论文信息 - Advances in oral nano-delivery systems for colon targeted drug delivery in inflammatory bowel disease: selective targeting to diseased versus healthy tissue.

Advances in oral nano-delivery systems for colon targeted drug delivery in inflammatory bowel disease: selective targeting to diseased versus healthy tissue.

UNLABELLED Colon targeted drug delivery is an active area of research for local diseases affecting the colon, as it improves the efficacy of therapeutics and enables localized treatment, which reduces systemic toxicity. Targeted delivery of therapeutics to the colon is particularly advantageous for the treatment of inflammatory bowel disease (IBD), which includes ulcerative colitis and Crohn's disease. Advances in oral drug delivery design have significantly improved the bioavailability of drugs to the colon; however in order for a drug to have therapeutic efficacy during disease, considerations must be made for the altered physiology of the gastrointestinal (GI) tract that is associated with GI inflammation. Nanotechnology has been used in oral dosage formulation design as strategies to further enhance uptake into diseased tissue within the colon. This review will describe some of the physiological challenges faced by orally administered delivery systems in IBD, the important developments in orally administered nano-delivery systems for colon targeting, and the future advances of this research. FROM THE CLINICAL EDITOR Inflammatory Bowel Disease (IBD) poses a significant problem for a large number of patients worldwide. Current medical therapy mostly aims at suppressing the active inflammatory episodes. In this review article, the authors described and discussed the various approaches current nano-delivery systems can offer in overcoming the limitations of conventional drug formulations.

[1] A. Lamprecht,et al. Surfactant-dependence of nanoparticle treatment in murine experimental colitis. , 2013, Journal of controlled release : official journal of the Controlled Release Society.

[2] A. Scarsbrook,et al. Prevalence of, and predictors of, bile acid malabsorption in outpatients with chronic diarrhea , 2012, Neurogastroenterology and motility : the official journal of the European Gastrointestinal Motility Society.

[3] Cui Tang,et al. Galactosylated trimethyl chitosan-cysteine nanoparticles loaded with Map4k4 siRNA for targeting activated macrophages. , 2013, Biomaterials.

[4] S. Chandran,et al. Multiparticulate formulation approach to colon specific drug delivery: current perspectives. , 2006, Journal of pharmacy & pharmaceutical sciences : a publication of the Canadian Society for Pharmaceutical Sciences, Societe canadienne des sciences pharmaceutiques.

[5] D. Podolsky,et al. Inflammatory bowel disease. , 2002, The New England journal of medicine.

[6] Stavroula Sofou,et al. Antibody-targeted liposomes in cancer therapy and imaging , 2008, Expert opinion on drug delivery.

[7] H. Merkle,et al. Evaluation of particle uptake in human blood monocyte-derived cells in vitro. Does phagocytosis activity of dendritic cells measure up with macrophages? , 2001, Journal of controlled release : official journal of the Controlled Release Society.

[8] David J Brayden,et al. Dexamethasone-pDMAEMA polymeric conjugates reduce inflammatory biomarkers in human intestinal epithelial monolayers. , 2009, Journal of controlled release : official journal of the Controlled Release Society.

[9] M. Sioud,et al. Gene silencing in mammalian cells by preformed small RNA duplexes. , 2002, Biochemical and biophysical research communications.

[10] B. Dortunç,et al. Preparation and in vitro evaluation of Eudragit microspheres containing acetazolamide. , 2004, International journal of pharmaceutics.

[11] Libo Yang,et al. Biorelevant dissolution testing of colon-specific delivery systems activated by colonic microflora. , 2008, Journal of controlled release : official journal of the Controlled Release Society.

[12] Toru Yoshitomi,et al. An orally administered redox nanoparticle that accumulates in the colonic mucosa and reduces colitis in mice. , 2012, Gastroenterology.

[13] W. Sandborn. Rational selection of oral 5-aminosalicylate formulations and prodrugs for the treatment of ulcerative colitis , 2002, American Journal of Gastroenterology.

[14] E. Chang,et al. Mechanisms and Treatment of Diarrhea in Inflammatory Bowel Diseases , 1997, Inflammatory bowel diseases.

