Your search keyword '"Jung, Yunjin"' showing total 45 results

1. Ionically bridged dexamethasone sodium phosphate-zinc-PLGA nanocomplex in alginate microgel for the local treatment of ulcerative colitis.

Author

Saparbayeva A, Lee J, Hlaing SP, Kim J, Kwak D, Kim H, Lee EH, Hwang S, Kim MS, Moon HR, Jung Y, and Yoo JW

Subjects

Mice, Animals, Zinc adverse effects, Alginates adverse effects, Colon pathology, Dextran Sulfate adverse effects, Disease Models, Animal, Colitis, Ulcerative drug therapy, Colitis, Ulcerative chemically induced, Colitis, Ulcerative pathology, Microgels therapeutic use, Colitis chemically induced

Abstract

Colon-targeted oral drug delivery systems comprising nanoparticles and microparticles have emerged as promising tools for the treatment of ulcerative colitis (UC) because they minimize side effects and maximize the local drug concentration. Dexamethasone sodium phosphate (DSP) is a potent anti-inflammatory glucocorticoid used for the treatment of UC. However, it remains a rather short-term treatment option owing to its side effects. In the present study, we developed the alginate gel encapsulating ionically bridged DSP-zinc-poly(lactic-co-glycolic acid) (PLGA) nanocomplex (DZP-NCs-in-microgel) for the oral local treatment of UC. The successful encapsulation of DSP-zinc-PLGA nanocomplex (DZP-NCs) in alginate microgel was confirmed by SEM imaging. The prepared gel released DZP-NCs in the stimulated intestinal fluid and dampened the release of DSP in the upper gastrointestinal tract. Furthermore, DZP-NCs-in-microgel alleviated colonic inflammation in a mouse model of dextran sodium sulfate-induced colitis by relieving clinical symptoms and histological marks. Our results suggest a novel approach for the oral colon-targeted delivery of dexamethasone sodium phosphate for the treatment of UC., (© 2023. The Pharmaceutical Society of Korea.)

Published

2023

2. N-Acetylserotonin is an oxidation-responsive activator of Nrf2 ameliorating colitis in rats.

Author

Kang C, Jeong S, Kim J, Ju S, Im E, Heo G, Park S, Yoo JW, Lee J, Yoon IS, and Jung Y

Subjects

Rats, Animals, NF-E2-Related Factor 2 metabolism, Heme Oxygenase-1 metabolism, Anti-Inflammatory Agents therapeutic use, Melatonin pharmacology, Melatonin therapeutic use, Colitis chemically induced, Colitis drug therapy, Colitis metabolism

Abstract

N-Acetylserotonin (NAS) is an intermediate in the melatonin biosynthetic pathway. We investigated the anti-inflammatory activity of NAS by focusing on its chemical feature oxidizable to an electrophile. NAS was readily oxidized by reaction with HOCl, an oxidant produced in the inflammatory state. HOCl-reacted NAS (Oxi-NAS), but not NAS, activated the anti-inflammatory nuclear factor erythroid 2-related factor 2 (Nrf2)-heme oxygenase (HO)-1 pathway in cells. Chromatographic and mass analyses demonstrated that Oxi-NAS was the iminoquinone form of NAS and could react with N-acetylcysteine possessing a nucleophilic thiol to form a covalent adduct. Oxi-NAS bound to Kelch-like ECH-associated protein 1, resulting in Nrf2 dissociation. Moreover, rectally administered NAS increased the levels of nuclear Nrf2 and HO-1 proteins in the inflamed colon of rats. Simultaneously, NAS was converted to Oxi-NAS in the inflamed colon. Rectal NAS mitigated colonic damage and inflammation. The anticolitic effects were significantly compromised by the coadministration of an HO-1 inhibitor., (© 2022 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2023

3. On-demand reconstitutable hyaluronic acid-doped azathioprine microcrystals effectively ameliorate ulcerative colitis via selective accumulation in inflamed tissues.

Author

Lee J, Oshi MA, Kwak D, Kim H, Kim J, Hlaing SP, Saparbayeva A, Hwang S, Jung Y, and Yoo JW

Subjects

Mice, Animals, Azathioprine adverse effects, Hyaluronic Acid therapeutic use, Colitis, Ulcerative drug therapy, Colitis, Ulcerative chemically induced, Colitis chemically induced, Colitis drug therapy

Abstract

Although CD44-targeted delivery of pure drug microcrystals of azathioprine (AZA) could be a desirable approach to treat ulcerative colitis (UC), premature drug release and systemic absorption before reaching the colitis region remain a major obstacle. In this study, to overcome these limitations, we developed on-demand reconstitutable HA-doped AZA microcrystals (EFS/HA-AZAs) via incorporating hyaluronic acid (HA)-doped AZA microcrystals (HA-AZAs) into a Eudragit FS (EFS) microcomposite. Since EFS acts as a protective layer, the premature release of AZA in the simulated conditions of the stomach and small intestine was substantially reduced, while HA-AZAs were successfully reconstituted from the EFS/HA-AZAs in the colonic environment, resulting from the pH-triggered dissolution of EFS. After complete reconstitution of HA-AZAs in the colon, HA-AZAs selectively accumulated in the inflamed region via the HA-CD44 interaction. Owing to successful colitis-targeted delivery, EFS/HA-AZAs showed potent anti-inflammatory effects in a dextran sulfate sodium-induced murine colitis model within 7 days without systemic toxicity. These results suggest that EFS/HA-AZAs could be a promising drug delivery system for UC treatment.

Published

2022

4. A Colon-Targeted Prodrug of Riluzole Improves Therapeutic Effectiveness and Safety upon Drug Repositioning of Riluzole to an Anti-Colitic Drug.

Author

Park S, Kang C, Kim J, Ju S, Yoo JW, Yoon IS, Kim MS, Lee J, and Jung Y

Subjects

Rats, Animals, Riluzole therapeutic use, Riluzole pharmacology, Drug Repositioning, Rats, Sprague-Dawley, Glycogen Synthase Kinase 3 beta, Colon, Anti-Inflammatory Agents chemistry, Prodrugs chemistry, Colitis chemically induced, Colitis drug therapy

Abstract

Riluzole (RLZ) is a neuroprotective drug indicated for amyotrophic lateral sclerosis. To examine the feasibility of RLZ for repositioning as an anti-inflammatory bowel disease (IBD) drug, RLZ (2, 5, and 10 mg/kg) was administered orally to rats with colitis induced by 2,4-dinitrobenzenesulfonic acid. Oral RLZ was effective against rat colitis in a dose-dependent manner, which was statistically significant at doses over 5 mg/kg. To address safety issues upon repositioning and further improve anti-colitic effectiveness, RLZ was coupled with salicylic acid (SA) via an azo-bond to yield RLZ-azo-SA (RAS) for the targeted colonic delivery of RLZ. Upon oral gavage, RAS (oral RAS) was efficiently delivered to and activated to RLZ in the large intestine, and systemic absorption of RLZ was substantially reduced. Oral RAS ameliorated colonic damage and inflammation in rat colitis and was more effective than oral RLZ and sulfasalazine, a current anti-IBD drug. Moreover, oral RAS potently inhibited glycogen synthase kinase 3β (GSK3β) in the inflamed distal colon, leading to the suppression of NFκB activity and an increase in the level of the anti-inflammatory cytokine interleukin-10. Taken together, RAS, which enables RLZ to be delivered to and inhibit GSK3β in the inflamed colon, may facilitate repositioning of RLZ as an anti-IBD drug.

Published

2022

5. Design and evaluation of IKK-activated GSK3β inhibitory peptide as an inflammation-responsive anti-colitic therapeutic.

Author

Hong S, Ju S, Yoo JW, Ha NC, and Jung Y

Subjects

Animals, Glycogen Synthase Kinase 3 beta, Inflammation chemically induced, Inflammation drug therapy, Peptides, Rats, Trinitrobenzenesulfonic Acid, Colitis chemically induced, Colitis drug therapy

Abstract

Glycogen synthase kinase-3β (GSK3β), a multi-functional kinase, is a promising therapeutic target for the treatment of inflammation. Inhibitory κB kinase (IKK)-activated GSK3β inhibitory peptide (IAGIP) was designed as an inflammation-responsive anti-colitic therapeutic. To optimize therapeutic efficiency, IAGIP was tested using two different drug delivery techniques: colon-targeted delivery and cell-permeable peptide modification. In cell-based experiments, in response to tumor necrosis factor (TNF)- and lipopolysaccharide (LPS)-mediated activation of IKK, cell-permeable IAGIP (CTP-IAGIP) inhibited GSK3β, leading to increased production of anti-inflammatory cytokine interleukin-10 (IL-10) and suppression of TNF- and LPS-induced NFκB activity. Oral gavage of CTP-IAGIP loaded in the colon-targeted capsule attenuated 2,4,6-trinitrobenzene sulfonic acid-induced rat colitis and lowered the expression levels of NFκB-regulated proteins in the inflamed colons. CTP-IAGIP further induced IL-10 production in the inflamed colonic tissues; however, the levels of IL-10 were not affected in the normal colonic tissue or colonic tissue in which inflammation had subsided. Collectively, our data suggest that IAGIP administered using the aforementioned drug delivery techniques is an orally active anti-colitic drug selectively responding to inflammation.

Published

2021

6. Preparation and Evaluation of Colon-Targeted Prodrugs of the Microbial Metabolite 3-Indolepropionic Acid as an Anticolitic Agent.

Author

Lee H, Park S, Ju S, Kim S, Yoo JW, Yoon IS, Min DS, and Jung Y

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents chemistry, Colitis chemically induced, Colitis immunology, Colitis pathology, Colon drug effects, Colon immunology, Colon pathology, Dinitrofluorobenzene administration & dosage, Dinitrofluorobenzene analogs & derivatives, Dinitrofluorobenzene toxicity, Disease Models, Animal, Drug Compounding methods, Humans, Indoles chemistry, Intestinal Mucosa drug effects, Intestinal Mucosa immunology, Intestinal Mucosa pathology, Male, Mice, Nicotinic Acids chemistry, Prodrugs chemistry, Propionates chemistry, RAW 264.7 Cells, Rats, Receptors, G-Protein-Coupled agonists, Sulfasalazine administration & dosage, Anti-Inflammatory Agents administration & dosage, Colitis drug therapy, Indoles administration & dosage, Nicotinic Acids administration & dosage, Prodrugs administration & dosage, Propionates administration & dosage

Abstract

Microbial metabolites play a critical role in mucosal homeostasis by mediating physiological communication between the host and colonic microbes, whose perturbation may lead to gut inflammation. The microbial metabolite 3-indolepropionic acid (3-IPA) is one such communication mediator with potent antioxidative and anti-inflammatory activity. To apply the metabolite for the treatment of colitis, 3-IPA was coupled with acidic amino acids to yield colon-targeted 3-IPA, 3-IPA-aspartic acid (IPA-AA) and 3-IPA-glutamic acid (IPA-GA). Both conjugates were activated to 3-IPA in the cecal contents, which occurred faster for IPA-AA. Oral gavage of IPA-AA (oral IPA-AA) delivered a millimolar concentration of IPA-AA to the cecum, liberating 3-IPA. In a 2,4-dinitrobenzene sulfonic acid (DNBS)-induced rat colitis model, oral IPA-AA ameliorated rat colitis and was less effective than sulfasalazine (SSZ), a current anti-inflammatory bowel disease drug. To enhance the anticolitic activity of 3-IPA, it was azo-linked with the GPR109 agonist 5-aminonicotinic acid (5-ANA) to yield IPA-azo-ANA, expecting a mutual anticolitic action. IPA-azo-ANA (activated to 5-ANA and 2-amino-3-IPA) exhibited colon specificity in in vitro and in vivo experiments. Oral IPA-azo-ANA mitigated colonic damage and inflammation and was more effective than SSZ. These results suggest that colon-targeted 3-IPA ameliorated rat colitis and its anticolitic activity could be enhanced by codelivery of the GPR109A agonist 5-ANA.

