Your search keyword '"J. J. de Gier"' showing total 125 results

1. Letter to the Editor and Reply on: 'Drugs and Driving,' Traffic Injury Prevention, 5:241 − 253, 2004

Author

Alain Verstraete, M. Walsh, J. J. de Gier, and A. Christopherson

Subjects

Engineering, Letter to the editor, Injury control, business.industry, Public Health, Environmental and Occupational Health, Poison control, Human factors and ergonomics, Traffic injury, medicine.disease, Suicide prevention, Occupational safety and health, Injury prevention, medicine, Medical emergency, business, Safety Research

Published

2005

2. Abstracts of papers

Author

W. E. Roorda, M. A. de Vries, C. Kosho, J. A. Bouwstra, H. E. Junginger, H. E. Boddé, C. Kleinjan, W. C. de Bruyn, W. T. Daems, T. Kranenburg, L. M. J. van Driel, R. Roosjen, H. F. L. Gulot, T. de Vringer, J. G. H. Joosten, H. Jousma, J. Bouwstra, G. Gooris, G. S. Gooris, H. L. G. M. Tiemessen, H. E. Junsinger, J. Verhoeven, J. J. H. U. de Groot, R. J. Schaeffer, L. J. C. Peschier, G. S. M. J. E. Duchateau, J. Zuldema, F. W. H. M. Merkus, F. A. J. M. Pieters, D. Dekker, L. van Blools, D. J. A. Crommelin, W. Jiskoot, J. C. A. Offringa, R. Plekkenpol, P. A. M. Peeters, A. C. M. Claessens, P. W. J. T. Leufkens, W. M. C. Eling, F. G. J. Poelma, J. J. Tukker, D. J. A. Cromnelin, G. Storm, L. van Bloois, M. Brouwer, H. Talsma, M. A. Blankenstein, J. W. R. Nortier, A. Bakri, J. Wilting, L. H. H. Janssen, P. J. A. Crommelin, A. M. Mathieu, M. van Ooteghem, A. Ludwig, D. D. Breimer, A. G. de Boer, C. H. Kleinbloesem, P. van Brummelen, M. Danhof, J. Urquhart, G. K. Bolhuis, H. V. van Kamp, J. H. Proost, C. F. Lerk, A. H. de Boer, H. Vromans, P. de Haan, A. J. M. Schoonen, G. W. de Vries-Nijboer, E. H. Bosch, K. D. Kussendrager, H. K. F. van Saene, H. F. Mahieu, J. J. M. van Saene, L. Baaijens, E. Middelbeek, R. van Rooy, M. J. C. Vissers, L. Baaljens, A. P. Sam, Y. Boer, D. Janknegt, H. L. M. Cox, P. J. J. de Meijer, P. H. A. M. Kloeg, C. K. Mensink, F. J. van de Vaart, W. Roggen, F. A. Boom, A. C. A. Paalman, Th. Vos, J. J. de Gier, A. Takken-Hillebrecht, J. A. L. van Lakwijk-Najoan, H. G. M. Leufkens, and A. H. P. Paes

Subjects

Pharmacology, Pharmacology (medical)

Published

1986

3. Abstracts of papers

Author

J. F. Rodrigues de Miranda, J. van der Weide, P. C. Tepper, J. B. de Vries, A. S. Horn, A. P. Ijzerman, T. Bultsma, H. Timmerman, M. Th. M. Tulp, L. H. M. Janssen, D. de Kaste, K. J. H. van Buuren, W. Soudijn, H. J. Kloosterboer, E. W. Bergink, Joop C. van Oene, John W. Kebabian, B. Rademnker, A. Bast, K. Kramer, B. Rademaker, A. Bakri, G. M. J. BeijersberRen van Henegouwen, H. de Vries, J. Wilting, W. J. M. Underberg, R. W. Busker, G. M. J. Beijersbergen van Henesouwen, G. M. J. Beijersbergen van Henegouwen, M. de Zwart, H. van der Goot, G. M. Donne-Op den Kelder, G. J. Bijloo, E. E. J. Haaksma, J. Ch. Eriks, Y. Severne, V. Nerme, G. Vauquelin, R. Leurs, M. M. Mennen, J. F. Plantjé, J. C. Stoof, B. J. 't Hart, J. J. de Gier, R. v. d. Straat, T. Kulkons, A. J. J. Debets, J. de Vries, H. P. E. Verneulen, J. F. van der Werf, A. C. van der Kuyl, J. M. S. van Maanen, C. de Ruiter, P. R. Kootstra, J. Broersen, M. V. M. Lafleur, J. Retèl, H. M. Pinedo, K. Wezel, E. I. Bakker, M. Wolf, A. J. Beld, and E. Mutschler

Subjects

Pharmacology, Pharmacology (medical)

