Your search keyword '"de Graaf IA"' showing total 43 results

1. Paraquat Exposure of Knapsack Spray Operators on Banana Plantations in Costa Rica

Author

S.B. Kromhout, B Wesseling, [No Value] De Graaf Ia, [No Value] Van Wendel de Joode Bn, and Inge de Graaf

Subjects

Paraquat, Air sampling, integumentary system, business.industry, Herbicides, Knapsack spray operators, Public Health, Environmental and Occupational Health, Systemic absorption, Respiratory exposure, Luchtkwaliteit, Dermal exposure, Air Quality, Toxicology, chemistry.chemical_compound, Biological monitoring, chemistry, Medicine, Occupational exposure, Urine sample, business, Working environment

Abstract

A study of occupational exposure to paraquat was performed among 11 knapsack spray operators at banana plantations in Costa Rica. External and internal exposures were quantified and determinants of exposure identified by measurements, observations, and interviews. Dermal exposure was measured with skin pads, respiratory exposure by personal air sampling, and internal exposure by urine sampling. The wrists, back, and legs were the areas with the highest levels of dermal exposure. Respiratory exposures appeared to be strongly influenced by differences between days, while dermal exposures varied mostly due to differences between plantations. The use of protective clothing did not effectively protect against dermal exposures. Both respiratory and dermal exposures were significantly related to internal exposures, and both should be considered possible routes for systemic absorption of paraquat. It cannot be excluded that measurable levels of exposure can lead to acute as well as chronic health effects. Furthermore, due to poor conditions within the working environment, the spray operators are continuously at risk for high exposures that could lead to severe intoxication, and therefore a strategy for control of exposure is necessary.

Published

1996

2. The consequence of regional gradients of P-gp and CYP3A4 for drug-drug interactions by P-gp inhibitors and the P-gp/CYP3A4 interplay in the human intestine ex vivo.

Author

Li M, de Graaf IA, van de Steeg E, de Jager MH, and Groothuis GM

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Adult, Aged, Aged, 80 and over, Cyclosporins pharmacology, Cytochrome P-450 CYP3A Inhibitors pharmacology, Drug Interactions, Female, Humans, In Vitro Techniques, Isoquinolines pharmacology, Ketoconazole pharmacology, Male, Middle Aged, Quinazolines pharmacology, Quinidine analogs & derivatives, Quinidine metabolism, Quinidine pharmacokinetics, Verapamil pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Colon metabolism, Cytochrome P-450 CYP3A metabolism, Ileum metabolism, Jejunum metabolism

Abstract

Intestinal P-gp and CYP3A4 work coordinately to reduce the intracellular concentration of drugs, and drug-drug interactions (DDIs) based on this interplay are of clinical importance and require pre-clinical investigation. Using precision-cut intestinal slices (PCIS) of human jejunum, ileum and colon, we investigated the P-gp/CYP3A4 interplay and related DDIs with P-gp inhibitors at the different regions of the human intestine with quinidine (Qi), dual substrate of P-gp and CYP3A4, as probe. All the P-gp inhibitors increased the intracellular concentrations of Qi by 2.1-2.6 fold in jejunum, 2.6-3.8 fold in ileum but only 1.2-1.3 fold in colon, in line with the different P-gp expression in these intestinal regions. The selective P-gp inhibitors (CP100356 and PSC833) enhanced 3-hydroxy-quinidine (3OH-Qi) in jejunum and ileum, while dual inhibitors of P-gp and CYP3A4 (verapamil and ketoconazole) decreased the 3OH-Qi production, despite of the increased intracellular Qi concentration, due to inhibition of CYP3A4. The outcome of DDIs based on P-gp/CYP3A4 interplay, shown as remarkable changes in the intracellular concentration of both the parent drug and the metabolite, varied among the intestinal regions, probably due to the different expression of P-gp and CYP3A4, and were different from those found in rat PCIS, which may have important implications for the disposition and toxicity of drugs and their metabolites., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

3. P-gp activity and inhibition in the different regions of human intestine ex vivo.

Author

Li M, de Graaf IA, de Jager MH, and Groothuis GM

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Adult, Aged, Biological Transport, Dose-Response Relationship, Drug, Duodenum drug effects, Duodenum metabolism, Female, Fluorescent Dyes metabolism, Humans, Ileum drug effects, Ileum metabolism, In Vitro Techniques, Jejunum drug effects, Jejunum metabolism, Kinetics, Male, Middle Aged, Rhodamine 123 metabolism, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Colon drug effects, Colon metabolism, Intestine, Small drug effects, Intestine, Small metabolism, Membrane Transport Modulators pharmacology

Abstract

Although intestinal P-glycoprotein (P-gp) has been extensively studied in vitro and in animals, its activity and the consequences of P-gp inhibition for drug disposition and toxicity in humans are still difficult to accurately extrapolate from these studies. Moreover, existing in vitro models do not take into consideration that the intestine is heterogeneous with respect to P-gp expression. Recently, we reported rat precision-cut intestinal slices (PCIS) as a physiological ex vivo model to study the regional gradient of P-gp activity and inhibition. Here we extended the application of PCIS to the human intestine. For this purpose rhodamine 123 (R123) accumulation in the presence or absence of the P-gp inhibitors verapamil, cyclosporine A, quinidine, ketoconazole, PSC833 and CP100356 was measured in PCIS of human duodenum, jejunum, ileum and colon. R123 accumulation in the presence of the P-gp inhibitors appeared to be most enhanced in the ileum compared to the other regions. Moreover, the regional differences in accumulation are in line with published differences in abundance of P-gp. The rank order of the potency of the P-gp inhibitors, reflected by their IC 50 , was comparable to that in rat PCIS. However, the increase in accumulation of the P-gp substrate R123 by the inhibitors was larger in human ileum PCIS than in rat PCIS, indicating species difference in P-gp abundance. These data show that human PCIS are an appropriate ex vivo model to study the activity of intestinal P-gp and predict the inhibitory effect of drugs and of transporter-mediated drug-drug interactions in the human intestine. Copyright © 2016 John Wiley & Sons, Ltd., (Copyright © 2016 John Wiley & Sons, Ltd.)

Published

2017

4. An integrative view of cisplatin-induced renal and cardiac toxicities: Molecular mechanisms, current treatment challenges and potential protective measures.

Author

Dugbartey GJ, Peppone LJ, and de Graaf IA

Subjects

Animals, DNA Damage drug effects, Heart Diseases metabolism, Heart Diseases pathology, Heart Diseases prevention & control, Humans, Kidney Diseases metabolism, Kidney Diseases pathology, Kidney Diseases prevention & control, Antineoplastic Agents toxicity, Cardiotoxicity pathology, Cardiotoxicity prevention & control, Cisplatin toxicity, Heart Diseases chemically induced, Kidney Diseases chemically induced

Abstract

Cisplatin is currently one of the most widely-used chemotherapeutic agents against various malignancies. Its clinical application is limited, however, by inherent renal and cardiac toxicities and other side effects, of which the underlying mechanisms are only partly understood. Experimental studies show cisplatin generates reactive oxygen species, which impair the cell's antioxidant defense system, causing oxidative stress and potentiating injury, thereby culminating in kidney and heart failure. Understanding the molecular mechanisms of cisplatin-induced renal and cardiac toxicities may allow clinicians to prevent or treat this problem better and may also provide a model for investigating drug-induced organ toxicity in general. This review discusses some of the major molecular mechanisms of cisplatin-induced renal and cardiac toxicities including disruption of ionic homeostasis and energy status of the cell leading to cell injury and cell death. We highlight clinical manifestations of both toxicities as well as (novel)biomarkers such as kidney injury molecule-1 (KIM-1), tissue inhibitor of metalloproteinase-1 (TIMP-1) and N-terminal pro-B-type natriuretic peptide (NT-proBNP). We also present some current treatment challenges and propose potential protective strategies including combination therapy with novel pharmacological compounds that might mitigate or prevent these toxicities, which include the use of hydrogen sulfide., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

5. Intracellular RIG-I Signaling Regulates TLR4-Independent Endothelial Inflammatory Responses to Endotoxin.

Author

Moser J, Heeringa P, Jongman RM, Zwiers PJ, Niemarkt AE, Yan R, de Graaf IA, Li R, Ravasz Regan E, Kümpers P, Aird WC, van Nieuw Amerongen GP, Zijlstra JG, Molema G, and van Meurs M

Subjects

Animals, Endothelial Cells pathology, Inflammation pathology, Mice, Mice, 129 Strain, Mice, Inbred C57BL, DEAD Box Protein 58 metabolism, Endothelial Cells immunology, Inflammation immunology, Lipopolysaccharides immunology, Signal Transduction, Toll-Like Receptor 4 immunology

Abstract

Sepsis is a systemic inflammatory response to infections associated with organ failure that is the most frequent cause of death in hospitalized patients. Exaggerated endothelial activation, altered blood flow, vascular leakage, and other disturbances synergistically contribute to sepsis-induced organ failure. The underlying signaling events associated with endothelial proinflammatory activation are not well understood, yet they likely consist of molecular pathways that act in an endothelium-specific manner. We found that LPS, a critical factor in the pathogenesis of sepsis, is internalized by endothelial cells, leading to intracellular signaling without the need for priming as found recently in immune cells. By identifying a novel role for retinoic acid-inducible gene-I (RIG-I) as a central regulator of endothelial activation functioning independent of TLR4, we provide evidence that the current paradigm of TLR4 solely being responsible for LPS-mediated endothelial responses is incomplete. RIG-I, as well as the adaptor protein mitochondrial antiviral signaling protein, regulates NF-κB-mediated induction of adhesion molecules and proinflammatory cytokine expression in response to LPS. Our findings provide essential new insights into the proinflammatory signaling pathways in endothelial cells and suggest that combined endothelial-specific inhibition of RIG-I and TLR4 will provide protection from aberrant endothelial responses associated with sepsis., (Copyright © 2016 by The American Association of Immunologists, Inc.)

Published

2016

6. The Consequence of Drug-Drug Interactions Influencing the Interplay between P-Glycoprotein and Cytochrome P450 3a: An Ex Vivo Study with Rat Precision-Cut Intestinal Slices.

