Your search keyword '"Keita, Åsa V"' showing total 14 results

1. Identification and validation of a blood-based diagnostic lipidomic signature of paediatric inflammatory bowel disease

Author

Salihovic, Samira, Nyström, Niklas, Bache-Wiig Mathisen, Charlotte, Kruse, Robert, Olbjørn, Christine, Andersen, Svend, J Noble, Alexandra, Dorn-Rasmussen, Maria, Bazov, Igor, Perminow, Gøri, Opheim, Randi, Espen Detlie, Trond, Huppertz-Hauss, Gert, Hedin, Charlotte R H, Carlson, Marie, Öhman, Lena, Magnusson, Maria K, Keita, Åsa V, Söderholm, Johan D, D'Amato, Mauro, Oresic, Matej, Wewer, Vibeke, Satsangi, Jack, Lindqvist, Carl Mårten, Burisch, Johan, Uhlig, Holm H, Repsilber, Dirk, Hyötyläinen, Tuulia, Lie Hoivik, Marte, Halfvarson, Jonas, Salihovic, Samira, Nyström, Niklas, Bache-Wiig Mathisen, Charlotte, Kruse, Robert, Olbjørn, Christine, Andersen, Svend, J Noble, Alexandra, Dorn-Rasmussen, Maria, Bazov, Igor, Perminow, Gøri, Opheim, Randi, Espen Detlie, Trond, Huppertz-Hauss, Gert, Hedin, Charlotte R H, Carlson, Marie, Öhman, Lena, Magnusson, Maria K, Keita, Åsa V, Söderholm, Johan D, D'Amato, Mauro, Oresic, Matej, Wewer, Vibeke, Satsangi, Jack, Lindqvist, Carl Mårten, Burisch, Johan, Uhlig, Holm H, Repsilber, Dirk, Hyötyläinen, Tuulia, Lie Hoivik, Marte, and Halfvarson, Jonas

Published

2024

2. Faecal biomarkers for diagnosis and prediction of disease course in treatment-naïve patients with IBD

Author

Ling Lundström, Maria, Peterson, Christer, Hedin, Charlotte R. H., Bergemalm, Daniel, Lampinen, Maria, Magnusson, Maria K., Keita, Åsa V., Kruse, Robert, Lindqvist, Carl Mårten, Repsilber, Dirk, D'Amato, Mauro, Hjortswang, Henrik, Strid, Hans, Söderholm, Johan D., Öhman, Lena, Venge, Per, Halfvarson, Jonas, Carlson, Marie, Ling Lundström, Maria, Peterson, Christer, Hedin, Charlotte R. H., Bergemalm, Daniel, Lampinen, Maria, Magnusson, Maria K., Keita, Åsa V., Kruse, Robert, Lindqvist, Carl Mårten, Repsilber, Dirk, D'Amato, Mauro, Hjortswang, Henrik, Strid, Hans, Söderholm, Johan D., Öhman, Lena, Venge, Per, Halfvarson, Jonas, and Carlson, Marie

Abstract

Background: Faecal biomarkers can be used to assess inflammatory bowel disease (IBD). Aim: To explore the performance of some promising biomarkers in diagnosing and predicting disease course in IBD. Methods: We included 65 patients with treatment-na & iuml;ve, new-onset Crohn's disease (CD), 90 with ulcerative colitis (UC), 67 symptomatic controls (SC) and 41 healthy controls (HC) in this prospective observational study. We analysed faecal samples for calprotectin (FC), myeloperoxidase (MPO), human neutrophil lipocalin (HNL), eosinophil cationic protein ECP and eosinophil-derived neurotoxin (EDN) and compared markers among groups. We assessed the diagnostic capability of biomarkers with receiver operating characteristic curves. Clinical disease course was determined for each patient with IBD and analysed the association with biomarkers by logistic regression. Results: All markers were elevated at inclusion in patients with IBD compared with HC (p < 0.001) and SC (p < 0.001). FC (AUC 0.85, 95% CI: 0.79-0.89) and MPO (AUC 0.85, 95% CI: 0.80-0.89) showed the highest diagnostic accuracy in distinguishing IBD from SC. The diagnostic ability of biomarkers differed between IBD subtypes with the highest performance for FC and MPO in CD. The diagnostic accuracy was further improved by combining FC and MPO (p = 0.02). Levels of FC, MPO and HNL at inclusion were predictive of an aggressive disease course with MPO showing the strongest association (p = 0.006). Conclusions: This study provides new insight into the diagnostic and prognostic capability of neutrophil and eosinophil biomarkers in IBD and suggests that MPO, alone or in combination with FC, may add to the diagnostic power of faecal biomarkers., This work was supported by the Swedish Foundation for Strategic Research (grant number RB13-016) (J.H.), Swedish Research Council (grant number 2020-02021) (J.H.), the Örebro University Hospital Research Foundation (grant numbers OLL-890291) (J.H.) and Medical Faculty, Uppsala University, Uppsala, Sweden M.C.

