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首页> 外文期刊>RSC Advances >Utilization of metabolic energy in treatment of ocular surface disorders: polyphosphate as an energy source for corneal epithelial cell proliferation
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Utilization of metabolic energy in treatment of ocular surface disorders: polyphosphate as an energy source for corneal epithelial cell proliferation

机译:用于治疗眼表面疾病的代谢能量:多磷酸盐作为角膜上皮细胞增殖的能源

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摘要

Impaired regeneration of the corneal epithelium, as found in many ocular surface diseases, is a major clinical problem in ophthalmology. We hypothesized that corneal epithelial regeneration can be promoted by the physiological, energy-delivering as well as "morphogenetically active" polymer, inorganic polyphosphate (polyP). Corneal limbal explants (diameter, 4 mm) were cultivated on collagen-coated well plates in the absence or presence of polyP (chain length, similar to 40 P-i units; 50 mu g ml(-1)) or human platelet lysate (hp-lysate; 5% v/v). Cell outgrowth and differentiation were analyzed after staining with DRAQ5 (nuclei) and rhodamine phalloidin (cytoskeleton), as well as by environmental scanning electron microscopy (ESEM). Cell growth/viability of hCECs was assessed by XTT assay. The expression of SDF-1 was quantitated by qRT-PCR. Exposure to hp-lysate (also containing polyP) increased cell migration already at day 1. Even stronger was the effect of polyP. This effect was blocked by a mast cell serine protease. The formation of cell multilayers was enhanced by hp-lysate or even more by polyP. ESEM revealed continuous cell junctions and prominent microvilli on the surface of adjacent cells exposed to polyP; those structures were only rarely seen in the controls. The hp-lysate and, more potently, polyP increased the proliferation of hCECs, as well as SDF-1 expression. The findings indicate the potential usefulness of the natural polymer, polyP, for topical treatment of corneal epithelial defects. Future studies are directed to develop suitable formulations of polyP, such as biomimetic polyP nano/microparticles showing an adjustable release kinetics.
机译:在许多眼部疾病中发现,角膜上皮的再生受损,是眼科的主要临床问题。我们假设角膜上皮再生可以通过生理,能量递送以及“形态学活性”聚合物,无机多磷酸(息肉)促进。在胶原蛋白涂层孔板上培养角膜缘外植体(直径,4毫米)在息肉或存在息肉(链长,类似于40 pi单元;50μgml(-1))或人血小板裂解物(HP-裂解物; 5%v / v)。用DRAQ5(核)和罗丹明氨基蛋白酶(细胞骨架)以及环境扫描电子显微镜(ESEM)染色术后分析细胞产物的产卵和分化。通过XTT测定评估HCEC的细胞生长/活力。通过QRT-PCR定量SDF-1的表达。暴露于HP-裂解物(也含有息肉)在第1天已经增加了细胞迁移。甚至更强是息肉的影响。这种效果被肥大细胞丝氨酸蛋白酶封闭。通过息肉通过HP裂解物或更多的细胞多层的形成。 ESEM在暴露于息肉的相邻电池表面上显示连续的细胞连接和显着的微血管;这些结构仅在对照中很少见到。 HP-裂解物和更棘手,息肉增加了HCEC的增殖,以及SDF-1表达。结果表明天然聚合物,息肉的潜在有用性,用于角膜上皮缺陷的局部处理。未来的研究旨在开发合适的息肉配方,例如染色息肉纳米/微粒,显示出可调节的释放动力学。

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  • 来源
    《RSC Advances》 |2019年第39期|共9页
  • 作者单位

    Johannes Gutenberg Univ Mainz Dept Ophthalmol Univ Med Ctr Johannes Gutenberg Langenbeckstr 1 D-55131 Mainz Germany;

    Johannes Gutenberg Univ Mainz ERC Adv Investigator Grant Res Grp Inst Physiol Chem Univ Med Ctr Duesbergweg 6 D-55128 Mainz Germany;

    Johannes Gutenberg Univ Mainz Inst Funct &

    Clin Anat Univ Med Ctr Johann Joachim Becher Weg 13 D-55099 Mainz Germany;

    Johannes Gutenberg Univ Mainz ERC Adv Investigator Grant Res Grp Inst Physiol Chem Univ Med Ctr Duesbergweg 6 D-55128 Mainz Germany;

    Johannes Gutenberg Univ Mainz ERC Adv Investigator Grant Res Grp Inst Physiol Chem Univ Med Ctr Duesbergweg 6 D-55128 Mainz Germany;

    Johannes Gutenberg Univ Mainz ERC Adv Investigator Grant Res Grp Inst Physiol Chem Univ Med Ctr Duesbergweg 6 D-55128 Mainz Germany;

    Johannes Gutenberg Univ Mainz Dept Ophthalmol Univ Med Ctr Johannes Gutenberg Langenbeckstr 1 D-55131 Mainz Germany;

    Johannes Gutenberg Univ Mainz ERC Adv Investigator Grant Res Grp Inst Physiol Chem Univ Med Ctr Duesbergweg 6 D-55128 Mainz Germany;

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  • 正文语种 eng
  • 中图分类 化学;
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