Published

1985

4. Abstracts of papers Rational use of drugs

Author

M. N. G. Dukes, Robert M. Elenbaas, G. Tognoni, Dorothy L. Smith, Inga Lunde, H. G. M. Leufkens, Y. A. Hekster, A. Bakker, G. Ostino, H. Petri, F. Sturmans, H. D. Banta, F. F. H. Rutten, L. L. Martens, P. R. Noyce, F. W. H. M. Merkus, Lolkje de Jong-v.d.Berg, Flora Haaijer-Ruskamp, Graham Dukes, B. -M. Vidgren, S. Vidgren, N. Martini, M. L. Sala, G. Scroccaro, P. Olivencia, D. C. McLcod, W. G. Coln, A. G. Hartzcma, C. F. Thaver, J. M. Rodriguez-Sasiain, B. Sangroniz, M. D. Mauleon, M. A. Wood, M. J. Martinez, O. Leinebø, J. N. Saugen, P. Marini, R. Olivato, C. Alberola, E. Cruz-Martos, T. Cruz, N. Marfagon, A. Herreros de Tejada, P. Denig, F. M. Haaijer-Ruskamp, H. Wesseling, A. Versluis, M. P. Gascón, Robert Horne, Jane Hough, N. S. Klazinga, J. J. -E. van Everdingen, P. J. van den Broek, D. K. Roberts, G. B. A. Veitch, K. K. C. Tan, D. A. Holland, M. C. Allwood, A. Nicholls, A. Astobieta, R. Calvo, J. M. Rodriquez-Sasiain, D. Barriquand, C. Pochon, G. Aulagner, A. Vial, C. Dumarest, P. H. Maire, R. W. Jelliffe, J. R. B. J. Brouwers, K. Cramer, J. Gulyas, H. J. vd Kam, J. Sijtsma, C. Donadio, G. Tramonti, G. Garcea, M. Costagli, A. Lucchetti, R. Giordani, G. Paizis, R. Pierotti, G. Falcone, C. Bianchi, C. Gallastegui, R. Farré, I. Jiménez, M. A. Mangues, E. Guasch, G. Ginovart, X. Sagrera, F. Raspall, J. M. Queralto, J. M. Kovarik, C. M. A. Rademaker, J. Verhoef, L. Silvestri, M. Caputo, M. Andrew, E. -L. Toverud, I. Jimenez, I. Castro, E. Alvarez, J. Altimiras, J. J. J. P. M. van de Leur, N. F. Muller, J. M. Van Turnhout, L. Mendizabal, J. M. Rodriguez Sasiain, G. Morana, K. Moss Ofstad, A. -M. Timenes, J. K. F. Vroom, L. T. W. de Jong-van den Berg, P. B. van den Berg, J. J. de Gier, J. Ferres, O. Recoder, Rio T. Sanchez, M. P. Garcia, A. Julia, A. Balet, R. Farre, M. A. Manques, T. Berod, E. Dufay, C. Naveau, M. Combe, A. Sauvageon, Erik Wind Hansen, Jens Dencker Christensen, L. Lie-A-Huen, J. H. Kinqma, D. K. P. Meijer, F. Le Meur, P. Isoard, M. S. Salek, A. Y. Finlay, G. K. Khan, D. K. Luscombe, A. Stuurman, M. P. Boidin, K. Wallenius, R. Ojala, A. Kariluoto, M. Ikonen, A. H. P. Paes, A. Th. G. Blom, S. Wallenius, H. Enlund, K. Vainio, C. Codina, M. Roca, P. Sardà, N. Corominas, J. Massó, J. Ribas, K. Kentra, M. Myllyntausta, M. Saarenpää, M. S. A. Airaksinen, L. Mendarte, A. Rimola, R. Meisters, Y. Hekster, W. Janssen, A. Cox, R. Kempen, S. J. A. Aerdts, R. van Dalen, H. A. L. Clasener, J. Festen, PP Schjphorst, HB Benraad, P. van Asten, R. de Wit, R. J. G. Limbeek, H. G. M. Nagel, R. H. B. Mgyboom, B. H. C. Stricker, B. A. M. van den Berg, T. H. A. Nelen, T. A. G. Tijssen, P. Wassink, M. J. E. Wassink-L'Ortije, P. Gascón, C. Selva, T. Bassons, C. Pardo, M. P. Mas, M. Saqalés, F. Sánchez, V. Mercade, R. Pujol, C. Agustí, M. Cano, T. Gurrera, M. Gorchs, X. Fabregas, L. L. Murgui, A. Verdaguer, W. P. J. Witjes, E. J. Vollaard, B. J. P. Crul, C. Limpens, K. Ahonen, T. Klaukka, I. Vohlonen, J. Martikainen, Daniel Goldenberg, Andres Brodsky, Ines Aparici, Cecilia Argeri, D. Goldenberg, C. Saidman, L. Sevinski, N. Allevato, B. Mujico, J. Ubogui, P. Dorfman, Lupo L. Rodriguez, M. Varela, J. Higa, Annie Fourrier, Philippe Larrouturou, Claire Samarran, Jacqueline Huchet, N. D. Barber, N. Party, P. Wilson, Grethe Eide, Kari Horvei, Angelika Kruse-Jensen, Ingrid Wold, Turid Møark, C. W. Barrett, A. C. Tugwell, B. Søndergaard, M. Rasmussen, F. Davidsen, H. Hey, L. Kierkeby, L. Riis, M. Korhonen, P. Vidgren, T. Ojanen, M. Vidqren, J. Ferrés, T. Sanchez, C. Gallastequi, A. Julià, R. M. C. Herings, B. H. Ch. Stricker, A. J. H. H. Janssen, Heike Dinter, A. J. H. M. Janssen, X. Barbaut, S. Proust, G. Amlagner, F. A. L. M. Eskens, E. Arnoldussen, E. Sieradzki, E. Wanat-Słupska, M. Zlółkowska, I. Pankowska, R. Mazur, B. Ksiazkiewicz, A. Jankowski, A. Marzec, C. Marzec, M. O. Marzec, J. P. Marzec, D. R. Mungall, Lynne Portnoy, F. Lucas, F. Kadir, A. Pijpers, A. Vulto, J. Zuidema, P. Sutton, Antal Samu, John E. Murphy, Ronnie Chapman, Nicolien Wieringa, J. Rolloos, M. T. P. J. Voesten, P. J. J. de Meijer, G. H. P. de Koning, S. Salek, E. Reerink, L. Farrow, G. Raskob, D. Rosenbloom, R. Hull, A. Torras, O. Recorder, C. Torras, J. Cubellsl, M. Font, R. Madridejos, A. Catalán, M. Huguet, N. Franquesa, J. Gratacós, M. Martinez, A. Saltó, E. van der Kleijn, R. J. M. ter Wee, N. Holmberg, and R. F. Brenninkmeijer

Subjects

Pharmacology, Medical education, business.industry, Pharmacology (medical), Pharmacy, business, Psychology, Rational use

Published

1989

5. Abstracts of Dutch Ph.D. Theses

Author

P. J. G. Cornelissen, J. J. De Gier, and A. P. De Jong

Subjects

Pharmacology, Pharmacology (medical)

Published

1981

6. Complications in correlation studies between serum, free serum and saliva concentrations of nitrazepam

Author

B J, Hart, J, Wilting, and J J, de Gier

Subjects

Adult, Male, Humans, Nitrazepam, Saliva, Dialysis, Serum Albumin, Protein Binding

Abstract

The relation between free serum and saliva concentrations of nitrazepam in healthy male volunteers has been studied. It was found that the average value of free serum concentrations from all volunteers was twice the average value of corresponding saliva concentrations. Sometimes mean values of serum, free serum and saliva concentrations are used in correlation studies. However, the data from individual volunteers showed that there was no correlation between them. Statistics can easily introduce false pictures for correlations between free serum and saliva concentrations of nitrazepam, whereas no correlation could be found on the basis of results from individuals. In response studies such as the effects of drugs on driving performance, the free serum and saliva concentrations of a drug from individual volunteers should therefore be considered. This will complicate the use of saliva in epidemiological studies on drugs and driving.

Published

1987

7. Diazepam-induced changes in signal detection performance. A comparison with the effects on the Critical Flicker-Fusion Frequency and the Digit Symbol Substitution Test

Author

A A, Jansen, J J, de Gier, and J L, Slangen

Subjects

Adult, Flicker Fusion, Male, Diazepam, Time Factors, Adolescent, Double-Blind Method, Pattern Recognition, Visual, Reaction Time, Humans, Attention, Psychomotor Performance, Probability

Abstract

The effects of 10 mg diazepam on signal detection theory measures (stimulus sensitivity, response bias) and reaction times were studied in a 1-hour visual signal detection task with high and low signal probability, and on performance in two short-duration tasks: Critical Flicker-Fusion Frequency (CFF) and the Digit Symbol Substitution Test (DSST). 12 healthy volunteers participated in this placebo-controlled, double-blind cross-over study. Diazepam affected the stimulus sensitivity and the reaction times of hits in the signal detection task. DSST performance was also impaired while CFF did not change after diazepam treatment. No relationship between serum diazepam concentration and change in task performance was found. It is concluded that diazepam affects signal detection performance, independent of signal probability. A short-duration task like the DSST is as sensitive to the effects of diazepam as the (long-duration) signal detection task.

