Project Summary Primary cilia are microtubule-based sensory structures found on the surface of most eukaryotic cells. Dysfunctional cilia lead to numerous syndromic disorders, often characterized by renal abnormalities. Unlike other cellular organelles, the ciliary lumen is open to the cytoplasm, making it unclear how cilia-essential and renal-physiology-related proteins, such as Polycystin 1 and 2 from ADPKD, reach the cilia. There is growing evidence to support the existence of a selective gate at cilia base that regulates the import of ciliogenic proteins. Despite the poorly studied transition fibers (TFs) being implied to be a vital part of the ciliary gate, there is a lack of molecular insight into the establishment of TFs, either in terms of their structure or function. Investigating the connection between cilia and disease in mammalian models can be challenging due to the essential roles of cilia in mammalian embryonic development. Thus, alternative experimental systems are needed. Caenorhabditis elegans has proven to be an effective model for studying ciliary proteins in their natural cellular environment due to its highly conserved cilia composition and signaling. Our laboratory pioneered the application of C. elegans to study the ciliary gate in past funding periods and made important discoveries about its composition, establishment, and significance in human diseases. Our recent findings have shown that the ARPKD protein DZIP1L plays a crucial role in establishing functional cilia gates in both C. elegans and human renal epithelial cilia. Building on our expertise in cilia research and utilizing the resources of the Mayo Clinic PKD Translational Center, our main objective is to fundamentally advance the understanding of the physiological importance of cilia gating in ciliopathies beyond Polycystic Kidney Disease. This proposal is based on a novel discovery that DZIP1L and ANKRD26 forms a conserved protein module to recruit other essential TF proteins to build a functional cilia gate; a paradigm that the activity of a poorly defined phosphoinositide signaling, mediated by the ciliary PIPKg, determines the proper localization of DZIP1L; and an exciting hypothesis that the ARPKD variants of DZIP1L may specifically impact cilia import of polycystins. Emerging evidence from our laboratory and others shows that polycystin dosage closely correlate with the severity of various PKD conditions, highlighting the therapeutic potential of targeting cilia gating to enhance the import of PKD proteins. To comprehensively understand the regulatory pathways of DZIP1L- regulated cilia gating, especially for PKD proteins, we will use both C. elegans and mammalian renal cell models and employ an interdisciplinary approach. Our goal is to gain critical insights into this understudied area in cilia and ciliopathies, establish its physiological significance, and link fundamental discoveries to the molecular connections between aberrant cilia gating and the d...