Author

Li M, de Graaf IA, Siissalo S, de Jager MH, van Dam A, and Groothuis GM

Subjects

Animals, Cyclosporins metabolism, Intestinal Absorption, Ketoconazole metabolism, Male, Quinidine metabolism, Rats, Rats, Wistar, Valine metabolism, Verapamil metabolism, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Cytochrome P-450 CYP3A metabolism, Drug Interactions physiology, Ileum metabolism, Jejunum metabolism, Pharmaceutical Preparations metabolism

Abstract

P-glycoprotein (P-gp) and cytochrome P450 3A (CYP3A) are differentially expressed along the intestine and work coordinately to reduce the intracellular concentration of xenobiotics and the absorption of orally taken drugs. Drug-drug interactions (DDIs) based on P-gp/CYP3A interplay are of clinical importance and require preclinical investigation. We investigated the P-gp/Cyp3a interplay and related DDIs with different P-gp inhibitors in the various regions of the rat intestine ex vivo using precision-cut intestinal slices (PCIS) with quinidine (Qi), a dual substrate of P-gp and Cyp3a, as the probe. The results showed that P-gp efflux was the main factor limiting the intracellular Qi content at concentrations below 5µM, whereas both efflux and metabolism were saturated at [Qi] > 50µM. The selective P-gp inhibitors CP100356 [N-(3,4-dimethoxyphenethyl)-4-(6,7-dimethoxy-3,4-dihydroisoquinolin-2[1H]-yl)-6,7-dimethoxyquinazolin-2-amine] and PSC833 [valspodar, 6-[(2S,4R,6E)-4-methyl-2-(methylamino)-3-oxo-6-octenoic acid]-7-l-valine-cyclosporin A] enhanced the Qi accumulation in slices in line with the different P-gp expression in the intestinal regions and, as a result, also enhanced metabolism in the jejunum and ileum. Dual inhibitors of both P-gp and Cyp3a (verapamil and ketoconazole) increased the concentration of Qi in the jejunum and ileum, but less 3-hydroxy-quinidine was produced due to inhibition of Cyp3a. The results indicate that the P-gp/Cyp3a interplay depends on the concentration of the drug and on the intestinal region under study. Furthermore, due to the P-gp/Cyp3a interplay, DDIs can lead to remarkable changes in the intracellular concentration of both the parent drug and the metabolite, which varies among the intestinal regions and depends on the selectivity of the inhibitors, with potentially important implications for disposition and toxicity of drugs and their metabolites., (Copyright © 2016 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2016

7. Precision-cut intestinal slices: alternative model for drug transport, metabolism, and toxicology research.

Author

Li M, de Graaf IA, and Groothuis GM

Subjects

Animals, Biological Transport, Cryopreservation methods, Humans, Reproducibility of Results, Toxicology methods, Translational Research, Biomedical methods, Xenobiotics adverse effects, Xenobiotics pharmacokinetics, Intestinal Mucosa metabolism, Models, Biological, Pharmaceutical Preparations metabolism

Abstract

Introduction: The absorption, distribution, metabolism, excretion and toxicity (ADME-tox) processes of drugs are of importance and require preclinical investigation intestine in addition to the liver. Various models have been developed for prediction of ADME-tox in the intestine. In this review, precision-cut intestinal slices (PCIS) are discussed and highlighted as model for ADME-tox studies., Areas Covered: This review provides an overview of the applications and an update of the most recent research on PCIS as an ex vivo model to study the transport, metabolism and toxicology of drugs and other xenobiotics. The unique features of PCIS and the differences with other models as well as the translational aspects are also discussed., Expert Opinion: PCIS are a simple, fast, and reliable ex vivo model for drug ADME-tox research. Therefore, PCIS are expected to become an indispensable link in the in vitro-ex vivo-in vivo extrapolation, and a bridge in translation of animal data to the human situation. In the future, this model may be helpful to study the effects of interorgan interactions, intestinal bacteria, excipients and drug formulations on the ADME-tox properties of drugs. The optimization of culture medium and the development of a (cryo)preservation technique require more research.

Published

2016

8. Adjusting the DNA Interaction and Anticancer Activity of Pt(II) N-Heterocyclic Carbene Complexes by Steric Shielding of the Trans Leaving Group.

Author

Muenzner JK, Rehm T, Biersack B, Casini A, de Graaf IA, Worawutputtapong P, Noor A, Kempe R, Brabec V, Kasparkova J, and Schobert R

Subjects

Cell Line, Tumor, Heterocyclic Compounds chemistry, Heterocyclic Compounds pharmacology, Humans, Methane chemistry, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, DNA drug effects, Methane analogs & derivatives, Platinum Compounds chemistry, Platinum Compounds pharmacology

Abstract

Five platinum(II) complexes bearing a (1,3-dibenzyl)imidazol-2-ylidene ligand but different leaving groups trans to it were examined for cytotoxicity, DNA and cell cycle interference, vascular disrupting properties, and nephrotoxicity. The cytotoxicity of complexes 3a-c increased with the steric shielding of their leaving chloride ligand, and complex 3c, featuring two triphenylphosphanes, was the most efficacious, with submicromolar IC50 concentrations. Complexes 3a-c interacted with DNA in electrophoretic mobility shift and ethidium bromide binding assays. The cationic complex 3c did not bind coordinatively to DNA but led to its aggregation, damage that is not amenable to the usual repair mechanisms. Accordingly, it arrested the cell cycle of melanoma cells in G1 phase, whereas cis-dichlorido[(1,3-dibenzyl)imidazol-2-ylidene](dimethyl sulfoxide) platinum(II) 3a induced G2/M phase arrest. Complex 3c also disrupted the blood vessels in the chorioallantoic membrane of fertilized chicken eggs. Ex vivo studies using precision-cut tissue slices suggested the nephrotoxicities of 3a-c to be clinically manageable.

Published

2015

9. Rat precision-cut intestinal slices to study P-gp activity and the potency of its inhibitors ex vivo.

Author

Li M, de Graaf IA, de Jager MH, and Groothuis GM

Subjects

Animals, Cyclosporine pharmacology, Cyclosporins pharmacology, In Vitro Techniques, Isoquinolines pharmacology, Ketoconazole pharmacology, Male, Quinazolines pharmacology, Quinidine pharmacology, Rats, Wistar, Rhodamine 123 metabolism, Verapamil pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Intestinal Mucosa metabolism

Abstract

Rat Precision-Cut Intestinal Slices (PCIS) were evaluated as ex vivo model to study the regional gradient of P-gp activity, and to investigate whether the rank order of inhibitory potency of P-gp inhibitors can be correctly reproduced in this model with more accurate IC50 values than with current in vitro models. PCIS were prepared from small intestine (duodenum, jejunum, ileum) and colon. Rhodamine 123 (R123) was used as P-gp substrate, while verapamil, cyclosporine A, quinidine, ketoconazole, PSC833 and CP100356 were employed as P-gp inhibitors. Increase in tissue accumulation of R123 in the presence of the inhibitors was considered as an indication of the inhibitory effect. The P-gp inhibitors increased the tissue accumulation of R123 in a concentration dependent manner. Fluorescence microscopy elucidated that this increase occurred predominantly in the enterocytes. The rank order of the corresponding IC50 values agreed well with reported values from cell lines expressing rat P-gp. The activity of and inhibitory effects on P-gp were significantly higher in ileum compared to the other regions. These data suggest that rat PCIS are a reliable ex vivo model to study the activity of intestinal P-gp and the inhibitory effect of drugs. PCIS have potential as ex vivo model for the prediction of transporter-mediated drug-drug interactions., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

10. Precision-cut rat, mouse, and human intestinal slices as novel models for the early-onset of intestinal fibrosis.

Author

Pham BT, van Haaften WT, Oosterhuis D, Nieken J, de Graaf IA, and Olinga P

Abstract

Intestinal fibrosis (IF) is a major complication of inflammatory bowel disease. IF research is limited by the lack of relevant in vitro and in vivo models. We evaluated precision-cut intestinal slices (PCIS) prepared from human, rat, and mouse intestine as ex vivo models mimicking the early-onset of (human) IF. Precision-cut intestinal slices prepared from human (h), rat (r), and mouse (m) jejunum, were incubated up to 72 h, the viability of PCIS was assessed by ATP content and morphology, and the gene expression of several fibrosis markers was determined. The viability of rPCIS decreased after 24 h of incubation, whereas mPCIS and hPCIS were viable up to 72 h of culturing. Furthermore, during this period, gene expression of heat shock protein 47 and plasminogen activator inhibitor 1 increased in all PCIS in addition to augmented expression of synaptophysin in hPCIS, fibronectin (Fn2) and TGF-β1 in rPCIS, and Fn2 and connective tissue growth factor (Ctgf) in mPCIS. Addition of TGF-β1 to rPCIS or mPCIS induced the gene expression of the fibrosis markers Pro-collagen1a1, Fn2, and Ctgf in both species. However, none of the fibrosis markers was further elevated in hPCIS. We successfully developed a novel ex vivo model that can mimic the early-onset of fibrosis in the intestine using human, rat, and mouse PCIS. Furthermore, in rat and mouse PCIS, TGF-β1 was able to even further increase the gene expression of fibrosis markers. This indicates that PCIS can be used as a model for the early-onset of IF., (© 2015 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of the American Physiological Society and The Physiological Society.)

Published

2015

11. Improved synthesis of N-benzylaminoferrocene-based prodrugs and evaluation of their toxicity and antileukemic activity.

Author

Daum S, Chekhun VF, Todor IN, Lukianova NY, Shvets YV, Sellner L, Putzker K, Lewis J, Zenz T, de Graaf IA, Groothuis GM, Casini A, Zozulia O, Hampel F, and Mokhir A

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents toxicity, Carbamates chemical synthesis, Carbamates chemistry, Cell Proliferation drug effects, Cell Survival drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Ferrous Compounds chemical synthesis, Ferrous Compounds chemistry, HL-60 Cells, Humans, In Vitro Techniques, Injections, Intraperitoneal, Liver drug effects, Male, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Models, Molecular, Molecular Structure, Prodrugs chemical synthesis, Prodrugs chemistry, Rats, Rats, Wistar, Structure-Activity Relationship, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Carbamates pharmacology, Carbamates toxicity, Ferrous Compounds pharmacology, Ferrous Compounds toxicity, Leukemia drug therapy, Prodrugs pharmacology, Prodrugs toxicity

Abstract

We report on an improved method of synthesis of N-benzylaminoferrocene-based prodrugs and demonstrate its applicability by preparing nine new aminoferrocenes. Their effect on the viability of selected cancer cells having different p53 status was studied. The obtained data are in agreement with the hypothesis that the toxicity of aminoferrocenes is not dependent upon p53 status. Subsequently the toxicity of a selected prodrug (4) was investigated ex vivo using rat precision cut liver slices and in vivo on hybrid male mice BDF1. In both experiments no toxicity was observed: ex vivo, up to 10 μM; in vivo, up to 6 mg/kg. Finally, prodrug 4 was shown to extend the survival of BDF1 mice carrying L1210 leukemia from 13.7 ± 0.6 days to 17.5 ± 0.7 days when injected daily 6 times at a dose of 26 μg/kg starting from the second day after injection of L1210 cells.