[15] R. Britton,et al. Role of the intestinal microbiota in resistance to colonization by Clostridium difficile. , 2014, Gastroenterology.

[16] Y. Barenholz,et al. Enhanced Transferrin Receptor Expression by Proinflammatory Cytokines in Enterocytes as a Means for Local Delivery of Drugs to Inflamed Gut Mucosa , 2011, PloS one.

[17] E. Yazaki,et al. Objective evaluation of small bowel and colonic transit time using pH telemetry in athletes with gastrointestinal symptoms , 2004, British Journal of Sports Medicine.

[18] N. Pace,et al. Molecular-phylogenetic characterization of microbial community imbalances in human inflammatory bowel diseases , 2007, Proceedings of the National Academy of Sciences.

[19] Willis,et al. Ligand-targeted liposomes. , 1998, Advanced drug delivery reviews.

[20] N. Ziats,et al. Acquired increase in leucocyte binding by intestinal microvascular endothelium in inflammatory bowel disease , 1998, The Lancet.

[21] D. Merlin,et al. Homeostatic and innate immune responses: role of the transmembrane glycoprotein CD98 , 2012, Cellular and Molecular Life Sciences.

[22] Yunwei Wang,et al. Lubiprostone Decreases Mouse Colonic Inner Mucus Layer Thickness and Alters Intestinal Microbiota , 2013, Digestive Diseases and Sciences.

[23] Bo Xiao,et al. Mannosylated bioreducible nanoparticle-mediated macrophage-specific TNF-α RNA interference for IBD therapy. , 2013, Biomaterials.

[24] J. Hanes,et al. Mucus-penetrating nanoparticles for drug and gene delivery to mucosal tissues. , 2009, Advanced drug delivery reviews.

[25] I. Wilding,et al. Variation in Gastrointestinal Transit of Pharmaceutical Dosage Forms in Healthy Subjects , 1991, Pharmaceutical Research.

[26] A. Beloqui,et al. Fate of nanostructured lipid carriers (NLCs) following the oral route: design, pharmacokinetics and biodistribution , 2014, Journal of microencapsulation.

[27] D. Rampton,et al. Intestinal luminal pH in inflammatory bowel disease: possible determinants and implications for therapy with aminosalicylates and other drugs , 2001, Gut.

[28] P. Legrand,et al. Polymeric nanocapsules as drug delivery systems. A review , 1999 .

[29] Bo Xiao,et al. Oral colon-specific therapeutic approaches toward treatment of inflammatory bowel disease , 2012, Expert opinion on drug delivery.

[30] R. Sartor. Genetics and environmental interactions shape the intestinal microbiome to promote inflammatory bowel disease versus mucosal homeostasis. , 2010, Gastroenterology.

[31] D. Podolsky. The future of IBD treatment. , 2003, Journal of gastroenterology.

[32] V. Préat,et al. Budesonide-loaded nanostructured lipid carriers reduce inflammation in murine DSS-induced colitis. , 2013, International journal of pharmaceutics.

[33] A. Basit,et al. Gut instincts: explorations in intestinal physiology and drug delivery. , 2008, International journal of pharmaceutics.

[34] Mansoor M Amiji,et al. Gastrointestinal distribution and in vivo gene transfection studies with nanoparticles-in-microsphere oral system (NiMOS). , 2007, Journal of controlled release : official journal of the Controlled Release Society.

[35] W. Sandborn. Rational selection of oral 5-aminosalicylate formulations and prodrugs for the treatment of ulcerative colitis. , 2002 .

[36] P. Venge,et al. Increased intraluminal release of eosinophil granule proteins EPO, ECP, EPX, and cytokines in ulcerative colitis and proctitis in segmental perfusion , 1999, American Journal of Gastroenterology.

[37] G. Macfarlane,et al. Fermentation in the Human Large Intestine: Its Physiologic Consequences and the Potential Contribution of Prebiotics , 2011, Journal of clinical gastroenterology.