Published

1986

8. The role of buffer composition during equilibrium dialysis in determining concentrations of free diazepam in serum

Author

J J, de Gier, B J, t Hart, and J, Wilting

Subjects

Male, Diazepam, Nordazepam, Humans, Buffers, Dialysis, Protein Binding

Abstract

Serum levels of free diazepam as determined with equilibrium dialysis depend on the composition of the dialyzing buffer with respect to Ca2+ and Cl-. Physiological concentrations of these ions double the obtained free serum levels, in line with data of diazepam containing albumin solutions. The diazepam binding capacity of serum was found to be higher than that of albumin alone, suggesting that albumin is probably not the only diazepam binding protein in serum. Evidence was also found that the diazepam binding to these other serum proteins is dependent on the presence of Ca2+ and Cl-.

Published

1983

9. The stability of benzodiazepines in saliva

Author

B J, Hart, J, Wilting, and J J, de Gier

Subjects

Male, Benzodiazepines, Drug Stability, Humans, Nitrazepam, Saliva, Specimen Handling

Abstract

The stability of some selected benzodiazepines in saliva has been studied. The benzodiazepines nitrazepam and clonazepam were found to be unstable in saliva at room temperature and nitrazepam was converted into 7-aminonitrazepam. The conversion rate of nitrazepam was strongly dependent on the composition of the subject's saliva. Nitro-reduction may complicate the use of saliva in epidemiological studies on drugs and driving. This could occur particularly if saliva drug concentrations are to be used as a quantitative measure of driving performance.

Published

1988

10. In vitro and in vivo effects of kisspeptin antagonists p234, p271, p354, and p356 on GPR54 activation.

Author

Albers-Wolthers CHJ, de Gier J, Walen M, van Kooten PJS, Lambalk CB, Leegwater PAJ, Roelen BAJ, Schaefers-Okkens AC, Rutten VPMG, Millar RPM, and Kooistra HS

Subjects

Animals, Dogs, Female, Humans, Rats, Receptors, Kisspeptin-1, Calcium metabolism, Kisspeptins pharmacology, Luteinizing Hormone blood, Receptors, G-Protein-Coupled antagonists & inhibitors, Signal Transduction drug effects

Abstract

Kisspeptins (KPs) and their receptor (GPR54 or KiSS1R) play a key-role in regulation of the hypothalamic-pituitary-gonadal axis and are therefore interesting targets for therapeutic interventions in the field of reproductive endocrinology. As dogs show a rapid and robust LH response after the administration of KP10, they can serve as a good animal model for research concerning KP signaling. The aims of the present study were to test the antagonistic properties of KP analogs p234, p271, p354, and p356 in vitro, by determining the intracellular Ca2+ response of CHEM1 cells that stably express human GPR54, and to study the in vivo effects of these peptides on basal plasma LH concentration and the KP10-induced LH response in female dogs. Exposure of the CHEM1 cells to KP-10 resulted in a clear Ca2+ response. P234, p271, p354, and p356 did not prevent or lower the KP10-induced Ca2+ response. Moreover, the in vivo studies in the dogs showed that none of these supposed antagonists lowered the basal plasma LH concentration and none of the peptides lowered the KP10-induced LH response. In conclusion, p234, p271, p354, and p356 had no antagonistic effects in vitro nor any effect on basal and kisspeptin-stimulated plasma LH concentration in female dogs.

Published

2017

11. Validation of a noninvasive diagnostic tool to verify neuter status in dogs: The urinary FSH to creatinine ratio.

Author

Albers-Wolthers CH, de Gier J, Oei CH, Schaefers-Okkens AC, and Kooistra HS

Subjects

Animals, Creatinine blood, Dogs, Female, Follicle Stimulating Hormone blood, Male, Reproducibility of Results, Sensitivity and Specificity, Creatinine urine, Follicle Stimulating Hormone urine, Hysterectomy veterinary, Immunoradiometric Assay veterinary, Orchiectomy veterinary, Ovariectomy veterinary

Abstract

Determining the presence of functional gonadal tissue in dogs can be challenging, especially in bitches during anestrus or not known to have been ovariectomized, or in male dogs with nonscrotal testes. Furthermore, in male dogs treated with deslorelin, a slow-release GnRH agonist implant for reversible chemical castration, the verification of complete downregulation of the hypothalamic-pituitary-gonadal (HPG) axis can be difficult, especially if pretreatment parameters such as the size of the testes or prostate gland are not available. The aims of this study were to validate an immunoradiometric assay for measurement of FSH in canine urine, to determine if the urinary FSH to creatinine ratio can be used to verify the neuter status in bitches and male dogs, as an alternative to the plasma FSH concentration, and to determine if downregulation of the HPG axis is achieved in male dogs during deslorelin treatment. Recovery of added canine FSH and serial dilutions of urine reported that the immunoradiometric assay measures urinary FSH concentration accurately and with high precision. Plasma FSH concentrations (the mean of two samples, taken 40 minutes apart) and the urinary FSH to creatinine ratio were determined before gonadectomy and 140 days (median, range 121-225 days) and 206 days (median, range 158-294 days) after gonadectomy of 13 bitches and five male dogs, respectively, and in 13 male dogs before and 132 days (median, range 117-174 days) after administration of a deslorelin implant. In both bitches and male dogs, the plasma FSH concentration and the urinary FSH to creatinine ratio were significantly higher after gonadectomy, with no overlapping of their ranges. Receiver operating characteristic analysis of the urinary FSH to creatinine ratio revealed a cut-off value of 2.9 in bitches and 6.5 in males to verify the presence or absence of functional gonadal tissue. In male dogs treated with deslorelin, the plasma FSH concentrations and urinary FSH to creatinine ratios were significantly lower after administration of the implant, but their ranges overlapped. We conclude that the urinary FSH to creatinine ratio can be used to verify the neuter status of bitches and male dogs. However, it cannot be used for the assessment of complete downregulation of the HPG axis after administration of a deslorelin implant. The urinary FSH to creatinine ratio is preferable over the plasma FSH concentration because it involves only one sample that can be collected relatively easy and noninvasively., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

12. The effects of kisspeptin agonist canine KP-10 and kisspeptin antagonist p271 on plasma LH concentrations during different stages of the estrous cycle and anestrus in the bitch.

