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潜伏转化生长因子-β结合蛋白 2 和 4 在微纤维发育中具有重要的重叠功能。

Latent TGF-β binding protein 2 and 4 have essential overlapping functions in microfibril development.

机构信息

Department of Pharmacology, Kansai Medical University, Osaka, 573-1010, Japan.

Department of Cardiology, Kansai Medical University, Osaka, 573-1010, Japan.

出版信息

Sci Rep. 2017 Mar 2;7:43714. doi: 10.1038/srep43714.

Abstract

Microfibrils are exracellular matrix components necessary for elastic fiber assembly and for suspending lenses. We previously reported that latent TGF-β binding protein 2 (LTBP-2), a microfibril-associated protein, is required for forming stable microfibril bundles in ciliary zonules. However, it was not understood why Ltbp2 null mice only showed an eye-specific phenotype, whereas LTBP-2 is abundantly expressed in other tissues containing microfibrils in wild type mice. Here, we show that LTBP-4, another microfibril-associated protein, compensates for the loss of LTBP-2 in microfibril formation. Ltbp2/4S double knockout (DKO) mice showed increased lethality due to emphysema, which was much more severe than that found in Ltbp4S null mice. Elastic fibers in the lungs of Ltbp2/4S DKO mice were severely disorganized and fragmented. Cultured mouse embryonic fibroblasts (MEFs) from Ltbp2/4S DKO embryos developed reduced microfibril meshwork in serum-free conditions, whereas the microfibril formation was restored by the addition of either recombinant LTBP-2 or -4. Finally, ectopic expression of LTBP-4 in the whole body restored ciliary zonule microfibril bundles in the eyes of Ltbp2 null mice. These data suggest that LTBP-2 and -4 have critical overlapping functions in forming the robust structure of microfibrils in vitro and in vivo.

摘要

微纤维是细胞外基质的组成部分,对于弹性纤维的组装和晶状体的悬浮是必需的。我们之前的研究报告表明,Latent TGF-β binding protein 2(LTBP-2),一种微纤维相关蛋白,对于睫状带的稳定微纤维束的形成是必需的。然而,尚不清楚为什么 Ltbp2 敲除小鼠仅表现出眼部特异性表型,而 LTBP-2 在野生型小鼠中含有微纤维的其他组织中大量表达。在这里,我们表明另一种微纤维相关蛋白 LTBP-4 可以补偿 LTBP-2 在微纤维形成中的缺失。Ltbp2/4S 双敲除(DKO)小鼠由于肺气肿导致的死亡率增加,比 Ltbp4S 敲除小鼠更为严重。Ltbp2/4S DKO 小鼠肺部的弹性纤维严重紊乱和碎片化。来自 Ltbp2/4S DKO 胚胎的培养的鼠胚胎成纤维细胞(MEFs)在无血清条件下发展出减少的微纤维网格,而添加重组 LTBP-2 或 -4 则恢复了微纤维的形成。最后,LTBP-4 的异位表达在 Ltbp2 敲除小鼠的整个身体中恢复了睫状带微纤维束。这些数据表明,LTBP-2 和 -4 在体外和体内形成稳健的微纤维结构方面具有关键的重叠功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/582a/5333096/241c80328f69/srep43714-f1.jpg

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