Published

2015

12. Consequences of Mrp2 deficiency for diclofenac toxicity in the rat intestine ex vivo.

Author

Niu X, de Graaf IA, van de Vegte D, Langelaar-Makkinje M, Sekine S, and Groothuis GM

Subjects

ATP Binding Cassette Transporter, Subfamily G, Member 2, ATP-Binding Cassette Transporters biosynthesis, Adenosine Triphosphate analysis, Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Diclofenac pharmacokinetics, Gene Expression drug effects, Intestinal Absorption drug effects, Intestines chemistry, Liver chemistry, Liver drug effects, Male, Rats, Tissue Culture Techniques, ATP-Binding Cassette Transporters deficiency, Anti-Inflammatory Agents, Non-Steroidal toxicity, Diclofenac toxicity, Intestines drug effects

Abstract

The non-steroidal anti-inflammatory drug diclofenac (DCF) has a high prevalence of intestinal side effects in humans and rats. It has been reported that Mrp2 transporter deficient rats (Mrp2) are more resistant to DCF induced intestinal toxicity. This was explained in vivo by impaired Mrp2-dependent biliary transport of DCF-acylglucuronide (DAG), leading to decreased intestinal exposure to DAG and DCF. However, it is not known to what extent adaptive changes in the Mrp2 intestine itself influence its sensitivity to DCF toxicity without the influence of liver metabolites. To investigate this, DCF toxicity and disposition were studied ex vivo by precision-cut intestinal slices and Ussing chamber using intestines from wild type(WT) and Mrp2 rats. The results show that adaptive changes due to Mrp2 deficiency concerning Mrp2, Mrp3 and BCRP gene expression, GSH content and DAG formation were different between liver and intestine. Furthermore, Mrp2 intestine was intrinsically more resistant to DCF toxicity than its WT counterpart ex vivo. This can at least partly be explained by a reduced DCF uptake by the Mrp2 intestine, but isnot related to the other adaptive changes in the intestine. The extrapolation of this data to humans with MRP2 deficiency is uncertain due to species differences in activity and regulation of transporters.

Published

2015

13. Diclofenac toxicity in human intestine ex vivo is not related to the formation of intestinal metabolites.

Author

Niu X, de Graaf IA, Langelaar-Makkinje M, Horvatovich P, and Groothuis GM

Subjects

Adenosine Triphosphate metabolism, Adult, Aged, Anti-Inflammatory Agents, Non-Steroidal metabolism, Caspase 3 metabolism, Diclofenac metabolism, Diclofenac toxicity, Female, Glucuronides metabolism, Humans, Immunohistochemistry, In Vitro Techniques, Jejunum pathology, L-Lactate Dehydrogenase metabolism, Male, Middle Aged, Anti-Inflammatory Agents, Non-Steroidal toxicity, Diclofenac analogs & derivatives, Glucuronides toxicity, Jejunum drug effects, Jejunum metabolism

Abstract

The use of diclofenac (DCF), a nonsteroidal anti-inflammatory drug, is associated with a high prevalence of gastrointestinal side effects. In vivo studies in rodents suggested that reactive metabolites of DCF produced by the liver or the intestine might be responsible for this toxicity. In the present study, precision-cut intestinal slices (PCIS) prepared from the jejunum of 18 human donors were used as an ex vivo model to investigate whether DCF intestinal metabolites are responsible for its intestinal toxicity in man. PCIS were incubated with a concentration range of DCF (0-600 µM) up to 24 h. DCF (≥400 µM) caused direct toxicity to the intestine as demonstrated by ATP depletion, morphological damage, caspase 3 activation, and lactate dehydrogenase leakage. Three main metabolites produced by PCIS (4'-hydroxy DCF, 5-hydroxy DCF, and DCF acyl glucuronide) were detected by HPLC. Protein adducts were detected by immunohistochemical staining and showed correlation with the intestinal metabolites. DCF induced similar toxicity to each of the samples regardless of the variation in metabolism among them. Less metabolites were produced by slices incubated with 400 µM DCF than with 100 µM DCF. The addition of the metabolic inhibitors such as ketoconazole, cimetidine, or borneol decreased the metabolite formation but increased the toxicity. The results suggest that DCF can induce intestinal toxicity in human PCIS directly at therapeutically relevant concentrations, independent of the reactive metabolites 4'-OH DCF, 5-OH DCF, or diclofenac acylglucuronide produced by the liver or formed in the intestine.

Published

2015

14. Precision cut intestinal slices are an appropriate ex vivo model to study NSAID-induced intestinal toxicity in rats.

Author

Niu X, de Graaf IA, van der Bij HA, and Groothuis GM

Subjects

Adenosine Triphosphate metabolism, Animals, Aspirin toxicity, Caspase 9 metabolism, Cell Survival drug effects, Diclofenac toxicity, Diflunisal toxicity, Endoplasmic Reticulum Stress, Gene Expression drug effects, Glutathione metabolism, Heat-Shock Proteins genetics, Heme Oxygenase (Decyclizing) genetics, Indomethacin toxicity, Jejunum metabolism, Jejunum pathology, Male, Naproxen toxicity, Rats, Wistar, Tissue Culture Techniques, Anti-Inflammatory Agents, Non-Steroidal toxicity, Jejunum drug effects

Abstract

Non-steroidal anti-inflammatory drugs (NSAIDs) are widely used therapeutic agents, however, they are associated with a high prevalence of intestinal side effects. In this investigation, rat precision cut intestinal slices (PCIS) were evaluated as an ex vivo model to study NSAID-induced intestinal toxicity. Firstly, PCIS were incubated with 0-200 μM diclofenac (DCF), one of the most intensively studied NSAIDs, to investigate whether they could correctly reflect the toxic mechanisms. DCF induced intestinal toxicity in PCIS was shown by morphological damage and ATP depletion. DCF induced endoplasmic-reticulum (ER) stress, mitochondrial injury and oxidative stress were reflected by up-regulated HSP-70 (heat shock protein 70) and BiP (binding immunoglobulin protein) gene expression, caspase 9 activation, GSH (glutathione) depletion and HO-1 (heme oxygenase 1) gene up-regulation respectively. Furthermore, DCF intestinal metabolites, which gave rise to protein adduct but not toxicity, were detected in PCIS. Secondly, PCIS were incubated with various concentrations of five NSAIDs. Typical NSAID-induced morphological changes were observed in PCIS. The ex vivo toxicity ranking (diflunisal> diclofenac = indomethacin > naproxen ≫ aspirin) showed good correlation with published in vitro and in vivo data, with diflunisal being the only exception. In conclusion, PCIS correctly reflect the various mechanisms of DCF-induced intestinal toxicity, and can serve as an ex vivo model for the prediction of NSAID-induced intestinal toxicity., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

15. Nanoparticle formulation of a poorly soluble cannabinoid receptor 1 antagonist improves absorption by rat and human intestine.

Author

Siissalo S, de Waard H, de Jager MH, Hayeshi R, Frijlink HW, Hinrichs WL, Dinter-Heidorn H, van Dam A, Proost JH, Groothuis GM, and de Graaf IA

Subjects

Animals, Brain metabolism, Cannabinoid Receptor Antagonists chemistry, Cannabinoid Receptor Antagonists pharmacokinetics, Chemistry, Pharmaceutical, Humans, Male, Rats, Rats, Wistar, Solubility, Cannabinoid Receptor Antagonists administration & dosage, Intestinal Absorption, Nanoparticles administration & dosage, Receptor, Cannabinoid, CB1 antagonists & inhibitors

Abstract

The inclusion of nanoparticles dispersed in a hydrophilic matrix is one of the formulation strategies to improve the bioavailability of orally administered Biopharmaceutics Classification System (BCS) class II and IV drugs by increasing their dissolution rate in the intestine. To confirm that the increased dissolution rate results in increased bioavailability, in vitro and in vivo animal experiments are performed, however, translation to the human situation is hazardous. In this study, we used a range of in vitro and ex vivo methods, including methods applying human tissue, to predict the in vivo oral bioavailability of a model BCS class II CB-1 antagonist, formulated as a nanoparticle solid dispersion. The enhanced dissolution rate from the nanoparticle formulation resulted in an increased metabolite formation in both rat and human precision-cut intestinal slices, suggesting increased uptake and intracellular drug concentration in the enterocytes. In Ussing chamber experiments with human tissue, both the metabolite formation and apical efflux of the metabolite were increased for the nanoparticulate solid dispersion compared with a physical mixture, in line with the results in intestinal slices. The pharmacokinetics of the different formulations was studied in rats in vivo. The nanoparticle formulation indeed improved the absorption of the cannabinoid receptor 1 (CB-1) antagonist and the delivery into the brain compared with the physical mixture. In conclusion, the combined approach provides a valuable set of tools to investigate the effects of formulation on the absorption of poorly soluble compounds in human intestine and may provide relevant information on the oral bioavailability in humans early in the development process.

Published

2013

16. Analysis of gene expression changes to elucidate the mechanism of chilling injury in precision-cut liver slices.

Author

Guan N, Blomsma SA, Fahy GM, Groothuis GM, and de Graaf IA

Subjects

Adenosine Triphosphate metabolism, Animals, Cell Survival drug effects, Gene Expression Profiling, In Vitro Techniques, Male, Oligonucleotide Array Sequence Analysis, Organ Preservation, RNA genetics, Rats, Rats, Wistar, Cold Temperature adverse effects, Cryoprotective Agents adverse effects, Liver injuries, Liver metabolism

Abstract

The exact mechanism of chilling injury (by a decrease of temperature to sub-physiological values), especially in the intact organ, is yet unknown. Precision-cut liver slices (PCLS), which closely resemble the organ from which they are derived, are an ideal in vitro model to study the mechanism of chilling injury in the intact organ. In the present study we were able to separate chilling injury from other damaging events such as cryoprotectant toxicity and ice-crystal injury and performed micro-array analysis of regulated genes. Pathway analysis revealed that different stress responses, lipid/fatty acid and cholesterol biosynthesis and metabolism were affected by chilling. This indicates that the cell-membrane might be the primary site and sensor for chilling, which may initiate and amplify downstream intracellular signaling events. Most importantly, we were able to identify gene expression responses from stellate cells and Kupffer cells suggesting the involvement of all liver cell types in the injury. In conclusion, a broad spectrum of previously unknown gene expression changes induced by chilling was identified in the tissue. This is the first report of a systematic investigation on the mechanism of chilling injury in integrated tissue by micro-array analysis under conditions in which other sources of injury are minimal., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

17. Evaluation of the intestinal toxicity and transport of xenobiotics utilizing precision-cut slices.

Author

Niu X, de Graaf IA, and Groothuis GM

Subjects

Animals, Biological Transport drug effects, Drug Evaluation, Preclinical methods, Humans, Intestines pathology, Microdissection methods, Organ Culture Techniques methods, Carrier Proteins metabolism, Gene Expression Regulation, Enzymologic drug effects, Intestinal Mucosa metabolism, Models, Biological, Xenobiotics adverse effects, Xenobiotics pharmacokinetics, Xenobiotics pharmacology

Abstract

1.The precision-cut intestinal slice (PCIS) technology is a relatively new addition to the battery of in vitro assays for evaluation of xenobiotic toxicity, metabolism, and transport. 2.The intestine is an important target for drug-induced toxicity due to its high exposure after oral administration. Therefore, the prediction of drug-induced intestinal side effects remains a significant safety issue in pharmaceutical development. Although animal experiments have been proven useful, species differences and the requirement for reduction of animal use warrant the development of in vitro methods which can apply human tissue. 3.The enterocytes lining the villi express high activities of enzymes and transporters involved in drug disposition. They vary highly in activities: along the length of the intestine and along the villi, gradients of expression levels of the enzymes and proteins exist, which necessitates an in vitro model that can reflect the different regions of the intestine. 4.In this chapter, the application of PCIS in studies on transport and toxicity of xenobiotics is reviewed. PCIS can be prepared from each region of the intestine and from various species in a similar manner, and the results published so far indicate that they represent a promising model to evaluate intestinal toxicity and transport.

