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米诺地尔对赖氨酰羟化酶1、2和3的基因表达具有不同的抑制作用:对胶原蛋白交联和纤维化治疗的影响

Minoxidil exerts different inhibitory effects on gene expression of lysyl hydroxylase 1, 2, and 3: implications for collagen cross-linking and treatment of fibrosis.

作者信息

Zuurmond Anne-Marie, van der Slot-Verhoeven Annemarie J, van Dura Ernst A, De Groot Jeroen, Bank Ruud A

机构信息

TNO Quality of Life, Biomedical Research, Department of Tissue Repair, P.O. Box 2215, 2301 CE Leiden, The Netherlands.

出版信息

Matrix Biol. 2005 Jun;24(4):261-70. doi: 10.1016/j.matbio.2005.04.002.

Abstract

Collagen deposits in fibrotic lesions often display elevated levels of hydroxyallysine (pyridinoline) cross-links. The relation between the occurrence of pyridinoline cross-links and the irreversibility of fibrosis suggests that these cross-links contribute to the aberrant accumulation of collagen. Based on its inhibitory effect on lysyl hydroxylase activity minoxidil has been postulated to possess anti-fibrotic properties by limiting the hydroxylysine supply for hydroxyallysine cross-linking. However, to interfere with hydroxyallysine cross-linking specifically lysyl hydroxylation of the collagen telopeptide should be inhibited, a reaction predominantly catalysed by lysyl hydroxylase (LH) 2b. In this study, we demonstrate that minoxidil treatment of cultured fibroblasts reduces LH1>>LH2b>LH3 mRNA levels dose-and time-dependently, but has essentially no effect on the total number of pyridinoline cross-links in the collagen matrix. Still the collagen produced in the presence of minoxidil displays some remarkable features: hydroxylation of triple helical lysine residues is reduced to 50% and lysylpyridinoline cross-linking is increased at the expense of hydroxylysylpyridinoline cross-linking. These observations can be explained by our finding that LH1 mRNA levels are the most sensitive to minoxidil treatment, corroborating that LH1 has a preference for triple helical lysine residues as substrate. In addition, the non-proportional increase in cross-links (20-fold) with respect to the decrease in lysyl hydroxylation state of the triple helix (2-fold) even suggests that LH1 preferentially hydroxylates triple helical lysine residues at the cross-link positions. We conclude that minoxidil is unlikely to serve as an anti-fibroticum, but confers features to the collagen matrix, which provide insight into the substrate specificity of LH1.

摘要

纤维化病变中的胶原蛋白沉积物通常显示出高含量的羟赖氨醛(吡啶啉)交联。吡啶啉交联的出现与纤维化的不可逆性之间的关系表明,这些交联有助于胶原蛋白的异常积累。基于其对赖氨酰羟化酶活性的抑制作用,有人推测米诺地尔通过限制用于羟赖氨醛交联的羟赖氨酸供应而具有抗纤维化特性。然而,要特异性地干扰羟赖氨醛交联,应抑制胶原蛋白端肽的赖氨酰羟化,这一反应主要由赖氨酰羟化酶(LH)2b催化。在本研究中,我们证明米诺地尔处理培养的成纤维细胞会剂量和时间依赖性地降低LH1>>LH2b>LH3的mRNA水平,但对胶原蛋白基质中吡啶啉交联的总数基本没有影响。不过,在米诺地尔存在下产生的胶原蛋白仍表现出一些显著特征:三螺旋赖氨酸残基的羟化减少到50%,赖氨酰吡啶啉交联增加,而羟赖氨酰吡啶啉交联减少。这些观察结果可以用我们的发现来解释,即LH1的mRNA水平对米诺地尔处理最敏感,这证实了LH1优先选择三螺旋赖氨酸残基作为底物。此外,交联增加(20倍)与三螺旋赖氨酸羟化状态降低(2倍)之间的非比例关系甚至表明,LH1优先在交联位置羟化三螺旋赖氨酸残基。我们得出结论,米诺地尔不太可能用作抗纤维化药物,但赋予胶原蛋白基质一些特性,这有助于深入了解LH1的底物特异性。

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