[38] Soriano,et al. The role of PEG on the stability in digestive fluids and in vivo fate of PEG-PLA nanoparticles following oral administration. , 2000, Colloids and surfaces. B, Biointerfaces.

[39] David J Brayden,et al. Chloride-led Disruption of the Intestinal Mucous Layer Impedes Salmonella Invasion: Evidence for an ‘Enteric Tear’ Mechanism , 2011, Cellular Physiology and Biochemistry.

[40] A. Basit,et al. Interplay Between Intestinal pH, Transit Time and Feed Status on the In Vivo Performance of pH Responsive Ileo-Colonic Release Systems , 2008, Pharmaceutical Research.

[41] N. Škalko-Basnet,et al. Mucoadhesive liposomal delivery systems: the choice of coating material , 2011, Drug development and industrial pharmacy.

[42] H. Takeuchi,et al. pH-Sensitive nanospheres for colon-specific drug delivery in experimentally induced colitis rat model. , 2009, European journal of pharmaceutics and biopharmaceutics : official journal of Arbeitsgemeinschaft fur Pharmazeutische Verfahrenstechnik e.V.

[43] G. Hansson,et al. A complex, but uniform O-glycosylation of the human MUC2 mucin from colonic biopsies analyzed by nanoLC/MSn. , 2009, Glycobiology.

[44] A. Lamprecht. IBD: Selective nanoparticle adhesion can enhance colitis therapy , 2010, Nature Reviews Gastroenterology &Hepatology.

[45] Michael P. Jones,et al. New Directions in the Assessment of Gastric Function: Clinical Applications of Physiologic Measurements , 2006, Digestive Diseases.

[46] J. Schulzke,et al. Nano- and microscaled particles for drug targeting to inflamed intestinal mucosa: a first in vivo study in human patients. , 2013, Journal of controlled release : official journal of the Controlled Release Society.

[47] J. Fallingborg,et al. Small Intestinal Transit Time and Intraluminal pH in Ileocecal Resected Patients with Crohn's Disease , 1998, Digestive Diseases and Sciences.

[48] D. Aggarwal,et al. Biopharmaceutical considerations and characterizations in development of colon targeted dosage forms for inflammatory bowel disease , 2013, Drug Delivery and Translational Research.

[49] K. Whaley,et al. Antibody diffusion in human cervical mucus. , 1994, Biophysical journal.

[50] Y. Mahida,et al. Respiratory burst activity of intestinal macrophages in normal and inflammatory bowel disease. , 1989, Gut.

[51] R. Price,et al. Ginkgo biloba extract EGb 761 has anti-inflammatory properties and ameliorates colitis in mice by driving effector T cell apoptosis. , 2008, Carcinogenesis.

[52] Claus-Michael Lehr,et al. Size-Dependent Bioadhesion of Micro- and Nanoparticulate Carriers to the Inflamed Colonic Mucosa , 2001, Pharmaceutical Research.

[53] A. Gasbarrini,et al. Adhesion molecules in inflammatory bowel disease: therapeutic implications for gut inflammation. , 2005, Digestive and liver disease : official journal of the Italian Society of Gastroenterology and the Italian Association for the Study of the Liver.

[54] G. Cairo,et al. Role of HIF-1 and NF-κB Transcription Factors in the Modulation of Transferrin Receptor by Inflammatory and Anti-inflammatory Signals* , 2008, Journal of Biological Chemistry.

[55] C. Probert,et al. Review article: steroid resistance in inflammatory bowel disease – mechanisms and therapeutic strategies , 2007, Alimentary pharmacology & therapeutics.

[56] Roland Ladurner,et al. Assessment of colonic transit time using MRI: a feasibility study , 2007, European Radiology.

[57] S. Phillips,et al. Inhibition of ileal water absorption by intraluminal fatty acids. Influence of chain length, hydroxylation, and conjugation of fatty acids. , 1974, The Journal of clinical investigation.

[58] Mansoor Amiji,et al. Oral TNF-α gene silencing using a polymeric microsphere-based delivery system for the treatment of inflammatory bowel disease. , 2011, Journal of controlled release : official journal of the Controlled Release Society.