Published

2024

3. Identification and validation of a blood- based diagnostic lipidomic signature of pediatric inflammatory bowel disease

Author

Salihovic, Samira, Nyström, Niklas, Mathisen, Charlotte Bache-Wiig, Kruse, Robert, Olbjørn, Christine, Andersen, Svend, Noble, Alexandra J., Dorn-Rasmussen, Maria, Bazov, Igor, Perminow, Gøri, Opheim, Randi, Detlie, Trond Espen, Huppertz-Hauss, Gert, Hedin, Charlotte R. H., Carlson, Marie, Öhman, Lena, Magnusson, Maria K., Keita, Åsa V., Söderholm, Johan D., D'Amato, Mauro, Oresic, Matej, Wewer, Vibeke, Satsangi, Jack, Lindqvist, Carl Mårten, Burisch, Johan, Uhlig, Holm H., Repsilber, Dirk, Hyötyläinen, Tuulia, Høivik, Marte Lie, Halfvarson, Jonas, Salihovic, Samira, Nyström, Niklas, Mathisen, Charlotte Bache-Wiig, Kruse, Robert, Olbjørn, Christine, Andersen, Svend, Noble, Alexandra J., Dorn-Rasmussen, Maria, Bazov, Igor, Perminow, Gøri, Opheim, Randi, Detlie, Trond Espen, Huppertz-Hauss, Gert, Hedin, Charlotte R. H., Carlson, Marie, Öhman, Lena, Magnusson, Maria K., Keita, Åsa V., Söderholm, Johan D., D'Amato, Mauro, Oresic, Matej, Wewer, Vibeke, Satsangi, Jack, Lindqvist, Carl Mårten, Burisch, Johan, Uhlig, Holm H., Repsilber, Dirk, Hyötyläinen, Tuulia, Høivik, Marte Lie, and Halfvarson, Jonas

Abstract

Improved biomarkers are needed for pediatric inflammatory bowel disease. Here we identify a diagnostic lipidomic signature for pediatric inflammatory bowel disease by analyzing blood samples from a discovery cohort of incident treatment-naïve pediatric patients and validating findings in an independent inception cohort. The lipidomic signature comprising of only lactosyl ceramide (d18:1/16:0) and phosphatidylcholine (18:0p/22:6) improves the diagnostic prediction compared with high-sensitivity C-reactive protein. Adding high-sensitivity C-reactive protein to the signature does not improve its performance. In patients providing a stool sample, the diagnostic performance of the lipidomic signature and fecal calprotectin, a marker of gastrointestinal inflammation, does not substantially differ. Upon investigation in a third pediatric cohort, the findings of increased lactosyl ceramide (d18:1/16:0) and decreased phosphatidylcholine (18:0p/22:6) absolute concentrations are confirmed. Translation of the lipidomic signature into a scalable diagnostic blood test for pediatric inflammatory bowel disease has the potential to support clinical decision making., This work was supported by the Swedish Foundation for Strategic Research [RB13-0160 to J.H.], the Swedish Research Council [2020-02021 to J.H.], the Örebro University Hospital research foundation [OLL-890291 to J.H.], NordForsk [90569 to J.H.].

Published

2024

4. Fecal Biomarkers of Neutrophil and Eosinophil Origin Reflect the Response to Biological Therapy and Corticosteroids in Patients With Inflammatory Bowel Disease

Author

Lundström, Maria Ling, Peterson, Christer, Lampinen, Maria, Hedin, Charlotte R. H., Keita, Åsa V., Kruse, Robert, Magnusson, Maria K., Lindqvist, Carl Mårten, Repsilber, Dirk, D'Amato, Mauro, Hjortswang, Henrik, Strid, Hans, Rönnblom, Anders, Söderholm, Johan D., Öhman, Lena, Venge, Per, Halfvarson, Jonas, Carlson, Marie, Lundström, Maria Ling, Peterson, Christer, Lampinen, Maria, Hedin, Charlotte R. H., Keita, Åsa V., Kruse, Robert, Magnusson, Maria K., Lindqvist, Carl Mårten, Repsilber, Dirk, D'Amato, Mauro, Hjortswang, Henrik, Strid, Hans, Rönnblom, Anders, Söderholm, Johan D., Öhman, Lena, Venge, Per, Halfvarson, Jonas, and Carlson, Marie