Published

2013

18. Precision-cut intestinal slices as in vitro tool for studies on drug metabolism.

Author

Groothuis GM and de Graaf IA

Subjects

Animal Testing Alternatives, Animals, Biological Transport, Drug Interactions, Humans, Organ Culture Techniques, Time Factors, Intestinal Mucosa metabolism, Models, Biological, Pharmaceutical Preparations metabolism

Abstract

The role of the intestine in drug metabolism has long been underestimated as a consequence of the technical difficulty to discern the role of the intestine from that of the liver in in vivo experiments and of the lack of in vitro models that are sufficiently viable and fully representing the physiology and anatomy of the intestine. Recently the precision-cut slice model, which is widely used for liver and kidney, was also adapted for the small and large intestine. In this review the application of precision-cut intestinal slices (PCIS) for research in drug metabolism and transport is discussed. PCIS can be prepared from animal and human tissues from all regions of the intestine allowing investigation of species differences and regional gradients of activities of metabolizing enzymes. They are viable for 8-24 h of incubation and show high activity of drug metabolizing enzymes, representative for the in vivo activity. They have been successfully used to study drug-drug interactions such as induction, inhibition and regulation of drug metabolizing enzymes, transporters and nuclear factors. Moreover they appear to be a suitable model for studies on cold preservation of donor organs for transplantation, and allow exploring inter-organ interactions by co-incubation with precision-cut slices of other organs. Their application as model for drug-induced intestinal toxicity is still in its infancy but appears to be promising. PCIS, prepared from human and animal tissues, represent a powerful translational model for drug metabolism, transport and toxicity studies and as such contributes to the reduction and replacement of animal experiments.

Published

2013

19. Cryopreservation of precision-cut tissue slices.

Author

Fahy GM, Guan N, de Graaf IA, Tan Y, Griffin L, and Groothuis GM

Subjects

Animals, Drug Evaluation, Preclinical methods, Humans, Rats, Cryopreservation methods, Freezing, Liver

Abstract

1.Cryopreservation of precision-cut tissue slices (PCTS) would have many advantages for drug development and would encourage more extensive use of the PCTS preparation. 2.Three methods have been studied to date: slow freezing, fast freezing, and vitrification. 3.Slow freezing can be very effective for some PCTS but is devastating to rat liver PCTS. Fast freezing can be successful for rat liver PCTS but is devastating to renal PCTS and has given inconsistent results even for rat liver PCTS. Vitrification has been effective for some slice systems but less effective for rat liver PCTS. Rat liver PCTS appear to be particularly difficult to cryopreserve well. 4.The general cryobiological principles of slow freezing, rapid freezing, and vitrification are reviewed. The empirical literature on the cryopreservation of PCTS has not taken sufficient account of these principles, and may, for example, include the effects of easily preventable osmotic injury. 5.More attention is needed to the effects of cryopreservation on specific cell types within PCTS and to the general integrity and viability of cryopreserved PCTS. Drug metabolism as a sole endpoint of study can be highly misleading. 6.Better application of cryobiological principles may enable improved results in the future.

Published

2013

20. Effects of cryoprotectant addition and washout methods on the viability of precision-cut liver slices.

Author

Guan N, Blomsma SA, van Midwoud PM, Fahy GM, Groothuis GM, and de Graaf IA

Subjects

Adenosine Triphosphate metabolism, Animals, Equipment Design, Liver ultrastructure, Male, Organ Preservation methods, Osmosis, Osmotic Pressure, Permeability, Rats, Rats, Wistar, Vitrification, Cryoprotective Agents metabolism, Liver metabolism, Organ Preservation instrumentation, Organ Preservation Solutions metabolism

Abstract

Successful vitrification of organ slices is hampered by both osmotic stress and chemical toxicity of cryoprotective agents (CPAs). In the present study, we focused on the effect of osmotic stress on the viability of precision-cut liver slices (PCLS) by comparing different CPA solutions and different methods of loading and unloading the slices with the CPAs. For this purpose, we developed a gradient method to load and unload CPAs with the intention of minimizing sudden changes in osmolarity and thereby avoiding osmotic stress in the slices in comparison with the commonly used step-wise loading/unloading approach. With this gradient method, the CPA solution was introduced at a constant rate into a specially designed mixing chamber containing the slices. We showed that immediate mixing of the infused CPA and the chamber constituents occurred, which enabled us to control the CPA concentration to which PCLS were exposed as a function of time. With this method, CPA concentration versus time profiles were varied using various commercially available CPA mixtures [VMP, VM3, M22, and modified M22 (mM22)]. The viability of PCLS was determined after CPA loading and unloading and subsequent incubation during 3h at 37°C. Despite the reduction of osmotic stress, the viability of slices did not improve with gradual loading and unloading and remained considerably lower than that of untreated slices. The toxicity of the three CPA solutions did not correlate with either their potential osmotic effects or their total concentrations, and did not change strongly with exposure time in 100% CPA. The most likely explanation for these observations is that PCLS are not very sensitive to osmotic changes of the magnitude imposed in our study, and chemical toxicity of the CPA solutions is the main barrier to be overcome. The chemical toxicity of the CPAs used in this study probably originates from a source other than the total concentration of the solutions. The presented gradient method using the specially designed chamber is more time and cost effective than the step-wise method and can be universally applied to efficiently evaluate different CPA solutions., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

21. Bilitranslocase is involved in the uptake of bromosulfophthalein in rat and human liver.

Author

Terdoslavich M, de Graaf IA, Proost JH, Cocolo A, Passamonti S, and Groothuis GM

Subjects

Animals, Antibodies immunology, Biological Transport, Ceruloplasmin, Humans, Male, Rats, Rats, Wistar, Species Specificity, Taurocholic Acid metabolism, Temperature, Liver metabolism, Membrane Proteins metabolism, Sulfobromophthalein pharmacokinetics

Abstract

Hepatic disposition of bromosulfophthalein (BSP), bilirubin and bile salts partially overlap, as these anions share both uptake and excretion mechanisms. Multiple organic anion transporters mediate hepatic BSP uptake, i.e. members of the SLCO and SLC22 gene families and bilitranslocase (TCDB #2.A.65.1.1). This study aimed at evaluating the relative contribution of bilitranslocase in BSP uptake in precision-cut human and rat liver slices. To this purpose, two different anti-sequence bilitranslocase antibodies were used as specific, functional inhibitors of bilitranslocase. The intact liver physiology was accurately reproduced in this BSP uptake assay, since uptake was strongly temperature-dependentand inhibited by hepatotropic organic anions, such as 50 nM bilirubin, 1 μM nicotinic acid, 2 μM digoxin, 5 μMindocyanine green and 100 μM taurocholate. The bilitranslocase antibodies inhibited BSP uptake both in rat and human liver slices. The combined use of bilitranslocase antibodies and taurocholate caused additive-type inhibition, confirming that bilitranslocase is not a bile salt transporter; by contrast, bilirubin caused no additive-type inhibition. In conclusion this data, indicate the role of the bilirubin transporter bilitranslocase as one of the transporters involved in the uptake of anions like BSP in parallel with other organic anion carriers. Moreover this data indicate the value of precision-cut liver slices for phenotypic drug uptake studies.

Published

2012

22. Transport of the coumarin metabolite 7-hydroxycoumarin glucuronide is mediated via multidrug resistance-associated proteins 3 and 4.

Author

Wittgen HG, van den Heuvel JJ, van den Broek PH, Siissalo S, Groothuis GM, de Graaf IA, Koenderink JB, and Russel FG

Subjects

Biological Transport, Active physiology, HEK293 Cells, Humans, Coumarins metabolism, Multidrug Resistance-Associated Proteins physiology, Umbelliferones metabolism

Abstract

Coumarin (1,2-benzopyrone) is a natural compound that has been used as a fragrance in the food and perfume industry and could have therapeutic usefulness in the treatment of lymphedema and different types of cancer. Several previous pharmacokinetic studies of coumarin have been performed in humans, which revealed extensive first-pass metabolism of the compound. 7-Hydroxycoumarin (7-HC) and its glucuronide (7-HC-G) are the main metabolites formed in humans, and via this route, 80 to 90% of the absorbed coumarin is excreted into urine, mainly as 7-HC-G. Active transport processes play a role in the urinary excretion of 7-HC-G; however, until now, the transporters involved remained to be elucidated. In this study, we investigated whether the efflux transporters multidrug resistance-associated proteins (MRP)1-4, breast cancer resistance protein, or P-glycoprotein play a role in 7-HC and 7-HC-G transport. For this purpose, we measured uptake of the metabolites into membrane vesicles overexpressing these transporters. Our results showed that 7-HC is not transported by any of the efflux transporters tested, whereas 7-HC-G was a substrate of MRP3 and MRP4. These results are in line with the pharmacokinetic profile of coumarin and suggest that MRP3 and MRP4 are the main transporters involved in the excretion of the coumarin metabolite 7-HC-G from liver and kidney.