[59] R. Macdermott,et al. Aberrant binding of lamina propria lymphocytes to vascular endothelium in inflammatory bowel diseases. , 1994, Gastroenterology.

[60] L. Ferguson,et al. Potential prospects of nanomedicine for targeted therapeutics in inflammatory bowel diseases. , 2012, World journal of gastroenterology.

[61] David J Brayden,et al. Restoration of rat colonic epithelium after in situ intestinal instillation of the absorption promoter, sodium caprate. , 2010, Therapeutic delivery.

[62] Russell J Mumper,et al. Doxorubicin and paclitaxel-loaded lipid-based nanoparticles overcome multidrug resistance by inhibiting P-glycoprotein and depleting ATP. , 2009, Cancer research.

[63] A. Lamprecht,et al. Nanoparticles in inflammatory bowel disease: particle targeting versus pH-sensitive delivery. , 2006, International journal of pharmaceutics.

[64] Y. Kawashima,et al. Biodegradable nanoparticles for targeted drug delivery in treatment of inflammatory bowel disease. , 2001, The Journal of pharmacology and experimental therapeutics.

[65] P. Artursson,et al. Transport of nanoparticles across an in vitro model of the human intestinal follicle associated epithelium. , 2005, European journal of pharmaceutical sciences : official journal of the European Federation for Pharmaceutical Sciences.

[66] Benjamin C. Tang,et al. Biodegradable polymer nanoparticles that rapidly penetrate the human mucus barrier , 2009, Proceedings of the National Academy of Sciences.

[67] Henry C. Lin,et al. The ileal brake: A fifteen-year progress report , 1999, Current gastroenterology reports.

[68] Jianfeng Chen,et al. Fabrication of porous hollow silica nanoparticles and their applications in drug release control. , 2004, Journal of controlled release : official journal of the Controlled Release Society.

[69] Shiu-Nan Chen,et al. Apoptotic cell: linkage of inflammation and wound healing , 2014, Front. Pharmacol..

[70] S. Muro,et al. Biodistribution and endocytosis of ICAM-1-targeting antibodies versus nanocarriers in the gastrointestinal tract in mice , 2012, International journal of nanomedicine.

[71] C. Lehr,et al. Nano- and microparticulate drug carriers for targeting of the inflamed intestinal mucosa. , 2012, Journal of controlled release : official journal of the Controlled Release Society.

[72] Y. van Kooyk,et al. Sweet preferences of MGL: carbohydrate specificity and function. , 2008, Trends in immunology.

[73] P. Savelkoul,et al. The Bacterial Flora in Inflammatory Bowel Disease: Current Insights in Pathogenesis and the Influence of Antibiotics and Probiotics , 2001, Scandinavian journal of gastroenterology. Supplement.

[74] S. Hua. Targeting sites of inflammation: intercellular adhesion molecule-1 as a target for novel inflammatory therapies , 2013, Front. Pharmacol..

[75] R. Fisher,et al. Measurement of Gastrointestinal Transit , 2005, Digestive Diseases and Sciences.

[76] C. Chou,et al. Effect of atropine on digested food-induced intestinal hyperemia. , 1985, The American journal of physiology.

[77] R Balfour Sartor,et al. Microbial influences in inflammatory bowel diseases. , 2008, Gastroenterology.

[78] P. Stahl,et al. Identification of the macrophage mannose receptor as a 175-kDa membrane protein. , 1986, Proceedings of the National Academy of Sciences of the United States of America.

[79] M. Sans,et al. VCAM-1 and ICAM-1 mediate leukocyte-endothelial cell adhesion in rat experimental colitis. , 1999, Gastroenterology.

[80] R. P. Thompson,et al. Basement membrane components , 2003, Journal of clinical pathology.

[81] T. Denning,et al. Targeting intestinal inflammation with CD98 siRNA/PEI-loaded nanoparticles. , 2014, Molecular therapy : the journal of the American Society of Gene Therapy.

[82] Edsel A. Peña,et al. American ginseng suppresses inflammation and DNA damage associated with mouse colitis , 2008, Carcinogenesis.