Abstract

Introduction: Fecal calprotectin (FC) is anoninvasive tool for examining response to biologics in inflammatory boweldisease (IBD), but its performance in relation to other novel fecal markers of various cellular origins is unknown. Methods: We performed a prospective multicenter cohort study and included patients with active IBD who provided a fecal sample at initiation of biological therapy. Levels of FC, myeloperoxidase (MPO), human neutrophil lipocalin (HNL), and eosinophil-derived neurotoxin (EDN) were analyzed and related to clinical remission status at 3 months. Changes in levels of markers at 3 months were calculated, and the impact of concomitant use of corticosteroids at baseline was estimated. Results: In patients achieving clinical remission (n = 27), a decrease in levels of FC (P = 0.005), MPO (P < 0.001), HNL (P < 0.001), and EDN (P < 0.001) was observed, whereas no significant decrease was seen in patients not achieving remission (n = 39). There was a significant difference in the change in the level of MPO (P = 0.01) and HNL (P = 0.02) between patients achieving clinical remission and those who did not, but changes in FC and EDN could not differentiate between these groups. Patients with concomitant systemic corticosteroids at inclusion had lower levels of HNL (P = 0.01) and EDN (P < 0.001) at baseline, compared with patients without corticosteroids. Discussion: Fecal MPO, HNL, and EDN are all promising biomarkers for assessing the treatment outcome of biologics in patients with IBD. Fecal levels of EDN and HNL are significantly affected by corticosteroids indicating a greater sensitivity to the effects of corticosteroids compared with levels of FC and MPO., This work was supported by the Swedish Foundation for Strategic Research (grant number RB13-016), Medical Faculty, Uppsala University, Uppsala, Sweden (M.C.) and the Orebro University Hospital Research Foundation (grant numbers OLL-936004, OLL-890291, OLL-790011, OLL-723021, and OLL-333321 to J.H.).

Published

2023

5. Elevated F-EDN correlates with mucosal eosinophil degranulation in patients with IBS : A possible association with microbiota?

Author

Casado-Bedmar, Maite, de-Faria, Felipe Meira, Biskou, Olga, Lindqvist, Carl Mårten, Ranasinghe, Purnika Damindi, Bednarska, Olga, Peterson, Christer, Walter, Susanna A., Carlson, Marie, Keita, Åsa V., Casado-Bedmar, Maite, de-Faria, Felipe Meira, Biskou, Olga, Lindqvist, Carl Mårten, Ranasinghe, Purnika Damindi, Bednarska, Olga, Peterson, Christer, Walter, Susanna A., Carlson, Marie, and Keita, Åsa V.

Abstract

Eosinophils have been linked to functional dyspepsia; however, less is known about their role in irritable bowel syndrome (IBS). This study tested the hypothesis of alterations in levels of fecal eosinophil-derived neurotoxin (F-EDN) and eosinophil density and degranulation within the colonic mucosa of IBS patients compared with healthy controls (HC). Colonic biopsies were collected from 37 IBS patients and 20 HC and analyzed for eosinophil numbers and local degranulation of eosinophil cationic protein (ECP) by histologic procedures. Fecal samples were collected for F-EDN and microbiota analysis. Differentiated 15HL-60 cells were used in vitro to investigate the direct effect of live bacteria on eosinophil activation measured by a colorimetric assay with o-phenylenediamine (OPD) substrate. We observed a higher number of eosinophils and increased extracellular ECP in the mucosa of IBS patients compared with HC. Moreover, F-EDN levels in IBS samples were elevated compared with HC and positively correlated to extracellular ECP. Metagenomic analysis showed significant correlations between bacterial composition and eosinophil measurements in both HC and IBS patients. In vitro experiments revealed an increased degranulation of 15HL-60 after stimulation with Salmonella typhimurium, Salmonella enterica, and Yersinia enterocolitica. To conclude, we could demonstrate alterations related to eosinophils in IBS, and, for the first time, a positive correlation between F-EDN levels and degranulated eosinophils in the colonic mucosa of IBS patients. Together our results suggest that eosinophils play a role in the pathophysiology of IBS and the mechanisms might be linked to an altered microbiota., Funding Agencies:Apotekare Hedberg Foundation Bengt Ihre Foundation SLS-788111 SLS-882561Ruth and Richard Julin Foundation 2017-00350 2019-00347County Council of Östergötland Lio-934618Mucosa Infection and Inflammation Center-MIIC Medical Faculty, Uppsala University, Uppsala Sweden

Published

2022

6. Mucosal Gene Transcript Signatures in Treatment Naïve Inflammatory Bowel Disease : A Comparative Analysis of Disease to Symptomatic and Healthy Controls in the European IBD-Character Cohort

Author

Vatn, Simen Svendsen, Lindstrøm, Jonas Christoffer, Moen, Aina E. F., Brackmann, Stephan, Tannæs, Tone M., Olbjørn, Christine, Bergemalm, Daniel, Keita, Åsa V., Gomollon, Fernando, Detlie, Trond Espen, Lüders, Torben, Kalla, Rahul, Adams, Alex, Satsangi, Jack, Jahnsen, Jørgen, Vatn, Morten H., Halfvarson, Jonas, Ricanek, Petr, Nilsen, Hilde, Vatn, Simen Svendsen, Lindstrøm, Jonas Christoffer, Moen, Aina E. F., Brackmann, Stephan, Tannæs, Tone M., Olbjørn, Christine, Bergemalm, Daniel, Keita, Åsa V., Gomollon, Fernando, Detlie, Trond Espen, Lüders, Torben, Kalla, Rahul, Adams, Alex, Satsangi, Jack, Jahnsen, Jørgen, Vatn, Morten H., Halfvarson, Jonas, Ricanek, Petr, and Nilsen, Hilde

