Your search keyword '"Ahmed M. I. Elfiky"' showing total 6 results

1. A BET Protein Inhibitor Targeting Mononuclear Myeloid Cells Affects Specific Inflammatory Mediators and Pathways in Crohn’s Disease

Author

Ahmed M. I. Elfiky, Ishtu L. Hageman, Marte A. J. Becker, Jan Verhoeff, Andrew Y. F. Li Yim, Vincent W. Joustra, Lieven Mulders, Ivan Fung, Inmaculada Rioja, Rab K. Prinjha, Nicholas N. Smithers, Rebecca C. Furze, Palwinder K. Mander, Matthew J. Bell, Christianne J. Buskens, Geert R. D’Haens, Manon E. Wildenberg, and Wouter J. de Jonge

Subjects

BET inhibitor, CES1, IBD, Cytology, QH573-671

Abstract

Background: Myeloid cells are critical determinants of the sustained inflammation in Crohn’s Disease (CD). Targeting such cells may be an effective therapeutic approach for refractory CD patients. Bromodomain and extra-terminal domain protein inhibitors (iBET) are potent anti-inflammatory agents; however, they also possess wide-ranging toxicities. In the current study, we make use of a BET inhibitor containing an esterase sensitive motif (ESM-iBET), which is cleaved by carboxylesterase-1 (CES1), a highly expressed esterase in mononuclear myeloid cells. Methods: We profiled CES1 protein expression in the intestinal biopsies, peripheral blood, and CD fistula tract (fCD) cells of CD patients using mass cytometry. The anti-inflammatory effect of ESM-iBET or its control (iBET) were evaluated in healthy donor CD14+ monocytes and fCD cells, using cytometric beads assay or RNA-sequencing. Results: CES1 was specifically expressed in monocyte, macrophage, and dendritic cell populations in the intestinal tissue, peripheral blood, and fCD cells of CD patients. ESM-iBET inhibited IL1β, IL6, and TNFα secretion from healthy donor CD14+ monocytes and fCD immune cells, with 10- to 26-fold more potency over iBET in isolated CD14+ monocytes. Transcriptomic analysis revealed that ESM-iBET inhibited multiple inflammatory pathways, including TNF, JAK-STAT, NF-kB, NOD2, and AKT signaling, with superior potency over iBET. Conclusions: We demonstrate specific CES1 expression in mononuclear myeloid cell subsets in peripheral blood and inflamed tissues of CD patients. We report that low dose ESM-iBET accumulates in CES1-expressing cells and exerts robust anti-inflammatory effects, which could be beneficial in refractory CD patients.

Published

2022

2. Carboxylesterase-1 Assisted Targeting of HDAC Inhibitors to Mononuclear Myeloid Cells in Inflammatory Bowel Disease

Author

Patricia van Hamersveld, Laura Tomlinson, Ishtu Hageman, Ahmed M. I. Elfiky, Sigrid E.M. Heinsbroek, Juan J. Garcia-Vallejo, Jan Verhoeff, Wouter J. de Jonge, Andrew Y. F. Li Yim, Matthew J Bell, Huw D. Lewis, Manon E. Wildenberg, Iris Admiraal, Rab K. Prinjha, Rebecca C. Furze, Richard Gregory, Mohammed Ghiboub, Palwinder K. Mander, Inmaculada Rioja, Manon de Krijger, Olaf Welting, Shafaque Rahman, Molecular cell biology and Immunology, Graduate School, Tytgat Institute for Liver and Intestinal Research, Amsterdam Gastroenterology Endocrinology Metabolism, AII - Inflammatory diseases, Human Genetics, ACS - Atherosclerosis & ischemic syndromes, Amsterdam Reproduction & Development (AR&D), and Gastroenterology and Hepatology

Subjects

Lipopolysaccharides, T cell, CD14, IBD, CD16, Inflammatory bowel disease, Monocytes, Mice, HDAC inhibitor, Crohn Disease, medicine, Macrophage, CES1, Animals, Humans, Myeloid Cells, Colitis, Intestinal Mucosa, CD68, business.industry, Gastroenterology, General Medicine, medicine.disease, Inflammatory Bowel Diseases, Histone Deacetylase Inhibitors, medicine.anatomical_structure, Monocyte differentiation, Cancer research, business, Carboxylic Ester Hydrolases