[83] M. Neurath,et al. Budesonide loaded nanoparticles with pH-sensitive coating for improved mucosal targeting in mouse models of inflammatory bowel diseases. , 2014, Journal of controlled release : official journal of the Controlled Release Society.

[84] G. Dalmasso,et al. Drug-loaded nanoparticles targeted to the colon with polysaccharide hydrogel reduce colitis in a mouse model. , 2010, Gastroenterology.

[85] Jane M. Young,et al. Patient Preferences Between Surgical and Medical Treatment in Crohn’s Disease , 2007, Diseases of the colon and rectum.

[86] Claus-Michael Lehr,et al. PEG-functionalized microparticles selectively target inflamed mucosa in inflammatory bowel disease. , 2013, European journal of pharmaceutics and biopharmaceutics : official journal of Arbeitsgemeinschaft fur Pharmazeutische Verfahrenstechnik e.V.

[87] Gang Lu,et al. A γ-Tocopherol–Rich Mixture of Tocopherols Inhibits Colon Inflammation and Carcinogenesis in Azoxymethane and Dextran Sulfate Sodium–Treated Mice , 2009, Cancer Prevention Research.

[88] Henry C. Lin,et al. Ileal brake: Neuropeptidergic control of intestinal transit , 2006, Current gastroenterology reports.

[89] S. Hua. Orally administered liposomal formulations for colon targeted drug delivery , 2014, Front. Pharmacol..

[90] G. Holmes,et al. Acid microclimate in coeliac and Crohn's disease: a model for folate malabsorption. , 1978, Gut.

[91] Alf Lamprecht,et al. The targeting of surface modified silica nanoparticles to inflamed tissue in experimental colitis. , 2008, Biomaterials.

[92] G. Radford-Smith,et al. Hypoxia and Integrin-Mediated Epithelial Restitution during Mucosal Inflammation , 2013, Front. Immunol..

[93] F. Barkas,et al. Electrolyte and acid-base disorders in inflammatory bowel disease , 2013, Annals of gastroenterology.

[94] J. Turner,et al. Myosin light chain kinase: pulling the strings of epithelial tight junction function , 2012, Annals of the New York Academy of Sciences.

[95] Linshu Liu,et al. Interaction of various pectin formulations with porcine colonic tissues. , 2005, Biomaterials.

[96] Y. Barenholz,et al. Differential Adhesion of Normal and Inflamed Rat Colonic Mucosa by Charged Liposomes , 2004, Pharmaceutical Research.

[97] D. Drossman,et al. Small intestinal bacterial overgrowth in irritable bowel syndrome: association with colon motility, bowel symptoms, and psychological distress , 2008, Neurogastroenterology and motility : the official journal of the European Gastrointestinal Motility Society.

[98] C. Bernstein,et al. Beta 2-integrin/intercellular adhesion molecule (ICAM) expression in the normal human intestine. , 1996, Clinical and Experimental Immunology.

[99] C. Kriegel,et al. Dual TNF-α/Cyclin D1 Gene Silencing With an Oral Polymeric Microparticle System as a Novel Strategy for the Treatment of Inflammatory Bowel Disease , 2011, Clinical and Translational Gastroenterology.

[100] S. Kshirsagar,et al. Preparation and characterization of nanocapsules for colon-targeted drug delivery system , 2012, Pharmaceutical development and technology.

[101] A. Nusrat,et al. Role of the intestinal barrier in inflammatory bowel disease. , 2008, World journal of gastroenterology.

[102] Clive G. Wilson,et al. The transit rate of different-sized model dosage forms through the human colon and the effects of a lactulose-induced catharsis , 1992 .

[103] S. Nuding,et al. Intestinal barrier in inflammatory bowel disease. , 2014, World journal of gastroenterology.

[104] T. Denning,et al. Fab'-bearing siRNA TNFα-loaded nanoparticles targeted to colonic macrophages offer an effective therapy for experimental colitis. , 2014, Journal of controlled release : official journal of the Controlled Release Society.