Abstract

Background: Studies of the mucosal transcriptomic landscape have given new insight into the pathogenesis of inflammatory bowel disease (IBD). Recently, the predictive biomarker potential of gene expression signatures has been explored. To further investigate the mucosal gene expression in IBD, we recruited a cohort of treatment naïve patients and compared them to both symptomatic and healthy controls. Methods: Altogether, 323 subjects were included: Crohn's disease (N = 75), ulcerative colitis (N = 87) and IBD unclassified (N = 3). Additionally, there were two control groups: symptomatic controls (N = 131) and healthy controls (N = 27). Mucosal biopsies were collected during ileocolonoscopy and gene expression in inflamed and non-inflamed mucosa was explored. Gene expression profiling was performed using Agilent G3 Human Gene Expression 860K v3 One-Color microarray. We recorded information about treatment escalation to anti-TNF agents or surgery, and anti-TNF response, to explore predictive opportunities of the mucosal transcriptome. Results: Gene expression profiles in symptomatic controls in whom IBD had been excluded resembled that of IBD patients and diverged from that of healthy controls. In non-inflamed Crohn's disease and ulcerative colitis, gene set enrichment analysis revealed dysregulation of pathways involved in basic cellular biological processes. Mitochondria-associated pathways were dysregulated both in non-inflamed and inflamed Crohn's disease and ulcerative colitis (>2.6 normalized enrichment scores <-1.8). Gene expression signatures of Crohn's disease and ulcerative colitis did not predict time for treatment escalation (p = 0.175). No significant association was found between gene expression signatures and anti-TNF response. Conclusion: Non-inflamed samples are probably superior to inflamed samples when exploring gene expression signatures in IBD and might reveal underlying mechanisms central for disease initiation. The gene expression signatu, Funding agencies:EU FP7 grant: IBD-CHARACTER 2858546South-Eastern Norway Regional Health Authority 2014011 2018001

Published

2022

7. Elevated F-EDN correlates with mucosal eosinophil degranulation in patients with IBS : A possible association with microbiota?

Author

Casado-Bedmar, Maite, de-Faria, Felipe Meira, Biskou, Olga, Lindqvist, Carl Mårten, Ranasinghe, Purnika Damindi, Bednarska, Olga, Peterson, Christer, Walter, Susanna A., Carlson, Marie, Keita, Åsa V., Casado-Bedmar, Maite, de-Faria, Felipe Meira, Biskou, Olga, Lindqvist, Carl Mårten, Ranasinghe, Purnika Damindi, Bednarska, Olga, Peterson, Christer, Walter, Susanna A., Carlson, Marie, and Keita, Åsa V.

Abstract

Eosinophils have been linked to functional dyspepsia; however, less is known about their role in irritable bowel syndrome (IBS). This study tested the hypothesis of alterations in levels of fecal eosinophil-derived neurotoxin (F-EDN) and eosinophil density and degranulation within the colonic mucosa of IBS patients compared with healthy controls (HC). Colonic biopsies were collected from 37 IBS patients and 20 HC and analyzed for eosinophil numbers and local degranulation of eosinophil cationic protein (ECP) by histologic procedures. Fecal samples were collected for F-EDN and microbiota analysis. Differentiated 15HL-60 cells were used in vitro to investigate the direct effect of live bacteria on eosinophil activation measured by a colorimetric assay with o-phenylenediamine (OPD) substrate. We observed a higher number of eosinophils and increased extracellular ECP in the mucosa of IBS patients compared with HC. Moreover, F-EDN levels in IBS samples were elevated compared with HC and positively correlated to extracellular ECP. Metagenomic analysis showed significant correlations between bacterial composition and eosinophil measurements in both HC and IBS patients. In vitro experiments revealed an increased degranulation of 15HL-60 after stimulation with Salmonella typhimurium, Salmonella enterica, and Yersinia enterocolitica. To conclude, we could demonstrate alterations related to eosinophils in IBS, and, for the first time, a positive correlation between F-EDN levels and degranulated eosinophils in the colonic mucosa of IBS patients. Together our results suggest that eosinophils play a role in the pathophysiology of IBS and the mechanisms might be linked to an altered microbiota., Funding Agencies:Apotekare Hedberg Foundation Bengt Ihre Foundation SLS-788111 SLS-882561Ruth and Richard Julin Foundation 2017-00350 2019-00347County Council of Östergötland Lio-934618Mucosa Infection and Inflammation Center-MIIC Medical Faculty, Uppsala University, Uppsala Sweden

Published

2022

8. Mucosal Gene Transcript Signatures in Treatment Naïve Inflammatory Bowel Disease : A Comparative Analysis of Disease to Symptomatic and Healthy Controls in the European IBD-Character Cohort