Published

2021

7. Colitis-targeted hybrid nanoparticles-in-microparticles system for the treatment of ulcerative colitis.

Author

Naeem M, Lee J, Oshi MA, Cao J, Hlaing SP, Im E, Jung Y, and Yoo JW

Subjects

Animals, Drug Carriers therapeutic use, Drug Delivery Systems, Drug Liberation, Mice, Colitis drug therapy, Colitis, Ulcerative drug therapy, Nanoparticles

Abstract

Nanoparticle (NP)-based drug delivery systems accumulate in the disrupted epithelium of inflamed colon tissue in ulcerative colitis. However, premature early drug release and uptake or degradation of NPs during their passage through the harsh gastric or intestinal environment compromise their therapeutic outcomes. This study aimed to develop an advanced colitis-targeted hybrid nanoparticles-in-microparticles (NPsinMPs) drug delivery system to overcome the aforementioned challenges. First, sustained drug releasing poly(lactic-co-glycolic acid) NPs were generated and further encapsulated in pH-sensitive Eudragit FS30D MPs to ensure complete drug protection in a gastric-like pH and for selective delivery of NPs to the colon. SEM and confocal microscopy for the NPsinMPs revealed successful NP encapsulation. NPsinMPs prevented drug release in an acidic gastric-like and intestinal-like pH and presented a sustained release thereafter at an ileal and colonic pH, indicating the degradation of the outer pH-sensitive MPs and release of NPs. Furthermore, in vivo imaging of gastrointestinal tract of a colitis mouse orally administered with fluorescent NPsinMPs revealed higher fluorescence intensities selectively in the colon, demonstrating the release of loaded NPs and their concomitant accumulation at the site of colon inflammation. NPsinMPs markedly mitigated experimental colitis in mice indicated by improved histopathological analysis, decreased myeloperoxidase activity, neutrophils and macrophage infiltration, and expression of proinflammatory cytokines in colonic tissues compared with NP-treated mice. The present results show the successful formulation of an NPsinMP-based drug delivery system and provide a platform to improve NP-based colon-targeted drug delivery through improved protection of encapsulated NPs and their payload in the early small intestine., Competing Interests: Declaration of Competing Interest None, (Copyright © 2020. Published by Elsevier Ltd.)

Published

2020

8. 5-Aminosalicylic Acid Azo-Coupled with a GPR109A Agonist Is a Colon-Targeted Anticolitic Codrug with a Reduced Risk of Skin Toxicity.

Author

Jeong S, Lee H, Kim S, Ju S, Kim W, Cho H, Kim HY, Heo G, Im E, Yoo JW, Yoon IS, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Anti-Inflammatory Agents, Non-Steroidal toxicity, Cell Line, Tumor, Chromatography, Liquid, Colitis metabolism, Colon pathology, Drug Delivery Systems, Humans, Inflammatory Bowel Diseases drug therapy, Inflammatory Bowel Diseases metabolism, Interleukin-10 metabolism, Male, Mesalamine blood, Mesalamine therapeutic use, Mice, NF-kappa B metabolism, Nicotinic Acids blood, Nicotinic Acids therapeutic use, Rats, Rats, Sprague-Dawley, Sulfasalazine pharmacology, Sulfasalazine therapeutic use, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Colitis drug therapy, Colon drug effects, Receptors, G-Protein-Coupled agonists

Abstract

To develop a 5-aminosalicylic acid (5-ASA)-based anticolitic drug with enhanced therapeutic activity, a colon-targeted codrug constituting 5-ASA and a GPR109A agonist was designed. 5-ASA azo-coupled with nicotinic acid (ASA-azo-NA) was synthesized, and the colon specificity and anticolitic effects were evaluated. Approximately 89% of ASA-azo-NA was converted to 5-aminonicotinic acid (5-ANA) and 5-ASA after 24 h of incubation in the cecal contents. 5-ANA was identified as a GPR109A agonist (concentration that gives half-maximal response (EC 50 ): 18 μM) in a cell-based assay. Upon oral gavage of ASA-azo-NA (oral ASA-azo-NA) and sulfasalazine (oral SSZ), a colon-targeted 5-ASA prodrug, cecal accumulation of 5-ASA was comparable, and 5-ANA was barely detectable in the blood, while it was detected up to 62.7 μM with oral 5-ANA. In parallel, oral ASA-azo-NA did not elicit an adverse skin response. In murine macrophage and human colon carcinoma cells, activation of GPR109A by 5-ANA elevated the level of the anti-inflammatory cytokine IL-10, suppressed NF-κB activation, and potentiated the inhibitory activity of 5-ASA on NF-κB. Oral ASA-azo-NA ameliorated rat colitis and was more effective than oral SSZ, which were substantially blunted following cotreatment with the GPR109A antagonist, mepenzolate. In conclusion, ASA-azo-NA is a colon-targeted anticolitic codrug with a reduced risk of skin toxicity induced by the GPR109A agonist, therapeutically surpassing a current 5-ASA-based anti-inflammatory bowel disease drug in a rat colitis model.

Published

2020

9. Sofalcone, a gastroprotective drug, covalently binds to KEAP1 to activate Nrf2 resulting in anti-colitic activity.

Author

Kim W, Lee H, Kim S, Joo S, Jeong S, Yoo JW, and Jung Y

Subjects

Animals, Chalcones therapeutic use, Colitis metabolism, Colitis pathology, Gastrointestinal Tract metabolism, Gastrointestinal Tract pathology, Male, Protein Binding, Rats, Rats, Sprague-Dawley, Chalcones metabolism, Chalcones pharmacology, Colitis drug therapy, Gastrointestinal Tract drug effects, Kelch-Like ECH-Associated Protein 1 metabolism, NF-E2-Related Factor 2 metabolism

Abstract

Sofalcone is a synthetic chalcone being used as a gastric mucosa protective agent in Japan. Sofalcone contains a 1,3-diaryl-2-propen-1-one moiety, which is a common chemical scaffold in naturally occurring chalcones. The α,β-unsaturated carbonyl group (Michael reaction acceptor) has electrophilic properties. We investigated the biochemical mechanisms by which sofalcone activated the cytoprotective and anti-inflammatory nuclear factor-erythroid 2 (NF-E2) p45-related factor 2 (Nrf2)-heme oxygenase (HO)-1 pathway. Furthermore, we investigated whether the activation of this pathway was involved in sofalcone -mediated protective effects in an experimental colitis model. Sofalcone induced HO-1 protein expression, which was dependent on increased nuclear accumulation of Nrf2 in human colon carcinoma cells. In addition, Sofalcone reacted with nucleophilic thiol compounds to form Michael adducts. A reduced form of sofalcone (SFCR) in which the Michael reaction acceptor was deactivated, did not exert biological or chemical activity. Biotin-tagged sofalcone bound to Kelch-like ECH-associated protein 1 (KEAP1), a cytosolic repressor of Nrf2. This binding was prevented by pretreatment with sofalcone and a thiol compound but not with SFCR. Furthermore, sofalcone treatment induced dissociation of the Nrf2-KEAP1 complex. Rectal administration of sofalcone alleviated colon damage and inflammation and increased colon nuclear accumulation of Nrf2 and HO-1 levels in a dinitrobenzene sulfonic acid-induced rat colitis model. The protective effects of sofalcone against colon damage and inflammation were significantly inhibited by co-administration of an HO-1 inhibitor. In conclusion, sofalcone activated the Nrf2-HO-1 pathway by covalently binding to KEAP1 via Michael addition, and may confer anti-colitic effects by inducing Nrf2 activation., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

10. Colon-Targeted Delivery Facilitates the Therapeutic Switching of Sofalcone, a Gastroprotective Agent, to an Anticolitic Drug via Nrf2 Activation.

Author

Kim W, Kim S, Ju S, Lee H, Jeong S, Yoo JW, Yoon IS, and Jung Y

Subjects

Administration, Oral, Amino Acids, Acidic administration & dosage, Amino Acids, Acidic chemistry, Animals, Anti-Ulcer Agents administration & dosage, Anti-Ulcer Agents chemistry, Chalcones administration & dosage, Chalcones chemistry, Colitis chemically induced, Dinitrofluorobenzene analogs & derivatives, Dinitrofluorobenzene pharmacology, Disease Models, Animal, Epithelial Cells metabolism, Gene Knockdown Techniques, HCT116 Cells, Heme Oxygenase-1 metabolism, Humans, Male, Mice, NF-E2-Related Factor 2 genetics, Protective Agents administration & dosage, Protective Agents chemistry, RAW 264.7 Cells, Rats, Rats, Sprague-Dawley, Signal Transduction drug effects, Sulfasalazine administration & dosage, Sulfasalazine therapeutic use, Transfection, Treatment Outcome, Anti-Ulcer Agents therapeutic use, Chalcones therapeutic use, Colitis drug therapy, Drug Delivery Systems methods, NF-E2-Related Factor 2 metabolism, Protective Agents therapeutic use

Abstract

We investigated if the therapeutic switching of sofalcone (SFC), a gastroprotective agent, to an anticolitic agent is feasible using colon-targeted drug delivery. SFC can activate the anti-inflammatory nuclear factor (erythroid-derived 2)-like 2 (Nrf2)-hemeoxygenase-1 (HO-1) pathway in human colon epithelial cells and murine macrophages. For the efficient treatment of colitis, SFC was coupled with acidic amino acids to yield SFC-aspartic acid (SFC-AA) and SFC-glutamic acid, and their colon targetability and therapeutic effects were assessed as an anticolitic agent in a 2,4-dinitrobenezenesulfonic acid-induced rat colitis model. The SFC derivatives were decoupled up to 72% in the cecal contents but remained stable in the small intestinal contents. Oral gavage of SFC-AA (oral SFC-AA, equivalent to 1.67 mg/kg of SFC) delivered SFC (maximal cecal concentration: 57.36 μM) to the cecum, while no SFC was detected with oral gavage of SFC (oral SFC, 1.67 mg/kg). Moreover, oral SFC-AA (equivalent to 10 mg/kg of SFC) did not afford detectable concentration of SFC in the blood but detected up to 4.64 μM with oral SFC (10 mg/kg), indicating efficient colonic delivery and limited systemic absorption of SFC upon oral SFC-AA. Oral SFC-AA ameliorated colonic damage and inflammation in rat colitis with elevating colonic levels of HO-1 and nuclear Nrf2 protein, and the anticolitic effects of SFC-AA were significantly undermined by an HO-1 inhibitor. At an equivalent dose of SFC, oral SFC-AA but not oral SFC increased colonic HO-1 and nuclear Nrf2 levels, and oral SFC-AA was more effective than oral SFC in treating rat colitis. Moreover, oral SFC-AA was as effective against colitis as oral sulfasalazine being used for the treatment of inflammatory bowel disease. In conclusion, colon-targeted delivery of SFC facilitated the therapeutic switching of the drug to an anticolitic drug via Nrf2 activation.

Published

2019

11. Therapeutic switching of sulpiride, an anti-psychotic and prokinetic drug, to an anti-colitic drug using colon-specific drug delivery.

Author

Kim D, Kim W, Jeong S, Kim D, Yoo JW, and Jung Y

Subjects

Animals, Benzamides chemical synthesis, Benzamides chemistry, Benzamides pharmacokinetics, Colitis chemically induced, Colitis metabolism, Colon drug effects, Dinitrofluorobenzene adverse effects, Dinitrofluorobenzene analogs & derivatives, Disease Models, Animal, Dose-Response Relationship, Drug, Down-Regulation, Drug Delivery Systems, Male, Peroxidase metabolism, Prodrugs chemical synthesis, Prodrugs chemistry, Prodrugs pharmacokinetics, Rats, Rats, Sprague-Dawley, Sulfasalazine pharmacokinetics, Benzamides administration & dosage, Colitis drug therapy, Colon chemistry, Prodrugs administration & dosage, Sulfasalazine administration & dosage, Sulpiride chemistry

Abstract

To test whether sulpiride (SP), an anti-psychotic and prokinetic drug, shows beneficial effects on experimental murine colitis, a colon-targeted prodrug of SP, 5-(aminoethanoylsulfamoyl)-N-[(1-ethylpyrrolidin-2-yl)methyl]-2-methoxybenzamide (glycylsulpiride (GSP)), was synthesized and its colonic delivery and therapeutic activity against 2,4-dinitrobenzenesulfonic acid (DNBS)-induced rat colitis were assessed. Synthesis of GSP was verified by infrared and proton nuclear magnetic resonance spectroscopy. GSP was converted to SP when incubated with the cecal contents but not when incubated with the small intestinal contents. The percent conversion was about 50.5% at 6 h and 67.7% at 10 h. Colonic delivery of GSP was examined by comparison with sulfasalazine (SSZ), a colon-specific prodrug of 5-aminosalicylic acid currently used for the treatment of inflammatory bowel disease. The two prodrugs accumulated similar concentrations of the corresponding parent drugs in the cecum at 2, 4, and 6 h after oral gavage. Although oral gavage of GSP released millimolar level of SP in the large intestine, SP was hardly detected in the blood. GSP improved colonic damage score and reduced myeloperoxidase activity up to 80.5% in the inflamed colon in a dose-dependent manner. Moreover, GSP was able to reduce the levels of inflammatory mediators in the inflamed colon. Overall, the anti-colitic effectiveness of GSP and SSZ was similar. In conclusion, colonic delivery of SP ameliorates DNBS-induced colitis in rats with no significant systemic absorption of SP. Thus, colon-targeted SP may be therapeutically switched to an anti-colitic drug.