[105] Michael C. Montalto,et al. Hypoxia-inducible factor-1-dependent regulation of the multidrug resistance (MDR1) gene. , 2002, Cancer research.

[106] R. H. Bridson,et al. Encapsulation of Liposomes within pH Responsive Microspheres for Oral Colonic Drug Delivery , 2012, International journal of biomaterials.

[107] B. McCormick,et al. Mucosal Inflammatory Response to Salmonella typhimurium Infection , 2014, Front. Immunol..

[108] I. Wilding,et al. The use of pharmacoscintigraphy to focus the development strategy for a novel 5-ASA colon targeting system (TIME CLOCK® system) , 1997 .

[109] Hebden,et al. Limited exposure of the healthy distal colon to orally‐dosed formulation is further exaggerated in active left‐sided ulcerative colitis , 2000, Alimentary Pharmacology and Therapeutics.

[110] Libo Yang,et al. Colon-specific drug delivery: new approaches and in vitro/in vivo evaluation. , 2002, International journal of pharmaceutics.

[111] D. Attwood,et al. An in vivo investigation into the suitability of pH dependent polymers for colonic targeting , 1993 .

[112] P. Moayyedi,et al. An Evidence-Based Systematic Review on Medical Therapies for Inflammatory Bowel Disease , 2011, The American Journal of Gastroenterology.

[113] A. Pfeiffer,et al. Effect of intestinal resection on human small bowel motility. , 1996, Gut.

[114] N. Shibata,et al. Application of a Biomagnetic Measurement System (BMS) to the Evaluation of Gastrointestinal Transit of Intestinal Pressure-Controlled Colon Delivery Capsules (PCDCs) in Human Subjects , 2000, Pharmaceutical Research.

[115] D. Rampton,et al. Chemiluminescence assay of mucosal reactive oxygen metabolites in inflammatory bowel disease. , 1992, Gastroenterology.

[116] L. Ursell,et al. Complex interactions among diet, gastrointestinal transit, and gut microbiota in humanized mice. , 2013, Gastroenterology.

[117] Yen Cu,et al. Controlled surface modification with poly(ethylene)glycol enhances diffusion of PLGA nanoparticles in human cervical mucus. , 2009, Molecular pharmaceutics.

[118] S. Rana,et al. Small Intestinal Bacterial Overgrowth and Orocecal Transit Time in Patients of Inflammatory Bowel Disease , 2013, Digestive Diseases and Sciences.

[119] A. Lamprecht,et al. Nanoparticle-based clodronate delivery mitigates murine experimental colitis. , 2012, Journal of controlled release : official journal of the Controlled Release Society.

[120] D. Merlin,et al. Nanoparticles with surface antibody against CD98 and carrying CD98 small interfering RNA reduce colitis in mice. , 2014, Gastroenterology.

[121] R. H. Bridson,et al. Evaluation of liposomes coated with a pH responsive polymer. , 2010, International journal of pharmaceutics.

[122] S. Mura,et al. Improving Oral Bioavailability and Pharmacokinetics of Liposomal Metformin by Glycerolphosphate–Chitosan Microcomplexation , 2013, AAPS PharmSciTech.

[123] Y. Kawashima,et al. Mucoadhesive properties of carbopol or chitosan-coated liposomes and their effectiveness in the oral administration of calcitonin to rats. , 2003, Journal of controlled release : official journal of the Controlled Release Society.

[124] R M Albrecht,et al. Gastrointestinal persorption and tissue distribution of differently sized colloidal gold nanoparticles. , 2001, Journal of pharmaceutical sciences.

[125] V. Préat,et al. pH-sensitive nanoparticles for colonic delivery of curcumin in inflammatory bowel disease. , 2014, International journal of pharmaceutics.

[126] H. Takeuchi,et al. Improved intestinal absorption of calcitonin by mucoadhesive delivery of novel pectin-liposome nanocomplexes. , 2008, Journal of controlled release : official journal of the Controlled Release Society.

[127] David J Brayden,et al. Drug delivery to inflamed colon by nanoparticles: comparison of different strategies. , 2013, International journal of pharmaceutics.