Author

Vatn, Simen Svendsen, Lindstrøm, Jonas Christoffer, Moen, Aina E. F., Brackmann, Stephan, Tannæs, Tone M., Olbjørn, Christine, Bergemalm, Daniel, Keita, Åsa V., Gomollon, Fernando, Detlie, Trond Espen, Lüders, Torben, Kalla, Rahul, Adams, Alex, Satsangi, Jack, Jahnsen, Jørgen, Vatn, Morten H., Halfvarson, Jonas, Ricanek, Petr, Nilsen, Hilde, Vatn, Simen Svendsen, Lindstrøm, Jonas Christoffer, Moen, Aina E. F., Brackmann, Stephan, Tannæs, Tone M., Olbjørn, Christine, Bergemalm, Daniel, Keita, Åsa V., Gomollon, Fernando, Detlie, Trond Espen, Lüders, Torben, Kalla, Rahul, Adams, Alex, Satsangi, Jack, Jahnsen, Jørgen, Vatn, Morten H., Halfvarson, Jonas, Ricanek, Petr, and Nilsen, Hilde

Abstract

Background: Studies of the mucosal transcriptomic landscape have given new insight into the pathogenesis of inflammatory bowel disease (IBD). Recently, the predictive biomarker potential of gene expression signatures has been explored. To further investigate the mucosal gene expression in IBD, we recruited a cohort of treatment naïve patients and compared them to both symptomatic and healthy controls. Methods: Altogether, 323 subjects were included: Crohn's disease (N = 75), ulcerative colitis (N = 87) and IBD unclassified (N = 3). Additionally, there were two control groups: symptomatic controls (N = 131) and healthy controls (N = 27). Mucosal biopsies were collected during ileocolonoscopy and gene expression in inflamed and non-inflamed mucosa was explored. Gene expression profiling was performed using Agilent G3 Human Gene Expression 860K v3 One-Color microarray. We recorded information about treatment escalation to anti-TNF agents or surgery, and anti-TNF response, to explore predictive opportunities of the mucosal transcriptome. Results: Gene expression profiles in symptomatic controls in whom IBD had been excluded resembled that of IBD patients and diverged from that of healthy controls. In non-inflamed Crohn's disease and ulcerative colitis, gene set enrichment analysis revealed dysregulation of pathways involved in basic cellular biological processes. Mitochondria-associated pathways were dysregulated both in non-inflamed and inflamed Crohn's disease and ulcerative colitis (>2.6 normalized enrichment scores <-1.8). Gene expression signatures of Crohn's disease and ulcerative colitis did not predict time for treatment escalation (p = 0.175). No significant association was found between gene expression signatures and anti-TNF response. Conclusion: Non-inflamed samples are probably superior to inflamed samples when exploring gene expression signatures in IBD and might reveal underlying mechanisms central for disease initiation. The gene expression signatu, Funding agencies:EU FP7 grant: IBD-CHARACTER 2858546South-Eastern Norway Regional Health Authority 2014011 2018001

Published

2022

9. Characterization of the circulating transcriptomic landscape in inflammatory bowel disease provides evidence for dysregulation of multiple transcription factors including NFE2, SPI1, CEBPB, and IRF2

Author

Nowak, Jan K., Adams, Alex T., Kalla, Rahul, Lindstrøm, Jonas C., Vatn, Simen, Bergemalm, Daniel, Keita, Åsa V., Gomollón, Fernando, Jahnsen, Jørgen, Vatn, Morten H., Ricanek, Petr, Ostrowski, Jerzy, Walkowiak, Jaroslaw, Halfvarson, Jonas, Satsangi, Jack, Nowak, Jan K., Adams, Alex T., Kalla, Rahul, Lindstrøm, Jonas C., Vatn, Simen, Bergemalm, Daniel, Keita, Åsa V., Gomollón, Fernando, Jahnsen, Jørgen, Vatn, Morten H., Ricanek, Petr, Ostrowski, Jerzy, Walkowiak, Jaroslaw, Halfvarson, Jonas, and Satsangi, Jack