Published

2019

12. Mesalazine Activates Adenosine Monophosphate-activated Protein Kinase: Implication in the Anti-inflammatory Activity of this Anti-colitic Drug.

Author

Park H, Kim W, Kim D, Jeong S, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Colitis metabolism, Colitis pathology, HCT116 Cells, Humans, Male, Mesalamine pharmacology, Mice, NF-kappa B metabolism, Phosphorylation drug effects, RAW 264.7 Cells, Rats, Sprague-Dawley, AMP-Activated Protein Kinases metabolism, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Colitis drug therapy, Enzyme Activation drug effects, Mesalamine therapeutic use

Abstract

Objective: Mesalazine, 5-aminosalicylic acid (5-ASA), is an anti-inflammatory drug that is most widely used for the treatment of Inflammatory Bowel Disease (IBD). Despite extensive clinical use, the exact pharmacological mechanism underlying the anti-colitic effects of 5-ASA has not yet been elucidated. A potential molecular mechanism underlying 5-ASA-mediated anti-colitic activity was investigated., Methods: An anti-inflammatory pharmacology of 5-ASA was scrutinized in human colon carcinoma cells and murine macrophages and in a TNBS-induced rat colitis model., Results: 5-ASA induced phosphorylation of adenosine monophosphate-activated protein kinase (AMPK) and its substrate acetyl-CoA carboxylase in cells. 5-ASA activation of AMPK occurred regardless of the presence of the pro-inflammatory mediators, Tumor Necrosis Factor Alpha (TNF-α) and lipopolysaccharide. 5-ASA inhibits TNF-α-dependent Nuclear Factor-Kappa B (NF-κB) activation, which was dampened by AMPK inhibition. Oral gavage of sulfasalazine (a colon-specific prodrug of 5- ASA) or rectal administration of 5-ASA ameliorated 2,4,6-trinitrobenzene sulfonic acid (TNBS)- induced rat colitis and activated AMPK in the inflamed colonic tissues while markedly diminishing the levels of NF-κB-regulated pro-inflammatory mediators cyclooxygenase-2, inducible nitric oxide synthase, and cytokine-induced neutrophil chemoattractant-3, elevated by the induction of inflammation. Rectal co-administration of 5-ASA and an AMPK inhibitor undermined 5-ASA-mediated activation of AMPK and its anti-colitic effects., Conclusion: These findings suggest that the activation of AMPK is involved in 5-ASA-mediated anticolitic effects at least partly via interference with pro-inflammatory NF-κB signaling., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2019

13. A colon-specific prodrug of metoclopramide ameliorates colitis in an experimental rat model.

Author

Yang Y, Kim W, Kim D, Jeong S, Yoo JW, and Jung Y

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Azo Compounds administration & dosage, Azo Compounds therapeutic use, Benzenesulfonates, Colitis chemically induced, Colitis pathology, Colon pathology, Male, Mesalamine administration & dosage, Mesalamine therapeutic use, Metoclopramide administration & dosage, Metoclopramide chemical synthesis, Prodrugs administration & dosage, Prodrugs chemical synthesis, Rats, Rats, Sprague-Dawley, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Colitis drug therapy, Colon drug effects, Disease Models, Animal, Metoclopramide therapeutic use, Prodrugs therapeutic use

Abstract

Background: We examined whether metoclopramide (MCP), a modulator of dopamine and serotonin receptors, alleviated colitis and had synergistic effects when coadministered with 5-aminosalicylic acid (5-ASA) in an experimental model of colitis., Methods: MCP azo-linked to 5-ASA (5-[4-chloro-2-{2-(diethylamino)ethylcarbamoyl}- 1-methoxyphenyl]azosalicylic acid, MCP-azo-ASA) was synthesized, where 5-ASA was used as a colon-targeting carrier and an anti-colitic agent, and the ability of MCP-azo-ASA to target the colon in vitro and in vivo was evaluated., Results: Our results indicate that MCP-azo-ASA was cleaved to MCP and 5-ASA in the cecal contents, but not in the contents of the small intestine. Oral gavage with equimolar concentrations of MCP-azo-ASA and sulfasalazine (SSZ, a colon-specific prodrug of 5-ASA widely used clinically) demonstrated that the two prodrugs delivered comparable amounts of 5-ASA to the cecum. MCP was barely detected in the blood after oral gavage with MCP-azo-ASA. In a rat model of 2,4-dinitrobenzene sulfonic acid hydrate (DNBS)-induced colitis, MCP-azo-ASA alleviated colonic damage in a dose-dependent manner. Moreover, MCP-azo-ASA reduced the concentrations of inflammatory mediators in the inflamed colon. At low equimolar doses, MCP-azo-ASA, but not SSZ, resulted in significant anti-colitic effects, which indicates that MCP has anti-colitic activity. MCP-azo-ASA had anti-colitic effects equal to those of SSZ at high equimolar doses., Conclusion: Thus, our results indicate that MCP-azo-ASA is a colon-specific prodrug of MCP. Targeted delivery of MCP to the colon ameliorated DNBS-induced colitis in rats, and we did not observe any synergistic effects of MCP after co-delivery with 5-ASA., Competing Interests: Disclosure The authors report no conflicts of interest in this work.

Published

2018

14. Colon-targeted dexamethasone microcrystals with pH-sensitive chitosan/alginate/Eudragit S multilayers for the treatment of inflammatory bowel disease.

Author

Oshi MA, Naeem M, Bae J, Kim J, Lee J, Hasan N, Kim W, Im E, Jung Y, and Yoo JW

Subjects

Alginates chemistry, Animals, Anti-Inflammatory Agents chemistry, Chitosan chemistry, Colitis chemically induced, Colitis metabolism, Colitis pathology, Colon drug effects, Colon metabolism, Colon pathology, Cytokines metabolism, Dexamethasone chemistry, Dextran Sulfate, Drug Liberation, Glucuronic Acid administration & dosage, Glucuronic Acid chemistry, Hexuronic Acids administration & dosage, Hexuronic Acids chemistry, Hydrogen-Ion Concentration, Male, Mice, Inbred ICR, Peroxidase metabolism, Polymethacrylic Acids chemistry, Alginates administration & dosage, Anti-Inflammatory Agents administration & dosage, Chitosan administration & dosage, Colitis drug therapy, Dexamethasone administration & dosage, Drug Delivery Systems, Polymethacrylic Acids administration & dosage

Abstract

Oral colon-targeted drug delivery has gained popularity as an effective strategy for treatment of inflammatory bowel disease (IBD). In this study, we prepared colon-targeted dexamethasone microcrystals (DXMCs) coated with multilayers of chitosan oligosaccharide (CH), alginate (AG), and finally Eudragit S 100 (ES) (ES 1 AG 4 CH 5 -DXMCs) using a layer-by-layer (LBL) coating technique. Particle size, surface charge, in vitro drug release, and in vivo anti-inflammatory activity of ES 1 AG 4 CH 5 -DXMCs were evaluated. ES 1 AG 4 CH 5 -DXMCs had an average particle size of 2.34 ± 0.19 μm and a negative surface charge of - 48 ± 9 mV. ES 1 AG 4 CH 5 -DXMCs demonstrated pH-dependent dexamethasone release, avoiding initial burst drug release in acidic pH conditions of the stomach and small intestine, and providing subsequent sustained drug release in the colonic pH. Importantly, ES 1 AG 4 CH 5 -DXMCs exhibited a significant therapeutic activity in a mouse model of colitis compared to other DXMCs. Overall, the LBL-coated DXMCs presented here could be a promising colon-targeted therapy for IBD., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

15. pH-triggered surface charge-reversal nanoparticles alleviate experimental murine colitis via selective accumulation in inflamed colon regions.

Author

Naeem M, Oshi MA, Kim J, Lee J, Cao J, Nurhasni H, Im E, Jung Y, and Yoo JW

Subjects

Animals, Anti-Inflammatory Agents administration & dosage, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Budesonide administration & dosage, Budesonide chemistry, Colitis chemically induced, Colitis immunology, Dextran Sulfate toxicity, Hydrogen-Ion Concentration, Inflammation immunology, Inflammation pathology, Mice, Nanoparticles chemistry, Polyethyleneimine chemistry, Budesonide pharmacology, Colitis prevention & control, Drug Delivery Systems, Inflammation metabolism, Lipopeptides chemistry, Nanoparticles administration & dosage, Polymethacrylic Acids chemistry

Abstract

In this study, we developed pH-triggered surface charge-reversal lipid nanoparticles (LNPs), loaded with budesonide, which could precisely deliver the drug to inflamed colon segments for the treatment of ulcerative colitis. Polyethyleneimine (PEI) was used to render LNPs cationic (PEI-LNPs), and Eudragit® S100 (ES) was coated on PEI-LNPs to obtain pH-triggered charge-reversal LNPs (ES-PEI-LNPs). ES coating avoided a burst drug release under acidic conditions mimicking the stomach and early small intestine environments and showed a sustained release in the colon. The surface charge of ES-PEI-LNPs switched from negative to positive under colonic conditions owing to pH-triggered removal of the ES coating. Bioimaging of the mouse gastrointestinal tract and confocal analysis of colon tissues revealed that ES-PEI-LNPs selectively accumulated in an inflamed colon. Furthermore, ES-PEI-LNPs mitigated experimental colitis in mice. These results suggest that the pH-triggered charge-reversal LNPs could be a promising drug carrier for ulcerative colitis therapy and other colon-targeted treatments., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

16. Colon-targeted delivery of cyclosporine A using dual-functional Eudragit ® FS30D/PLGA nanoparticles ameliorates murine experimental colitis.

Author

Naeem M, Bae J, Oshi MA, Kim MS, Moon HR, Lee BL, Im E, Jung Y, and Yoo JW

Subjects

Administration, Oral, Animals, Body Weight, Colitis chemically induced, Colitis pathology, Cytokines metabolism, Drug Carriers administration & dosage, Drug Liberation, Hydrogen-Ion Concentration, Immunosuppressive Agents therapeutic use, Inflammation Mediators metabolism, Macrophages drug effects, Macrophages pathology, Mice, Inbred ICR, Nanoparticles administration & dosage, Nanoparticles ultrastructure, Particle Size, Peroxidase metabolism, Polylactic Acid-Polyglycolic Acid Copolymer, Treatment Outcome, Colitis drug therapy, Colon pathology, Cyclosporine administration & dosage, Cyclosporine therapeutic use, Drug Delivery Systems, Lactic Acid chemistry, Methylmethacrylates chemistry, Nanoparticles chemistry, Polyglycolic Acid chemistry

Abstract

Background: Colon-targeted oral nanoparticles (NPs) have emerged as an ideal, safe, and effective therapy for ulcerative colitis (UC) owing to their ability to selectively accumulate in inflamed colonic mucosa. Cyclosporine A (CSA), an immunosuppressive agent, has long been used as rescue therapy in severe steroid-refractory UC. In this study, we developed CSA-loaded dual-functional polymeric NPs composed of Eudragit ® FS30D as a pH-sensitive polymer for targeted delivery to the inflamed colon, and poly(lactic-co-glycolic acid) (PLGA) as a sustained-release polymer., Methods: CSA-loaded Eudragit FS30D nanoparticles (ENPs), PLGA nanoparticles (PNPs), and Eudragit FS30D/PLGA nanoparticles (E/PNPs) were prepared using the oil-in-water emulsion method. Scanning electron microscope images and zeta size data showed successful preparation of CSA-loaded NPs., Results: PNPs exhibited a burst drug release of >60% at pH 1.2 (stomach pH) in 0.5 h, which can lead to unwanted systemic absorption and side effects. ENPs effectively inhibited the burst drug release at pH 1.2 and 6.8 (proximal small intestine pH); however, nearly 100% of the CSA in ENPs was released rapidly at pH 7.4 (ileum-colon pH) owing to complete NP dissolution. In contrast to single-functional PNPs and ENPs, the dual-functional E/PNPs minimized burst drug release (only 18%) at pH 1.2 and 6.8, and generated a sustained release at pH 7.4 thereafter. Importantly, in distribution studies in the gastrointestinal tracts of mice, E/PNPs significantly improved CSA distribution to the colon compared with PNPs or ENPs. In a mouse model of colitis, E/PNP treatment improved weight loss and colon length, and decreased rectal bleeding, spleen weight, histological scoring, myeloperoxidase activity, macrophage infiltration, and expression of proinflammatory cytokines compared with PNPs or ENPs., Conclusion: Overall, this work confirms the benefits of CSA-loaded E/PNPs for efficiently delivering CSA to the colon, suggesting their potential for UC therapy., Competing Interests: Disclosure The authors report no conflicts of interest in this work.

Published

2018

17. 5-Aminosalicylic Acid Azo-Linked to Procainamide Acts as an Anticolitic Mutual Prodrug via Additive Inhibition of Nuclear Factor kappaB.

