RRC ID 76020
Author Mosquera JV, Bacher MC, Priess JR.
Title Nuclear lipid droplets and nuclear damage in Caenorhabditis elegans.
Journal PLoS Genet
Abstract Fat stored in the form of lipid droplets has long been considered a defining characteristic of cytoplasm. However, recent studies have shown that nuclear lipid droplets occur in multiple cells and tissues, including in human patients with fatty liver disease. The function(s) of stored fat in the nucleus has not been determined, and it is possible that nuclear fat is beneficial in some situations. Conversely, nuclear lipid droplets might instead be deleterious by disrupting nuclear organization or triggering aggregation of hydrophobic proteins. We show here that nuclear lipid droplets occur normally in C. elegans intestinal cells and germ cells, but appear to be associated with damage only in the intestine. Lipid droplets in intestinal nuclei can be associated with novel bundles of microfilaments (nuclear actin) and membrane tubules that might have roles in damage repair. To increase the normal, low frequency of nuclear lipid droplets in wild-type animals, we used a forward genetic screen to isolate mutants with abnormally large or abundant nuclear lipid droplets. Genetic analysis and cloning of three such mutants showed that the genes encode the lipid regulator SEIP-1/seipin, the inner nuclear membrane protein NEMP-1/Nemp1/TMEM194A, and a component of COPI vesicles called COPA-1/α-COP. We present several lines of evidence that the nuclear lipid droplet phenotype of copa-1 mutants results from a defect in retrieving mislocalized membrane proteins that normally reside in the endoplasmic reticulum. The seip-1 mutant causes most germ cells to have nuclear lipid droplets, the largest of which occupy more than a third of the nuclear volume. Nevertheless, the nuclear lipid droplets do not trigger apoptosis, and the germ cells differentiate into gametes that produce viable, healthy progeny. Thus, our results suggest that nuclear lipid droplets are detrimental to intestinal nuclei, but have no obvious deleterious effect on germ nuclei.
Volume 17(6)
Pages e1009602
Published 2021-6-1
DOI 10.1371/journal.pgen.1009602
PII PGENETICS-D-21-00328
PMID 34133414
PMC PMC8208577
MeSH Actin Cytoskeleton / metabolism Actin Cytoskeleton / ultrastructure Animals Caenorhabditis elegans / genetics Caenorhabditis elegans / metabolism* Caenorhabditis elegans Proteins / genetics* Caenorhabditis elegans Proteins / metabolism Cell Nucleus / metabolism* Cell Nucleus / ultrastructure Coatomer Protein / genetics* Coatomer Protein / metabolism Endoplasmic Reticulum / genetics Endoplasmic Reticulum / metabolism Gene Expression Regulation Germ Cells / cytology Germ Cells / metabolism Intestinal Mucosa / metabolism* Intestinal Mucosa / pathology Intestines / pathology Lipid Droplets / metabolism* Lipid Droplets / ultrastructure Lipid Metabolism / genetics* Lipids / chemistry Membrane Proteins / genetics* Membrane Proteins / metabolism Mutation Nuclear Proteins / genetics Nuclear Proteins / metabolism Organ Specificity ran GTP-Binding Protein / genetics ran GTP-Binding Protein / metabolism
Resource
C.elegans tm4221