Abstract

AIM: To assess the pathobiological and translational importance of whole blood transcriptomic analysis in inflammatory bowel disease (IBD). METHODS: We analyzed whole blood expression profiles from paired-end sequencing in a discovery cohort of 590 Europeans recruited across six countries in the IBD Character initiative (newly diagnosed patients with Crohn's disease [CD, n = 156], ulcerative colitis [UC, n = 167], and controls [n = 267]), exploring differential expression (DESeq2), co-expression networks (WGCNA), and transcription factor involvement (EPEE, ChEA, DoRothEA). Findings were validated by analysis of an independent replication cohort (99 CD, 100 UC, and 95 controls). In the discovery cohort, we also defined baseline expression correlates of future treatment escalation using cross-validated elastic-net and random forest modelling, along with a pragmatic ratio detection procedure. RESULTS: Disease-specific transcriptomes were defined in IBD (8697 transcripts), CD (7152), and UC (8521), with the most highly significant changes in single genes, including CD177 (log2-fold change [LFC] = 4.63, p = 4.05 × 10 -118), MCEMP1 (LFC = 2.45, p = 7.37 × 10 -109), and S100A12 (LFC = 2.31, p = 2.15 × 10 -93). Significantly over-represented pathways included IL-1 (p = 1.58 × 10 -11), IL-4, and IL-13 (p = 8.96 × 10 -9). Highly concordant results were obtained using multiple regulatory activity inference tools applied to the discovery and replication cohorts. These analyses demonstrated central roles in IBD for the transcription factors NFE2, SPI1 (PU.1), CEBPB, and IRF2, all regulators of cytokine signaling, based on a consistent signal across cohorts and transcription factor ranking methods. A number of simple transcriptome-based models were associated with the need for treatment escalation, including the binary CLEC5A/CDH2 expression ratio in UC (hazard ratio = 23.4, 95% CI 5.3-102.0). CONCLUSION: Transcriptomic analysis has allowed for a detailed characterization of IBD, Funding agency:Polish National Science Centre 2017/25/B/NZ5/02783

Published

2022

10. Systemic Inflammation in Preclinical Ulcerative Colitis

Author

Bergemalm, Daniel, Andersson, Erik, Hultdin, Johan, Eriksson, Carl, Rush, Stephen T., Kalla, Rahul, Adams, Alex T., Keita, Åsa V., D'Amato, Mauro, Gomollon, Fernando, Jahnsen, Jørgen, Arnott, Ian D., Bayes, Monica, Bonfiglio, Ferdinando, Boyapati, Ray K., Carstens, Adam, Casén, Christina, Ciemniejewska, Ewa, Dahl, Fredrik A., Detlie, Trond Espen, Drummond, Hazel E., Ekeland, Gunn S., Ekman, Daniel, Frengen, Anna B., Gullberg, Mats, Gut, Ivo G., Gut, Marta, Heath, Simon C., Hjelm, Fredrik, Hjortswang, Henrik, Ho, Gwo-Tzer, Jonkers, Daisy, Söderholm, Johan, Kennedy, Nicholas A., Lees, Charles W., Lindahl, Torbjørn, Lindqvist, Mårten, Merkel, Angelika, Modig, Eddie, Moen, Aina E.F., Nilsen, Hilde, Nimmo, Elaine R., Noble, Colin L., Nordberg, Niklas, O'Leary, Kate R., Ocklind, Anette, Olbjørn, Christine, Pettersson, Erik, Pierik, Marieke, Dominique, Ricanek, Petr, Satsangi, Jack, Repsilber, Dirk, Karling, Pontus, Halfvarson, Jonas, Bergemalm, Daniel, Andersson, Erik, Hultdin, Johan, Eriksson, Carl, Rush, Stephen T., Kalla, Rahul, Adams, Alex T., Keita, Åsa V., D'Amato, Mauro, Gomollon, Fernando, Jahnsen, Jørgen, Arnott, Ian D., Bayes, Monica, Bonfiglio, Ferdinando, Boyapati, Ray K., Carstens, Adam, Casén, Christina, Ciemniejewska, Ewa, Dahl, Fredrik A., Detlie, Trond Espen, Drummond, Hazel E., Ekeland, Gunn S., Ekman, Daniel, Frengen, Anna B., Gullberg, Mats, Gut, Ivo G., Gut, Marta, Heath, Simon C., Hjelm, Fredrik, Hjortswang, Henrik, Ho, Gwo-Tzer, Jonkers, Daisy, Söderholm, Johan, Kennedy, Nicholas A., Lees, Charles W., Lindahl, Torbjørn, Lindqvist, Mårten, Merkel, Angelika, Modig, Eddie, Moen, Aina E.F., Nilsen, Hilde, Nimmo, Elaine R., Noble, Colin L., Nordberg, Niklas, O'Leary, Kate R., Ocklind, Anette, Olbjørn, Christine, Pettersson, Erik, Pierik, Marieke, Dominique, Ricanek, Petr, Satsangi, Jack, Repsilber, Dirk, Karling, Pontus, and Halfvarson, Jonas

