SIDT2 RNA transporter promotes lung and gastrointestinal tumor development

Nguyen, Tracy; Bieging-Rolett, Kathryn; Putoczki, Tracy L.; Wicks, Ian P.; Attardi, Laura D.; Pang, Ken C

doi:10.1101/724237

Cited by 1 publication

(1 citation statement)

References 48 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…SIDT2 overexpression enhances siRNA transport, while knockdown reduces RNA degradation, and a knockout disturbs the glucose homeostasis [15,24]. Like SIDT1, SIDT2 is also implicated in crucial biological processes such as lysosomal membrane permeability, hepatic lipid homeostasis, apoptosis, and tumor proliferation [14,20,25,26]. Despite SIDTs being a potential target for therapeutics against tumor progression, liver diseases, and Type II diabetes, their exploration as potential drug targets has been impeded by the lack of in vitro transport kinetic studies and high-resolution 3D structures of SIDTs.…”

Section: Introductionmentioning

confidence: 99%

Structure of the human systemic RNAi defective transmembrane protein 1 (hSIDT1) reveals the conformational flexibility of its lipid binding domain

Navratna,

Kumar,

Rana

et al. 2023

Preprint

View full text Add to dashboard Cite

InC. elegans, the inter-cellular transport of the small non-coding RNA that causes systemic RNA interference (RNAi) is mediated by the transmembrane protein SID1, encoded by thesid1gene in the systemic RNA interference-defective (sid) loci. SID1 shares remarkable structural and sequence similarity with cholesterol uptake protein 1 (CHUP1), and they are classified together as members of the cholesterol uptake family (ChUP). Although systemic RNAi is not an evolutionarily conserved process, thesidgene products are found across the animal kingdom, suggesting a potential for the existence of other novel gene regulatory mechanisms mediated by small non-coding RNAs. Human homologs ofsidgene products – hSIDT1 and hSIDT2 – are believed to mediate contact-dependent lipophilic small non-coding dsRNA transport. Here, we report the structure of recombinant full-length human SIDT1. We find that the extra-cytosolic domain (ECD) of hSIDT1 adopts a double jelly roll fold, and the transmembrane domain (TMD) exists as two modules – a flexible lipid binding domain (LBD) and a rigid TMD core. Our structural analyses provide insights into the potential role of the lipid binding domain in the function of hSIDT1 and other cholesterol uptake (ChUP) family members.

show abstract