Laboratory of Cytoskeleton and Cilia Biology, Nencki Institute of Experimental Biology, Polish Academy of Sciences, 3 Pasteur Street, 02-093 Warsaw, Poland.
Faculty of Chemistry, University of Warsaw, 1 Pasteur Street, 02-093 Warsaw, Poland.
Int J Mol Sci. 2022 Feb 3;23(3):1749. doi: 10.3390/ijms23031749.
Primary ciliary dyskinesia (PCD) is a hereditary genetic disorder caused by the lack of motile cilia or the assembxly of dysfunctional ones. This rare human disease affects 1 out of 10,000-20,000 individuals and is caused by mutations in at least 50 genes. The past twenty years brought significant progress in the identification of PCD-causative genes and in our understanding of the connections between causative mutations and ciliary defects observed in affected individuals. These scientific advances have been achieved, among others, due to the extensive motile cilia-related research conducted using several model organisms, ranging from protists to mammals. These are unicellular organisms such as the green alga , the parasitic protist , and free-living ciliates, and , the invertebrate , and vertebrates such as zebrafish, , and mouse. Establishing such evolutionarily distant experimental models with different levels of cell or body complexity was possible because both basic motile cilia ultrastructure and protein composition are highly conserved throughout evolution. Here, we characterize model organisms commonly used to study PCD-related genes, highlight their pros and cons, and summarize experimental data collected using these models.
原发性纤毛运动障碍(PCD)是一种遗传性遗传疾病,由缺乏运动纤毛或功能失调的纤毛组装引起。这种罕见的人类疾病影响每 10000-20000 人中的 1 人,由至少 50 个基因的突变引起。在过去的二十年中,在鉴定 PCD 致病基因方面取得了重大进展,我们对致病突变与受影响个体中观察到的纤毛缺陷之间的联系有了更好的理解。这些科学进展除其他外,是由于使用几种模式生物(从原生动物到哺乳动物)进行了广泛的与运动纤毛相关的研究而实现的。这些模式生物包括单细胞生物,如绿藻、寄生原生动物和自由生活的纤毛虫,以及无脊椎动物和脊椎动物,如斑马鱼、鸡和老鼠。之所以能够建立具有不同细胞或身体复杂性水平的这种进化上相距甚远的实验模型,是因为基本的运动纤毛超微结构和蛋白质组成在整个进化过程中都高度保守。在这里,我们描述了常用于研究 PCD 相关基因的模式生物,突出了它们的优缺点,并总结了使用这些模型收集的实验数据。
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