DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection

Dipeptidyl peptidase 9 (DPP9) is a member of the dipeptidyl peptidase IV family. Inhibition of DPP9 has recently been shown to activate the nucleotide-binding domain leucine-rich repeat 1 (NLRP1) inflammasome. NLRP1 is known to bind nucleic acids with high affinity and directly interact with double...

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Autores principales: del Castillo-Izquierdo, Ángela, Moreno-Navarrete, José María, Latorre, Jessica, Arnoriaga-Rodríguez, María, Ballanti, Marta, Monteleone, Giovanni, Alessandro Paoluzi, Omero, Mingrone, Geltrude, Puig, Josep, Ramos, Rafael, Garre-Olmo, Josep, Jové, Mariona, Pamplona, Reinald, Portero-Otín, Manuel, Sol, Joaquim, Lefebvre, Philippe, Staels, Bart, Federici, Massimo, Fernández-Real, José Manuel, Mayneris-Perxachs, Jordi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9686780/
https://www.ncbi.nlm.nih.gov/pubmed/36358551
http://dx.doi.org/10.3390/antiox11112177
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author del Castillo-Izquierdo, Ángela
Moreno-Navarrete, José María
Latorre, Jessica
Arnoriaga-Rodríguez, María
Ballanti, Marta
Monteleone, Giovanni
Alessandro Paoluzi, Omero
Mingrone, Geltrude
Puig, Josep
Ramos, Rafael
Garre-Olmo, Josep
Jové, Mariona
Pamplona, Reinald
Portero-Otín, Manuel
Sol, Joaquim
Lefebvre, Philippe
Staels, Bart
Federici, Massimo
Fernández-Real, José Manuel
Mayneris-Perxachs, Jordi
author_facet del Castillo-Izquierdo, Ángela
Moreno-Navarrete, José María
Latorre, Jessica
Arnoriaga-Rodríguez, María
Ballanti, Marta
Monteleone, Giovanni
Alessandro Paoluzi, Omero
Mingrone, Geltrude
Puig, Josep
Ramos, Rafael
Garre-Olmo, Josep
Jové, Mariona
Pamplona, Reinald
Portero-Otín, Manuel
Sol, Joaquim
Lefebvre, Philippe
Staels, Bart
Federici, Massimo
Fernández-Real, José Manuel
Mayneris-Perxachs, Jordi
author_sort del Castillo-Izquierdo, Ángela
collection PubMed
description Dipeptidyl peptidase 9 (DPP9) is a member of the dipeptidyl peptidase IV family. Inhibition of DPP9 has recently been shown to activate the nucleotide-binding domain leucine-rich repeat 1 (NLRP1) inflammasome. NLRP1 is known to bind nucleic acids with high affinity and directly interact with double stranded RNA, which plays a key role in viral replication. DPP9 has also recently emerged as a key gene related to lung-inflammation in critical SARS-CoV-2 infection. Importantly, DPP9 activity is strongly dependent on the oxidative status. Here, we explored the potential role of DPP9 in the gastrointestinal tract. We performed transcriptomics analyses of colon (microarray, n = 37) and jejunal (RNA sequencing, n = 31) biopsies from two independent cohorts as well as plasma metabolomics analyses in two independent cohorts (n = 37 and n = 795). The expression of DPP9 in the jejunum, colon, and blood was significantly associated with circulating biomarkers of oxidative stress (uric acid, bilirubin). It was also associated positively with the expression of transcription factors (NRF-2) and genes (SOD, CAT, GPX) encoding for antioxidant enzymes, but negatively with that of genes (XDH, NOX) and transcription factors (NF-KB) involved in ROS-generating enzymes. Gene co-expression patterns associated with DPP9 identified several genes participating in antiviral pathways in both tissues. Notably, DPP9 expression in the colon and plasma was strongly positively associated with several circulating nucleotide catabolites (hypoxanthine, uric acid, 3-ureidopropionic acid) with important roles in the generation of ROS and viral infection, as well as other metabolites related to oxidative stress (Resolvin D1, glutamate-containing dipeptides). Gene-drug enrichment analyses identified artenimol, puromycin, anisomycin, 3-phenyllactic acid, and linezolid as the most promising drugs targeting these DPP9-associated genes. We have identified a novel potential pathogenic mechanism of viral infection in the digestive tract and promising existing drugs that can be repositioned against viral infection.
