Adenovirus 36 seropositivity is related to the expression of anti-adipogenic lncRNAs GAS5 and MEG3 in adipose tissue obtained from subjects with obesity
Background Human Adenovirus D-36 (HAdV-D36) promotes adipogenesis in cellular and animal models and may contribute to the development of human obesity. Induction of PPARγ by HAdV-D36 seems to have a central role in the maintenance of adipogenic status. There is limited information about epigenetic m...
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Veröffentlicht in: | International Journal of Obesity 2024-10, Vol.48 (10), p.1414-1420 |
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Sprache: | eng |
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Zusammenfassung: | Background
Human Adenovirus D-36 (HAdV-D36) promotes adipogenesis in cellular and animal models and may contribute to the development of human obesity. Induction of PPARγ by HAdV-D36 seems to have a central role in the maintenance of adipogenic status. There is limited information about epigenetic mechanisms contributing to this process in human adipose tissue. This study evaluated the expression of lncRNAs (
ADINR, GAS5
and
MEG3
) and miRNAs (
miR-18a
and
miR-140
) involved in the adipogenic process in visceral adipose tissue (VAT) of subjects with obesity with previous HAdV-D36 infection (seropositive) and unexposed (seronegative) subjects with obesity.
Methods
Individuals with obesity were grouped according to the presence of antibodies against HAdV-D36 (Seropositive: HAdV-D36[+],
n
= 29; and Seronegative: HAdV-D36[−],
n
= 28). Additionally, a group of individuals without obesity (
n
= 17) was selected as a control group. The HAdV-D36 serology was carried out by ELISA. Biopsies of VAT were obtained during an elective and clinically indicated surgery (bariatric or cholecystectomy). RNA extraction from VAT was performed and the expression of
PPARG
and non-coding RNAs was evaluated by qPCR.
Results
HAdV-D36[+] individuals had lower expression of anti-adipogenic lncRNAs
GAS5
(
p
= 0.016) and
MEG3
(
p
= 0.035) compared with HAdV-D36[-] subjects with obesity. HAdV-D36[+] subjects also presented increased expression of the adipogenic miRNA
miR-18a
(
p
= 0.042), which has been reported to be modulated by
GAS5
through a RNA sponging mechanism during adipogenic differentiation. Additionally, an inverse correlation of
GAS5
with
PPARG
expression was observed (r = −0.917,
p
= 0.01).
Conclusion
Our results suggest that HAdV-D36 is related to non-coding RNAs implicated in adipogenesis, representing a potential mechanism by which previous HAdV-D36 infection could be associated with the long-term maintenance of adipogenic status, probably through the
GAS5/miR-18a
axis. |
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ISSN: | 0307-0565 1476-5497 1476-5497 |
DOI: | 10.1038/s41366-024-01555-x |