Published

2012

23. On-line HPLC analysis system for metabolism and inhibition studies in precision-cut liver slices.

Author

van Midwoud PM, Janssen J, Merema MT, de Graaf IA, Groothuis GM, and Verpoorte E

Subjects

Animals, Diclofenac metabolism, Eosine I Bluish pharmacology, In Vitro Techniques, Inactivation, Metabolic, Liver cytology, Male, Microtomy, Rats, Rats, Wistar, Umbelliferones metabolism, Chromatography, High Pressure Liquid methods, Liver drug effects, Liver metabolism, Online Systems, Pharmaceutical Preparations metabolism

Abstract

A novel approach for on-line monitoring of drug metabolism in continuously perifused, precision-cut liver slices (PCLS) in a microfluidic system has been developed using high-performance liquid chromatography with UV detection (HPLC-UV). In this approach, PCLS are incubated in a microfluidic device made of poly(dimethylsiloxane) (PDMS) by continuous, single-pass perifusion with fresh medium. Two syringe pumps are incorporated into the system to infuse substrates or inhibitors at varying concentrations into the perfusion medium just before the chip entrance. The medium containing the metabolites produced by the PCLS is directed toward an injection loop. Once filled, the content of this injection loop is automatically injected onto an HPLC for analysis. The on-line analysis of metabolites was tested by using the substrate, 7-hydroxycoumarin (7-HC). Rapid switching between substrate and solvent control was possible, and a direct metabolic response of the liver slice to perifusion with substrate was detected. Very stable phase II metabolism over a period of 24 h was observed. The inhibitory effect of phloxine B on the formation of 7-hydroxycoumarin glucuronide (phase II product of 7-HC) was also investigated. Phloxine B was injected into the incubation medium in increasing concentrations varying from 0 to 200 μM. The results showed a concentration-dependent inhibition of 7-HC glucuronide formation and allowed the calculation of an IC50 value (concentration in which 50% of the enzyme is inhibited) of ∼85 μM using one single liver slice. On-line detection was also shown to be advantageous for the detection of unstable metabolites. This was demonstrated by determination of the metabolites of the drug diclofenac. The reactive metabolite, acyl glucuronide, was detected at relatively high concentrations which remained very constant over a period of 4 h. In contrast, only low and decreasing amounts of diclofenac acyl glucuronide could be measured in the conventional well-plate incubation system. The advantages of this novel on-line analysis system for PCLS include the capability to obtain direct information about tissue function, assess the concentration dependence of drug-drug interactions in one single slice, and detect unstable metabolites. The system also enables fast analysis without the need to store samples, thus eliminating the associated freeze-thaw problems, and allows the simultaneous analysis of multiple metabolites.

Published

2011

24. Reduced ischemia-reoxygenation injury in rat intestine after luminal preservation with a tailored solution.

Author

Roskott AM, Nieuwenhuijs VB, Leuvenink HG, Dijkstra G, Ottens P, de Jager MH, Gonalves Dias Pereira P, Fidler V, Groothuis GM, Ploeg RJ, and de Graaf IA

Subjects

Adenosine, Allopurinol, Animals, Cell Survival, Gene Expression Regulation, Glutathione, Ice, Insulin, Intestinal Mucosa cytology, Intestinal Mucosa pathology, Intestines cytology, Intestines pathology, Microvilli pathology, Microvilli physiology, Organ Preservation Solutions, RNA, Messenger genetics, RNA, Messenger isolation & purification, Raffinose, Rats, Intestines physiopathology, Ischemia prevention & control, Organ Preservation methods

Abstract

Background: The intestine is extremely sensitive to ischemic preservation and reoxygenation injury. Current vascular perfusion and cold storage with University of Wisconsin (UW) solution neglect the intestinal lumen and the ongoing mucosal metabolism during hypothermia. This study was designed to test the effects of luminal preservation with an alternative preservation solution in addition to the common vascular flush with UW solution on graft viability after preservation and ex vivo reoxygenation., Methods: Rat intestine was preserved on ice for 6 hr in UW solution or Williams Medium E with additional buffering, impermeants, and a colloid (WMEplus) after being stapled or after flushing and filling the lumen with the respective preservation solution. Tissue slices were prepared from fresh and preserved intestines and were incubated with oxygen for 6 hr at 37°C to assess the viability after reoxygenation., Results: Directly after preservation, histologic damage was mild and unaffected by preservation strategy. Contrary to luminal preservation, closed preservation resulted in significantly decreased ATP levels compared with control. Reoxygenation aggravated damage and revealed differences between the strategies. Luminal preservation better maintained the ATP levels and histologic integrity (vs. closed preservation) for both solutions. Histomorphologic integrity was superior after preservation with WMEplus (vs. UW solution). Expression of stress responsive genes was least up-regulated in the slices from tissue preserved luminally with WMEplus., Conclusions: In conclusion, preservation and reoxygenation injury can be attenuated by luminal preservation with WMEplus.

Published

2010

25. Preparation and incubation of precision-cut liver and intestinal slices for application in drug metabolism and toxicity studies.

Author

de Graaf IA, Olinga P, de Jager MH, Merema MT, de Kanter R, van de Kerkhof EG, and Groothuis GM

Subjects

Adenosine Triphosphate metabolism, Animals, Humans, Intestinal Mucosa metabolism, Intestines drug effects, Intestines pathology, Liver drug effects, Liver pathology, Microtomy instrumentation, Rats, Xenobiotics toxicity, Liver metabolism, Microtomy methods, Tissue Culture Techniques instrumentation, Xenobiotics metabolism

Abstract

Precision-cut tissue slices (PCTS) are viable ex vivo explants of tissue with a reproducible, well defined thickness. They represent a mini-model of the organ under study and contain all cells of the tissue in their natural environment, leaving intercellular and cell-matrix interactions intact, and are therefore highly appropriate for studying multicellular processes. PCTS are mainly used to study the metabolism and toxicity of xenobiotics, but they are suitable for many other purposes. Here we describe the protocols to prepare and incubate rat and human liver and intestinal slices. Slices are prepared from fresh liver by making a cylindrical core using a drill with a hollow bit, from which slices are cut with a specially designed tissue slicer. Intestinal tissue is embedded in cylinders of agarose before slicing. Slices remain viable for 24 h (intestine) and up to 96 h (liver) when incubated in 6- or 12-well plates under 95% O(2)/5% CO(2) atmosphere.

Published

2010

26. Targeted transfection increases siRNA uptake and gene silencing of primary endothelial cells in vitro--a quantitative study.

Author

Asgeirsdóttir SA, Talman EG, de Graaf IA, Kamps JA, Satchell SC, Mathieson PW, Ruiters MH, and Molema G

Subjects

Aged, Antibodies, Monoclonal metabolism, Binding Sites, Biological Transport, Cadherins immunology, Cell Culture Techniques, Cells, Cultured, Endothelial Cells immunology, Humans, Inflammation immunology, Kidney immunology, Male, Middle Aged, Particle Size, Pyridinium Compounds metabolism, Tissue Culture Techniques, Antigens, CD genetics, Cadherins genetics, Endothelial Cells metabolism, Inflammation metabolism, Kidney metabolism, RNA Interference, RNA, Small Interfering metabolism, Transfection

Abstract

Applications of small-interfering RNA (siRNA) call for specific and efficient delivery of siRNA into particular cell types. We developed a novel, non-viral targeting system to deliver siRNA specifically into inflammation-activated endothelial cells. This was achieved by conjugating the cationic amphiphilic lipid SAINT to antibodies recognizing the inflammatory cell adhesion molecule E-selectin. These anti-E-selectin-SAINT lipoplexes (SAINTarg) maintained antigen recognition capacity of the parental antibody in vitro, and ex vivo in human kidney tissue slices subjected to inflammatory conditions. Regular SAINT mediated transfection resulted in efficient gene silencing in human microvascular endothelial cells (HMEC-1) and conditionally immortalized glomerular endothelial cells (ciGEnC). However, primary human umbilical vein endothelial cells (HUVEC) transfected poorly, a phenomenon that we could quantitatively correlate with a cell-type specific capacity to facilitate siRNA uptake. Importantly, SAINTarg increased siRNA uptake and transfection specificity for activated endothelial cells. Transfection with SAINTarg delivered significantly more siRNA into activated HUVEC, compared to transfection with non-targeted SAINT. The enhanced uptake of siRNA was corroborated by improved silencing of both gene- and protein expression of VE-cadherin in activated HUVEC, indicating that SAINTarg delivered functionally active siRNA into endothelial cells. The obtained results demonstrate a successful design of a small nucleotide carrier system with improved and specific siRNA delivery into otherwise difficult-to-transfect primary endothelial cells, which in addition reduced considerably the amount of siRNA needed for gene silencing., (Copyright 2009 Elsevier B.V. All rights reserved.)

Published

2010

27. Shock-induced stress induces loss of microvascular endothelial Tie2 in the kidney which is not associated with reduced glomerular barrier function.

Author

van Meurs M, Kurniati NF, Wulfert FM, Asgeirsdottir SA, de Graaf IA, Satchell SC, Mathieson PW, Jongman RM, Kümpers P, Zijlstra JG, Heeringa P, and Molema G

Subjects

Aged, Albuminuria metabolism, Albuminuria physiopathology, Animals, Cell Line, Disease Models, Animal, Down-Regulation, Endothelium, Vascular physiopathology, Humans, In Vitro Techniques, Kidney blood supply, Kidney physiopathology, Lipopolysaccharides, Male, Mice, Mice, Inbred C57BL, Microvessels metabolism, Middle Aged, Neutrophils metabolism, RNA, Messenger metabolism, Receptor Protein-Tyrosine Kinases genetics, Receptor, TIE-2 genetics, Shock, Hemorrhagic physiopathology, Shock, Septic chemically induced, Shock, Septic physiopathology, Time Factors, Tumor Necrosis Factor-alpha metabolism, Capillary Permeability, Endothelium, Vascular metabolism, Glomerular Filtration Rate, Kidney metabolism, Receptor Protein-Tyrosine Kinases metabolism, Receptor, TIE-2 metabolism, Shock, Hemorrhagic metabolism, Shock, Septic metabolism

Abstract

Both hemorrhagic shock and endotoxemia induce a pronounced vascular activation in the kidney which coincides with albuminuria and glomerular barrier dysfunction. We hypothesized that changes in Tie2, a vascular restricted receptor tyrosine kinase shown to control microvascular integrity and endothelial inflammation, underlie this loss of glomerular barrier function. In healthy murine and human kidney, Tie2 is heterogeneously expressed in all microvascular beds, although to different extents. In mice subjected to hemorrhagic and septic shock, Tie2 mRNA and protein were rapidly, and temporarily, lost from the renal microvasculature, and normalized within 24 h after initiation of the shock insult. The loss of Tie2 protein could not be attributed to shedding as both in mice and healthy volunteers subjected to endotoxemia, sTie2 levels in the systemic circulation did not change. In an attempt to identify the molecular control of Tie2, we activated glomerular endothelial cell cultures and human kidney slices in vitro with LPS or TNF-alpha, but did not observe a change in Tie2 mRNA levels. In parallel to the loss of Tie2 in vivo, an overt influx of neutrophils in the glomerular compartment, which coincided with proteinuria, was seen. As neutrophil-endothelial cell interactions may play a role in endothelial adaptation to shock, and these effects cannot be mimicked in vitro, we depleted neutrophils before shock induction. While this neutrophil depletion abolished proteinuria, Tie2 was not rescued, implying that Tie2 may not be a major factor controlling maintenance of the glomerular filtration barrier in this model.

