Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function

Monocytes play a vital role in the development of cardiovascular diseases. Type 2 diabetes mellitus (T2DM) is a major CVD risk factor, and T2DM-induced aberrant activation and enhanced migration of monocytes is a vital pathomechanism that leads to atherogenesis. We recently reported the upregulation...

Descripción completa

Detalles Bibliográficos
Autores principales: Dorenkamp, Marc, Nasiry, Madina, Semo, Dilvin, Koch, Sybille, Löffler, Ivonne, Wolf, Gunter, Reinecke, Holger, Godfrey, Rinesh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9914555/
https://www.ncbi.nlm.nih.gov/pubmed/36766855
http://dx.doi.org/10.3390/cells12030513
_version_ 1784885692903456768
author Dorenkamp, Marc
Nasiry, Madina
Semo, Dilvin
Koch, Sybille
Löffler, Ivonne
Wolf, Gunter
Reinecke, Holger
Godfrey, Rinesh
author_facet Dorenkamp, Marc
Nasiry, Madina
Semo, Dilvin
Koch, Sybille
Löffler, Ivonne
Wolf, Gunter
Reinecke, Holger
Godfrey, Rinesh
author_sort Dorenkamp, Marc
collection PubMed
description Monocytes play a vital role in the development of cardiovascular diseases. Type 2 diabetes mellitus (T2DM) is a major CVD risk factor, and T2DM-induced aberrant activation and enhanced migration of monocytes is a vital pathomechanism that leads to atherogenesis. We recently reported the upregulation of SHP-2 phosphatase expression in mediating the VEGF resistance of T2DM patient-derived monocytes or methylglyoxal- (MG, a glucose metabolite and advanced glycation end product (AGE) precursor) treated monocytes. However, the exact mechanisms leading to SHP-2 upregulation in hyperglycemic monocytes are unknown. Since inflammation and accumulation of AGEs is a hallmark of T2DM, we hypothesise that inflammation and AGE-RAGE (Receptor-for-AGEs) signalling drive SHP-2 expression in monocytes and blockade of these pathways will repress SHP-2 function. Indeed, monocytes from T2DM patients revealed an elevated SHP-2 expression. Under normoglycemic conditions, the serum from T2DM patients strongly induced SHP-2 expression, indicating that the T2DM serum contains critical factors that directly regulate SHP-2 expression. Activation of pro-inflammatory TNFα signalling cascade drove SHP-2 expression in monocytes. In line with this, linear regression analysis revealed a significant positive correlation between TNFα expression and SHP-2 transcript levels in T2DM monocytes. Monocytes exposed to MG or AGE mimetic AGE-BSA, revealed an elevated SHP-2 expression and co-treatment with an NFκB inhibitor or genetic inhibition of p65 reversed it. The pharmacological inhibition of RAGE was sufficient to block MG- or AGE-BSA-induced SHP-2 expression and activity. Confirming the importance of RAGE-NFκB signalling in regulating SHP-2 expression, the elevated binding of NFκB to the SHP-2 promoter—induced by MG or AGE-BSA—was reversed by RAGE and NFκB inhibition. Besides, we detected elevated RAGE levels in human and murine T2DM monocytes and monocytes exposed to MG or AGE-BSA. Importantly, MG and AGE-BSA treatment of non-T2DM monocytes phenocopied the aberrant pro-migratory phenotype of T2DM monocytes, which was reversed entirely by either SHP-2- or RAGE inhibition. In conclusion, these findings suggest a new therapeutic approach to prevent accelerated atherosclerosis in T2DM patients since inhibiting the RAGE-NFκB-SHP-2 axis impeded the T2DM-driven, SHP-2-dependent monocyte activation.
format Online
Article
Text
id pubmed-9914555
