首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Collagen fibril assembly during postnatal development and dysfunctional regulation in the lumican-deficient murine cornea.
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Collagen fibril assembly during postnatal development and dysfunctional regulation in the lumican-deficient murine cornea.

机译:产后发育过程中的胶原蛋白原纤维组装以及在缺乏发光素的小鼠角膜中的功能失调。

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The transparent cornea is the outer barrier of the eye and is its major refractive surface. Development of a functional cornea requires a postnatal maturation phase involving development, growth and organization of the stromal extracellular matrix. Lumican, a leucine-rich proteoglycan, is implicated in regulating assembly of collagen fibrils and the highly organized extracellular matrix essential for corneal transparency. We investigated the regulatory role(s) of lumican in fibril assembly during postnatal corneal development using wild type (Lum+/+) and lumican-null (Lum-/-) mice. In Lum+/+ mice, a regular architecture of small-diameter fibrils is achieved in the anterior stroma by postnatal day 10 (P10), while the posterior stroma takes longer to reach this developmental maturity. Thus, the anterior and the posterior stroma follow distinct developmental timelines and may be under different regulatory mechanisms. In Lum-/- mice, it is the posterior stroma where abnormal lateral associations of fibrilsand thicker fibrils with irregular contours are evident as early as P10. In contrast, the anterior stroma is minimally perturbed by the absence of lumican. In Lum+/+ mice, lumican is expressed throughout the developing stroma at P10, with strong expression limited to the posterior stroma in the adult. Therefore, the posterior stroma, which is most vulnerable to lumican-deficiency, demonstrates an early developmental defect in fibril structure and architecture in the Lum-/- mouse. These defects underlie the reported increased light scattering and opacity detectable in the adult. Our findings emphasize the early regulation of collagen structure by lumican during postnatal development of the cornea.
机译:透明角膜是眼睛的外部屏障,是其主要的折射表面。功能性角膜的发育需要产后成熟期,其中涉及基质细胞外基质的发育,生长和组织。 Lumican是一种富含亮氨酸的蛋白聚糖,与调节胶原纤维和角膜透明度必不可少的高度组织化的细胞外基质的组装有关。我们调查了使用野生型(Lum + / +)和null的lumican-null(Lum-/-)小鼠在产后角膜发育过程中lumican在原纤维组装中的调节作用。在Lum + / +小鼠中,到出生后第10天(P10),在前间质中即可形成小直径原纤维的常规结构,而后间质要花费更长的时间才能达到这种发育成熟。因此,前基质和后基质的发育时间不同,可能处于不同的调节机制下。在Lum-/-小鼠中,最早是在P10时,在后基质中就可以看到原纤维的异常侧向结合以及轮廓不规则的较粗纤维的异常结合。相比之下,不存在lumican对前间质的影响最小。在Lum + / +小鼠中,Lumican在P10的整个发育中的基质中表达,在成年后基质中有很强的表达。因此,最容易发生lumican缺乏症的后基质显示Lum-/-小鼠的原纤维结构和结构的早期发育缺陷。这些缺陷是据报道成人中增加的光散射和不透明度的基础。我们的研究结果强调了卢米肯在角膜产后发育过程中对胶原蛋白结构的早期调节。

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