Abstract

Background & Aims: Preclinical ulcerative colitis is poorly defined. We aimed to characterize the preclinical systemic inflammation in ulcerative colitis, using a comprehensive set of proteins. Methods: We obtained plasma samples biobanked from individuals who developed ulcerative colitis later in life (n = 72) and matched healthy controls (n = 140) within a population-based screening cohort. We measured 92 proteins related to inflammation using a proximity extension assay. The biologic relevance of these findings was validated in an inception cohort of patients with ulcerative colitis (n = 101) and healthy controls (n = 50). To examine the influence of genetic and environmental factors on these markers, a cohort of healthy twin siblings of patients with ulcerative colitis (n = 41) and matched healthy controls (n = 37) were explored. Results: Six proteins (MMP10, CXCL9, CCL11, SLAMF1, CXCL11 and MCP-1) were up-regulated (P < .05) in preclinical ulcerative colitis compared with controls based on both univariate and multivariable models. Ingenuity Pathway Analyses identified several potential key regulators, including interleukin-1β, tumor necrosis factor, interferon-gamma, oncostatin M, nuclear factor-κB, interleukin-6, and interleukin-4. For validation, we built a multivariable model to predict disease in the inception cohort. The model discriminated treatment-naïve patients with ulcerative colitis from controls with leave-one-out cross-validation (area under the curve = 0.92). Consistently, MMP10, CXCL9, CXCL11, and MCP-1, but not CCL11 and SLAMF1, were significantly up-regulated among the healthy twin siblings, even though their relative abundances seemed higher in incident ulcerative colitis. Conclusions: A set of inflammatory proteins are up-regulated several years before a diagnosis of ulcerative colitis. These proteins were highly predictive of an ulcerative colitis diagnosis, and some seemed to be up-regulated already at exposure to genetic and environ

Published

2021

11. Systemic Inflammation in Preclinical Ulcerative Colitis

Author

Bergemalm, Daniel, Andersson, Erik, Hultdin, Johan, Eriksson, Carl, Rush, Stephen T., Kalla, Rahul, Adams, Alex T., Keita, Åsa V., D'Amato, Mauro, Gomollon, Fernando, Jahnsen, Jorgen, Ricanek, Petr, Satsangi, Jack, Repsilber, Dirk, Karling, Pontus, Halfvarson, Jonas, Bergemalm, Daniel, Andersson, Erik, Hultdin, Johan, Eriksson, Carl, Rush, Stephen T., Kalla, Rahul, Adams, Alex T., Keita, Åsa V., D'Amato, Mauro, Gomollon, Fernando, Jahnsen, Jorgen, Ricanek, Petr, Satsangi, Jack, Repsilber, Dirk, Karling, Pontus, and Halfvarson, Jonas

Abstract

BACKGROUND & AIMS: Pre-clinical ulcerative colitis is poorly defined. We aimed to characterize the pre-clinical systemic inflammation in ulcerative colitis, using a comprehensive set of proteins. METHODS: We obtained plasma samples, biobanked from individuals who later in life developed ulcerative colitis (n=72), and matched healthy controls (n=140), within a population-based screening cohort. We measured 92 proteins related to inflammation using a proximity extension assay. The biological relevance of these findings were validated in an inception cohort of ulcerative colitis patients (n=101), and healthy controls (n=50). To examine the influence of genetic and environmental factors on these markers, a cohort of healthy twin siblings of ulcerative colitis patients (n=41) and matched healthy controls (n=37) were explored. RESULTS: Six proteins (MMP10, CXCL9, CCL11, SLAMF1, CXCL11 and MCP1) were upregulated (p<0.05) in pre-clinical ulcerative colitis compared to controls based on both univariate and mulativariable models. Ingenuity Pathway Analyses identified several potential key regulators, including IL-1b, TNF, IFN-gamma, OSM, NFĸB, IL-6 and IL-4. For validation, we built a multivariable model to predict disease in the inception cohort. The model discriminated treatment-naïve ulcerative colitis patients from controls with leave-one-out cross-validation (AUC=0.92). Consistently, MMP10, CXCL9, CXCL11, and MCP-1, but not CCL11 and SLAMF1, were significantly upregulated among the healthy twin siblings, even though their relative abundances seemed higher in incident ulcerative colitis. CONCLUSIONS: A set of inflammatory proteins are upregulated several years before a diagnosis of ulcerative colitis. These proteins were highly predictive of an ulcerative colitis diagnosis, and some seemed to be upregulated already at exposure to genetic and environmental risk factors., Funding agencies:Bengt Ihre research foundationOrebro University Hospital Research Foundation OLL-709831 OLL-936004 OLL-890291 OLL-790011 OLL-723021

Published

2021

12. Altered interaction between enteric glial cells and mast cells in the colon of women with irritable bowel syndrome

Author

de-Faria, Felipe Meira, Casado-Bedmar, Maite, Lindqvist, Carl Mårten, Jones, Michael P., Walter, Susanna A., Keita, Åsa V., de-Faria, Felipe Meira, Casado-Bedmar, Maite, Lindqvist, Carl Mårten, Jones, Michael P., Walter, Susanna A., and Keita, Åsa V.