Author

Kim W, Nam J, Lee S, Jeong S, and Jung Y

Subjects

Animals, Azo Compounds chemistry, Colon drug effects, Male, Mesalamine chemistry, Procainamide chemistry, Prodrugs chemistry, Rats, Rats, Sprague-Dawley, Trinitrobenzenesulfonic Acid chemistry, Trinitrobenzenesulfonic Acid pharmacology, Azo Compounds pharmacology, Colitis drug therapy, Mesalamine pharmacology, NF-kappa B metabolism, Procainamide pharmacology, Prodrugs pharmacology

Abstract

To improve the anticolitic efficacy of 5-aminosalicylic acid (5-ASA), a colon-specific mutual prodrug of 5-ASA was designed. 5-ASA was coupled to procainamide (PA), a local anesthetic, via an azo bond to prepare 5-(4-{[2-(diethylamino)ethyl]carbamoyl}phenylazo)salicylic acid (5-ASA-azo-PA). 5-ASA-azo-PA was cleaved to 5-ASA and PA up to about 76% at 10 h in the cecal contents while remaining stable in the small intestinal contents. Oral gavage of 5-ASA-azo-PA and sulfasalazine, a colon-specific prodrug currently used in clinic, to rats showed similar efficiency in delivery of 5-ASA to the large intestine, and PA was not detectable in the blood after 5-ASA-azo-PA administration. Oral gavage of 5-ASA-azo-PA alleviated 2,4,6-trinitrobenzenesulfonic acid-induced rat colitis. Moreover, combined intracolonic treatment with 5-ASA and PA elicited an additive ameliorative effect. Furthermore, combined treatment with 5-ASA and PA additively inhibited nuclear factor-kappaB (NFκB) activity in human colon carcinoma cells and inflamed colonic tissues. Finally, 5-ASA-azo-PA administered orally was able to reduce inflammatory mediators, NFκB target gene products, in the inflamed colon. 5-ASA-azo-PA may be a colon-specific mutual prodrug acting against colitis, and the mutual anticolitic effects occurred at least partly through the cooperative inhibition of NFκB activity.

Published

2016

18. Dextran-5-(4-ethoxycarbonylphenylazo)salicylic acid ester, a polymeric colon-specific prodrug releasing 5-aminosalicylic acid and benzocaine, ameliorates TNBS-induced rat colitis.

Author

Nam J, Kim W, Lee S, Jeong S, Yoo JW, Kim MS, and Jung Y

Subjects

Administration, Oral, Animals, Cecum drug effects, Cecum metabolism, Colitis chemically induced, Colitis metabolism, Colon metabolism, Inflammation Mediators metabolism, Male, Rats, Rats, Sprague-Dawley, Trinitrobenzenesulfonic Acid pharmacology, Benzocaine pharmacology, Colitis drug therapy, Colon drug effects, Dextrans pharmacology, Mesalamine pharmacology, Polymers pharmacology, Prodrugs pharmacology

Abstract

Local anesthetics have beneficial effects on colitis. Dextran-5-(4-ethoxycarbonylphenylazo)salicylic acid ester (Dex-5-ESA), designed as a polymeric colon-specific prodrug liberating 5-ASA and benzocaine in the large intestine, was prepared and its therapeutic activity against colitis was evaluated using a TNBS-induced rat colitis model. Dex-5-ESA liberated 5-ASA and benzocaine in the cecal contents while (bio)chemically stable in the small intestinal contents and mucosa. Oral administration of Dex-5-ESA (equivalent to 10 mg 5-ASA/kg, twice a day) alleviated colonic injury and reduced MPO activity in the inflamed colon. In parallel, pro-inflammatory mediators, COX-2, iNOS and CINC-3, elevated by TNBS-induced colitis, were substantially diminished in the inflamed colon. Dex-5-ESA was much more effective for the treatment of colitis than 5-(4-ethoxycarbonylphenylazo)salicylic acid (5-ESA) that may not deliver benzocaine to the large intestine. Our data suggest that Dex-5-ESA is a polymeric colon-specific prodrug, liberating 5-ASA and benzocaine in the target site (large intestine), probably exerting anti-colitic effects by combined action of 5-ASA and benzocaine.

Published

2016

19. Colonic delivery of celecoxib is a potential pharmaceutical strategy for repositioning the selective COX-2 inhibitor as an anti-colitic agent.

Author

Kim W, Lee Y, Jeong S, Nam J, Lee S, and Jung Y

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents administration & dosage, Anti-Inflammatory Agents pharmacokinetics, Anti-Inflammatory Agents pharmacology, Colitis pathology, Colon pathology, Cyclooxygenase 2 Inhibitors pharmacokinetics, Cyclooxygenase 2 Inhibitors pharmacology, Disease Models, Animal, Drug Repositioning, Glutamates pharmacokinetics, Glutamates pharmacology, HCT116 Cells, Humans, Male, NF-kappa B metabolism, Prodrugs, Rats, Rats, Sprague-Dawley, Sulfonamides pharmacokinetics, Sulfonamides pharmacology, Colitis drug therapy, Colon metabolism, Cyclooxygenase 2 Inhibitors administration & dosage, Glutamates administration & dosage, Sulfonamides administration & dosage

Abstract

Celecoxib is a selective cyclooxygenase-2 inhibitor applied to the treatment of arthritis. Repositioning the anti-inflammatory drug as an anti-inflammatory bowel disease drug has obstacles such as controversial anti-colitic efficacy and potential side effects. We examined whether colonic delivery of celecoxib could circumvent the therapeutic limitations. N-succinylglutam-1-yl celecoxib (SG1C), a colon-specific prodrug of celecoxib), was administered orally to rats with colitis and the anti-inflammatory activity and pharmacologic mechanisms were investigated. SG1C alleviated the colonic injury and lowered myeloperoxidase activity in the inflamed colonic tissues much more effectively than conventional celecoxib. While suppressing expression of pro-inflammatory nuclear factor kappaB gene products including cyclooxygenase-2, SG1C elevated an anti-inflammatory nuclear factor-erythroid 2 p45 (NF-E2)-related factor 2 (Nrf2) and its target gene product heme oxygenase (HO)-1 in the inflamed colon. In contrast, no significant molecular effects were observed with conventional celecoxib. Unlike conventional celecoxib, SG1C did not lower the serum level of 6-keto-PGF1α, an inverse indicator of cardiovascular adverse effects. Collectively, colonic delivery of celecoxib, likely improving therapeutic and toxicological properties of celecoxib, may be a feasible pharmaceutical strategy to therapeutically switch celecoxib to an anti-colitic drug.

Published

2015

20. Colon-targeted delivery of piceatannol enhances anti-colitic effects of the natural product: potential molecular mechanisms for therapeutic enhancement.

Author

Yum S, Jeong S, Lee S, Nam J, Kim W, Yoo JW, Kim MS, Lee BL, and Jung Y

Subjects

Administration, Oral, Administration, Rectal, Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents metabolism, Biomarkers metabolism, Capsules, Chemistry, Pharmaceutical, Colitis chemically induced, Colitis genetics, Colitis metabolism, Colitis pathology, Colon metabolism, Colon pathology, Disease Models, Animal, Gastrointestinal Agents chemistry, Gastrointestinal Agents metabolism, Gelatin chemistry, Gene Expression Regulation, HCT116 Cells, Humans, Inflammation Mediators metabolism, Male, Mice, RAW 264.7 Cells, Rats, Sprague-Dawley, Signal Transduction drug effects, Stilbenes chemistry, Stilbenes metabolism, Technology, Pharmaceutical methods, Transfection, Trinitrobenzenesulfonic Acid, Anti-Inflammatory Agents administration & dosage, Colitis prevention & control, Colon drug effects, Gastrointestinal Agents administration & dosage, Stilbenes administration & dosage

Abstract

Piceatannol (PCT), an anti-colitic natural product, undergoes extensive Phase II hepatic metabolism, resulting in very low bioavailability. We investigated whether colon-targeted delivery of PCT could enhance anti-colitic effects and how therapeutic enhancement occurred at the molecular level. Molecular effects of PCT were examined in human colon carcinoma cells and inflamed colons. The anti-colitic effects of PCT in a colon-targeted capsule (colon-targeted PCT) were compared with PCT in a gelatin capsule (conventional PCT) in a trinitrobenzene sulfonic acid-induced rat colitis model. Colon-targeted PCT elicited greatly enhanced recovery of the colonic inflammation. In HCT116 cells, PCT inhibited nuclear factor kappaB while activating anti-colitic transcription factors, nuclear factor-erythroid 2 (NF-E2) p45-related factor 2, and hypoxia-inducible factor-1. Colon-targeted PCT, but not conventional PCT, modulated production of the target gene products of the transcription factors in the inflamed colonic tissues. Rectal administration of PCT, which simulates the therapeutic action of colon-targeted PCT, also ameliorated rat colitis and reproduced the molecular effects in the inflamed colonic tissues. Colon-targeted delivery increased therapeutic efficacy of PCT against colitis, likely resulting from multitargeted effects exerted by colon-targeted PCT. The drug delivery technique may be useful for therapeutic optimization of anti-colitic lead compounds including natural products.

Published

2015

21. Colon-targeted delivery of budesonide using dual pH- and time-dependent polymeric nanoparticles for colitis therapy.

Author

Naeem M, Choi M, Cao J, Lee Y, Ikram M, Yoon S, Lee J, Moon HR, Kim MS, Jung Y, and Yoo JW

Subjects

Acrylic Resins chemistry, Animals, Anti-Inflammatory Agents pharmacokinetics, Anti-Inflammatory Agents pharmacology, Budesonide pharmacokinetics, Budesonide pharmacology, Colitis pathology, Colon metabolism, Colon pathology, Delayed-Action Preparations, Dextran Sulfate toxicity, Disease Models, Animal, Drug Liberation, Hydrogen-Ion Concentration, Male, Mice, Mice, Inbred ICR, Nanoparticles, Polymethacrylic Acids chemistry, Time Factors, Anti-Inflammatory Agents administration & dosage, Budesonide administration & dosage, Colitis drug therapy, Drug Delivery Systems

Abstract

Single pH-dependent drug delivery systems have been widely used for colon-targeted delivery, but their efficiency is often hampered by the variation in gut pH. To overcome the limitation of single pH-dependent delivery systems, in this study, we developed and evaluated the therapeutic potential of budesonide-loaded dual pH/time-dependent nanoparticles (NPs) for the treatment of colitis. Eudragit FS30D was used as a pH-dependent polymer, and Eudragit RS100 as a time-dependent controlled release polymer. Single pH-dependent NPs (pH_NPs), single time-dependent NPs (Time_NPs), and dual pH/time-dependent NPs (pH/Time_NPs) were prepared using the oil-in-water emulsion method. The physicochemical properties and drug release profiles of these NPs in gastrointestinal (GI) tract conditions were investigated. The therapeutic potential and in vivo distribution of the NPs were evaluated in a dextran sulfate sodium (DSS)-induced colitis mice model. The pH/Time_NPs prevented a burst drug release in acidic pH conditions and showed sustained release at a colonic pH. The in vivo distribution study in the mice GI tract demonstrated that pH/Time_NPs were more efficiently delivered to the inflamed colon than pH_NPs were. Compared to the single pH_NPs-treated group, the pH/Time_NPs-treated group showed increased body weight and colon length and markedly decreased disease activity index, colon weight/length ratios, histological damage, and inflammatory cell infiltration in colon tissue. Our results demonstrate that the dual pH/time-dependent NPs are an effective oral colon-targeted delivery system for colitis therapy.

Published

2015

22. Enhanced therapeutic efficacy of budesonide in experimental colitis with enzyme/pH dual-sensitive polymeric nanoparticles.

Author

Naeem M, Cao J, Choi M, Kim WS, Moon HR, Lee BL, Kim MS, Jung Y, and Yoo JW

Subjects

Animals, Cell Line, Cell Survival drug effects, Disease Models, Animal, Hydrogen-Ion Concentration, Rats, Budesonide chemistry, Budesonide pharmacology, Budesonide therapeutic use, Colitis drug therapy

Abstract

Current colon-targeted drug-delivery approaches for colitis therapy often utilize single pH-triggered systems, which are less reliable due to the variation of gut pH in individuals and in disease conditions. Herein, we prepared budesonide-loaded dual-sensitive nanoparticles using enzyme-sensitive azo-polyurethane and pH-sensitive methacrylate copolymer for the treatment of colitis. The therapeutic potential of the enzyme/pH dual-sensitive nanoparticles was evaluated using a rat colitis model and compared to single pH-triggered nanoparticles. Clinical activity scores, colon/body weight ratios, myeloperoxidase activity, and proinflammatory cytokine levels were markedly decreased by dual-sensitive nanoparticles compared to single pH-triggered nanoparticles and budesonide solution. Moreover, dual-sensitive nanoparticles accumulated selectively in inflamed segments of the colon. In addition, dual-sensitive nanoparticle plasma concentrations were lower than single pH-triggered nanoparticles, and no noticeable in vitro or in vivo toxicity was observed. Our results demonstrate that enzyme/pH dual-sensitive nanoparticles are an effective and safe colon-targeted delivery system for colitis therapy.

