Myotis bat STING attenuates aging-related inflammation in female mice.

Myotis bat STING attenuates aging-related inflammation in female mice.

Publication date: Sep 18, 2024

Bats, notable as the only flying mammals, serve as natural reservoir hosts for various highly pathogenic viruses in humans (e. g., SARS-CoV and Ebola virus). Furthermore, bats exhibit an unparalleled longevity among mammals relative to their size, particularly the Myotis bats, which can live up to 40 years. However, the mechanisms underlying these distinctive traits remain incompletely understood. In our prior research, we demonstrated that bats exhibit dampened STING-interferon activation, potentially conferring upon them the capacity to mitigate virus- or aging-induced inflammation. To substantiate this hypothesis, we established the first in vivo bat-mouse model for aging studies by integrating Myotis davidii bat STING ( MdSTING) into the mouse genome. We monitored the genotypes of these mice and performed a longitudinal comparative transcriptomic analysis on MdSTING and wild-type mice over a 3-year aging process. Blood transcriptomic analysis indicated a reduction in aging-related inflammation in female MdSTING mice, as evidenced by significantly lower levels of pro-inflammatory cytokines and chemokines, immunopathology, and neutrophil recruitment in aged female MdSTING mice compared to aged wild-type mice in vivo. These results indicated that MdSTING knock-in attenuates the aging-related inflammatory response and may also improve the healthspan in mice in a sex-dependent manner. Although the underlying mechanism awaits further study, this research has critical implications for bat longevity research, potentially contributing to our comprehension of healthy aging in humans.

Concepts Keywords
Aging Aging
Flying Aging-related inflammation
Immunopathology Animals
Mice Bat
Reservoir Chiroptera
Cytokines
Cytokines
Female
Inflammation
Longevity
Membrane Proteins
Membrane Proteins
Mice
STING
Sting1 protein, mouse
Virus reservoir host

Semantics

Type Source Name
disease MESH inflammation
disease VO Viruses
disease IDO process
disease IDO blood
disease IDO host

Original Article

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