Author

Albers-Wolthers CH, de Gier J, Rutten VP, van Kooten PJ, Leegwater PA, Schaefers-Okkens AC, and Kooistra HS

Subjects

Animals, Estrous Cycle physiology, Female, Gene Expression Regulation drug effects, Gene Expression Regulation physiology, Kisspeptins pharmacology, Peptides antagonists & inhibitors, Dogs physiology, Estrous Cycle drug effects, Kisspeptins antagonists & inhibitors, Luteinizing Hormone blood

Abstract

Kisspeptin (KP) plays a key role in the regulation of the hypothalamic-pituitary-gonadal axis via the release of GnRH. As normal KP signaling is essential for reproductive function, it could be an interesting new target for therapeutic interventions, e.g., nonsurgical contraception in dogs. The aims of the present study were to investigate the effect of KP-10 administration on plasma LH concentration in different stages of the reproductive cycle and to investigate the suitability of p271 as KP antagonist in the bitch. Two groups of six adult Beagle bitches were used. In one group, plasma LH concentration was determined before (40 and 0 minutes) and 10, 20, 40, and 60 minutes after the intravenous administration of 0.5-μg/kg body weight (BW) canine KP-10. In the other group, the bitches received a continuous intravenous infusion with p271 (50 μg/kg BW/h) for 3 hours, and 0.5-μg/kg BW canine KP-10 was administered intravenously 2 hours after the start of the p271 infusion. Their plasma LH concentration was determined before (-40 and 0 minutes) and 30, 60, 90, 120, 130, 140, 160, and 180 minutes after the start of the p271 infusion. In both groups, the experiments were performed during the follicular phase, the first and second half of the luteal phase, and during anestrus. Canine KP-10 induced an increase of plasma LH concentration during all estrous cycle stages and anestrus. There was no difference in LH response between the two groups. The lowest LH response was seen during the follicular phase and the highest response during anestrus. The area under the curve (AUC) for LH and LH increment in the follicular phase were lower than those in anestrus. The AUC LH and LH increment in the first half of the luteal phase were lower than those in the second half of the luteal phase and anestrus. The AUC LH and LH increment in the second half of the luteal phase were not different from those in anestrus. Continuous administration of the antagonist p271 did not alter basal plasma LH concentration and could not prevent or lower the LH response to KP-10 in any of the cycle stages and anestrus. It can be concluded that the LH response to KP-10 is dependent on estrous cycle stage and that peripheral administrated p271 cannot be used as KP antagonist in the dog. This provides new insight in reproductive endocrinology of the bitch, which is important when KP signaling is considered for therapeutic interventions, such as for estrus induction or nonsurgical contraception in the bitch., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

13. Successful treatment for subinvolution of placental sites in the bitch with low oral doses of progestagen.

Author

Voorhorst MJ, van Brederode JC, Albers-Wolthers CH, de Gier J, and Schaefers-Okkens AC

Subjects

Administration, Oral, Animals, Antineoplastic Agents, Hormonal administration & dosage, Antineoplastic Agents, Hormonal pharmacology, Antineoplastic Agents, Hormonal therapeutic use, Dog Diseases pathology, Dogs, Dose-Response Relationship, Drug, Female, Megestrol Acetate administration & dosage, Megestrol Acetate pharmacology, Parturition, Postpartum Period, Pregnancy, Puerperal Disorders drug therapy, Dog Diseases drug therapy, Megestrol Acetate therapeutic use, Puerperal Disorders veterinary

Abstract

Subinvolution of placental sites (SIPS) is the major cause of persistent sanguineous vaginal discharge after parturition in the bitch. Spontaneous remission is common but may take several months, and hence, medical therapy to end the discharge is often requested. In this retrospective study, we evaluated the effect of treatment for SIPS with low oral doses of a progestagen. Nine bitches with SIPS, but otherwise clinically healthy, were found in the computer database of the Department of Clinical Sciences of Companion Animals. Seven of these bitches were treated with low oral doses of a progestagen (megestrol acetate, 0.1 mg/kg body weight (bw) once daily for the 1st week, then 0.05 mg/kg bw once daily for the 2nd week). The other two bitches were untreated. Treatment results were evaluated by a telephone questionnaire. Progestagen treatment was successful in all of the treated dogs; sanguineous vaginal discharge stopped within the treatment period. One of the two untreated dogs remained symptomatic until the next oestrus, approximately 120 days after parturition, and the other remained symptomatic until 6 weeks before the start of the next pro-oestrus, 270 days after parturition. No side effects of the progestagen treatment were observed. Subsequent gestations, parturitions and puerperal periods of 5 mated bitches were uneventful. One bitch did not become pregnant after mating. In conclusion, the results of this study indicate that oral administration of low doses of progestagen for 2 weeks is effective in stopping persistent sanguineous vaginal discharge in bitches with SIPS, with neither side effects nor reduced subsequent fertility., (© 2013 Blackwell Verlag GmbH.)

Published

2013

14. Progesterone receptor isoforms in the mammary gland of cats and dogs.

Author

Gracanin A, de Gier J, Zegers K, Bominaar M, Rutteman GR, Schaefers-Okkens AC, Kooistra HS, and Mol JA

Subjects

Amino Acid Sequence, Animals, Female, Molecular Sequence Data, Protein Isoforms, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Progesterone classification, Species Specificity, Cats metabolism, Dogs metabolism, Mammary Glands, Animal metabolism, Receptors, Progesterone metabolism

Abstract

Progesterone exerts its effect by binding to specific progesterone receptors (PR) within the cell. In dogs and cats, no data are available on PR isoforms as found in other species. We therefore investigated the sequence of the PR gene and encoded protein in dogs and cats, the expression of PR isoforms in mammary tissue using Western blots and the presence of PR in mammary tissue using immunohistochemistry. Comparison of the amino acid sequence of the canine and feline PR with human PR revealed major differences in the PR-B-specific upstream segment (BUS). However, the essential activation function 3 (AF3) domain was intact in the cat but mutated in the dog. The DNA and ligand-binding domains were highly similar among the species. In cats with fibroadenomatous hyperplasia (FAH), high expression of PR mRNA together with growth hormone (GH), GH receptor (GHR) and IGF-I mRNA was found in comparison with feline mammary carcinomas. Immunohistochemical analysis showed strong nuclear as well as cytoplasmic staining for PR in FAH. Western blot analysis revealed expression of the PR-A and PR-B isoforms in the feline mammary gland. In canine mammary tissue, the most abundant PR staining was found in proliferative zones of the mammary gland. Western blot analyses showed mainly staining for PR-A with lower PR-B staining. It is concluded that in dogs and cats both PR isoforms are expressed. The role of mutations found in the canine PR-B is discussed., (© 2012 Blackwell Verlag GmbH.)

