Novel, soluble 3-heteroaryl-substituted tanshinone mimics attenuate the inflammatory response in murine macrophages
The RNA binding protein Human Antigen R (HuR) has been identified as a main regulator of the innate immune response and its inhibition can lead to beneficial anti-inflammatory effects. To this aim, we previously synthesized a novel class of small molecules named Tanshinone Mimics (TMs) able to inter...
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Veröffentlicht in: | Scientific reports 2024-10, Vol.14 (1), p.24501-19, Article 24501 |
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Sprache: | eng |
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Zusammenfassung: | The RNA binding protein Human Antigen R (HuR) has been identified as a main regulator of the innate immune response and its inhibition can lead to beneficial anti-inflammatory effects. To this aim, we previously synthesized a novel class of small molecules named Tanshinone Mimics (TMs) able to interfere with HuR-RNA binding, and that dampen the LPS-induced immune response. Herein, we present a novel series of TMs, encompassing thiophene
3/TM9
and
4/TM10
, furan
5/TM11
and
6/TM12
, pyrrole
7b/TM13
, and pyrazole
8.
The furan-containing
5
(
TM11
) showed the greatest inhibitory effect of the series on HuR-RNA complex formation, as suggested by RNA Electromobility Shift Assay and Time-Resolved FRET. Molecular Dynamics Calculation of HuR −
5/TM11
interaction, quantum mechanics approaches and Surface Plasmon Resonance data, all indicates that, within the novel heteroaryl substituents, the furan ring better recapitulates the chemical features of the RNA bound to HuR. Compound
5/TM11
also showed improved aqueous solubility compared to previously reported TMs. Real-time monitoring of cell growth and flow cytometry analyses showed that
5
/
TM11
preferentially reduced cell proliferation rather than apoptosis in murine macrophages at immunomodulatory doses. We observed its effects on the innate immune response triggered by lipopolysaccharide (LPS) in macrophages, showing that
5
/
TM11
significantly reduced the expression of proinflammatory cytokines as
Cxcl10
and
Il1b
. |
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ISSN: | 2045-2322 2045-2322 |
DOI: | 10.1038/s41598-024-73309-8 |