[128] S. Gupta,et al. Effect of dosing time on the total intestinal transit time of non-disintegrating systems. , 2000, International journal of pharmaceutics.

[129] Y. Barenholz,et al. Transferrin as a luminal target for negatively charged liposomes in the inflamed colonic mucosa. , 2009, Molecular pharmaceutics.

[130] Shubiao Zhang,et al. Cationic lipids and polymers mediated vectors for delivery of siRNA. , 2007, Journal of controlled release : official journal of the Controlled Release Society.

[131] G. Leitinger,et al. Chemical coupling of thiolated chitosan to preformed liposomes improves mucoadhesive properties , 2012, International journal of nanomedicine.

[132] L. A. Christensen,et al. Very low intraluminal colonic pH in patients with active ulcerative colitis , 1993, Digestive Diseases and Sciences.

[133] V. Sinha,et al. Polysaccharides in colon-specific drug delivery. , 2001, International journal of pharmaceutics.

[134] R. Spiller,et al. Further characterisation of the 'ileal brake' reflex in man--effect of ileal infusion of partial digests of fat, protein, and starch on jejunal motility and release of neurotensin, enteroglucagon, and peptide YY. , 1988, Gut.

[135] G. Mullin,et al. Increased oxidative stress and decreased antioxidant defenses in mucosa of inflammatory bowel disease , 1996, Digestive Diseases and Sciences.

[136] Y. Kawashima,et al. A pH-sensitive microsphere system for the colon delivery of tacrolimus containing nanoparticles. , 2005, Journal of controlled release : official journal of the Controlled Release Society.

[137] J. Harris,et al. Activated fluid transport regulates bacterial-epithelial interactions and significantly shifts the murine colonic microbiome , 2012, Gut microbes.

[138] G. Wu,et al. Diet and the intestinal microbiome: associations, functions, and implications for health and disease. , 2014, Gastroenterology.

[139] N. Ziats,et al. Enhanced leukocyte binding by intestinal microvascular endothelial cells in inflammatory bowel disease. , 1997, Gastroenterology.

[140] Didier Merlin,et al. Orally delivered thioketal nanoparticles loaded with TNF-α-siRNA target inflammation and inhibit gene expression in the intestines. , 2010, Nature materials.

[141] Hyun-Jae Shin,et al. Improved oral bioavailability of alendronate via the mucoadhesive liposomal delivery system. , 2012, European journal of pharmaceutical sciences : official journal of the European Federation for Pharmaceutical Sciences.

[142] K. Gradauer,et al. Liposomes coated with thiolated chitosan enhance oral peptide delivery to rats , 2013, Journal of controlled release : official journal of the Controlled Release Society.

[143] Y. Kawashima,et al. Nanoparticles Enhance Therapeutic Efficiency by Selectively Increased Local Drug Dose in Experimental Colitis in Rats , 2005, Journal of Pharmacology and Experimental Therapeutics.

[144] D. Fatouros,et al. In vitro lipid digestion models in design of drug delivery systems for enhancing oral bioavailability , 2008, Expert opinion on drug metabolism & toxicology.

[145] R. Müller,et al. Lipid Nanoparticles with a Solid Matrix (SLN®, NLC®, LDC®) for Oral Drug Delivery , 2008, Drug development and industrial pharmacy.

[146] Bo Xiao,et al. Glycoprotein CD98 as a receptor for colitis-targeted delivery of nanoparticle. , 2014, Journal of materials chemistry. B.

[147] D. Merlin,et al. Activation of epithelial CD98 glycoprotein perpetuates colonic inflammation , 2005, Laboratory Investigation.

[148] A. Munakata,et al. Improved localizing method of radiopill in measurement of entire gastrointestinal pH profiles: colonic luminal pH in normal subjects and patients with Crohn's disease. , 1997, The American journal of gastroenterology.

[149] Y. Raab,et al. A new method for the quantification of neutrophil and eosinophil cationic proteins in feces: establishment of normal levels and clinical application in patients with inflammatory bowel disease , 2002, American Journal of Gastroenterology.