Published

2012

15. Disorders of sexual development and associated changes in the pituitary-gonadal axis in dogs.

Author

Buijtels JJ, de Gier J, Kooistra HS, Grinwis GC, Naan EC, Zijlstra C, and Okkens AC

Subjects

Animals, Disorders of Sex Development pathology, Disorders of Sex Development physiopathology, Dogs, Estradiol blood, Female, Follicle Stimulating Hormone blood, Genes, sry genetics, Gonadal Dysgenesis veterinary, Gonadotropin-Releasing Hormone, Luteinizing Hormone blood, Male, Ovary pathology, Ovotesticular Disorders of Sex Development veterinary, Progesterone blood, RNA, Messenger analysis, Testis pathology, Testosterone blood, Disorders of Sex Development veterinary, Dog Diseases physiopathology, Ovary physiopathology, Pituitary Gland physiopathology, Testis physiopathology

Abstract

Normal sexual differentiation depends on completion of chromosomal sex determination, gonadal differentiation, and development of the phenotypic sex. An irregularity in any of these three steps can lead to a disorder in sexual development (DSD). We examined nine dogs with DSD by abdominal ultrasonography, laparotomy, histologic examination of the gonads, and reproductive tract, cytogenetic analysis, and mRNA expression of the SRY gene. We also determined the plasma concentrations of luteinizing hormone (LH), estradiol-17β, and testosterone before and after administration of gonadotropin-releasing hormone (GnRH) and compared these results with those obtained in anestrous bitches and male control dogs. The gonads of three dogs with DSD contained both testicular and ovarian tissue, while in the other six only testicular tissue was found. Each of the dogs had a uterus. Based on gynecologic examination, cytogenetic analysis, and the histology of the gonads, seven of the nine dogs appeared to be XX sex reversals. Three of these were XX true hermaphrodites and four were XX males; the other two dogs had incomplete XY gonadal dysgenesis. All seven XX sex-reversed dogs were found to be negative for the SRY gene by polymerase chain reaction. The basal plasma luteinizing hormone (LH) concentration was significantly higher in dogs with DSD than in anestrous bitches but not significantly different from that in male dogs. The basal plasma LH concentration increased significantly after GnRH administration in all dogs with DSD. The basal plasma estradiol concentration was significantly higher in dogs with DSD than in anestrous bitches but not significantly different from that in male dogs. The basal plasma testosterone concentration was lower in dogs with DSD than in male dogs. In all dogs with DSD both the basal and GnRH-induced plasma testosterone concentrations were above the upper limit of their respective ranges in the anestrous bitches. In conclusion, the secretion of LH and estradiol in these dogs with DSD, all of which had testicular tissue in their gonads, was similar to that in male control dogs. These results indicate that the basal and/or GnRH-stimulated plasma testosterone concentration might be used to detect the presence of testicular tissue in dogs with DSD., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

16. Effects of gonadotropin-releasing hormone administration on the pituitary-gonadal axis in male and female dogs before and after gonadectomy.

Author

de Gier J, Buijtels JJ, Albers-Wolthers CH, Oei CH, Kooistra HS, and Okkens AC

Subjects

Animals, Dogs, Estradiol blood, Female, Follicle Stimulating Hormone blood, Gonads physiology, Luteinizing Hormone blood, Male, Orchiectomy veterinary, Ovariectomy veterinary, Ovary drug effects, Ovary physiology, Pituitary Gland physiology, Testis drug effects, Testis physiology, Testosterone blood, Castration, Gonadotropin-Releasing Hormone pharmacology, Gonads drug effects, Pituitary Gland drug effects

Abstract

GnRH-stimulation tests were performed in 14 female and 14 male client-owned dogs of several breeds, before and 4 to 5 mo after gonadectomy. The aim of the study was to obtain more insight into the pituitary-gonadal axis in intact and neutered dogs and to establish reference values. Basal plasma luteinizing hormone (LH) and follicle-stimulating hormone (FSH) concentrations were increased significantly after gonadectomy in both bitches and male dogs. In both males and females ranges of the basal plasma FSH concentrations, before and after gonadectomy, did not overlap as opposed to the overlap in ranges of the basal plasma LH concentrations. Before gonadectomy basal plasma LH concentrations were lower and basal plasma FSH concentrations were higher in bitches than in male dogs. After gonadectomy these basal values did not differ significantly. GnRH administration before gonadectomy resulted in an increase in plasma LH and FSH concentrations in both genders. GnRH administration after gonadectomy produced an increase only in plasma LH concentrations in both genders, and a just significant increase in plasma FSH in castrated male dogs. GnRH administration before gonadectomy resulted in a significant increase in plasma testosterone concentration in both genders. In males ranges of basal and GnRH-stimulated plasma testosterone concentrations before and after gonadectomy did not overlap. Basal plasma estradiol concentrations were significantly higher in intact males than in castrated males and their ranges did not overlap. The basal estradiol concentrations in bitches before and after ovariectomy were not significantly different. At 120 min after GnRH administration, ranges of plasma estradiol concentration of intact and ovariectomized bitches no longer overlapped. In conclusion, basal plasma FSH concentration appears to be more reliable than basal plasma LH concentration for verification of neuter status in both male and female dogs. The basal plasma testosterone concentration appears to be reliable for verification of neuter status in male dogs. The plasma estradiol concentration at 120 min after GnRH administration can be used to discriminate between bitches with and without functional ovarian tissue., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

17. Questionnaire-based survey of parturition in the queen.

Author

Musters J, de Gier J, Kooistra HS, and Okkens AC

Subjects

Animals, Birth Weight, Female, Litter Size, Male, Pregnancy, Reference Values, Sex Ratio, Stillbirth veterinary, Time Factors, Cats physiology, Parturition physiology, Pregnancy, Animal physiology

Abstract

The lack of scientific data concerning whether parturition in the queen proceeds normally or not may prevent veterinarians and cat owners from recognizing parturition problems in time. A questionnaire-based study of parturition in 197 queens was performed to determine several parameters of parturition and their influence on its progress. The mean length of gestation was 65.3 days (range 57 to 72 days) and it decreased with increasing litter size (P = 0.02). The median litter size was 4.5 kittens (range 1 to 9), with more males (53%) than females (46%) (P = 0.05). Sixty-nine percent of the kittens were born in anterior presentation and 31% in posterior presentation, indicating that either can be considered normal in the cat. Males were born in posterior position (34%) more often than females (26%) (P = 0.03). The mean birth weight was 98 g (range of 35 to 167 g) and decreased with increasing litter size (P < 0.01). Mean birth weight was higher in males and kittens born in posterior presentation (P < 0.01). Forty-four (5%) of the 887 kittens were stillborn. This was not correlated with the presentation at expulsion but stillborn kittens were more often female (P = 0.02) and weighed less than those born alive (P = 0.04). The median interkitten time was 30 min (range 2 to 343 min) and 95% were born within 100 min after expulsion of the preceding kitten. The interkitten time as a measure of the progress of parturition was not influenced by the kitten's gender, presentation at expulsion, birth weight, or stillbirth, or by the parity of the queen. The results of this study can be used to develop reference values for parturition parameters in the queen, both to determine whether a given parturition is abnormal and as the basis for a parturition protocol., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

18. Effects of the 3β-hydroxysteroid dehydrogenase inhibitor trilostane on luteal progesterone production in the dog.

Author

de Gier J, Wolthers CH, Galac S, Okkens AC, and Kooistra HS

Subjects

17-Hydroxysteroid Dehydrogenases antagonists & inhibitors, Adrenal Cortex drug effects, Adrenal Cortex metabolism, Adrenal Cortex physiology, Animals, Dihydrotestosterone pharmacology, Enzyme Inhibitors pharmacology, Female, Luteal Phase blood, Luteal Phase metabolism, Luteal Phase physiology, Ovulation blood, Ovulation drug effects, Ovulation metabolism, Ovulation physiology, Pregnancy, Progesterone blood, Prolactin blood, Prolactin metabolism, Time Factors, Dihydrotestosterone analogs & derivatives, Dogs, Luteal Phase drug effects, Progesterone metabolism

