Laboratoire de Génétique Médicale UMRS1112, Centre de Recherche Biomédicale de Strasbourg, CRBS, Institut de Génétique Médicale d'Alsace, IGMA, Strasbourg 67000, France.
Cold Spring Harb Perspect Med. 2023 Jan 3;13(1):a041303. doi: 10.1101/cshperspect.a041303.
Retinal degeneration due to photoreceptor ciliary-related proteins dysfunction accounts for more than 25% of all inherited retinal dystrophies. The cilium, being an evolutionarily conserved and ubiquitous organelle implied in many cellular functions, can be investigated by way of many models from invertebrate models to nonhuman primates, all these models have massively contributed to the pathogenesis understanding of human ciliopathies. Taking the Bardet-Biedl syndrome (BBS) as an emblematic example as well as other related syndromic ciliopathies, the contribution of a wide range of models has enabled to characterize the role of the BBS proteins in the archetypical cilium but also at the level of the connecting cilium of the photoreceptors. There are more than 24 BBS genes encoding for proteins that form different complexes such as the BBSome and the chaperone proteins complex. But how they lead to retinal degeneration remains a matter of debate with the possible accumulation of proteins in the inner segment and/or accumulation of unwanted proteins in the outer segment that cannot return in the inner segment machinery. Many BBS proteins (but not the chaperonins for instance) can be modeled in primitive organisms such as , , , and These models have enabled clarifying the role of a subset of BBS proteins in the primary cilium as well as their relations with other modules such as the intraflagellar transport (IFT) module, the nephronophthisis (NPHP) module, or the Meckel-Gruber syndrome (MKS)/Joubert syndrome (JBTS) module mostly involved with the transition zone of the primary cilia. Assessing the role of the primary cilia structure of the connecting cilium of the photoreceptor cells has been very much studied by way of zebrafish modeling () as well as by a plethora of mouse models. More recently, large animal models have been described for three BBS genes and one nonhuman primate model in rhesus macaque for In completion to animal models, human cell models can now be used notably thanks to gene editing and the use of induced pluripotent stem cells (iPSCs). All these models are not only important for pathogenesis understanding but also very useful for studying therapeutic avenues, their pros and cons, especially for gene replacement therapy as well as pharmacological triggers.
由于光感受器纤毛相关蛋白功能障碍导致的视网膜变性占所有遗传性视网膜营养不良的 25%以上。纤毛作为一种进化上保守且普遍存在的细胞器,参与许多细胞功能,可以通过从无脊椎动物模型到非人类灵长类动物的多种模型进行研究,所有这些模型都为理解人类纤毛病的发病机制做出了巨大贡献。以 Bardet-Biedl 综合征 (BBS) 为例,以及其他相关的综合征性纤毛病,广泛的模型研究使人们能够描述 BBS 蛋白在典型纤毛中的作用,也能够描述其在光感受器连接纤毛中的作用。超过 24 个 BBS 基因编码形成不同复合物的蛋白质,如 BBSome 和伴侣蛋白复合物。但是,它们如何导致视网膜变性仍然存在争议,可能是由于内节中蛋白质的积累和/或外节中无法返回内节机制的无用蛋白质的积累。许多 BBS 蛋白(但不是伴侣蛋白)可以在原始生物中建模,如、、和。这些模型阐明了一组 BBS 蛋白在初级纤毛中的作用,以及它们与其他模块(如内纤毛运输 (IFT) 模块、肾单位-纤毛发育不全 (NPHP) 模块或 Meckel-Gruber 综合征 (MKS)/Joubert 综合征 (JBTS) 模块)的关系,这些模块主要与初级纤毛的过渡区有关。评估光感受器连接纤毛的初级纤毛结构的作用已通过斑马鱼建模 () 和大量的小鼠模型进行了大量研究。最近,已为三个 BBS 基因和一个非人类灵长类猕猴模型描述了大型动物模型。除了动物模型,现在还可以使用人类细胞模型,这要归功于基因编辑和诱导多能干细胞 (iPSC) 的使用。所有这些模型不仅对发病机制的理解很重要,而且对研究治疗方法也非常有用,特别是对基因替代疗法和药物触发剂。
