Pseudoxanthoma Elasticum (PXE): Ultrastructural and Biochemical Study on Proteoglycan and Proteoglycan-Associated Material Produced by Skin Fibroblasts In Vitro

R. Tiozzo^costa , M. Baccarani Contri , M.R. Cingi , I. Pasquali^ronchetti , R. Salvini , S. Rindi , G. De Luca
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引用次数: 53

Abstract

Pseudoxanthoma elasticum is a genetic disease characterized by progressive mineralization of elastic fibers. Previous studies suggested that other components, apart from elastin, might be involved in the alterations of this connective tissue disorder (Martinez-Hernandez and Huf f er, 1974; Pasquali Ronchetti et al., 1981; 1986). Evidence is presented that proteoglycan metabolism is altered in PXE-affected patient. Urinary GAGs suggests an increased degradation of glucosamine-containing GAGs in the patient. Pulse and chase experiments on in vitro skin fibroblasts indicated a decreased rate of synthesis of 35SO4 containing GAGs or an increase of their turnover rate in PXE. Moreover, when PGs produced from skin fibroblasts were identified by ultracentrifugation and gel filtration in associative conditions, PXE fibroblasts produced a significantly higher amount of the high molecular weight fraction of sulfated PGs. This high molecular weight material was present both in the medium and in the matrix and disappeared under dissociative conditions or after treatment with hyaluronidase or with pancreas elastase. By electron microscopy, PXE fibroblasts appeared to produce and secrete an enormous amount of toluidine blue 0 positive material organized as filaments and amorphous masses. These data are in agreement with previous observations of the presence of abnormal masses of microfilaments, in the dermis of PXE patients, which were sensitive to hyaluronidase and partially to trypsin and elastase (Pasquali Ronchetti et al., 1986). The results seem to confirm that at least some of the alterations of connective tissues in PXE are due to abnormal PGs metabolism and to their tendency to form abnormal aggregates in the extracellular space.

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皮肤成纤维细胞体外产生蛋白聚糖及蛋白聚糖相关物质的超微结构和生化研究
弹性假黄瘤是一种以弹性纤维进行性矿化为特征的遗传性疾病。先前的研究表明,除了弹性蛋白外,其他成分可能参与这种结缔组织疾病的改变(Martinez-Hernandez and Huf er, 1974;Pasquali Ronchetti et al., 1981;1986)。有证据表明pxe患者的蛋白多糖代谢发生改变。尿中GAGs提示患者体内含有葡萄糖胺的GAGs降解增加。体外皮肤成纤维细胞的脉冲和追逐实验表明,PXE中含有GAGs的35SO4的合成速率降低或其周转率增加。此外,当通过超离心和凝胶过滤在相关条件下鉴定皮肤成纤维细胞产生的pg时,PXE成纤维细胞产生的高分子量硫酸pg含量显著增加。这种高分子量物质既存在于培养基中,也存在于基质中,在解离条件下或用透明质酸酶或胰腺弹性酶处理后消失。电镜下,PXE成纤维细胞产生并分泌大量的甲苯胺蓝0阳性物质,呈细丝状和无定形团块。这些数据与之前观察到的PXE患者真皮中存在异常的微丝团一致,这些微丝团对透明质酸酶敏感,部分对胰蛋白酶和弹性酶敏感(Pasquali Ronchetti et al., 1986)。结果似乎证实,PXE中结缔组织的至少一些改变是由于PGs代谢异常以及它们在细胞外空间形成异常聚集体的倾向。
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