首页> 外文期刊>Virchows Archiv: an international journal of pathology >Immunohistochemical localization and mRNA expression of matrix Gla protein and fetuin-A in bone biopsies of hemodialysis patients.
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Immunohistochemical localization and mRNA expression of matrix Gla protein and fetuin-A in bone biopsies of hemodialysis patients.

机译:血液透析患者骨活检的免疫组织化学定位和基质Gla蛋白和胎球蛋白-A的mRNA表达。

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Matrix Gla protein (MGP) and fetuin-A are inhibitors of arterial calcifications. In blood of rats, calcium-phosphate-fetuin-MGP complexes, produced in bone, have been identified. Indeed, an association between bone resorption, release of such complexes, and arterial calcifications has been reported. We have investigated the synthesis and localization of fetuin-A and MGP in bone of hemodialysis patients and the possible contribution of bone cells in arterial calcifications. Bone biopsies from 11 hemodialysis patients were used for histology, in situ hybridization of fetuin-A and MGP messenger RNA (mRNA), immunohistochemistry of fetuin-A, and total, carboxylated, and non-carboxylated MGP proteins. Patients showed various types of renal osteodystrophy, or normal bone. MGP was synthesized and expressed (total and carboxylated) by osteoblasts, osteocytes, and most osteoclasts, while fetuin-A by osteoblasts and osteocytes. Fetuin-A and carboxylated MGP proteins were positive in the calcified matrix, while total MGP was negative. Osteoid seams were negative to fetuin-A, lightly positive to carboxylated MGP, and occasionally positive to total MGP. Undercarboxylated MGP was mostly undetectable. In adult humans, fetuin-A is produced also by osteoblasts, and not only by hepatocytes, as previously believed. MGP, essentially carboxylated, is synthesized by osteoblasts and most osteoclasts. Increased bone turnover can be an important contributor to arterial calcifications.
机译:基质Gla蛋白(MGP)和胎球蛋白A是动脉钙化的抑制剂。在大鼠血液中,已经鉴定出在骨骼中产生的磷酸钙-胎球蛋白-MGP复合物。实际上,已经报道了骨吸收,此类复合物的释放与动脉钙化之间的关联。我们已经研究了血液透析患者骨骼中胎球蛋白A和MGP的合成和定位,以及骨细胞在动脉钙化中的可能贡献。来自11名血液透析患者的骨活检用于组织学,胎球蛋白-A和MGP信使RNA(mRNA)的原位杂交,胎球蛋白-A的免疫组织化学以及总的,羧化的和非羧化的MGP蛋白。患者表现出各种类型的肾性骨营养不良或正常骨骼。 MGP由成骨细胞,成骨细胞和大多数破骨细胞合成并表达(全部和羧化),而胎球蛋白-A由成骨细胞和成骨细胞表达。 Fetuin-A和羧化的MGP蛋白在钙化基质中呈阳性,而总MGP呈阴性。类固醇接缝对胎球蛋白-A阴性,对羧化MGP轻微阳性,偶尔对总MGP阳性。羧基不足的MGP大多无法检测到。在成年人类中,胎蛋白-A也由成骨细胞产生,而不仅是由肝细胞产生,如先前所相信的。 MGP,基本上是羧化的,是由成骨细胞和大多数破骨细胞合成的。骨转换增加可能是动脉钙化的重要原因。

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