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spelling pubmed-96867802022-11-25 DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection del Castillo-Izquierdo, Ángela Moreno-Navarrete, José María Latorre, Jessica Arnoriaga-Rodríguez, María Ballanti, Marta Monteleone, Giovanni Alessandro Paoluzi, Omero Mingrone, Geltrude Puig, Josep Ramos, Rafael Garre-Olmo, Josep Jové, Mariona Pamplona, Reinald Portero-Otín, Manuel Sol, Joaquim Lefebvre, Philippe Staels, Bart Federici, Massimo Fernández-Real, José Manuel Mayneris-Perxachs, Jordi Antioxidants (Basel) Article Dipeptidyl peptidase 9 (DPP9) is a member of the dipeptidyl peptidase IV family. Inhibition of DPP9 has recently been shown to activate the nucleotide-binding domain leucine-rich repeat 1 (NLRP1) inflammasome. NLRP1 is known to bind nucleic acids with high affinity and directly interact with double stranded RNA, which plays a key role in viral replication. DPP9 has also recently emerged as a key gene related to lung-inflammation in critical SARS-CoV-2 infection. Importantly, DPP9 activity is strongly dependent on the oxidative status. Here, we explored the potential role of DPP9 in the gastrointestinal tract. We performed transcriptomics analyses of colon (microarray, n = 37) and jejunal (RNA sequencing, n = 31) biopsies from two independent cohorts as well as plasma metabolomics analyses in two independent cohorts (n = 37 and n = 795). The expression of DPP9 in the jejunum, colon, and blood was significantly associated with circulating biomarkers of oxidative stress (uric acid, bilirubin). It was also associated positively with the expression of transcription factors (NRF-2) and genes (SOD, CAT, GPX) encoding for antioxidant enzymes, but negatively with that of genes (XDH, NOX) and transcription factors (NF-KB) involved in ROS-generating enzymes. Gene co-expression patterns associated with DPP9 identified several genes participating in antiviral pathways in both tissues. Notably, DPP9 expression in the colon and plasma was strongly positively associated with several circulating nucleotide catabolites (hypoxanthine, uric acid, 3-ureidopropionic acid) with important roles in the generation of ROS and viral infection, as well as other metabolites related to oxidative stress (Resolvin D1, glutamate-containing dipeptides). Gene-drug enrichment analyses identified artenimol, puromycin, anisomycin, 3-phenyllactic acid, and linezolid as the most promising drugs targeting these DPP9-associated genes. We have identified a novel potential pathogenic mechanism of viral infection in the digestive tract and promising existing drugs that can be repositioned against viral infection. MDPI 2022-11-03 /pmc/articles/PMC9686780/ /pubmed/36358551 http://dx.doi.org/10.3390/antiox11112177 Text en © 2022 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
del Castillo-Izquierdo, Ángela
Moreno-Navarrete, José María
Latorre, Jessica
Arnoriaga-Rodríguez, María
Ballanti, Marta
Monteleone, Giovanni
Alessandro Paoluzi, Omero
Mingrone, Geltrude
Puig, Josep
Ramos, Rafael
Garre-Olmo, Josep
Jové, Mariona
Pamplona, Reinald
Portero-Otín, Manuel
Sol, Joaquim
Lefebvre, Philippe
Staels, Bart
Federici, Massimo
Fernández-Real, José Manuel
Mayneris-Perxachs, Jordi
DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title_full DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title_fullStr DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title_full_unstemmed DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title_short DPP9 as a Potential Novel Mediator in Gastrointestinal Virus Infection
title_sort dpp9 as a potential novel mediator in gastrointestinal virus infection
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9686780/
https://www.ncbi.nlm.nih.gov/pubmed/36358551
http://dx.doi.org/10.3390/antiox11112177
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