the majority of the protein was digested resulting in a truncated amelogenin lacking the C-terminal segment. In rP172-rhMMP-20 samples, the occlusion of amelogenin into the calcite crystals was drastically decreased. Truncated amelogenin (rP147) and the 25-residue C-terminal domain produced crystals with regular shape and less occluded organic material. Removal of the C-terminal diminished the affinity of amelogenin to the crystals and therefore prevented occlusion. We hypothesize that HAP and calcite interact with amelogenin in a similar manner. In the case of each material, full-length amelogenin binds most strongly, truncated amelogenin binds weakly and the C-terminus alone has the weakest interaction. Regarding enamel crystal growth, the prevention of occlusion into maturing enamel crystals might be a major benefit resulting from the selective cleavage of amelogenin at the C-terminus by MMP-20. Our data have important implications for understanding the hypomineralized enamel phenotype in cases of amelogenesis imperfecta resulting from MMP-20 mutations and will contribute to the design of enamel inspired biomaterials.
机译:方解石晶体在全长釉蛋白原存在下并在其蛋白水解过程中通过重组人基质金属蛋白酶20(rhMMP-20)生长。重组猪牙釉蛋白(rP172)通过抑制{104}面上台阶的生长而改变了方解石晶体的形状,并被包藏在晶体内部。共添加rhMMP-20后,大部分蛋白质被消化,导致缺少C末端片段的截短的釉蛋白原。在rP172-rhMMP-20样品中,釉质生成素在方解石晶体中的吸留率大大降低。截短的釉质生成素(rP147)和25个残基的C末端结构域产生的晶体具有规则的形状和较少的有机物闭塞。 C-末端的去除减少了釉原蛋白对晶体的亲和力,因此防止了闭塞。我们假设HAP和方解石以类似方式与amelogenin相互作用。在每种材料中,全长釉生成素结合最强,截短的釉生成素结合很弱,仅C末端的相互作用最弱。关于牙釉质晶体的生长,防止MAGE-20在C端选择性分裂釉蛋白原可能是防止釉质晶体成熟的主要障碍。我们的数据对于理解由MMP-20突变引起的牙釉质发育不全的情况下理解矿化程度低的牙釉质表型具有重要意义,并将有助于珐琅质生物材料的设计。

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