Abstract

Interference with the pregnancy-maintaining influence of progesterone is the basis of most methods for termination of unwanted pregnancy in dogs. The currently available methods are based on induction of luteolysis or blocking of the progesterone receptor. Inhibition of progesterone synthesis using a competitive inhibitor of 3β-hydroxysteroid dehydrogenase (3β-HSD) could be another strategy to terminate unwanted pregnancies. In this study we investigated the effects of the 3β-HSD inhibitor trilostane on corpus luteum function in non-pregnant bitches. Trilostane was administered orally for seven consecutive days in either the pituitary-independent part of the luteal phase (PIP, start of treatment on D11 after ovulation, n = 6) or the pituitary-dependent part (PDP, start of treatment on D31 after ovulation, n = 6), in an oral dose of about 4.5 mg/kg bw, twice daily. Results were compared with those obtained in control bitches (n = 6). ACTH stimulation tests were performed to assess adrenocortical reserve capacity. Trilostane caused no apparent side effects and ACTH stimulation tests revealed good suppression of cortisol secretion. Trilostane also caused a significant decrease in plasma progesterone concentration. When it was stopped during PIP, progesterone secretion was completely restored and there was no difference in the length of the luteal phase between those dogs and control dogs (99 days, range 70-138 d and 99 d, range 60-112 d, respectively). When trilostane was stopped during PDP there was no post-treatment recovery of progesterone secretion and although the luteal phase tended to be shorter (66 d, range 41-101 d) the difference was not significant (P = 0.09). Plasma prolactin concentration did not increase after the trilostane-induced decrease in plasma progesterone. The interoestrous interval in dogs treated during PIP (234 d, range 175-269 d) or PDP (198 d, range 120-287 d) was not significantly shorter than the control interval (247 d, range 176-313 d). In conclusion, trilostane treatment was effective in decreasing plasma progesterone concentration in bitches during the luteal phase, but the dose regimen used in this study produced less clear-cut inhibition of ovarian steroidogenesis than have other strategies to decrease plasma progesterone concentration. Further studies are warranted to determine whether trilostane can be used to terminate unwanted pregnancy in the bitch without inducing adrenocortical insufficiency., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

19. The pituitary-ovarian axis in dogs with remnant ovarian tissue.

Author

Buijtels JJ, de Gier J, Kooistra HS, Naan EC, Oei CH, and Okkens AC

Subjects

Animals, Estradiol blood, Estrous Cycle blood, Female, Gonadotropin-Releasing Hormone pharmacology, Luteinizing Hormone blood, Ovariectomy veterinary, Ovary diagnostic imaging, Ovary surgery, Progesterone blood, Ultrasonography, Dogs physiology, Ovary pathology, Pituitary Gland physiology

Abstract

It can be difficult to confirm the presence of remnant ovarian tissue (ROT) in bitches that are presumed to be ovariohysterectomised. A GnRH stimulation test can be used to distinguish ovariectomised bitches from those in anoestrus, but it is uncertain whether the GnRH-induced changes in plasma LH and oestradiol concentrations that occur in intact bitches also occur in ROT-bitches. We report here eighteen ROT-bitches and compare the results of GnRH stimulation tests with those of six ovariectomised and six bitches in anoestrus. The basal (n = 17) and/or GnRH-stimulated (n = 18) plasma oestradiol concentration was above the detection limit of the assay, i.e., < 7 pmol/l, in all ROT-bitches but below the detection limit in all ovariectomised bitches. Basal plasma LH concentration was significantly higher in ROT-bitches (4.1 ± 0.7 μg/L) than those in anoestrus (0.64 ± 0.04 μg/L), and significantly lower than in ovariectomised bitches (20.2 ± 3.6 μg/L). Basal plasma LH concentration was relatively high in bitches in which there was a long interval between ovariectomy and appearance of oestrus. GnRH administration resulted in a significant increase in plasma LH and oestradiol concentrations in ROT-bitches. The GnRH-induced increase and subsequent decline in plasma LH concentration were significantly less in ROT-bitches than in either ovariectomised bitches or those in anoestrus. The GnRH-induced increase in plasma oestradiol concentration was significantly smaller in ROT-bitches than in those in anoestrus. In conclusion, the results of this study demonstrate that in dogs ROT is associated with noticeable changes in the pituitary-ovarian axis and suggest that a GnRH stimulation test may be used to distinguish between completely ovariectomised bitches and those with ROT., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

20. Alterations of the pituitary-ovarian axis in dogs with a functional granulosa cell tumor.

Author

Buijtels JJ, de Gier J, Kooistra HS, Kroeze EJ, and Okkens AC

Subjects

Animals, Dogs, Estradiol blood, Female, Gonadotropin-Releasing Hormone pharmacology, Granulosa Cell Tumor diagnostic imaging, Granulosa Cell Tumor metabolism, Luteinizing Hormone blood, Ovarian Neoplasms diagnostic imaging, Ovarian Neoplasms metabolism, Ovariectomy, Ovary drug effects, Ovary pathology, Pituitary Gland drug effects, Ultrasonography, Dog Diseases metabolism, Granulosa Cell Tumor veterinary, Ovarian Neoplasms veterinary, Ovary metabolism, Pituitary Gland metabolism

Abstract

Information on the pituitary-ovarian axis in dogs with a granulosa cell tumor (GCT) is lacking. Therefore, we investigated the plasma concentrations of luteinizing hormone (LH) and estradiol before and after gonadotropin-releasing hormone (GnRH) administration in seven bitches with a functional GCT (GCT-total), of which three were intact (GCT-intact) and four had remnant ovarian tissue (GCT-ROT). The results of the GnRH stimulation test were compared with those in six anestrous and six ovariectomized bitches. The most noteworthy results were as follows. The basal plasma LH concentrations of the GCT-ROT bitches were higher (P<0.05) than those of the anestrous bitches. The increment in the plasma LH concentration after GnRH administration in the GCT-total bitches was lower (P<0.001) than the increments in both the anestrous and ovariectomized bitches. The basal plasma estradiol concentrations in the GCT-total bitches were higher (P<0.001) than those in the anestrous and ovariectomized bitches. In conclusion, the pituitary-ovarian axis is affected in bitches with a functional GCT and is characterized by relatively high plasma LH concentrations in GCT-ROT bitches and a subnormal LH response to GnRH stimulation in all GCT bitches compared with those in anestrous and ovariectomized bitches. The relatively high proportion of dogs with remnant ovarian tissue among the GCT bitches suggests a pathogenetic role for elevated gonadotropin secretion in the pathogenesis of GCT.

