Investigating the Impact of Birt–hogg–dubé Syndrome Associated Folliculin (Flcn) and Retinitis Pigmentosa 2 (Rp2) Loss on Cilia Function and Morphology
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Date
2024
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Open Access Color
GOLD
Green Open Access
Yes
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58
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173
Publicly Funded
No
Abstract
Folliculin (FLCN), a GTPase-activating protein (GAP), has been linked to Birt–Hogg–Dubé syndrome, the mTORC1 signaling pathway and cilia. Disruptions in cilia structure and function lead to a group of diseases known as ciliopathies. Birt-Hogg-Dubé syndrome is one of 35 different ciliopathy diseases and there are more than 250 genes that cause ciliopathy diseases. FLCN interacts with kinesin-2 along cilia. The specific role of FLCN in regulating Kinesin-IFT trafficking has, however, remained unclear. In the current study, we investigated the effects of flcn-1 loss (the human ortholog of FLCN) on kinesin and IFT trafficking in C. elegans. The loss of flcn-1 alone did not result in any apparent alterations to kinesin or IFT trafficking within the cilia. However, when we combined the deletion of flcn-1 with the deletion of Retinitis Pigmentosa 2 (RP2), another GAP protein, the ciliary entry of a non-ciliary membrane protein TRAM-1 (Translocation Associated Membrane Protein 1) occured. Additionally, although cilia length was unaltered, our analysis of double mutants revealed the extra branch in wing AWB cilia morphology but not the single rod-like PHA/PHB cilia. In summary, our study reveals the previously unknown functions of FLCN in ciliary gating and cilia morphology in C. elegans
Description
Keywords
Biyoloji, Hücre Biyolojisi, Folliculin;Cilia;Retinitis pigmentosa 2;Ciliary gate, Biochemistry and Cell Biology (Other), Biyokimya ve Hücre Biyolojisi (Diğer), Cilia, Folliculin, Ciliary gate, Retinitis pigmentosa 2
Turkish CoHE Thesis Center URL
Fields of Science
0301 basic medicine, 0303 health sciences, 03 medical and health sciences
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N/A
Source
Cumhuriyet Science Journal
Volume
45
Issue
2
Start Page
235
End Page
239
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