Abstract

Background: Enteric glial cells (EGC) and mast cells (MC) are intimately associated with gastrointestinal physiological functions. We aimed to investigate EGC-MC interaction in irritable bowel syndrome (IBS), a gut-brain disorder linked to increased intestinal permeability, and MC. Methods: Parallel approaches were used to quantify EGC markers in colonic biopsies from healthy controls (HC) and patients with IBS. Data were correlated with MC, vasoactive intestinal polypeptide (VIP) and VIP receptors (VPAC1/VPAC2) expressions, and bacterial translocation through biopsies mounted in Ussing chambers. In addition, we investigated the effects of EGC mediators on colonic permeability and the pharmacological-induced responses of EGC and MC cell lines. Key Results: Immunofluorescence of IBS colonic mucosa, as well as Western blotting and ELISA of IBS biopsy lysates, revealed increased glial fibrillary intermediate filament (GFAP) expression, indicating EGC activation. Mucosal GFAP correlated with increased MC and VPAC1(+)MC numbers and decreased VIP+MC, which seemed to control bacterial translocation in HC. In the contrary, EGC activation in IBS correlated with less MC and VPAC1(+) MC numbers, and more VIP+ MC. In vitro, MC and EGC cell lines showed intracellular calcium responses to each other's mediators. Furthermore, EGC mediators prevented VIP-induced MC degranulation, while MC mediators induced a reactive EGC phenotype. In Ussing chambers, EGC mediators decreased paracellular passage through healthy colonic biopsies. Conclusions & Inferences: Findings suggest the involvement of EGC and MC in the control of barrier function in the human colon and indicate a potential EGC-MC interaction that seems altered in IBS, with detrimental consequences to colonic permeability. Altogether, results suggest that imbalanced EGC-MC communication contributes to the pathophysiology of IBS., Funding Agencies:Apotekare Hedberg Foundation Bengt Ihre Foundation SLS-788111 SLS-882561Ruth and Richard Julin Foundation 2017-00350 2019-00347Mucosa Infection and Inflammation Center-MIIC AFA Insurance Research Foundation County Council of Östergötland Lio-934618 Lio-902661

Published

2021

13. The Intestinal Barrier and Current Techniques for the Assessment of Gut Permeability

Author

Schoultz, Ida, Keita, Åsa V., Schoultz, Ida, and Keita, Åsa V.

Abstract

The intestinal barrier is essential in human health and constitutes the interface between the outside and the internal milieu of the body. A functional intestinal barrier allows absorption of nutrients and fluids but simultaneously prevents harmful substances like toxins and bacteria from crossing the intestinal epithelium and reaching the body. An altered intestinal permeability, a sign of a perturbed barrier function, has during the last decade been associated with several chronic conditions, including diseases originating in the gastrointestinal tract but also diseases such as Alzheimer and Parkinson disease. This has led to an intensified interest from researchers with diverse backgrounds to perform functional studies of the intestinal barrier in different conditions. Intestinal permeability is defined as the passage of a solute through a simple membrane and can be measured by recording the passage of permeability markers over the epithelium via the paracellular or the transcellular route. The methodological tools to investigate the gut barrier function are rapidly expanding and new methodological approaches are being developed. Here we outline and discuss, in vivo, in vitro and ex vivo techniques and how these methods can be utilized for thorough investigation of the intestinal barrier., Funding Agencies:Faculty of Medicine and Health, Örebro University, Sweden LIONS international Foundation Faculty of Medicine and Health Sciences, Linköping University

Published

2020

14. Effects of Dietary Fibres on Acute Indomethacin-Induced Intestinal Hyperpermeability in the Elderly : A Randomised Placebo Controlled Parallel Clinical Trial

Author

Ganda Mall, John Peter, Fart, Frida, Sabet, Julia A., Lindqvist, Carl Mårten, Nestestog, Ragnhild, Hegge, Finn Terje, Keita, Åsa, V, Brummer, Robert Jan, Schoultz, Ida, Ganda Mall, John Peter, Fart, Frida, Sabet, Julia A., Lindqvist, Carl Mårten, Nestestog, Ragnhild, Hegge, Finn Terje, Keita, Åsa, V, Brummer, Robert Jan, and Schoultz, Ida

Abstract

The effect of dietary fibres on intestinal barrier function has not been well studied, especially in the elderly. We aimed to investigate the potential of the dietary fibres oat beta-glucan and wheat arabinoxylan to strengthen the intestinal barrier function and counteract acute non-steroid anti-inflammatory drug (indomethacin)-induced hyperpermeability in the elderly. A general population of elderly subjects (>= 65 years,n= 49) was randomised to a daily supplementation (12g/day) of oat beta-glucan, arabinoxylan or placebo (maltodextrin) for six weeks. The primary outcome was change in acute indomethacin-induced intestinal permeability from baseline, assessed by an in vivo multi-sugar permeability test. Secondary outcomes were changes from baseline in: gut microbiota composition, systemic inflammatory status and self-reported health. Despite a majority of the study population (85%) showing a habitual fibre intake below the recommendation, no significant effects on acute indomethacin-induced intestinal hyperpermeability in vivo or gut microbiota composition were observed after six weeks intervention with either dietary fibre, compared to placebo., Funding Agencies:European Union (EU) 289517Bo Rydin foundation F0514

Published

2020