Published

2015

23. HIF-prolyl hydroxylase is a potential molecular target for esculetin-mediated anti-colitic effects.

Author

Yum S, Jeong S, Lee S, Kim W, Nam J, and Jung Y

Subjects

Animals, Colitis chemically induced, Disease Models, Animal, HCT116 Cells drug effects, Humans, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Male, Rats, Rats, Sprague-Dawley, Vascular Endothelial Growth Factor A metabolism, Colitis drug therapy, Hypoxia-Inducible Factor-Proline Dioxygenases metabolism, Umbelliferones pharmacology

Abstract

We investigated a potential molecular target for anti-colitic effects of esculetin, 6,7-dihydroxycoumarin. Esculetin administered rectally effectively ameliorated TNBS-induced rat colitis and attenuated the expression of pro-inflammatory mediators in the inflamed colon. In human colon carcinoma HCT116 cells, esculetin induced hypoxia-inducible factor-1α (HIF-1α), leading to secretion of vascular endothelial growth factor, a HIF-1 target gene product involved in ulcer healing of the gastrointestinal mucosa. Esculetin directly inhibited HIF prolyl hydroxylase-2 (HPH-2), an enzyme playing a major role in negatively regulating HIF-1α protein stability. Esculetin inhibition of HPH and consequent induction of HIF-1α were attenuated by escalating dose of either ascorbate or 2-ketoglutarate, the required factors of the enzyme. Structurally, the catechol moiety in esculetin was required for HPH inhibition. Collectively, HPH may be a molecular target for esculetin-mediated anti-colitic effects and the catechol moiety in esculetin is the pharmacophore for HPH inhibition., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

24. Lipophilic modification enhances anti-colitic properties of rosmarinic acid by potentiating its HIF-prolyl hydroxylases inhibitory activity.

Author

Jeong S, Park H, Hong S, Yum S, Kim W, and Jung Y

Subjects

Animals, Ascorbic Acid pharmacology, Carboxylic Acids chemistry, Cell Line, Tumor, Cinnamates therapeutic use, Coenzymes physiology, Colitis chemically induced, Colitis metabolism, Colitis pathology, Depsides therapeutic use, Enzyme Inhibitors therapeutic use, Esters, Humans, Hydroxylation drug effects, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Hypoxia-Inducible Factor-Proline Dioxygenases metabolism, Ketoglutaric Acids pharmacology, Protein Stability drug effects, Rats, Signal Transduction drug effects, Structure-Activity Relationship, Trinitrobenzenesulfonic Acid adverse effects, Vascular Endothelial Growth Factor A metabolism, Rosmarinic Acid, Cinnamates chemistry, Cinnamates pharmacology, Colitis drug therapy, Depsides chemistry, Depsides pharmacology, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Hydrophobic and Hydrophilic Interactions, Hypoxia-Inducible Factor-Proline Dioxygenases antagonists & inhibitors

Abstract

Inhibition of hypoxia inducible factor-prolyl hydroxylase-2 (HPH), leading to activation of hypoxia inducible factor (HIF)-1 is a potential therapeutic strategy for the treatment of colitis. Rosmarinic acid (RA), an ester of caffeic acid and 3,4-dihydroxyphenyllactic acid is a naturally occurring polyphenolic compound with two catechols, a or inhibition of HPH. To improve accessibility of highly hydrophilic RA to HPH, an intracellular target, RA was chemically modified to decrease hydrophilicity. Of the less-hydrophilic derivatives, rosmarinic acid methyl ester (RAME) most potently inhibited HPH. Accordingly, RAME prevented hydroxylation of HIF-1α and consequently stabilized HIF-1α protein in cells. RAME inhibition of HPH and induction of HIF-1α were diminished by elevated doses of the required factors of HPH, 2-ketoglutarate and ascorbate. RAME induction of HIF-1α led to activation of an ulcer healing pathway, HIF-1-vascular endothelial growth factor (VEGF), in human colon carcinoma cells. RAME administered rectally ameliorated TNBS-induced rat colitis and substantially decreased the levels of pro-inflammatory mediators in the inflamed colonic tissue. In parallel with the cellular effects of RAME, RAME up-regulated HIF-1α and VEGF in the inflamed colonic tissue. Thus, lipophilic modification of RA improves its ability to inhibit HPH, leading to activation of the HIF-1-VEGF pathway. RAME, a lipophilic RA derivative, may exert anti-colitic effects via activation of the ulcer healing pathway., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

25. Colon-targeted celecoxib ameliorates TNBS-induced rat colitis: a potential pharmacologic mechanism and therapeutic advantages.

Author

Lee Y, Kim W, Hong S, Park H, Yum S, Yoon JH, and Jung Y

Subjects

6-Ketoprostaglandin F1 alpha blood, Animals, Celecoxib, Cell Line, Colitis blood, Colitis metabolism, Colon metabolism, Cyclooxygenase 2 Inhibitors metabolism, Cyclooxygenase 2 Inhibitors therapeutic use, Gene Expression Regulation drug effects, Humans, Male, Mice, Prodrugs metabolism, Pyrazoles metabolism, Pyrazoles therapeutic use, Rats, Sulfonamides metabolism, Sulfonamides therapeutic use, Colitis chemically induced, Colitis drug therapy, Colon drug effects, Cyclooxygenase 2 Inhibitors pharmacology, Pyrazoles pharmacology, Sulfonamides pharmacology, Trinitrobenzenesulfonic Acid adverse effects

Abstract

The clinical usefulness of celecoxib, a selective cyclooxygenase-2 (COX-2) inhibitor, for treatment of inflammatory bowel disease (IBD) is controversial in terms of efficacy and toxicity. To overcome these problems, colon-specific drug delivery was adopted, which generally confers therapeutic and toxicological advantages of drugs for treatment of colonic diseases. N-succinylaspart-1-yl celecoxib (SA1C), a colon-specific prodrug of celecoxib, was administered orally to rats with experimental colitis, and the anti-colitic effects and a molecular mechanism were investigated and compared to those of conventional celecoxib. SA1C, which delivered a much greater amount of celecoxib to the inflamed colon, alleviated the colonic injury, lowered myeloperoxidase activity in the inflamed colonic tissues and was much more effective than conventional celecoxib. SA1C but not conventional celecoxib significantly attenuated expression of NFκB target gene products in the inflamed tissues. Consistent with this, SA1C effectively prevented nuclear accumulation of p65 in the inflamed tissues. Moreover, while conventional celecoxib lowered the serum level of 6-keto-PGF1α, an inverse indicator of cardiovascular toxicity, SA1C did not change its serum level. Our data suggest that colonic delivery of celecoxib is a feasible strategy for treatment of IBD with improved therapeutic and toxicological properties.

Published

2014

26. N-(2-Mercaptopropionyl)-glycine, a diffusible antioxidant, activates HIF-1 by inhibiting HIF prolyl hydroxylase-2: implication in amelioration of rat colitis by the antioxidant.

Author

Yum S, Park H, Hong S, Jeong S, Kim W, and Jung Y

Subjects

Animals, Antioxidants pharmacology, Ascorbic Acid metabolism, Basic Helix-Loop-Helix Transcription Factors antagonists & inhibitors, Colitis pathology, Diffusion, Enzyme Activation drug effects, HCT116 Cells, Humans, Male, Rats, Rats, Sprague-Dawley, Tiopronin pharmacology, Trinitrobenzenesulfonic Acid, Vascular Endothelial Growth Factor A metabolism, Antioxidants therapeutic use, Basic Helix-Loop-Helix Transcription Factors metabolism, Colitis drug therapy, Colitis enzymology, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Prolyl Hydroxylases metabolism, Tiopronin therapeutic use

Abstract

We investigated anti-colitic effects of N-(2-mercaptopropionyl)-glycine (NMPG), a diffusible antioxidant, in TNBS-induced rat colitis model and a potential molecular mechanism underlying the pharmacologic effect of the antioxidant. NMPG alleviated colonic injury and effectively lowered myeloperoxidase activity. Moreover, NMPG substantially attenuated expression of pro-inflammatory mediators in the inflamed colon. NMPG induced hypoxia-inducible factor-1α (HIF-1α) in human colon carcinoma cells, leading to elevated secretion of vascular endothelial growth factor (VEGF), a target gene product of HIF-1 involved in ulcer healing of gastrointestinal mucosa. NMPG induction of HIF-1α occurred by inhibiting HIF prolyl hydroxylase-2 (HPH-2), an enzyme that plays a major role in negatively regulating HIF-1α protein stability. In in vitro Von Hippel-Lindau protein binding assay, the inhibitory effect of NMPG on HPH-2 was attenuated by escalating dose of ascorbate but not 2-ketoglutarate, cofactors of the enzyme. Consistent with this, cell-permeable ascorbate significantly attenuated NMPG induction of HIF-1α in cells. Our data suggest that NMPG is an anti-colitic antioxidant that exerts its pharmacologic effects at least partly through activation of an ulcer healing pathway, HIF-1-VEGF., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2014

27. Caffeic acid phenethyl ester activation of Nrf2 pathway is enhanced under oxidative state: structural analysis and potential as a pathologically targeted therapeutic agent in treatment of colonic inflammation.

Author

Kim H, Kim W, Yum S, Hong S, Oh JE, Lee JW, Kwak MK, Park EJ, Na DH, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents chemistry, Blotting, Western, Caffeic Acids chemistry, Cell Line, Tumor, Chromatography, High Pressure Liquid, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay, Humans, Immunoprecipitation, Oxidative Stress drug effects, Phenylethyl Alcohol chemistry, Phenylethyl Alcohol pharmacology, Rats, Reverse Transcriptase Polymerase Chain Reaction, Structure-Activity Relationship, Anti-Inflammatory Agents pharmacology, Caffeic Acids pharmacology, Colitis metabolism, NF-E2-Related Factor 2 metabolism, Phenylethyl Alcohol analogs & derivatives, Signal Transduction drug effects

Abstract

Caffeic acid phenethyl ester (CAPE) is a polyphenolic natural product that possesses numerous biological activities including anti-inflammatory effects. CAPE-mediated nuclear factor-erythroid 2 p45 (NF-E2)-related factor 2 (Nrf2) activation is likely responsible for some of its biological effects. CAPE was chemically modified to yield CAPE analogues that were subjected to experiments examining cellular Nrf2 activity. CAPE and the CAPE analogue with a catechol moiety, but not the other analogues, activated the Nrf2 pathway. In addition, only biotin-labeled CAPE analogues with the catechol moiety precipitated Kelch-like ECH associated protein 1 (Keap1) when incubated with cell lysates and streptavidin agarose beads. Sodium hypochlorite (NaOCl) oxidation of the catechol moiety in CAPE produced an oxidized, electrophilic form of CAPE (Oxi-CAPE) and greatly enhanced the ability of CAPE to activate Nrf2 and to bind to Keap1. Rectal administration of CAPE ameliorated 2,4,6-trinitrobenzene sulfonic acid-induced rat colitis and activated the Nrf2 pathway in the inflamed colon, and incubation of CAPE in the lumen of the inflamed distal colon generated Oxi-CAPE. However, these biological effects and chemical change of CAPE were not observed in the normal colon. Our data suggest that CAPE requires the catechol moiety for the oxidation-enhanced activation of the Nrf2 pathway and has potential as a pathologically targeted Nrf2-activating agent that is exclusively activated in pathological states with oxidative stress such as colonic inflammation., (© 2013 Elsevier Inc. All rights reserved.)

Published

2013

28. Glycyrrhizin enhances therapeutic activity of a colon-specific methylprednisolone prodrug against experimental colitis.