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-99145552023-02-11 Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function Dorenkamp, Marc Nasiry, Madina Semo, Dilvin Koch, Sybille Löffler, Ivonne Wolf, Gunter Reinecke, Holger Godfrey, Rinesh Cells Article Monocytes play a vital role in the development of cardiovascular diseases. Type 2 diabetes mellitus (T2DM) is a major CVD risk factor, and T2DM-induced aberrant activation and enhanced migration of monocytes is a vital pathomechanism that leads to atherogenesis. We recently reported the upregulation of SHP-2 phosphatase expression in mediating the VEGF resistance of T2DM patient-derived monocytes or methylglyoxal- (MG, a glucose metabolite and advanced glycation end product (AGE) precursor) treated monocytes. However, the exact mechanisms leading to SHP-2 upregulation in hyperglycemic monocytes are unknown. Since inflammation and accumulation of AGEs is a hallmark of T2DM, we hypothesise that inflammation and AGE-RAGE (Receptor-for-AGEs) signalling drive SHP-2 expression in monocytes and blockade of these pathways will repress SHP-2 function. Indeed, monocytes from T2DM patients revealed an elevated SHP-2 expression. Under normoglycemic conditions, the serum from T2DM patients strongly induced SHP-2 expression, indicating that the T2DM serum contains critical factors that directly regulate SHP-2 expression. Activation of pro-inflammatory TNFα signalling cascade drove SHP-2 expression in monocytes. In line with this, linear regression analysis revealed a significant positive correlation between TNFα expression and SHP-2 transcript levels in T2DM monocytes. Monocytes exposed to MG or AGE mimetic AGE-BSA, revealed an elevated SHP-2 expression and co-treatment with an NFκB inhibitor or genetic inhibition of p65 reversed it. The pharmacological inhibition of RAGE was sufficient to block MG- or AGE-BSA-induced SHP-2 expression and activity. Confirming the importance of RAGE-NFκB signalling in regulating SHP-2 expression, the elevated binding of NFκB to the SHP-2 promoter—induced by MG or AGE-BSA—was reversed by RAGE and NFκB inhibition. Besides, we detected elevated RAGE levels in human and murine T2DM monocytes and monocytes exposed to MG or AGE-BSA. Importantly, MG and AGE-BSA treatment of non-T2DM monocytes phenocopied the aberrant pro-migratory phenotype of T2DM monocytes, which was reversed entirely by either SHP-2- or RAGE inhibition. In conclusion, these findings suggest a new therapeutic approach to prevent accelerated atherosclerosis in T2DM patients since inhibiting the RAGE-NFκB-SHP-2 axis impeded the T2DM-driven, SHP-2-dependent monocyte activation. MDPI 2023-02-03 /pmc/articles/PMC9914555/ /pubmed/36766855 http://dx.doi.org/10.3390/cells12030513 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Dorenkamp, Marc
Nasiry, Madina
Semo, Dilvin
Koch, Sybille
Löffler, Ivonne
Wolf, Gunter
Reinecke, Holger
Godfrey, Rinesh
Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title_full Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title_fullStr Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title_full_unstemmed Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title_short Pharmacological Targeting of the RAGE-NFκB Signalling Axis Impedes Monocyte Activation under Diabetic Conditions through the Repression of SHP-2 Tyrosine Phosphatase Function
title_sort pharmacological targeting of the rage-nfκb signalling axis impedes monocyte activation under diabetic conditions through the repression of shp-2 tyrosine phosphatase function
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9914555/
https://www.ncbi.nlm.nih.gov/pubmed/36766855
http://dx.doi.org/10.3390/cells12030513
work_keys_str_mv AT dorenkampmarc pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT nasirymadina pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT semodilvin pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT kochsybille pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT lofflerivonne pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT wolfgunter pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT reineckeholger pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction
AT godfreyrinesh pharmacologicaltargetingoftheragenfkbsignallingaxisimpedesmonocyteactivationunderdiabeticconditionsthroughtherepressionofshp2tyrosinephosphatasefunction

Ejemplares similares