Published

2009

28. Induction of metabolism and transport in human intestine: validation of precision-cut slices as a tool to study induction of drug metabolism in human intestine in vitro.

Author

van de Kerkhof EG, de Graaf IA, Ungell AL, and Groothuis GM

Subjects

Adenosine Triphosphate metabolism, Colon enzymology, Cytochrome P-450 CYP1A1 biosynthesis, Cytochrome P-450 CYP1A1 genetics, Cytochrome P-450 CYP3A biosynthesis, Cytochrome P-450 CYP3A genetics, Humans, In Vitro Techniques, Jejunum enzymology, Microtomy methods, RNA, Messenger biosynthesis, RNA, Messenger genetics, Reproducibility of Results, Colon metabolism, Jejunum metabolism, Pharmaceutical Preparations metabolism

Abstract

Induction of drug enzyme activity in the intestine can strongly determine plasma levels of drugs. It is therefore important to predict drug-drug interactions in human intestine in vitro. We evaluated the applicability of human intestinal precision-cut slices for induction studies in vitro. Morphological examination and intracellular ATP levels indicated tissue integrity up to 24 h of incubation, whereas in proximal jejunum slices, the metabolic rate toward most substrates remained at 40 to 50% of initial values. In colon slices, the cytochrome P450 conversions were below the detection limit, but conjugation rates remained relatively constant during incubation. The inducibility of drug-metabolizing enzymes and P-glycoprotein was evaluated using prototypical inducers for five induction pathways. beta-Naphthoflavone (aryl hydrocarbon receptor ligand) induced CYP1A1 (132-fold in colon and 362-fold in proximal jejunum) and UDP glucuronosyltransferase (UGT) 1A6 mRNA (9.8-fold in colon and 3.2-fold in proximal jejunum). In proximal jejunum, rifampicin (RIF) [pregnane X receptor (PXR) ligand] induced CYP3A4 (5.2-fold), CYP2B6 (2-fold), UGT1A6 (2.2-fold), and multidrug resistance-1 (MDR1)/ABCB1 mRNA (2.7-fold), whereas 6beta-hydroxytestosterone formation (CYP3A4) increased 2-fold. In colon, RIF induced UGT1A6 32-fold and MDR1 2.2-fold. Dexamethasone (glucocorticoid receptor and PXR ligand) induced CYP3A4 mRNA (3.5-fold) and activity (5-fold) in proximal jejunum. Phenobarbital (constitutive androstane receptor activator) induced CYP3A4 (4.1-fold, only in jejunum), CYP2B6 (4.9-fold in colon and 2.3-fold in proximal jejunum), and MDR1/ABCB1 mRNA and CYP3A4 activity (2-fold only proximal jejunum). Quercetin (nuclear factor-E2-related factor 2 activator) induced UGT1A6 mRNA (6.7-fold in colon and 2.2-fold in proximal jejunum). In conclusion, this study shows that human intestinal precision-cut slices are useful to study induction of drug-metabolizing enzymes and transporters in the human intestine.

Published

2008

29. In vitro methods to study intestinal drug metabolism.

Author

van de Kerkhof EG, de Graaf IA, and Groothuis GM

Subjects

Animals, Biological Availability, Drug Interactions, Enzymes metabolism, Humans, Intestinal Mucosa metabolism, Pharmaceutical Preparations metabolism, Species Specificity, Biotransformation, Drug Evaluation, Preclinical methods, Models, Biological

Abstract

Although the liver has long been thought to play the major role in drug metabolism, also the metabolic capacity of the intestine is more and more recognized. In vivo studies eventually pointed out not only the significance of first-pass metabolism by the intestinal wall for the bioavailability of several compounds, but also the relevance of transporters in this process. Only a few methods are available to study drug metabolism in vivo or in situ and with most of these methods it remains difficult to discriminate between the contribution of liver and extrahepatic tissues. To study intestinal drug metabolism in vitro, apart from subcellular fractions, several intact cell systems are nowadays available. This review discusses the available intestinal in vitro methods to study drug metabolism. The advantages and limitations of intact cell systems (isolated intestinal perfusion, everted sac, Ussing chamber preparations, biopsies, precision-cut slices, primary cells), subcellular fractions (S9 fractions, microsomes) and intestinal cell lines (caco-2, LS180 cells amongst others) are discussed. Their applicability to different species and to study phase I and II metabolism/transport and drug-drug interactions are summarized. Furthermore, causes of variation within and between methods are discussed and metabolic rates obtained with different methods are compared. Whereas subcellular fractions and cell lines are efficient methods to study mechanistic aspects of drug metabolism at the enzyme level, the isolated intestinal perfusion, everted sac and Ussing chamber appear particularly useful for studying drug metabolism of rapidly metabolised drugs and interactions with transporters. Biopsies, precision-cut slices and primary cells seem all appropriate to study induction and metabolism of slowly metabolised drugs.

Published

2007

30. Induction of phase I and II drug metabolism in rat small intestine and colon in vitro.

Author

van de Kerkhof EG, de Graaf IA, de Jager MH, and Groothuis GM

Subjects

Adenosine Triphosphate metabolism, Alkaline Phosphatase metabolism, Animals, Coumarins metabolism, Glyceraldehyde 3-Phosphate Dehydrogenase (NADP+) genetics, In Vitro Techniques, Male, Metabolic Detoxication, Phase I, Metabolic Detoxication, Phase II, Microfilament Proteins genetics, Pharmacokinetics, RNA, Messenger metabolism, Rats, Rats, Wistar, Testosterone metabolism, Umbelliferones metabolism, Colon metabolism, Intestine, Small metabolism

Abstract

The aim of this study was to evaluate drug metabolism in rat small intestinal and colon precision-cut slices during 24 h of incubation and the applicability of these slices for enzyme induction studies. Various parameters were evaluated: intracellular levels of ATP (general viability marker), alkaline phosphatase activity (specific epithelial marker), villin expression (specific epithelial marker), and metabolic rates of 7-ethoxycoumarin (CYP1A), testosterone (CYP3A and CYP2B), and 7-hydroxycoumarin (glucuronide and sulfate conjugation) conversions. ATP and villin remained constant up to, respectively, 5 and 8 h in small intestine and up to 24 h in colon. The metabolic rate remained constant in small intestinal slices up to 8 h and decreased afterward to 24 to 92%, depending on the substrate studied. The inducibility of metabolism in small intestinal and colon slices was tested with several inducers at various concentrations and incubation times. The following inducers were used: 3-methylcholanthrene, beta-naphthoflavone, indirubin, and tert-butylhydroquinone (aryl hydrocarbon receptor ligands), dexamethasone (glucocorticoid receptor/pregnane X receptor ligand) and phenobarbital (constitutive androstane receptor ligand). After incubation with inducers, metabolic rates were evaluated with 7-ethoxycoumarin and testosterone (phase I) and 7-hydroxycoumarin (phase II) as substrate. All inducers elevated the metabolic rates consistent with the available published in vivo induction data. Induction of enzyme activity was already detectable after 5 h (small intestine) and after 8 h (colon) for 3-methylcholanthrene and beta-naphthoflavone and was clearly detectable for all tested inducers after 24 h (up to 20-fold compared with noninduced controls). In conclusion, small intestinal and colon precision-cut slices are useful for metabolism and enzyme induction studies.

Published

2007

31. Cryopreservation of rat precision-cut liver and kidney slices by rapid freezing and vitrification.

Author

de Graaf IA, Draaisma AL, Schoeman O, Fahy GM, Groothuis GM, and Koster HJ

Subjects

Adenosine Triphosphate metabolism, Animals, Cryoprotective Agents pharmacology, Freezing, Rats, Rats, Wistar, Temperature, Cryopreservation methods, Kidney anatomy & histology, Liver anatomy & histology

Abstract

Precision-cut tissue slices of both hepatic and extra-hepatic origin are extensively used as an in vitro model to predict in vivo drug metabolism and toxicity. Cryopreservation would greatly facilitate their use. In the present study, we aimed to improve (1) rapid freezing and warming (200 degrees C/min) using 18% Me(2)SO as cryoprotectant and (2) vitrification with high molarity mixtures of cryoprotectants, VM3 and VS4, as methods to cryopreserve precision-cut rat liver and kidney slices. Viability after cryopreservation and subsequent 3-4h of incubation at 37 degrees C was determined by measuring ATP content and by microscopical evaluation of histological integrity. Confirming earlier studies, viability of rat liver slices was maintained at high levels by rapid freezing and thawing with 18% Me(2)SO. However, vitrification of liver slices with VS4 resulted in cryopreservation damage despite the fact that cryoprotectant toxicity was low, no ice was formed during cooling and devitrification was prevented. Viability of liver slices was not improved by using VM3 for vitrification. Kidney slices were found not to survive cryopreservation by rapid freezing. In contrast, viability of renal medullary slices was almost completely maintained after vitrification with VS4, however vitrification of renal cortex slices with VS4 was not successful, partly due to cryoprotectant toxicity. Both kidney cortex and medullary slices were vitrified successfully with VM3 (maintaining viability at 50-80% of fresh slice levels), using an optimised pre-incubation protocol and cooling and warming rates that prevented both visible ice-formation and cracking of the formed glass. In conclusion, vitrification is a promising approach to cryopreserve precision-cut (kidney) slices.

Published

2007

32. Innovative methods to study human intestinal drug metabolism in vitro: precision-cut slices compared with ussing chamber preparations.

Author

van de Kerkhof EG, Ungell AL, Sjöberg AK, de Jager MH, Hilgendorf C, de Graaf IA, and Groothuis GM

Subjects

Adenosine Triphosphate analysis, Colon enzymology, Cytochrome P-450 Enzyme System metabolism, Diffusion Chambers, Culture, Humans, Intestine, Small enzymology, Metabolic Detoxication, Phase I, Metabolic Detoxication, Phase II, Organ Culture Techniques, Substrate Specificity, Tissue Distribution, Colon metabolism, Intestine, Small metabolism, Pharmaceutical Preparations metabolism

Abstract

Predictive in vitro methods to investigate drug metabolism in the human intestine using intact tissue are of high importance. Therefore, we studied the metabolic activity of human small intestinal and colon slices and compared it with the metabolic activity of the same human intestinal segments using the Ussing chamber technique. The metabolic activity was evaluated using substrates to both phase I and phase II reactions: testosterone, 7-hydroxycoumarin (7HC), and a mixture of cytochrome P450 (P450) substrates (midazolam, diclofenac, coumarin, and bufuralol). In slices of human proximal jejunum, the metabolic activity of several P450-mediated and conjugation reactions remained constant up to4hof incubation. In the colon slices, conjugation rates were virtually equal to those in small intestine, whereas P450-mediated conversions occurred much slower. In both organs, morphological evaluation and ATP content implied tissue integrity within this period. P450 conversions using the Ussing chamber technique showed that the metabolic rate (sum of metabolites measured in apical, basolateral, and tissue compartments) was constant up to 3 h. For 7HC conjugations, the metabolic rate remained constant up to 4 h. The distribution of the metabolites in the compartments differed between the substrates. Overall, metabolic rates were surprisingly similar in both techniques and appear similar to or even higher than in liver. In conclusion, this study shows that both human intestinal precision-cut slices and Ussing chamber preparations provide useful tools for in vitro biotransformation studies.