Author

Lee Y, Jeong S, Kim W, Kim H, Yoon JH, Jeong SH, and Jung Y

Subjects

Adrenal Glands drug effects, Animals, Anti-Inflammatory Agents metabolism, Colitis metabolism, Drug Evaluation, Preclinical, Drug Synergism, Male, Methylprednisolone metabolism, Prodrugs therapeutic use, Rats, Rats, Sprague-Dawley, Anti-Inflammatory Agents therapeutic use, Colitis drug therapy, Glycyrrhizic Acid therapeutic use, Methylprednisolone therapeutic use

Abstract

Background: Co-administration of a reduction inhibitor and a colon-specific prodrug of a glucocorticoid susceptible to colonic reductive metabolism is suggested as a strategy to circumvent the therapeutic loss of the glucocorticoid delivered to and acting locally at the large intestine., Aims: We examined whether the strategy was feasible as a pharmacotherapy for treatment of inflammatory bowel disease., Methods: Glycyrrhizin (GCZ), a reduction inhibitor, was tested for its inhibition of the colonic metabolism of methylprednisolone (MP). Therapeutic activity against TNBS-induced rat colitis and adrenal suppression were compared after oral administration of methylprednisolone 21-sulfate sodium (MPS), a colon-specific prodrug of MP, or MPS/GCZ to colitic rats., Results: Upon incubation of MP with the cecal contents, MP disappeared, and this was delayed by addition of GCZ. In addition, more MP produced from MPS in the cecal contents accumulated in the presence of GCZ. Consistent with these results, upon oral administration of MPS/GCZ, MPS or MP, MP was detected at a greater level in the large intestine for MPS/GCZ. MPS/GCZ ameliorated TNBS-induced colitis of rats, and this therapeutic effect was superior to that of MPS and MP. Moreover, MPS/GCZ decreased the plasma levels of corticosterone and ACTH to a greater extent than MPS, but less than MP., Conclusions: Co-administration of GCZ, a reduction inhibitor, may be a plausible strategy to reduce the therapeutic loss of MP produced from MPS in the large intestine, thus improving the therapeutic property of the prodrug against inflammatory bowel disease.

Published

2013

29. Structure-activity relationship of salicylic acid derivatives on inhibition of TNF-α dependent NFκB activity: Implication on anti-inflammatory effect of N-(5-chlorosalicyloyl)phenethylamine against experimental colitis.

Author

Kim J, Kang S, Hong S, Yum S, Kim YM, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cell Survival drug effects, Chemokine CXCL2 analysis, Chemokine CXCL2 metabolism, HCT116 Cells, Humans, Inhibitory Concentration 50, Magnetic Resonance Spectroscopy, Mass Spectrometry, Mice, Molecular Structure, NF-kappa B metabolism, Rats, Salicylates chemistry, Salicylates pharmacology, Spectrophotometry, Infrared, Structure-Activity Relationship, Tumor Necrosis Factor-alpha pharmacology, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Colitis drug therapy, NF-kappa B antagonists & inhibitors, Salicylates chemical synthesis, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

To develop a more potent NFκB inhibitor from salicylic acid which is known to inhibit activity of NFκB, a transcription factor regulating genes involved in immunity, inflammation and tumorigenesis, derivatives of salicylic acid (SA) where the 5 position, carboxyl or hydroxyl group was modified were treated in HCT116 cells transfected with an NFκB dependent luciferase gene and LPS-stimulated RAW264.7 cells. Amidation of the carboxylic group or substitution of chlorine at the 5 position increased the ability of SA to suppress the expression of NFκB dependent luciferase and inducible nitric oxide synthase, a product of an NFκB target gene. Moreover, simultaneous amidation and chlorination of SA (5-chlorosalicylamide; 5-CSAM) conferred an additive NFκB inhibitory activity on SA. To further enhance the inhibitory activity, N-modification was imposed on 5-CSAM. N-(5-chlorosalicyloyl)phenethylamine (5-CSPA), N-(5-chlorosalicyloyl)3-phenylpropylamine (5-CSPPA) and N-(5-chlorosalicyloyl)4-hydroxyphenylethylamine (5-CSHPA) showed greater potencies for inhibiting NFκB activity than other derivatives. Their IC(50)s' in the luciferase assay measured 15μM (5-CSPA), 17μM (5-CSPPA) and 91μM (5-CSHPA). Rectal administration of 5-CSPA ameliorated TNBS-induced rat colitis, which was more effective than a conventional drug, 5-aminosalicylic acid. These data may provide useful information for development of a therapeutic agent for treatment of diseases where NFκB plays a critical role in the pathogenic progresses., (Copyright © 2011 Elsevier Masson SAS. All rights reserved.)

Published

2012

30. An anti-inflammatory mechanism of taurine conjugated 5-aminosalicylic acid against experimental colitis: taurine chloramine potentiates inhibitory effect of 5-aminosalicylic acid on IL-1beta-mediated NFkappaB activation.

Author

Joo K, Lee Y, Choi D, Han J, Hong S, Kim YM, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Cell Line, Tumor, Colitis metabolism, Dose-Response Relationship, Drug, Drug Synergism, Enzyme Activation drug effects, Humans, I-kappa B Kinase metabolism, Mesalamine therapeutic use, Prodrugs metabolism, Taurine chemistry, Taurine pharmacology, Colitis drug therapy, Interleukin-1beta metabolism, Mesalamine chemistry, Mesalamine pharmacology, NF-kappa B metabolism, Taurine analogs & derivatives

Abstract

Previously, we reported that oral administration of taurine conjugated 5-aminosalicylic acid, a colon-specific prodrug of 5-aminosalicylic acid (5-ASA), is effective in ameliorating experimental colitis and taurine elicits an additive anti-inflammatory effect upon cotreatment with 5-ASA. To explore a molecular mechanism for the anti-inflammatory property of the prodrug, we investigated the effect of the conjugate on IL-1beta-mediated NFkappaB activation. In human colon carcinoma Caco-2 and HCT116 cells, NFkappaB activity was accessed by a luciferase reporter assay and IL-6 secretion. Protein levels were determined by Western blotting. IL-6 levels were monitored by an Elisa kit. Treatment with either 5-ASA or taurine chloramine (TauCl) inhibited IL-1beta-mediated NFkappaB dependent luciferase expression and IL-6 secretion. In HCT116 cells, the inhibitory effect by TauCl or 5-ASA was through preventing IL-1beta-induced IkappaB kinase activation and subsequently interfering with IkappaBalpha degradation and p65 nuclear accumulation. Furthermore, combined TauCl/5-ASA treatment interfered additively with the activation process, leading to additive inhibitory effect on IL-1beta-mediated NFkappaB activation. Our results suggest that the anti-inflammatory effect of the prodrug on experimental colitis is attributed to the inhibition of the IL-1beta-mediated NFkappaB activation and the taurine effect is through TauCl potentiating the ability of 5-ASA to inhibit IL-1beta dependent NFkappaB activation.

Published

2009

31. Sulfate-conjugated methylprednisolone as a colon-targeted methylprednisolone prodrug with improved therapeutic properties against rat colitis.

Author

Kong H, Lee Y, Hong S, Han J, Choi B, Jung Y, and Kim YM

Subjects

Administration, Oral, Adrenal Glands drug effects, Animals, Disease Models, Animal, Drug Delivery Systems, Glucocorticoids adverse effects, Glucocorticoids chemistry, Male, Methylprednisolone adverse effects, Methylprednisolone chemistry, Prodrugs, Rats, Rats, Sprague-Dawley, Sulfates chemistry, Thymus Gland drug effects, Trinitrobenzenesulfonic Acid, Colitis drug therapy, Colon metabolism, Glucocorticoids pharmacokinetics, Methylprednisolone pharmacokinetics

Abstract

Methylprednisolone (MP) is one of the most widely used corticosteroids for the treatment of inflammatory bowel disease (IBD). However, systemic adverse effects of MP limit its availability for the disease. In present study, sulfate-conjugated methylprednisolone (MPS) was evaluated in vivo as a colon-targeted prodrug of MP and its therapeutic properties against 2,4,6-trinitrobenzenesulfonic acid-induced rat colitis were investigated. Upon oral administration, a large fraction of MPS reached the large intestine, where MPS was converted to MP implying that MPS would deliver MP effectively to the large intestine. The fecal recovery of MP (after MPS administration) was much greater than that after MP administration and the urinary recovery of MP (after MPS administration) was much less than that after MP administration, suggesting that MPS should exhibit enhanced therapeutic activity and reduced systemic adverse effects. Consistent with this notion, MPS was more effective than MP in ameliorating rat colitis. Moreover, the adverse effects of MPS on adrenal function and thymus were much lower than those of MP. Taken together, MPS may be therapeutically superior to MP in IBD treatment.

Published

2009

32. Dexamethasone 21-sulfate improves the therapeutic properties of dexamethasone against experimental rat colitis by specifically delivering the steroid to the large intestine.

Author

Kim I, Kong H, Lee Y, Hong S, Han J, Jung S, Jung Y, and Kim YM

Subjects

Administration, Oral, Adrenal Glands drug effects, Adrenal Glands metabolism, Adrenocorticotropic Hormone blood, Animals, Anti-Inflammatory Agents administration & dosage, Anti-Inflammatory Agents pharmacokinetics, Colitis chemically induced, Colitis metabolism, Colitis pathology, Colon metabolism, Colon pathology, Dexamethasone administration & dosage, Dexamethasone analogs & derivatives, Dexamethasone pharmacokinetics, Disease Models, Animal, Feces chemistry, Gastrointestinal Agents administration & dosage, Gastrointestinal Agents pharmacokinetics, Hydrocortisone blood, Intestinal Absorption, Male, Prodrugs administration & dosage, Prodrugs pharmacokinetics, Rats, Rats, Sprague-Dawley, Sulfates administration & dosage, Sulfates pharmacokinetics, Trinitrobenzenesulfonic Acid, Anti-Inflammatory Agents pharmacology, Colitis prevention & control, Colon drug effects, Dexamethasone pharmacology, Gastrointestinal Agents pharmacology, Prodrugs pharmacology, Sulfates pharmacology

Abstract

Purpose: We investigated in vivo-colon targetability and therapeutic properties of DS against experimental rat colitis., Methods: The systemic absorption and colonic delivery of D after oral administration of DS was analyzed by examining the concentration of drugs in the GI tract, plasma, urine and feces. Therapeutic activity of DS was determined using a TNBS-induced rat colitis model. Adrenal suppression by DS administration was evaluated by monitoring the concentration of ACTH and corticosterone in the plasma., Results: DS administered orally was delivered efficiently to the large intestine resulting in D accumulation at the target site. In addition, DS was not detectable in the plasma and was detected very low in the urine after DS administration. The fecal and urinary recovery of D (after DS administration) was much greater and less than that after D administration, suggesting that DS should exhibit enhanced therapeutic activity and reduced systemic side effects. Consistent with this notion, DS was more effective than D in healing rat colitis. Moreover, oral administration of either D or DS reduced the plasma corticosterone and ACTH levels from the normal levels, which is significantly greater for D., Conclusion: DS is a promising colon specific prodrug that improves therapeutic properties of D.

Published

2009

33. N,N'-Bis(5-aminosalicyl)-L-cystine is a potential colon-specific 5-aminosalicylic acid prodrug with dual therapeutic effects in experimental colitis.

Author

Kim H, Huh J, Jeon H, Choi D, Han J, Kim Y, and Jung Y

Subjects

Aminosalicylic Acids chemistry, Animals, Colitis metabolism, Colon metabolism, Cystine administration & dosage, Cystine chemistry, Male, Prodrugs chemistry, Rats, Rats, Sprague-Dawley, Aminosalicylic Acids administration & dosage, Colitis drug therapy, Colon drug effects, Cystine analogs & derivatives, Prodrugs administration & dosage

Abstract

To evaluate N,N'-bis(5-aminosalicyl)-L-cystine (5-ASA-Cys) as a potential colon-specific 5-aminosalicylic acid prodrug with dual therapeutic effects in experimental colitis, the pharmacokinetics and therapeutic activity were investigated after oral administration of 5-ASA-Cys and amelioration of experimental colitis was compared after rectal administration of 5-aminosalicylic acid (5-ASA) and/or cysteine. In addition, the gluthathione (GSH) level in the inflamed colonic tissue was examined after administration of cysteine or 5-ASA-Cys. Oral administration of 5-ASA-Cys delivered much greater amount of 5-ASA to the large intestine and excreted lower amount of 5-ASA via urine than that of free 5-ASA. Oral administration of 5-ASA-Cys ameliorated experimental colitis of rats induced by TNBS, which was more effective than that of sulfasalazine. Although cysteine administered rectally was not significantly effective, intracolonic treatment with both 5-ASA and cysteine showed a synergic effect in alleviating the rat colitis. Furthermore, not only 5-ASA-Cys administered orally but also cysteine administered rectally increased the glutathione level in the inflamed colonic tissue. Taken together, these results suggest that 5-ASA-Cys is a potential colon specific 5-ASA prodrug with dual therapeutic effects on experimental colitis and cysteine modulation of the glutathione level may be relevant to the dual effects of the prodrug., ((c) 2008 Wiley-Liss, Inc. and the American Pharmacists Association)

Published

2009

34. Evaluation of 5-aminosalicyltaurine as a colon-specific prodrug of 5-aminosalicylic acid for treatment of experimental colitis.