Abstract

Background and AimsHistone deacetylase inhibitors [HDACi] exert potent anti-inflammatory effects. Because of the ubiquitous expression of HDACs, clinical utility of HDACi is limited by off-target effects. Esterase-sensitive motif [ESM] technology aims to deliver ESM-conjugated compounds to human mononuclear myeloid cells, based on their expression of carboxylesterase 1 [CES1]. This study aims to investigate utility of an ESM-tagged HDACi in inflammatory bowel disease [IBD].MethodsCES1 expression was assessed in human blood, in vitro differentiated macrophage and dendritic cells, and Crohn’s disease [CD] colon mucosa, by mass cytometry, quantitative polymerase chain reaction [PCR], and immunofluorescence staining, respectively. ESM-HDAC528 intracellular retention was evaluated by mass spectrometry. Clinical efficacy of ESM-HDAC528 was tested in dextran sulphate sodium [DSS]-induced colitis and T cell transfer colitis models using transgenic mice expressing human CES1 under the CD68 promoter.ResultsCES1 mRNA was highly expressed in human blood CD14+ monocytes, in vitro differentiated and lipopolysaccharide [LPS]-stimulated macrophages, and dendritic cells. Specific hydrolysis and intracellular retention of ESM-HDAC528 in CES1+ cells was demonstrated. ESM-HDAC528 inhibited LPS-stimulated IL-6 and TNF-α production 1000 times more potently than its control, HDAC800, in CES1high monocytes. In healthy donor peripheral blood, CES1 expression was significantly higher in CD14++CD16- monocytes compared with CD14+CD16++ monocytes. In CD-inflamed colon, a higher number of mucosal CD68+ macrophages expressed CES1 compared with non-inflamed mucosa. In vivo, ESM-HDAC528 reduced monocyte differentiation in the colon and significantly improved colitis in a T cell transfer model, while having limited potential in ameliorating DSS-induced colitis.ConclusionsWe demonstrate that monocytes and inflammatory macrophages specifically express CES1, and can be preferentially targeted by ESM-HDAC528 to achieve therapeutic benefit in IBD.

Published

2022

3. Selective targeting of epigenetic readers and histone deacetylases in autoimmune and inflammatory diseases: Recent advances and future perspectives

Author

Nicola Harker, Menno P.J. de Winther, Wouter J. de Jonge, Ahmed M. I. Elfiky, David F. Tough, and Mohammed Ghiboub

Subjects

Inhibitor, Medicine (miscellaneous), Bromodomain, Context (language use), Review, Bioinformatics, Chromatin remodeling, 03 medical and health sciences, 0302 clinical medicine, Histone deacetylases, Medicine, Epigenetics, Esterase sensitive motif, 030304 developmental biology, 0303 health sciences, biology, Drug discovery, business.industry, Translation (biology), Autoimmune and inflammatory diseases, Histone, Targeted drug delivery, 030220 oncology & carcinogenesis, biology.protein, business

Abstract

Histone deacetylases (HDACs) and bromodomain-containing proteins (BCPs) play a key role in chromatin remodeling. Based on their ability to regulate inducible gene expression in the context of inflammation and cancer, HDACs and BCPs have been the focus of drug discovery efforts, and numerous small-molecule inhibitors have been developed. However, dose-limiting toxicities of the first generation of inhibitors, which typically target multiple HDACs or BCPs, have limited translation to the clinic. Over the last decade, an increasing effort has been dedicated to designing class-, isoform-, or domain-specific HDAC or BCP inhibitors, as well as developing strategies for cell-specific targeted drug delivery. Selective inhibition of the epigenetic modulators is helping to elucidate the functions of individual epigenetic proteins and has the potential to yield better and safer therapeutic strategies. In accordance with this idea, several in vitro and in vivo studies have reported the ability of more selective HDAC/BCP inhibitors to recapitulate the beneficial effects of pan-inhibitors with less unwanted adverse events. In this review, we summarize the most recent advances with these strategies, discussing advantages and limitations of these approaches as well as some therapeutic perspectives, focusing on autoimmune and inflammatory diseases.

