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使用角蛋白酶生成的 BKS-1(+)新表位对大鼠脊柱组织中的硫酸角质素进行免疫定位:表达模式与 II 类 SLRPs、 lumican 和 keratocan 的相关性。

Immunolocalization of Keratan Sulfate in Rat Spinal Tissues Using the Keratanase Generated BKS-1(+) Neoepitope: Correlation of Expression Patterns with the Class II SLRPs, Lumican and Keratocan.

机构信息

Bioimaging Research Hub, Cardiff School of Biosciences, Cardiff University, Cardiff CF10 3AX, Wales, UK.

Graduate School of Biomedical Engineering, University of New South Wales, Sydney 2052, NSW, Australia.

出版信息

Cells. 2020 Mar 30;9(4):826. doi: 10.3390/cells9040826.

Abstract

This study has identified keratan sulfate in fetal and adult rat spinal cord and vertebral connective tissues using the antibody BKS-1(+) which recognizes a reducing terminal N-acetyl glucosamine-6-sulfate neo-epitope exposed by keratanase-I digestion. Labeling patterns were correlated with those of lumican and keratocan using core protein antibodies to these small leucine rich proteoglycan species. BKS-1(+) was not immunolocalized in fetal spinal cord but was apparent in adult cord and was also prominently immunolocalized to the nucleus pulposus and inner annulus fibrosus of the intervertebral disc. Interestingly, BKS-1(+) was also strongly associated with vertebral body ossification centers of the fetal spine. Immunolocalization of lumican and keratocan was faint within the vertebral body rudiments of the fetus and did not correlate with the BKS-1(+) localization indicating that this reactivity was due to another KS-proteoglycan, possibly osteoadherin (osteomodulin) which has known roles in endochondral ossification. Western blotting of adult rat spinal cord and intervertebral discs to identify proteoglycan core protein species decorated with the BKS-1(+) motif confirmed the identity of 37 and 51 kDa BKS-1(+) positive core protein species. Lumican and keratocan contain low sulfation KS-I glycoforms which have neuroregulatory and matrix organizational properties through their growth factor and morphogen interactive profiles and ability to influence neural cell migration. Furthermore, KS has interactive capability with a diverse range of neuroregulatory proteins that promote neural proliferation and direct neural pathway development, illustrating key roles for keratocan and lumican in spinal cord development.

摘要

本研究使用识别由角蛋白酶 I 消化暴露的还原末端 N-乙酰氨基葡萄糖-6-硫酸新表位的抗体 BKS-1(+),鉴定了胎儿和成年大鼠脊髓和脊柱连接组织中的硫酸角质素。使用这些小富含亮氨酸的蛋白聚糖种类的核心蛋白抗体,将标记模式与 lumican 和 keratocan 的标记模式相关联。BKS-1(+) 在胎儿脊髓中未免疫定位,但在成年脊髓中明显存在,并且在椎间盘的髓核和内纤维环中也明显免疫定位。有趣的是,BKS-1(+) 也与胎儿脊柱的椎体骨化中心强烈相关。lumican 和 keratocan 在胎儿椎体原基中的免疫定位较弱,与 BKS-1(+)定位不相关,表明这种反应性是由于另一种 KS 蛋白聚糖,可能是骨粘连蛋白(骨调节素)所致,它在软骨内骨化中具有已知的作用。用 BKS-1(+) 基序标记鉴定成年大鼠脊髓和椎间盘的蛋白聚糖核心蛋白种类的 Western 印迹证实了 37 和 51 kDa BKS-1(+) 阳性核心蛋白种类的身份。Lumican 和 keratocan 含有低硫酸化的 KS-I 糖型,通过其生长因子和形态发生素相互作用谱以及影响神经细胞迁移的能力,具有神经调节和基质组织特性。此外,KS 具有与多种神经调节蛋白相互作用的能力,这些蛋白促进神经增殖并指导神经途径发育,表明 keratocan 和 lumican 在脊髓发育中具有关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99f0/7226845/eea0b2cf9b03/cells-09-00826-g001.jpg

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