Published

2006

33. Empirical validation of a rat in vitro organ slice model as a tool for in vivo clearance prediction.

Author

de Graaf IA, de Kanter R, de Jager MH, Camacho R, Langenkamp E, van de Kerkhof EG, and Groothuis GM

Subjects

Animals, Drug Evaluation, Preclinical, Intestinal Mucosa metabolism, Kidney metabolism, Kinetics, Liver metabolism, Male, Protein Binding, Rats, Rats, Sprague-Dawley, Rats, Wistar, Reproducibility of Results, Tissue Culture Techniques, Coumarins metabolism, Serum Albumin, Bovine metabolism, Testosterone metabolism, Umbelliferones metabolism

Abstract

Tissue slices have been shown to be a valuable tool to predict metabolism of novel drugs. However, besides the numerous advantages of their use for this purpose, some potential drawbacks also exist, including reported poor penetration of drugs into the inner cell layers of slices and loss of metabolic capacity during prolonged incubation, leading to underprediction of metabolic clearance. In the present study, we empirically identified (and quantified) sources of underprediction using rat tissue slices of lung, intestine, kidney, and liver and found that thin liver slices (+/-100 mum) metabolized model substrates (7-hydroxycoumarin, testosterone, warfarin, 7-ethoxycoumarin, midazolam, haloperidol, and quinidine) as rapidly as isolated hepatocytes. Furthermore, it was found that organ slices remain metabolically active for sufficient periods of incubation, enabling study of the kinetics of low clearance compounds. In addition, we determined the influence of albumin on the clearance prediction of six model substrates. For three of these substrates, the intrinsic clearance in the presence of albumin was approximately 3 times higher than that obtained from incubations without albumin, but corrected for unbound fraction. This resulted in a much more accurate prediction of in vivo whole body metabolic clearance for these compounds. Collectively, these results show that drawbacks of the use of slices for clearance prediction are largely surmountable. Provided that thin liver slices and physiological albumin concentration are used, whole body metabolic clearance is predicted with acceptable (2-fold) accuracy with organ slices. These results emphasize the applicability of organ slices in this field of research.

Published

2006

34. Characterization of rat small intestinal and colon precision-cut slices as an in vitro system for drug metabolism and induction studies.

Author

van de Kerkhof EG, de Graaf IA, de Jager MH, Meijer DK, and Groothuis GM

Subjects

Animals, Colon enzymology, Coumarins metabolism, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System metabolism, Enzyme Induction drug effects, Enzyme Inhibitors pharmacology, Glucuronides metabolism, Intestine, Small enzymology, Ketoconazole pharmacology, Male, Models, Animal, Rats, Rats, Wistar, Testosterone metabolism, Time Factors, Tissue Culture Techniques, Umbelliferones metabolism, beta-Naphthoflavone pharmacology, Colon metabolism, Cytochrome P-450 Enzyme System biosynthesis, Intestine, Small metabolism

Abstract

The aim of this study was to characterize rat small intestinal and colon tissue slices as a tool to study intestinal metabolism and to investigate gradients of drug metabolism along the intestinal tract as well as drug-induced inhibition and induction of biotransformation. Tissue morphology and the intestinal mucus layer remained intact in small intestinal and colon slices during 3 h of incubation, while alkaline phosphatase was retained and the rate of metabolism of three model compounds (7-hydroxycoumarin, 7-ethoxycoumarin, and testosterone) appeared constant. Phase I and phase II metabolic gradients, decreasing from stomach toward colon were shown to be clearly different for the model compounds used. Furthermore, the observed slice activities were similar or even higher compared with the literature data concerning metabolism of in vitro intestinal systems. Preincubation with beta-naphthoflavone for 24 h induced the O-deethylation of 7-ethoxycoumarin from nearly undetectable to 140 pmol/min/mg protein in small intestine (fresh slices, 43 pmol/min/mg protein) and to 100 pmol/min/mg protein in colon slices (fresh slices, undetectable). Ketoconazole inhibited metabolism of testosterone by 40% and that of 7-ethoxycoumarin by 100%. In conclusion, we showed that the intestinal slice model is an excellent model to study drug metabolism in the intestine in vitro, since we found that the viability parameters remain constant and the measured enzyme activities are relevant, sensitive to inhibitors, and inducible. Therefore, it is a promising tool to study intestinal drug metabolism in human intestine in vitro in the future.

Published

2005

35. A new technique for preparing precision-cut slices from small intestine and colon for drug biotransformation studies.

Author

de Kanter R, Tuin A, van de Kerkhof E, Martignoni M, Draaisma AL, de Jager MH, de Graaf IA, Meijer DK, and Groothuis GM

Subjects

Adenosine Triphosphate analysis, Animals, Colon cytology, Coumarins metabolism, Intestine, Small cytology, Lidocaine metabolism, Male, RNA analysis, Rats, Rats, Wistar, Testosterone metabolism, Umbelliferones metabolism, Biotransformation, Colon metabolism, Intestine, Small metabolism, Microtomy methods

Abstract

Introduction: A new technique was developed to prepare precision-cut slices from small intestine and colon with the object of studying the biotransformation of drugs in these organs., Methods: Rat intestinal slices were prepared in two different ways. In the first method, slices were punched out of the small intestine. In the second method, precision-cut slices were made from agarose-filled and -embedded intestines, using the Krumdieck tissue slicer. This method was also applied to colon tissue. Viability of the slices was determined by analysis of intracellular ATP and RNA levels and morphology. Drug metabolizing activity was studied using lidocaine, testosterone, and 7-ethoxycoumarin (7-EC) as phase I substrates, and 7-hydroxycoumarin (7-HC) as a phase II substrate., Results: Precision-cut slices made from agarose-filled and -embedded intestine better preserved ATP levels than tissue that was punched out of the intestinal wall. After 24 h of incubation, morphology in precision cut-slices showed was quite well preserved while punched out tissue was almost completely autolytic after incubation. In addition, total RNA amount and quality was much better maintained in precision-cut slices, when compared to punched out tissue. Both intestinal slices and punched-out tissue showed high, and comparable, phase I and phase II biotransformation activities., Discussion: It is concluded that preparing precision-cut 0.25 mm slices out of agarose-filled and -embedded intestine provides an improvement, compared with punched-out tissue, and that both intestinal and colon slices are useful preparations for in vitro biotransformation studies.

Published

2005

36. Prediction of whole-body metabolic clearance of drugs through the combined use of slices from rat liver, lung, kidney, small intestine and colon.

Author

De Kanter R, Monshouwer M, Draaisma AL, De Jager MH, de Graaf IA, Proost JH, Meijer DK, and Groothuis GM

Subjects

Animals, Biotransformation, Colon metabolism, In Vitro Techniques, Intestine, Small metabolism, Kidney metabolism, Liver metabolism, Lung metabolism, Male, Microtomy, Organ Specificity, Predictive Value of Tests, Rats, Rats, Wistar, Coumarins metabolism, Coumarins pharmacokinetics, Pharmaceutical Preparations metabolism, Umbelliferones metabolism, Umbelliferones pharmacokinetics

Abstract

1: The aim was to investigate whether precision-cut rat tissue slices could be used to predict metabolic drug clearance in vivo. To obtain a complete picture, slices not only from liver, but also from lung, kidney, small intestine and colon were included. 2: The metabolic clearances of 7-ethoxycoumarin, 7-hydroxycoumarin, testosterone, methyltestosterone and warfarin were determined by measuring the disappearance of these compounds during incubation with slices prepared from liver, lung, kidney, small intestine and colon. 3: The total in vitro metabolic clearance was determined by adding the individual in vitro organ clearances from the slices. Prediction based on the in vitro clearance was within an order of magnitude to the corresponding in vivo values. Interestingly, the relative contribution of extrahepatic metabolic clearance of the studied compounds to total clearance was remarkably high, ranging from 35 to 72% of the total metabolic clearance. 4: It is concluded that the model of multi-organ precision-cut slices is a useful in vitro tool for prediction of in vivo metabolic clearance. In addition, it provides information about the relative contribution of the liver, lung, kidney, small intestine and colon to the total metabolic clearance., (Copyright 2004 Taylor and Francis Ltd.)

Published

2004

37. Cryopreservation of precision-cut tissue slices for application in drug metabolism research.

Author

de Graaf IA and Koster HJ

Subjects

Humans, Reproducibility of Results, Tissue Banks, Water, Cryopreservation methods, Pharmacokinetics, Tissue Fixation methods

Abstract

Cryopreservation of tissue slices greatly facilitates their use in drug metabolism research, leading to efficient use of human organ material and a decrease of laboratory animal use. In the present review, various mechanisms of cryopreservation such as equilibrium slow freezing, rapid freezing and vitrification, and their application to cryopreservation of tissue slices are discussed as well as the viability parameters often used to evaluate the success of cryopreservation. Equilibrium freezing prevents intracellular ice formation by inducing cellular dehydration, but (large) ice crystals are still formed in the interstitial space of the slices. Upon rapid freezing, (small) intra- and extracellular ice crystals are formed which slices from some tissues can resist. Vitrification prevents the formation of both intra- and extracellular ice crystals while an amorphous glass is formed of the slice liquid constituents. To vitrify, however, high molarity solutions of cryoprotectants are required that may be toxic to the slices. The use of mixtures of high molarity of cryoprotectants overcomes this problem. We conclude that vitrification is the approach that most likely will lead to the development of universal cryopreservation methods for tissue slices of various organs from various animal species. In the future this may lead to the formation of a tissue slice bank from which slices can be derived at any desirable time point for in vitro experimentation.