Published

2010

21. Minimal external masculinization in a SRY-negative XX male Podenco dog.

Author

Buijtels JJ, de Gier J, van Haeften T, Kooistra HS, Spee B, Veldhuis Kroeze EJ, Zijlstra C, and Okkens AC

Subjects

Animals, DNA analysis, Disorders of Sex Development, Estradiol blood, Female, Genitalia, Female anatomy & histology, Genitalia, Female diagnostic imaging, Gonadotropin-Releasing Hormone administration & dosage, Luteinizing Hormone blood, Male, Phenotype, Polymerase Chain Reaction, Sex Determination Processes, Sex-Determining Region Y Protein genetics, Testis anatomy & histology, Testis growth & development, Testosterone blood, Ultrasonography, Dogs genetics, Sex Differentiation genetics, Sex-Determining Region Y Protein analysis

Abstract

Normal mammalian sex differentiation takes place in three genetically controlled steps: chromosomal sex determination (XX or XY), gonadal differentiation and development of the phenotypic sex. Animals are considered to be sex reversed if chromosomal sex determination and gonadal development are not in agreement. In this report, sex reversal is described in a 1.5-year-old Podenco dog that was referred because of suspected recurrent growth of a previously removed os clitoridis in the vulva. With that exception the dog was phenotypically female, but had never been in oestrus and exhibited male behaviour. Abdominal ultrasonography showed a small tubular structure dorsal to the bladder, consistent with a uterus. An ovoid structure resembling a gonad was visible between the right kidney and inguinal canal. Plasma testosterone concentrations before and after GnRH administration indicated the presence of functional testicular tissue. Two testes, each with its epididymis and ductus deferens, and a complete bicornuate uterus were removed surgically. Cytogenetic analysis of peripheral blood lymphocytes showed a normal female karyotype (78, XX). These findings are consistent with the diagnosis of an XX male. PCR analysis of genomic DNA revealed that the SRY gene was absent. In summary, this report describes the first SRY-negative XX male Podenco dog with an almost complete female phenotype despite high basal and stimulated plasma testosterone concentrations. It is hypothesized that the clinical observations in this dog may have been caused by reduced and delayed Müllerian-inhibiting substance secretion and the absence of conversion of testosterone to dihydrotestosterone due to 5alpha-reductase deficiency.

Published

2009

22. Physiology of the canine anoestrus and methods for manipulation of its length.

Author

de Gier J, Beijerink NJ, Kooistra HS, and Okkens AC

Subjects

Animals, Bromocriptine, Dogs blood, Estrous Cycle blood, Estrous Cycle physiology, Estrus drug effects, Estrus physiology, Female, Follicle Stimulating Hormone blood, Gonadotropin-Releasing Hormone blood, Luteinizing Hormone blood, Prolactin antagonists & inhibitors, Prolactin blood, Time Factors, Anestrus blood, Anestrus drug effects, Anestrus physiology, Dogs physiology, Dopamine Agonists pharmacology, Estrous Cycle drug effects, Serotonin Antagonists pharmacology

Abstract

Progression from early to late anoestrus is characterized by the appearance of a larger number of gonadotrophin-releasing hormone (GnRH) pulses with a higher amplitude, an increase in the sensitivity of the pituitary to GnRH, an increase in ovarian responsiveness to gonadotrophins, and an increase in basal plasma follicle-stimulating hormone (FSH) concentration. A period of increased luteinizing hormone (LH) pulsatility has been observed shortly before the onset of pro-oestrus. Apart from these changes in the hypothalamus-pituitary-ovary axis, the initiation of a new follicular phase in the bitch is also stimulated by dopaminergic influences other than the accompanying plasma prolactin decrease. Metergoline, a drug which in a low dosage lowers the plasma prolactin concentration via a serotonin-antagonistic pathway, does not shorten the anoestrus; while bromocriptine, in a dosage insufficient to cause a decrease in the plasma prolactin concentration, does prematurely induce a follicular phase. These observations indicate that it is not the decrease in the plasma prolactin concentration, but another dopamine-agonistic influence that plays a crucial role in the transition to a new follicular phase. The dopamine-agonist induced oestrus is associated with a rapid rise in the basal plasma FSH concentration, similar to what is observed during the physiological late anoestrus. Administration of GnRH, eCG and oestrogens may also be used to induce oestrus but with variable results. Oestrus can be prevented surgically or medically, for which purpose progestagens are the most important drugs. The mechanism is still unclear, although it has been demonstrated that with continuing medroxyprogesterone acetate (MPA) treatment the FSH response to GnRH stimulation decreases and changes occur in the pulsatile release of the gonadotrophins. In general, LH pulses coincide with a FSH pulse, but during MPA treatment, LH pulses were observed while there was such a small increase in FSH that it was not recognized as significant FSH pulse.

Published

2008

23. Estriolum treatment in the bitch: a risk for uterine infection?

Author

Schotanus BA, de Gier J, van der Lugt JJ, and Okkens AC

Subjects

Animals, Diagnosis, Differential, Dog Diseases diagnostic imaging, Dog Diseases etiology, Dog Diseases pathology, Dogs, Empyema diagnosis, Empyema etiology, Estriol administration & dosage, Female, Hysterectomy veterinary, Ovariectomy veterinary, Ultrasonography, Urinary Incontinence drug therapy, Urinary Incontinence veterinary, Uterine Diseases diagnosis, Uterine Diseases etiology, Dog Diseases diagnosis, Empyema veterinary, Estriol adverse effects, Uterine Diseases veterinary

Abstract

Purulent vaginal discharge in a bitch in which ovariohysterectomy has been performed is often caused by inflammation of the uterine stump. The inflammation is due to either cystic endometrial hyperplasia (CEH) induced primarily by progesterone from remnant ovarian tissue or exogenous progestagens, or it is due to the presence of unabsorbed suture material. This report describes a 9-year-old Irish setter with hemopurulent vaginal discharge and non-pruritic symmetrical alopecia, which had undergone ovariohysterectomy 3.5 years ago and which had been treated with estriolum daily for the past 2.5 years because of urinary incontinence. Vaginoscopy revealed hemopurulent discharge throughout the vagina and vestibule. Cytological examination of ultrasound-guided fine-needle aspiration biopsies of a large mass in the hypogastricum, which appeared to be the uterine cervical stump, revealed septic purulent inflammation. The concentration of plasma progesterone was low and the concentration of plasma 17-ss oestradiol did not increase after gonadotrophin-releasing hormone administration. No remnant ovarian tissue was found by abdominal ultrasonography, laparotomy, or histological examination of mesovarian pedicles. Laparotomy revealed uterine stump empyema. Histological examination of the surgically removed mass excluded both CEH and unabsorbed suture material as the cause of the stump empyema. Instead, it is hypothesized that the long-term treatment with estriolum was a causative factor. This suggests that bitches treated with estriolum should be examined regularly.