Author

Jung Y, Kim HH, Kim H, Kong H, Choi B, Yang Y, and Kim Y

Subjects

Aminosalicylic Acids chemistry, Aminosalicylic Acids pharmacokinetics, Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Chromatography, High Pressure Liquid, Colitis chemically induced, Colon drug effects, Drug Delivery Systems, Feces chemistry, Gastrointestinal Agents therapeutic use, Intestinal Absorption, Male, Mesalamine chemistry, Mesalamine pharmacokinetics, Prodrugs chemistry, Prodrugs pharmacokinetics, Rats, Rats, Sprague-Dawley, Sulfasalazine therapeutic use, Taurine chemistry, Taurine pharmacokinetics, Taurine therapeutic use, Trinitrobenzenesulfonic Acid, Aminosalicylic Acids therapeutic use, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Colitis drug therapy, Mesalamine therapeutic use, Prodrugs therapeutic use, Taurine analogs & derivatives

Abstract

We previously reported that 5-aminosalicyltaurine (taurine-conjugated 5-ASA, 5-ASA-Tau) showed a potential as a colon-specific prodrug of 5-aminosalicylic acid (5-ASA) by in vitro evaluation. In this report, we in vivo-evaluated 5-ASA-Tau as a colon-specific prodrug for treatment of experimental colitis. Taurine conjugation of 5-ASA greatly reduced absorption of 5-ASA from the intestine. Oral administration of taurine-conjugated 5-ASA not only increased the colonic delivery efficiency of 5-ASA but also decreased the systemic absorption of free 5-ASA as compared with that of 5-ASA and, moreover, taurine is similarly effective to known colon-specific carriers for 5-ASA, glycine and aspartic acid, suggesting that taurine conjugation is an efficient way to increase the therapeutic effect and to reduce the adverse effects of 5-ASA. Intracolonic treatment with combined 5-ASA/taurine additively ameliorated TNBS-induced colitis rats indicating that taurine acted as not only a promoiety but also a therapeutically active agent. Furthermore, 5-ASA-Tau is slightly more effective than sulfasalazine in alleviating the colonic inflammation induced by TNBS. Taken together, our data suggest that 5-ASA-Tau is a potential colon-specific prodrug of 5-aminosalicylic acid with improved therapeutic activity against inflammatory bowel disease.

Published

2006

35. A molecular mechanism for the anti-inflammatory effect of taurine-conjugated 5-aminosalicylic acid in inflamed colon.

Author

Kim H, Jeon H, Kong H, Yang Y, Choi B, Kim YM, Neckers L, and Jung Y

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Cell Line, Chromatography, High Pressure Liquid, Colitis metabolism, Colon metabolism, Colon pathology, Dose-Response Relationship, Drug, Humans, Mesalamine chemistry, Mesalamine therapeutic use, NF-kappa B chemistry, NF-kappa B metabolism, Phosphorylation, Rats, Serine metabolism, Taurine analogs & derivatives, Taurine pharmacology, Tumor Necrosis Factor-alpha pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Colitis drug therapy, Colon drug effects, Mesalamine pharmacology, Taurine chemistry

Abstract

In previous reports, a novel colon-specific prodrug, 5-aminosalicyltaurine (5-ASA-Tau) administered orally, is successfully delivered to and liberates 5-aminosalicylic acid (5-ASA) and taurine in the inflamed large intestine of rats. Furthermore, the prodrug ameliorates the 2,4,6-trinitrobenzene-sulfonic acid-induced colitis, and taurine acts not only as a carrier but also as an active therapeutic agent. In this study, we investigated the anti-inflammatory properties of the prodrug at a molecular level. After rectal administration of taurine, formation of taurine chloramine (TauCl) in the inflamed colonic tissue was examined using high-performance liquid chromatography. In human colon epithelial cell lines, nuclear factor-kappaB (NF-kappaB) activity was accessed using an NF-kappaB-dependent luciferase reporter gene. Protein levels were monitored by Western blotting. DNA binding activity of the NF-kappaB subunit p65 was determined using a DNA binding assay kit. A millimolar level of TauCl was formed in the inflamed tissue. TauCl inhibited tumor necrosis factor (TNF)-dependent NF-kappaB activation by modifying thiol(s) on p65 and blocking DNA binding. In addition, 5-ASA inhibited phosphorylation of p65 at serine 536, which is critical for transcriptional activity of NF-kappaB. Furthermore, combined TauCl/5-ASA treatment additively inhibited TNF-dependent NF-kappaB activation. Together, our data suggest that the colon-specific carrier taurine contributes to the clinical effect of the prodrug by potentiating the inhibitory effect of the active ingredient 5-ASA on a major proinflammatory signal, TNF-dependent NF-kappaB activation in the inflamed large intestine.

Published

2006

36. N-Succinylaspartic-Acid-Conjugated Riluzole Is a Safe and Potent Colon-Targeted Prodrug of Riluzole against DNBS-Induced Rat Colitis.

Author

Kim, Jaejeong, Kang, Changyu, Yoo, Jin-Wook, Yoon, In-Soo, and Jung, Yunjin

Subjects

COLITIS, RILUZOLE, COLON (Anatomy), ORAL drug administration, INTESTINAL diseases, SALICYLIC acid

Abstract

In our previous study, riluzole azo-linked to salicylic acid (RAS) was prepared as a colon-targeted prodrug of riluzole (RLZ) to facilitate the repositioning of RLZ as an anticolitic drug. RAS is more effective against rat colitis than RLZ and sulfasalazine, currently used as an anti-inflammatory bowel disease drug. The aim of this study is to further improve colon specificity, anticolitic potency, and safety of RAS. N-succinylaspart-1-ylRLZ (SAR) and N-succinylglutam-1-ylRLZ (SGR) were synthesized and evaluated as a "me-better" colon-targeted prodrug of RLZ against rat colitis. SAR but not SGR was converted to RLZ in the cecal contents, whereas both conjugates remained intact in the small intestine. When comparing the colon specificity of SAR with that of RAS, the distribution coefficient and cell permeability of SAR were lower than those of RAS. In parallel, oral SAR delivered a greater amount of RLZ to the cecum of rats than oral RAS. In a DNBS-induced rat model of colitis, oral SAR mitigated colonic damage and inflammation and was more potent than oral RAS. Moreover, upon oral administration, SAR had a greater ability to limit the systemic absorption of RLZ than RAS, indicating a reduced risk of systemic side effects of SAR. Taken together, SAR may be a "me-better" colon-targeted prodrug of RLZ to improve the safety and anticolitic potency of RAS, an azo-type colon-targeted prodrug of RLZ. [ABSTRACT FROM AUTHOR]

Published

2023

37. Colon-Targeted Trans-Cinnamic Acid Ameliorates Rat Colitis by Activating GPR109A.

Author

Kang, Changyu, Kim, Jaejeong, Ju, Sanghyun, Cho, Heeyeong, Kim, Hyun Young, Yoon, In-Soo, Yoo, Jin-Wook, and Jung, Yunjin

Subjects

INFLAMMATORY bowel diseases, COLITIS, ASPARTIC acid, GLUTAMIC acid, CELL permeability, CECUM

Abstract

We designed colon-targeted trans-cinnamic acid (tCA) and synthesized its conjugates with glutamic acid (tCA-GA) and aspartic acid (tCA-AA). We evaluated the anti-colitic activity of colon-targeted tCA using a dinitrobenzenesulfonic acid-induced rat colitis model. The conjugates lowered the distribution coefficient and Caco-2 cell permeability of tCA and converted to tCA in the cecum, with higher rates and percentages with tCA-GA than with tCA-AA. Following oral gavage, tCA-GA delivered a higher amount of tCA to the cecum and exhibited better anti-colitic effects than tCA and sulfasalazine (SSZ), which is the current treatment for inflammatory bowel disease. In the cellular assay, tCA acted as a full agonist of GPR109A (EC50: 530 µM). The anti-colitic effects of tCA-GA were significantly compromised by the co-administration of the GPR109A antagonist, mepenzolate. Collectively, colon-targeted tCA potentiated the anti-colitic activity of tCA by effectively activating GPR109A in the inflamed colon, enabling tCA to elicit therapeutic superiority over SSZ. [ABSTRACT FROM AUTHOR]

Published

2023

38. Hyaluronic Acid-Conjugated PLGA Nanoparticles Alleviate Ulcerative Colitis via CD44-Mediated Dual Targeting to Inflamed Colitis Tissue and Macrophages.

Author

Hlaing, Shwe Phyu, Cao, Jiafu, Lee, Juho, Kim, Jihyun, Saparbayeva, Aruzhan, Kwak, Dongmin, Kim, Hyunwoo, Hwang, Seonghwan, Yun, Hwayoung, Moon, Hyung Ryong, Jung, Yunjin, and Yoo, Jin-Wook

Subjects

ULCERATIVE colitis, INFLAMMATORY bowel diseases, COLITIS, TARGETED drug delivery, RECTAL administration, NANOMEDICINE, MACROPHAGES

Abstract

Although various local anti-inflammatory therapies for ulcerative colitis have been developed, rapid drug elimination from inflamed colitis tissue and off-target side effects reduce their therapeutic efficacy. In this study, we synthesized curcumin (Cur)-loaded hyaluronic acid (HA)-conjugated nanoparticles (Cur-HA-PLGA-NPs) that target inflamed colitis tissue via HA-CD44 interaction with resident colonic epithelial cells and subsequently target activated macrophages for ulcerative colitis therapy. The synthesized spherical Cur-HA-PLGA-NPs showed physicochemical properties similar to those of non-HA-conjugated Cur-PLGA-NPs. HA-PLGA-NPs exhibited selective accumulation in inflamed colitis tissue with minimal accumulation in healthy colon tissue. HA functionalization enhanced targeted drug delivery to intestinal macrophages, significantly increasing HA-PLGA-NP cellular uptake. Importantly, the rectal administration of Cur-HA-PLGA-NPs exhibited better therapeutic efficacy than Cur-PLGA-NPs in animal studies. Histological examination revealed that Cur-HA-PLGA-NPs reduced inflammation with less inflammatory cell infiltration and accelerated recovery with re-epithelialization signs. Our results suggest that Cur-HA-PLGA-NPs are a promising delivery platform for treating ulcerative colitis. [ABSTRACT FROM AUTHOR]

Published

2022

39. Colon-targeted delivery of cyclosporine A using dual-functional Eudragit® FS30D/PLGA nanoparticles ameliorates murine experimental colitis

Author

Naeem, Muhammad, Bae, Junhwan, Oshi, Murtada A, Kim, Min-Soo, Moon, Hyung Ryong, Lee, Bok Luel, Im, Eunok, Jung, Yunjin, and Yoo, Jin-Wook

Subjects

Colon, colon-targeted nanoparticles, Administration, Oral, Drug Delivery Systems, Polylactic Acid-Polyglycolic Acid Copolymer, Animals, Methylmethacrylates, Lactic Acid, Particle Size, Original Research, ulcerative colitis, Peroxidase, Drug Carriers, Mice, Inbred ICR, Macrophages, Body Weight, Hydrogen-Ion Concentration, Colitis, sustained and pH-sensitive release, Drug Liberation, Treatment Outcome, Cyclosporine, Cytokines, Nanoparticles, Inflammation Mediators, cyclosporine A, Immunosuppressive Agents, Polyglycolic Acid

Abstract

Background Colon-targeted oral nanoparticles (NPs) have emerged as an ideal, safe, and effective therapy for ulcerative colitis (UC) owing to their ability to selectively accumulate in inflamed colonic mucosa. Cyclosporine A (CSA), an immunosuppressive agent, has long been used as rescue therapy in severe steroid-refractory UC. In this study, we developed CSA-loaded dual-functional polymeric NPs composed of Eudragit® FS30D as a pH-sensitive polymer for targeted delivery to the inflamed colon, and poly(lactic-co-glycolic acid) (PLGA) as a sustained-release polymer. Methods CSA-loaded Eudragit FS30D nanoparticles (ENPs), PLGA nanoparticles (PNPs), and Eudragit FS30D/PLGA nanoparticles (E/PNPs) were prepared using the oil-in-water emulsion method. Scanning electron microscope images and zeta size data showed successful preparation of CSA-loaded NPs. Results PNPs exhibited a burst drug release of >60% at pH 1.2 (stomach pH) in 0.5 h, which can lead to unwanted systemic absorption and side effects. ENPs effectively inhibited the burst drug release at pH 1.2 and 6.8 (proximal small intestine pH); however, nearly 100% of the CSA in ENPs was released rapidly at pH 7.4 (ileum–colon pH) owing to complete NP dissolution. In contrast to single-functional PNPs and ENPs, the dual-functional E/PNPs minimized burst drug release (only 18%) at pH 1.2 and 6.8, and generated a sustained release at pH 7.4 thereafter. Importantly, in distribution studies in the gastrointestinal tracts of mice, E/PNPs significantly improved CSA distribution to the colon compared with PNPs or ENPs. In a mouse model of colitis, E/PNP treatment improved weight loss and colon length, and decreased rectal bleeding, spleen weight, histological scoring, myeloperoxidase activity, macrophage infiltration, and expression of proinflammatory cytokines compared with PNPs or ENPs. Conclusion Overall, this work confirms the benefits of CSA-loaded E/PNPs for efficiently delivering CSA to the colon, suggesting their potential for UC therapy.

