Doherty Dan
University of Washington and Seattle Children's Hospital, Seattle, WA, USA.
Semin Pediatr Neurol. 2009 Sep;16(3):143-54. doi: 10.1016/j.spen.2009.06.002.
Joubert syndrome (JS) is a primarily autosomal recessive condition characterized by hypotonia, ataxia, abnormal eye movements, and intellectual disability with a distinctive mid-hindbrain malformation (the "molar tooth sign"). Variable features include retinal dystrophy, cystic kidney disease, liver fibrosis and polydactyly. Recently, substantial progress has been made in our understanding of the genetic basis of JS, including identification of seven causal genes (NPHP1, AHI1, CEP290, RPGRIP1L, TMEM67/MKS3, ARL13B and CC2D2A). Despite this progress, the known genes account for <50% of cases and few strong genotype-phenotype correlations exist in JS; however, genetic testing can be prioritized based on clinical features. While all seven JS genes have been implicated in the function of the primary cilium/basal body organelle (PC/BB), little is known about how the PC/BB is required for brain, kidney, retina and liver development/function, nor how disruption of PC/BB function leads to diseases of these organs. Recent work on the function of the PC/BB indicates that the organelle is required for multiple signaling pathways including sonic hedgehog, WNT and platelet derived growth factor. Due to shared clinical features and underlying molecular pathophysiology, JS is included in the rapidly expanding group of disorders called ciliopathies. The ciliopathies are emerging as models for more complex diseases, where sequence variants in multiple genes contribute to the phenotype expressed in any given patient.
乔伯特综合征(JS)是一种主要为常染色体隐性遗传的疾病,其特征为肌张力减退、共济失调、异常眼动以及智力残疾,并伴有独特的中后脑畸形(“磨牙征”)。可变特征包括视网膜营养不良、多囊肾病、肝纤维化和多指畸形。最近,我们对JS的遗传基础有了实质性进展,包括鉴定出7个致病基因(NPHP1、AHI1、CEP290、RPGRIP1L、TMEM67/MKS3、ARL13B和CC2D2A)。尽管有这一进展,但已知基因仅占病例的不到50%,且JS中几乎没有强的基因型-表型相关性;然而,可根据临床特征对基因检测进行优先排序。虽然所有7个JS基因都与初级纤毛/基体细胞器(PC/BB)的功能有关,但对于PC/BB在脑、肾、视网膜和肝脏发育/功能中的作用机制,以及PC/BB功能的破坏如何导致这些器官的疾病,我们知之甚少。最近关于PC/BB功能的研究表明,该细胞器参与包括音猬因子、WNT和血小板衍生生长因子在内的多种信号通路。由于具有共同的临床特征和潜在的分子病理生理学,JS被纳入了迅速扩大的一组称为纤毛病的疾病中。纤毛病正逐渐成为更复杂疾病的模型,在这些疾病中,多个基因的序列变异会导致任何给定患者所表现出的表型。