A suppressive oligodeoxynucleotide expressing TTAGGG motifs modulates cellular energetics through the mTOR signaling pathway

buir.contributor.authorYazar, Volkan
buir.contributor.authorKılıç, Gizem
buir.contributor.authorBulut, Özlem
buir.contributor.authorCanavar-Yıldırım, Tuğçe
buir.contributor.authorYağcı, Fuat C.
buir.contributor.authorGamze, Aykut
buir.contributor.authorGürsel, İhsan
dc.citation.epage48en_US
dc.citation.issueNumber1en_US
dc.citation.spage39en_US
dc.citation.volumeNumber32en_US
dc.contributor.authorYazar, Volkan
dc.contributor.authorKılıç, Gizem
dc.contributor.authorBulut, Özlem
dc.contributor.authorCanavar-Yıldırım, Tuğçe
dc.contributor.authorYağcı, Fuat C.
dc.contributor.authorGamze, Aykut
dc.contributor.authorKlinman, D. M.
dc.contributor.authorGürsel, M.
dc.contributor.authorGürsel, İhsan
dc.date.accessioned2021-02-17T08:06:53Z
dc.date.available2021-02-17T08:06:53Z
dc.date.issued2020
dc.departmentDepartment of Molecular Biology and Geneticsen_US
dc.description.abstractImmune-mediated inflammation must be down-regulated to facilitate tissue remodeling during homeostatic restoration of an inflammatory response. Uncontrolled or over-exuberant immune activation can cause autoimmune diseases, as well as tissue destruction. A151, the archetypal example of a chemically synthesized suppressive oligodeoxynucleotide (ODN) based on repetitive telomere-derived TTAGGG sequences, was shown to successfully down-regulate a variety of immune responses. However, the degree, duration and breadth of A151-induced transcriptome alterations remain elusive. Here, we performed a comprehensive microarray analysis in combination with Ingenuity Pathway Analysis (IPA) using murine splenocytes to investigate the underlying mechanism of A151-dependent immune suppression. Our results revealed that A151 significantly down-regulates critical mammalian target of rapamycin (mTOR) activators (Pi3kcd, Pdpk1 and Rheb), elements downstream of mTOR signaling (Rps6ka1, Myc, Stat3 and Slc2a1), an important component of the mTORC2 protein complex (Rictor) and Mtor itself. The effects of A151 on mTOR signaling were doseand time-dependent. Moreover, flow cytometry and immunoblotting analyses demonstrated that A151 is able to reverse mTOR phosphorylation comparably to the well-known mTOR inhibitor rapamycin. Furthermore, Seahorse metabolic assays showed an A151 ODN-induced decrease in both oxygen consumption and glycolysis implying that a metabolically inert state in macrophages could be triggered by A151 treatment. Overall, our findings suggested novel insights into the mechanism by which the immune system is metabolically modulated by A151 ODN.en_US
dc.description.provenanceSubmitted by Onur Emek (onur.emek@bilkent.edu.tr) on 2021-02-17T08:06:53Z No. of bitstreams: 1 A_suppressive_oligodeoxynucleotide_expressing_TTAGGG_motifs_modulates_cellular_energetics_through_the_mTOR_signaling_pathway.pdf: 2041704 bytes, checksum: c3e9126e309231883359ceb37d3ba05e (MD5)en
dc.description.provenanceMade available in DSpace on 2021-02-17T08:06:53Z (GMT). No. of bitstreams: 1 A_suppressive_oligodeoxynucleotide_expressing_TTAGGG_motifs_modulates_cellular_energetics_through_the_mTOR_signaling_pathway.pdf: 2041704 bytes, checksum: c3e9126e309231883359ceb37d3ba05e (MD5) Previous issue date: 2020en
dc.description.sponsorshipThis work was partially supported by the Scientific and Technological Research Council of Turkey (TUBITAK) (grant number: 115S492 to I.G.), (grant number: 115S837 to I.G.) and the Ministry of Development (grant name: UMRAM-ASI, project #: 2015BSV302 to I.G.).en_US
dc.identifier.doi10.1093/intimm/dxz059en_US
dc.identifier.issn0953-8178
dc.identifier.urihttp://hdl.handle.net/11693/73894
dc.language.isoEnglishen_US
dc.publisherOxford University Pressen_US
dc.relation.isversionofhttps://dx.doi.org/10.1093/intimm/dxz059en_US
dc.source.titleInternational Immunologyen_US
dc.subjectA151 ODNen_US
dc.subjectImmunometabolismen_US
dc.subjectImmunosuppressionen_US
dc.subjectMicroarrayen_US
dc.titleA suppressive oligodeoxynucleotide expressing TTAGGG motifs modulates cellular energetics through the mTOR signaling pathwayen_US
dc.typeArticleen_US

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