image: An artist's impression of cGAS-STING pathway response model for micronucleus. Before, cGAS's accumulation in micronuclei was considered to be an indicator of cGAS activation. Now, it was found that micronuclei were inert to cGAS.
Credit: KyotoU GTobiyama/Makoto Hayashi
Kyoto, Japan -- Cells possess an innate immune system that defends against invasive pathogens such as bacteria and viruses. Previous studies have mapped out the cytoplasmic cGAS-STING pathway in the cytoplasm, known for responding to foreign nucleic acids, such as double-stranded DNA.
Micronuclei -- or MN, abnormal intracellular structures containing the cell's DNA -- have also been suspected of triggering the pathway. However, no conclusive evidence exists of pathway activation by MN-induced cyclic GMP-AMP synthase, or cGAS.
Now, Kyoto University and the AIRC Institute of Molecular Oncology, or IFOM, have collaborated to develop the reporter cell line Fusion Visualization system 2 -- FuVis2 -- designed to help researchers visualize cellular nuclei with chromosome fusion and resulting MN. Using FuVis2, they examined whether MN influences the cGAS-STING response in live cells, where STING refers to stimulators of interferon genes.
"Our findings suggest cGAS more commonly recognizes MN during cell division without activating STING in the following cell cycle, contrary to the existing theory that cGAS-bound MN leads to STING activation," says lead author Makoto Hayashi at the IFOM-KU Joint Research Laboratory at KyotoU's Graduate School of Medicine.
The team also showed that cGAS-STING activation by gamma irradiation leads to mitochondrial DNA leakage into the cytoplasm and is not associated with MN formation. The observed MN inactivity against innate immune responses may suggest chromosomal abnormalities with severe consequences.
Radiation-generated MN had been reported to activate the cGAS-STING pathway, so the researchers began using MN as a model for cGAS activation.
"However, we were excited to obtain the opposite results," says Yuki Sato at KyotoU's Graduate School of Biostudies.
Previous correlative results have also suggested that an MN-mediated innate immune response may drive cellular senescence and suppress cancer. However, Hayashi's team now feels the need to revisit this model.
"Given that these findings were derived specifically from the human colon cancer cell type HCT116, we should also conduct further analyses across different cell types and species before establishing theories about the MN-activated pathway," concludes Hayashi.
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The paper "Micronucleus is not a potent inducer of the cGAS/STING pathway" appeared on 2 February 2024 in Life Science Alliance, with doi: 10.26508/lsa.202302424
About Kyoto University
Kyoto University is one of Japan and Asia's premier research institutions, founded in 1897 and responsible for producing numerous Nobel laureates and winners of other prestigious international prizes. A broad curriculum across the arts and sciences at undergraduate and graduate levels complements several research centers, facilities, and offices around Japan and the world. For more information, please see: http://www.kyoto-u.ac.jp/en
Journal
Life Science Alliance
Method of Research
Experimental study
Subject of Research
Cells
Article Title
Micronucleus is not a potent inducer of the cGAS/STING pathway
Article Publication Date
2-Feb-2024
COI Statement
The authors declare that they have no conflict of interest.