Published

2003

38. Comparison of in vitro preparations for semi-quantitative prediction of in vivo drug metabolism.

Author

De Graaf IA, Van Meijeren CE, Pektaş F, and Koster HJ

Subjects

Animals, Drug Evaluation, Preclinical methods, Forecasting, In Vitro Techniques, Intestine, Small metabolism, Kidney metabolism, Liver metabolism, Lung metabolism, Male, Pharmaceutical Preparations chemistry, Rats, Rats, Sprague-Dawley, Rats, Wistar, Species Specificity, Tissue Distribution physiology, Pharmaceutical Preparations metabolism

Abstract

Various in vitro preparations were compared with respect to their ability to mimic in vivo metabolism. For this purpose, S9-liver homogenate, microsomes, cryopreserved hepatocytes, cryopreserved liver slices and fresh liver, lung, kidney, and intestinal slices were incubated with three drugs in development, which are metabolized in vivo by a wide range of biotransformation pathways. Metabolites were identified and quantified with liquid chromatography-mass spectometry/UV from the in vitro incubations and compared with metabolite patterns in feces, urine, and bile of dosed rats. In vitro systems with intact liver cells produced the same metabolites as the rat in vivo and are a valuable tool to study drug metabolism. Phase I metabolites were almost all conjugated in intact cells, whereas S9-homogenate only conjugated by sulfation and N-acetylation. Microsomes and S9-homogenate are useful to study phase I metabolism but not for the prediction of in vivo metabolism. Extra-hepatic organ slices did not form any metabolites that were not produced by liver cells, but the relative amounts of the various metabolites differed considerably. Small intestinal slices were more active than liver slices in the formation of the N-glucuronide of compound C, which is the major metabolite in vivo. When the relative contribution of liver and small intestinal slices to the metabolism of this compound was taken into account, it appeared that the in vivo metabolite pattern could be well predicted. Results indicate that for adequate prediction of in vivo metabolism, fresh or cryopreserved liver slices or hepatocytes in combination with slices of the small intestines should be used.

Published

2002

39. Incubation at 37 degrees C prior to cryopreservation decreases viability of liver slices after cryopreservation by rapid freezing.

Author

de Graaf IA, Geerlinks A, and Koster HJ

Subjects

Adenosine pharmacology, Adenosine Triphosphate metabolism, Allopurinol pharmacology, Animals, Body Water, Calcium, Chelating Agents pharmacology, Free Radical Scavengers pharmacology, Glutathione pharmacology, Insulin pharmacology, Male, Microtomy, Organ Preservation Solutions pharmacology, Oxygen pharmacology, Potassium pharmacology, Raffinose pharmacology, Rats, Rats, Wistar, Temperature, Cryopreservation methods, Liver drug effects, Liver metabolism, Specimen Handling methods

Abstract

Precision-cut liver slices are to some extent resistant to ice formation induced by rapid freezing. Susceptibility to rapid freezing damage has been shown to be (partly) dependent on intrinsic properties of cells. In the present study an attempt was made to decrease the susceptibility of rat liver slices for rapid freezing damage: the slices were pre-incubated at 37 degrees C under oxygen, prior to cryopreservation to recover from low ATP levels, impaired ion regulation and cell swelling induced by their preparation. It was shown that, unexpectedly, recovery of cellular homeostasis prior to the cryopreservation procedure by the 37 degrees C pre-incubation markedly decreased viability of rapidly frozen slices (in which ice was formed), but not of vitrified slices (in which no ice was formed), in a time- and temperature-dependent manner. UW was found to protect slices from this 'warm pre-incubation phenomenon.' Apparently, pre-incubation prior to freezing causes certain cellular alterations that render slices more susceptible to rapid freezing damage.

Published

2002

40. Water crystallization within rat precision-cut liver slices in relation to their viability.

Author

de Graaf IA and Koster HJ

Subjects

Animals, Cryoprotective Agents, Crystallization, Ice, In Vitro Techniques, Male, Rats, Rats, Wistar, Thermodynamics, Water metabolism, Cryopreservation methods, Liver anatomy & histology, Liver physiology, Tissue Preservation methods

Abstract

This study examined whether tissue vitrification, promoted by partitioning within the tissue, could be the mechanism explaining the high viability of rat liver slices, rapidly frozen after preincubation with 18% Me2SO or VS4 (a 7.5 M mixture of Me2SO, 1,2-propanediol, and formamide with weight ratio 21.5:15:2.4). To achieve this, we first determined the extent to which crystallization or vitrification occurred in cryoprotectant solutions (Me2SO and VS4) and within liver slices impregnated with these solutions. Second, we determined how these events were related to survival of slices after thawing. Water crystallization was evaluated by differential scanning calorimetry and viability was determined by histomorphological examination of the slices after culturing at 37 degrees C for 4 h. VS4-preincubated liver slices indeed behaved differently from bulk VS4 solution, because, when vitrified, they had a lower tendency to devitrify. Vitrified VS4-preincubated slices that were warmed sufficiently rapid to prevent devitrification had a high viability. When VS4 was diluted (to 75%) or if warming was not fast enough to prevent ice formation, slices had a low viability. With 45% Me2SO, low viability of cryopreserved slices was caused by cryoprotectant toxicity. Surprisingly, liver slices preincubated with 18% Me2SO or 50% VS4 had a high viability despite the formation of ice within the slice. In conclusion, tissue vitrification provides a mechanism that explains the high viability of VS4-preincubated slices after ultrarapid freezing and thawing (>800 degrees C/min). Slices that are preincubated with moderately concentrated cryoprotectant solutions (18% Me2SO, 50% VS4) and cooled rapidly (100 degrees C/min) survive cryopreservation despite the formation of ice crystals within the slice., (Copyright 2001 Elsevier Science (USA).)

Published

2001

41. Increased post-thaw viability and phase I and II biotransformation activity in cryopreserved rat liver slices after improvement of a fast-freezing method.

Author

de Graaf IA, van der Voort D, Brits JH, and Koster HJ

Subjects

Animals, Biotransformation, Cell Survival drug effects, Chromatography, High Pressure Liquid, Cold Temperature, Cryopreservation methods, Dimethyl Sulfoxide pharmacology, In Vitro Techniques, Liver cytology, Liver drug effects, Male, Potassium metabolism, Rats, Rats, Wistar, Temperature, Testosterone pharmacokinetics, Time Factors, Tissue Preservation, Cryopreservation standards, Freezing, Liver metabolism

Abstract

An existing cryopreservation method for liver slices applies 12% dimethylsulfoxide and rapid freezing. We found that cells in rat liver slices cryopreserved in this manner deteriorated rapidly upon culturing. To improve this cryopreservation method, we varied the dimethylsulfoxide concentration (0, 12, 18, and 30%), the cryopreservation medium (Williams medium E, fetal calf serum, and University of Wisconsin medium), slice thickness, and the storage period at 4 degrees C during slice preparation before cryopreservation. After thawing, slices were cultured for 4 h at 37 degrees C before their viability was evaluated by their potassium content and the number of intact cells determined histomorphologically. The biotransformation capacity of liver slices cryopreserved by the improved method was assessed by testosterone oxidation, hydroxycoumarin sulfation, and glucuronidation. Best results were obtained with 18% dimethylsulfoxide in Williams medium E: the potassium content of cryopreserved slices was higher than 65%, and the number of intact cells was higher than 60% of that in fresh slices; with 12% dimethylsulfoxide, potassium content was less than 40%, and the number of intact cells was less than 30%. Results did not differ between the three cryopreservation media. Viability of thin slices (8-10 cell layers) was better maintained than that of thicker slices (>14 cell layers). Storage at 4 degrees C of slices before cryopreservation decreased viability after cryopreservation. Both oxidative and conjugation activities were better than 60% of fresh values. Although results varied, slices cryopreserved with this improved method and cultured for 4 h retained viability between 50 and 80%, and biotransformation activity between 60 and 90% of fresh slices.

Published

2000

42. Intercellular communication and cell proliferation in precision-cut rat liver slices: effect of medium composition and DDT.

Author

de Graaf IA, Tajima O, Groten JP, and Wolterbeek AP

Subjects

Animals, Blotting, Western, Bromodeoxyuridine metabolism, Cell Division drug effects, Cells, Cultured, Connexins metabolism, Dose-Response Relationship, Drug, Gap Junctions metabolism, Immunohistochemistry, In Vitro Techniques, L-Lactate Dehydrogenase metabolism, Male, Rats, Rats, Wistar, Time Factors, Gap Junction beta-1 Protein, Culture Media, DDT pharmacology, Liver drug effects, Liver metabolism, Signal Transduction drug effects

Abstract

Gap junctional intercellular communication (GJIC) and cell proliferation were studied in control and 1,1'-bis(p-chlorophenyl)-2, 2,2,-trichloroethane (DDT) treated precision-cut liver slices of rat by evaluating connexin 32 (Cx32) expression and 5-bromo-2'-deoxyuridine (BrdU) incorporation. In addition, the effect of different culture media (RPMI and WME) on control and DDT influenced Cx32 expression and cell proliferation was determined. Cx32 expression in control precision-cut liver slices was maintained during 8 h of culturing, but decreased after prolonged culturing. Control cell proliferation was significantly higher when WME was used as culture medium than when RPMI was used. In slices treated with DDT Cx32 expression was decreased. In slices cultured in RPMI medium, this decrease preceded a dose-dependent increase in cell proliferation. These results show the usefulness of precision-cut liver slices in studying cellular proliferation and intercellular communication.

Published

2000

43. Assessment of some critical factors in the freezing technique for the cryopreservation of precision-cut rat liver slices.

Author

Maas WJ, de Graaf IA, Schoen ED, Koster HJ, van de Sandt JJ, and Groten JP

Subjects

Adenosine Triphosphate metabolism, Animals, Dinitrochlorobenzene metabolism, Evaluation Studies as Topic, Glutathione metabolism, Glutathione Transferase metabolism, In Vitro Techniques, L-Lactate Dehydrogenase metabolism, Male, Microtomy, Potassium metabolism, Proteins metabolism, Rats, Rats, Wistar, Testosterone metabolism, Urea metabolism, Cryopreservation methods, Liver anatomy & histology, Liver metabolism, Tissue Preservation methods

Abstract

A number of studies on the cryopreservation of precision-cut liver slices using various techniques have been reported. However, the identification of important factors that determine cell viability following cryopreservation is difficult because of large differences between the various methods published. The aim of this study was to evaluate some important factors in the freezing process in an effort to find an optimized approach to the cryopreservation of precision-cut liver slices. A comparative study of a slow and a fast freezing technique was carried out to establish any differences in tissue viability for a number of endpoints. Both freezing techniques aim at the prevention of intracellular ice formation, which is thought to be the main cause of cell death after cryopreservation. Subsequently, critical variables in the freezing process were studied more closely in order to explain the differences in viability found in the two methods in the first study. For this purpose, a full factorial experimental design was used with 16 experimental groups, allowing a number of variables to be studied at different levels in one single experiment. It is demonstrated that ATP and K(+) content and histomorphology are sensitive parameters for evaluating slice viability after cryopreservation. Subsequently, it is shown that freezing rate and the cryopreservation medium largely determine the residual viability of liver slices after cryopreservation and subsequent culturing. It is concluded that a cryopreservation protocol with a fast freezing step and using William's Medium E as cryopreservation medium was the most promising approach to successful freezing of rat liver slices of those tested in this study., (Copyright 2000 Academic Press.)

Published

2000