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Type IV collagen is a novel DEJ biomarker that is reduced by radiotherapy

机译:IV型胶原蛋白是一种新型的DEJ生物标志物,可通过放疗减少

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The dental basement membrane (BM) is composed of collagen types IV, VI, VII, and XVII, fibronectin, and laminin and plays an inductive role in epithelial-mesenchymal interactions during tooth development. The BM is degraded and removed during later-stage tooth morphogenesis; however, its original position defines the location of the dentin-enamel junction (DEJ) in mature teeth. We recently demonstrated that type VII collagen is a novel component of the inner enamel organic matrix layer contiguous with the DEJ. Since it is frequently co-expressed with and forms functional complexes with type VII collagen, we hypothesized that type IV collagen should also be localized to the DEJ in mature human teeth. To identify collagen IV, we first evaluated defect-free erupted teeth from various donors. To investigate a possible stabilizing role, we also evaluated extracted teeth exposed to high-dose radiotherapy - teeth that manifest post-radiotherapy DEJ instability. We now show that type IV collagen is a component within the morphological DEJ of posterior and anterior teeth from individuals aged 18 to 80 yr. Confocal microscopy revealed that immunostained type IV collagen was restricted to the 5- to 10-μm-wide optical DEJ, while collagenase treatment or previous in vivo tooth-level exposure to > 60 Gray irradiation severely reduced immunoreactivity. This assignment was confirmed by Western blotting with whole-tooth crown and enamel extracts. Without reduction, type IV collagen contained macromolecular α-chains of 225 and 250 kDa. Compositionally, our results identify type IV collagen as the first macromolecular biomarker of the morphological DEJ of mature teeth. Given its network structure and propensity to stabilize the dermal-epidermal junction, we propose that a collagen-IV-enriched DEJ may, in part, explain its well-known fracture toughness, crack propagation resistance, and stability. In contrast, loss of type IV collagen may represent a biochemical rationale for the DEJ instability observed following oral cancer radiotherapy.
机译:牙齿基底膜(BM)由IV,VI,VII和XVII型胶原,纤连蛋白和层粘连蛋白组成,并在牙齿发育过程中在上皮-间质相互作用中起诱导作用。 BM在后期牙齿形态发生过程中被降解和去除;但是,它的原始位置定义了成熟牙中牙本质-牙釉质结合部(DEJ)的位置。我们最近证明,VII型胶原蛋白是与DEJ相邻的内部搪瓷有机基质层的新型成分。由于它经常与VII型胶原蛋白共表达并与功能性复合物形成复合物,因此我们假设IV型胶原蛋白也应在成熟的人牙中定位于DEJ。为了鉴定胶原蛋白IV,我们首先评估了来自各种供体的无缺陷爆发牙齿。为了研究可能的稳定作用,我们还评估了暴露于大剂量放疗的拔牙-放疗后DEJ不稳定性的牙齿。我们现在显示,IV型胶原蛋白是年龄在18至80岁之间的前后牙形态DEJ中的一个组成部分。共聚焦显微镜显示,免疫染色的IV型胶原蛋白仅限于5至10μm宽的光学DEJ,而胶原酶处理或先前体内的牙齿水平暴露于> 60 Gray辐射则严重降低了免疫反应性。通过用全齿冠和牙釉质提取物进行的蛋白质印迹法证实了这种归属。未经还原,IV型胶原含有225和250 kDa的大分子α链。从结构上讲,我们的结果确定IV型胶原蛋白是成熟牙齿形态DEJ的第一个大分子生物标记。考虑到其网络结构和稳定真皮-表皮连接的倾向,我们建议富含胶原蛋白IV的DEJ可以部分解释其众所周知的断裂韧性,抗裂纹扩展性和稳定性。相反,IV型胶原蛋白的损失可能代表了口腔癌放疗后观察到的DEJ不稳定性的生化原理。

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