Published

2018

40. Eletrophilic Chemistry of Tranilast Is Involved in Its Anti-Colitic Activity via Nrf2-HO-1 Pathway Activation.

Author

Jeong, Seongkeun, Kang, Changyu, Park, Sohee, Ju, Sanghyun, Yoo, Jin-Wook, Yoon, In-Soo, Yun, Hwayoung, and Jung, Yunjin

Subjects

NUCLEAR factor E2 related factor, PHARMACEUTICAL chemistry, SULFHYDRYL group, DRUG utilization, ANTIALLERGIC agents, TRYPTOPHAN

Abstract

Tranilast (TRL), a synthetic derivative of a tryptophan metabolite, is an anti-allergic drug used to treat bronchial asthma. We investigated how TRL activated the nuclear factor-erythroid 2 p45-related factor 2 (Nrf2)-hemeoxygenase-1 (HO-1) pathway based on the electrophilic chemistry of the drug and whether TRL activity contributed to the treatment of rat colitis. In human colon carcinoma cells, TRL activated Nrf2, as represented by an increase in nuclear Nrf2 and induction of Nrf2-dependent luciferase and, subsequently, HO-1, a target gene product of Nrf2. TRL activation of Nrf2 and induction of HO-1 were completely prevented by chemical reduction of the electrophilic functional group (α, β-unsaturated carbonyl group) in the drug. In parallel, TRL was reactive with the nucleophilic thiol group in N-acetylcysteine, forming a covalent adduct. Moreover, TRL, but not reduced TRL, binds to Kelch-like ECH-associated protein 1 (KEAP1), releasing Nrf2. TRL administration ameliorated colonic damage and inflammation in rats with dinitrobenzene sulfonic acid-induced colitis, which was partly compromised by the chemical reduction of TRL or co-treatment with an HO-1 inhibitor. Our results suggest that TRL activated the Nrf2-HO-1 pathway via covalent binding to KEAP1, partly contributing to TRL amelioration in rat colitis. [ABSTRACT FROM AUTHOR]

Published

2021

41. A Colon-Targeted Prodrug, 4-Phenylbutyric Acid-Glutamic Acid Conjugate, Ameliorates 2,4-Dinitrobenzenesulfonic Acid-Induced Colitis in Rats.

Author

Kim, Soojin, Lee, Seunghyun, Lee, Hanju, Ju, Sanghyun, Park, Sohee, Kwon, Doyoung, Yoo, Jin-Wook, Yoon, In-Soo, Min, Do Sik, Jung, Young-Suk, and Jung, Yunjin

Subjects

COLITIS, LARGE intestine, COLON (Anatomy), ENDOPLASMIC reticulum, INFLAMMATORY bowel diseases, RATS

Abstract

An elevated level of endoplasmic reticulum (ER) stress is considered an aggravating factor for inflammatory bowel disease (IBD). To develop an ER-stress attenuator that is effective against colitis, 4-phenylbutyric acid (4-PBA), a chemical chaperone that alleviates ER stress, was conjugated with acidic amino acids to yield 4-PBA-glutamic acid (PBA-GA) and 4-PBA-aspartic acid (PBA-AA) conjugates. The PBA derivatives were converted to 4-PBA in the cecal contents, and the conversion was greater with PBA-GA than that with PBA-AA. After oral administration of PBA-GA (oral PBA-GA), up to 2.7 mM PBA was detected in the cecum, whereas 4-PBA was not detected in the blood, indicating that PBA-GA predominantly targeted the large intestine. In 2,4-dinitrobenzenesulfonic acid-induced colitis in rats, oral PBA-GA alleviated the damage and inflammation in the colon and substantially reduced the elevated levels of ER stress marker proteins in the inflamed colon. Moreover, PBA-GA was found to be as effective as the currently used anti-IBD drug, sulfasalazine. In conclusion, PBA-GA is a colon-targeted prodrug of 4-PBA and is effective against rat colitis probably via the attenuation of ER stress in the inflamed colon. [ABSTRACT FROM AUTHOR]

Published

2020

42. Conjugation of Amisulpride, an Anti-Psychotic Agent, with 5-Aminosalicylic Acid via an Azo Bond Yields an Orally Active Mutual Prodrug against Rat Colitis.

Author

Kim, Wooseong, Kim, Dayoon, Jeong, Seongkeun, Ju, Sanghyun, Lee, Hanju, Kim, Soojin, Yoo, Jin-Wook, Yoon, In-Soo, and Jung, Yunjin

Subjects

COLITIS, AMISULPRIDE, GASTROINTESTINAL contents, INFLAMMATORY mediators, RATS, INFLAMMATORY bowel diseases

Abstract

Amisulpride (ASP), an anti-psychotic agent, is a pharmacologically equivalent to sulpiride (SP). Because SP demonstrates anti-ulcer and anti-colitic activities, ASP with an aniline moiety was azo-coupled to salicylic acid to generate 5-(aminoethanoylsulfamoyl)-N-[(1-ethylpyrrolidin-2-yl)methyl]-2-methoxybenzamide (ASP-azo-ASA), with the expectation that it would act as a colon-specific mutual prodrug against colitis. Following a 24 h incubation, approximately 80% of ASP-azo-ASA was cleaved to form ASP and 5-aminosalicylic acid (5-ASA) in the cecal contents, whereas it remained stable in the small intestinal contents. Oral gavage of ASP-azo-ASA (oral ASP-azo-ASA) delivered 5-ASA to the cecum to levels comparable with those observed for sulfasalazine (SSZ; clinical colon-specific prodrug of 5-ASA) and without detectable concentrations of ASP in the blood, indicating efficient colonic delivery. Oral ASP-azo-ASA ameliorated 2, 4-dinitrobenzenesulfonic acid hydrate (DNBS)-induced colitis in rats more effectively than oral SSZ. Additionally, oral ASP-azo-ASA lowered the levels of inflammatory mediators in the inflamed distal colon more effectively than oral SSZ. Combined treatment with 5-ASA and ASP via the rectal route more effectively reversed colonic damage and inflammation than treatment with 5-ASA or ASP alone, confirming the mutual anti-colitic actions of 5-ASA and ASP. In conclusion, ASP-azo-ASA is an orally active mutual prodrug against rat colitis with limited systemic absorption of ASP. [ABSTRACT FROM AUTHOR]

Published

2019

43. Oxidized 5-aminosalicylic acid activates Nrf2-HO-1 pathway by covalently binding to Keap1: Implication in anti-inflammatory actions of 5-aminosalicylic acid.

Author

Kang, Sookjin, Kim, Wooseong, Jeong, Seongkeun, Nam, Joon, Lee, Sunyoung, Jung, Yunjin, and Lee, Yonghyun

Subjects

*MESALAMINE, *COLON diseases, *COVALENT bonds, *OXIDATION, *HYPOCHLORITES, *THERAPEUTICS

Abstract

Mesalazine (5-aminosalicylic acid, 5-ASA), a currently used drug for anti-inflammatory bowel disease, is easily oxidized by HOCl, a strong oxidant generated in gut inflammation, to produce electrophilic quinones. We investigated whether this chemical feature has an implication in the anti-inflammatory pharmacology of 5-ASA. Human colon carcinoma HCT116 cells were treated with HOCl-reacted 5-ASA. Oxidized 5-ASA activated Nrf2 while 5-ASA itself was not effective. Activation of Nrf2 led to induction of hemeoxygenase (OH)-1, an anti-inflammatory enzyme. Western blot analysis of Keap1, a cytosolic repressor of Nrf2, following precipitation of biotin-labeled proteins in cell lysates treated with biotin-tagged 5-ASA, revealed a much greater amount of Keap1 when biotin-tagged 5-ASA was oxidized with HOCl. Precipitation of Keap1 was attenuated markedly by pretreatment with oxidized 5-ASA or a sulfhydryl donor. In addition, treatment with oxidized 5-ASA in cell lysates reduced the Keap1 amount that coimmunoprecipitated with Nrf2. In parallel, rectal administration of 5-ASA increased the level of HO-1 and nuclear Nrf2 in the inflamed colonic tissues, but not in normal colonic tissues. Moreover, oral gavage of sulfasalazine, a colon-specific prodrug of 5-ASA currently used clinically, activated the Nrf2-HO-1 pathway in the colonic tissues where inflammation was in progress, which was not observed when inflammation subsided. Collectively, our data suggest that Nrf2-HO-1 pathway is involved in the anti-inflammatory pharmacology of 5-ASA, which was likely being exerted exclusively in the inflammatory state. [ABSTRACT FROM AUTHOR]

Published

2017

44. Enzyme/pH dual sensitive polymeric nanoparticles for targeted drug delivery to the inflamed colon.

Author

Naeem, Muhammad, Kim, Wooseong, Cao, Jiafu, Jung, Yunjin, and Yoo, Jin-Wook

Subjects

*NANOPARTICLES, *DRUG delivery systems, *HYDROGEN-ion concentration, *COLITIS, *POLYURETHANES

Abstract

Novel nanoparticles whose drug release profiles are controlled by both enzyme and pH were prepared for the colon-specific drug delivery using a polymeric mixture of enzyme-sensitive azo-polyurethane and pH-sensitive Eudragit S100 (ES-Azo.pu). The enzyme/pH dual sensitive nanoparticles were designed to release a drug based on a two-fold approach which specifically aimed to target drug delivery to the inflamed colon while preventing the burst release of drugs in the stomach and small intestine. Single pH-sensitive (ES) and dual sensitive (ES-Azo.pu) nanoparticles were prepared using an oil-in-water emulsion solvent evaporation method and coumarin-6 (C-6) was used as a model drug. The successful formation of ES and ES-azo.pu nanoparticles that have 214 nm and 244 nm in mean particle size, respectively, was confirmed by scanning electron microscopy and qNano. ES nanoparticles showed almost 100% of burst drug release at pH 7.4, whereas ES-Azo.pu nanoparticles prevented the burst drug release at pH 7.4, followed by a sustained release phase thereafter. Furthermore, ES-Azo.pu nanoparticles exhibited enzyme-triggered drug release in the presence of rat cecal contents obtained from a rat model of colitis. An in vivo localization study in rat gastrointestinal tract demonstrated that ES-Azo.pu nanoparticles were selectively distributed in the inflamed colon, showing 5.5-fold higher C-6 than ES nanoparticles. In conclusion, the enzyme/pH dual sensitive nanoparticles presented in this study can serve as a promising strategy for colon-specific drug delivery against inflammatory bowel disease and other colon disorders. [ABSTRACT FROM AUTHOR]

Published

2014

45. Piceatannol, a hydroxystilbene natural product, stabilizes HIF-1α protein by inhibiting HIF prolyl hydroxylase

Author

Yum, Soohwan, Doh, Hea-Jeong, Hong, Sungchae, Jeong, Seongkeun, Kim, Dae-Duk, Park, Misun, and Jung, Yunjin

Subjects

*PICEATANNOL, *STILBENE, *VASCULAR endothelial growth factors, *HEME oxygenase, *HYPOXIA-inducible factor 1, *COLITIS, *HYDROXYLASES

Abstract

Abstract: To investigate the mechanisms underlying the biological activity of piceatannol (PCT), a hydroxystilbene natural product that has anti-colitic properties, we examined whether PCT could modulate hypoxia-inducible factor (HIF)-1 activity in human colon carcinoma cells. PCT induced HIF-1α protein, leading to induction of its target gene products, vascular endothelial growth factor and heme oxygenase-1, which are involved in amelioration of colitis. PCT induction of HIF-1α resulted from HIF-1α protein stabilization, which occurred through inhibition of HIF-prolyl hydroxylase-2 (HPH-2). PCT inhibition of HPH-2 was reversed by addition of ascorbate, a cofactor of HPH-2, but not the cosubstrate, 2-ketoglutarate, to the reaction mixture of an in vitro von Hippel–Lindau (VHL) capture assay, and pretreatment with ascorbate abrogated PCT induction of cellular HIF-1α. Moreover, PCT prevented hydroxylation of cellular HIF-1α and attenuated coimmunoprecipitation of Flag-VHL protein and HA–HIF-1α over-expressed in human embryonic kidney 293 cells. Structural analysis using derivatives of PCT revealed that the catechol moiety in PCT was required for the stabilization of HIF-1α protein. Taken together, PCT activation of HIF-1 resulting from inhibition of HPH-2 may be a molecular mechanism for an anti-colitic effect of the natural product. [Copyright &y& Elsevier]

Published

2013