Published

2021

4. P032 MiR-511 deficiency aggravates T cell transfer colitis in mice

Author

Theodorus B. M. Hakvoort, Ahmed M. I. Elfiky, Caroline Verseijden, P H P van Hamersveld, Sigrid E.M. Heinsbroek, W J de Jonge, Shafaque Rahman, Sybren L. Meijer, and Olaf Welting

Subjects

medicine.diagnostic_test, business.industry, T cell, Gastroenterology, Spleen, Inflammation, General Medicine, medicine.disease, Flow cytometry, FOXP3 gene, medicine.anatomical_structure, Cancer research, medicine, Transfer technique, Colitis, medicine.symptom, business, Interleukin 4

Abstract

Background MiR-511 is embedded in intron region 5 of the CD206/MRC1 gene, expressed by macrophage and dendritic cell populations. In this study, we aimed to investigate the effect of MiR-511 deficiency on intestinal inflammation in a murine T cell transfer colitis model. Methods A double MiR-511- and Rag-1 (knockout) KO mouse was generated and a T cell transfer colitis was induced by intraperitoneal injection of naïve T cells from donor WT mice. Since these mice lack mature T and B cells, first signs of inflammation appeared at week 3 after T cell injection. An endoscopy score was obtained to determine inflammation at week 3 and 5, respectively. The experiment was terminated at week 5 and severity of inflammation was assessed on the basis of weight loss, colon weight/length ratio, histology score, spleen weight and disease activity index. In addition, flow cytometry was performed for analysing immune cell populations (monocyte, macrophages, dendritic cells, neutrophils) in the colons of both control and colitis groups and T cells in the spleens of colitis group, respectively. Results Following the induction of T cell transfer colitis, colon weight/length ratio, spleen weight and endoscopic score were significantly increased in the double KO mice compared to Rag-1 KO control mice. A higher histology score and disease activity index in the double KO with no change in weight loss compared to Rag-1 KO control mice was observed. A significant increase in monocyte population in the colons of double KO was seen and increased numbers of monocytes was also observed in the double KO control group with no inflammation. Also, a higher influx of T cells in the double KO mice with a significant increase in Foxp3 and IL4 population was observed in the group with colitis. Conclusion MiR-511 deficiency aggravates intestinal inflammation compared to Rag-1 KO control mice. Also, a higher presence of monocyte as well as T cell populations were observed in these mice. Together these data show that MiR-511 is involved in the regulation of intestinal health. Future research will focus on underlying mechanisms.

Published

2021

5. Fr481 CARBOXYLESTERASE-1 ASSISTED TARGETING OF HDAC INHIBITOR TO MONONUCLEAR MYELOID CELLS ATTENUATES COLON INFLAMMATION IN T CELL TRANSFER COLITIS MURINE MODEL

Author

Patricia van Hamersveld, Jan Verhoeff, Ishtu Hageman, Rebecca C. Furze, Pal Mander, Sigrid E.M. Heinsbroek, Juan J. Garcia-Vallejo, Wouter J. de Jonge, Ahmed M. I. Elfiky, Manon E. Wildenberg, Nicholas Smithers, Inmaculada Rioja, Matthew J Bell, Huw D. Lewis, Olaf Welting, and M Becker

Subjects

Hepatology, Chemistry, T cell, Carboxylesterase 1, Gastroenterology, Colon inflammation, medicine.disease, medicine.anatomical_structure, Murine model, Myeloid cells, medicine, HDAC inhibitor, Cancer research, Colitis

Published

2021

6. Mo1104 MONONUCLEAR MYELOID CELL TARGETED HISTONE DEACETYLASE (HDAC) INHIBITOR DEMONSTRATES POTENT ACTIVITY IN MONOCYTES AND IMPAIRS COLON MONOCYTES TO MACROPHAGE DIFFERENTIATION DURING ACUTE DSS COLITIS

Author

Patricia van Hamersveld, Ahmed M. I. Elfiky, Wouter J. de Jonge, Rebecca C. Furze, Olaf Welting, Mohammed Ghiboub, M Becker, Manon E. Wildenberg, Pal Mander, Sigrid E.M. Heinsbroek, Matthew J Bell, Menno P.J. de Winther, Huw D. Lewis, Shafaque Rahman, and iris van den berg

Subjects

medicine.anatomical_structure, Myeloid, Hepatology, Macrophage differentiation, Chemistry, Cell, Gastroenterology, medicine, HDAC inhibitor, Cancer research, Histone deacetylase, Colitis, medicine.disease

Published

2020