Published

2008

24. Hormonal changes in spontaneous and aglépristone-induced parturition in dogs.

Author

Baan M, Taverne MA, de Gier J, Kooistra HS, Kindahl H, Dieleman SJ, and Okkens AC

Subjects

Adrenocorticotropic Hormone blood, Animals, Dinoprost analogs & derivatives, Dinoprost blood, Estradiol blood, Female, Follicle Stimulating Hormone blood, Hydrocortisone blood, Labor, Induced methods, Luteinizing Hormone blood, Pregnancy, Progesterone blood, Prolactin blood, Dogs physiology, Estrenes administration & dosage, Hormones blood, Labor, Induced veterinary, Parturition physiology

Abstract

To increase our understanding of the endocrine changes associated with parturition in dogs, plasma concentrations of progesterone (P4), 15-ketodihydroprostaglandin F(2alpha) (PGFM), estradiol-17-beta (E2beta), cortisol, ACTH, prolactin (PRL), LH, and FSH were measured in six spontaneously whelping bitches and in six bitches in which parturition was induced with the progesterone-receptor blocker aglépristone on day 58 of pregnancy. Expulsion of pups in the induced group took place in the presence of P4 concentrations that were still elevated. PGFM concentrations increased before parturition in both groups, but levels were lower in the induced bitches. PGFM levels reached a maximum in both groups during parturition and quickly decreased in the spontaneously whelping group after parturition, but remained elevated in the induced group. In both groups, cortisol concentrations reached similar maximum levels during the last 30 h before the onset of expulsion. During the 3 days postpartum, cortisol concentrations were higher in the induced group. The highly variable ACTH concentrations did not differ significantly throughout the study within or between groups. In both groups, E2beta concentrations decreased and PRL concentrations increased between the late gestational period and the 30-h period before parturition. Concentrations of both LH (spontaneously whelping group) and FSH (both groups) decreased between late gestation and the postpartum period. The results of this study illustrate the hormonal changes around parturition in the bitch, and reveal that aglépristone-induced parturition is associated with still incomplete luteolysis, an altered PGFM profile, and elevated postpartum cortisol concentrations as compared with spontaneously whelping dogs.

Published

2008

25. Differential regulation of the secretion of luteinizing hormone and follicle-stimulating hormone around the time of ovulation in the bitch.

Author

de Gier J, Kooistra HS, Djajadiningrat-Laanen SC, Dieleman SJ, and Okkens AC

Subjects

Animals, Dogs blood, Follicle Stimulating Hormone blood, Luteinizing Hormone blood, Progesterone blood, Time Factors, Dogs physiology, Estrous Cycle physiology, Follicle Stimulating Hormone metabolism, Luteinizing Hormone metabolism, Ovulation physiology

Abstract

Plasma concentrations of luteinizing hormone (LH) and follicle stimulating hormone (FSH) were determined 3-6 times daily in six Beagle bitches from the start of the follicular phase until 5 d after the estimated day of ovulation. The aim of the study was to gain more detailed information regarding the changes in and the temporal relation between these hormones around the time of ovulation. In all bitches, the pre-ovulatory LH surge was accompanied by a pre-ovulatory FSH surge. The mean duration of the pre-ovulatory FSH surge (110 +/- 8 h) was significantly longer than that of the pre-ovulatory LH surge (36 +/- 5 h). The FSH surge started concomitantly with the pre-ovulatory LH surge in four bitches, and 12 h before the start of the LH surge in the other two bitches. The pre-ovulatory LH surge had a bifurcated pattern in four bitches. The mean plasma LH concentration before (1.9 +/- 0.4 microg/L) and after (1.9 +/- 0.3 microg/L) the pre-ovulatory LH surge were similar. The mean plasma FSH concentration during the period 72-28 h before the pre-ovulatory LH surge (1.6 +/- 0.3 U/L) was lower (P < 0.001) than that during the period 100-144 h after the pre-ovulatory LH surge (3.1 +/- 0.2U/L). In conclusion, this study demonstrated concurrent pre-ovulatory surges of FSH and LH and provided more evidence for differential regulation of the secretion of FSH and LH.

Published

2006

26. Temporal relations between plasma concentrations of luteinizing hormone, follicle-stimulating hormone, estradiol-17beta, progesterone, prolactin, and alpha-melanocyte-stimulating hormone during the follicular, ovulatory, and early luteal phase in the bitch.

Author

de Gier J, Kooistra HS, Djajadiningrat-Laanen SC, Dieleman SJ, and Okkens AC

Subjects

Animals, Female, Follicle Stimulating Hormone blood, Luteinizing Hormone blood, Ovulation physiology, Time Factors, alpha-MSH blood, Dogs blood, Estradiol blood, Estrous Cycle blood, Gonadotropins, Pituitary blood, Progesterone blood, Prolactin blood

Abstract

Compared with other domestic animals, relatively little is known about the changes in, and temporal relations between, reproductive hormones around the time of ovulation in the domestic bitch. Therefore, plasma concentrations of luteinizing hormone (LH), follicle-stimulating hormone (FSH), estradiol-17beta, progesterone, prolactin (PRL), and alpha-melanocyte-stimulating hormone (alpha-MSH) were determined one to six times daily from the start of the follicular phase until 5 days after the estimated day of ovulation in six Beagle bitches. In all bitches, the pre-ovulatory LH surge was accompanied by a pre-ovulatory FSH surge. A pre-ovulatory PRL or alpha-MSH surge was not observed. The pre-ovulatory FSH and LH surges started concomitantly in four bitches, but in two bitches the FSH surge started 12 h earlier than the LH surge. The FSH surge (110+/-8 h) lasted significantly longer than the LH surge (36+/-5 h). In contrast with the pre-ovulatory FSH surge, the pre-ovulatory LH surge was bifurcated in four of six bitches. The mean plasma LH concentrations before (1.9+/-0.4 microg/L) and after (1.9+/-0.3 microg/L) the LH surge were similar, but the mean plasma FSH concentration before the FSH surge (1.6+/-0.3 U/L) was significantly lower than that after the FSH surge (3.1+/-0.2 U/L). In most bitches the highest plasma estradiol-17beta concentration coincided with or followed the start of the pre-ovulatory LH surge. In five of the six bitches the plasma progesterone concentration started to rise just before or concurrently with the start of the LH surge. In conclusion, the results of this study provide evidence for the differential regulation of the secretion of LH and FSH in the bitch. In addition, the interrelationship of the plasma profiles of estradiol-17beta and LH suggests a positive feedback effect of estradiol-17beta on LH surge release. The start of the pre-ovulatory LH surge is associated with an increase in the plasma progesterone concentration in this species.

Published

2006

27. Induction of parturition in the bitch with the progesterone-receptor blocker aglépristone.

Author

Baan M, Taverne MA, Kooistra HS, de Gier J, Dieleman SJ, and Okkens AC

Subjects

Animals, Animals, Newborn, Birth Weight, Female, Hematocrit, Labor, Induced methods, Litter Size, Male, Pregnancy, Progesterone blood, Dogs physiology, Estrenes therapeutic use, Labor, Induced veterinary, Parturition drug effects, Receptors, Progesterone antagonists & inhibitors

Abstract

The triggering mechanism for parturition in the bitch remains unclear. Consequently, the development of drugs to successfully induce parturition in the dog has been difficult. The aim of this study was to evaluate the efficacy of the progesterone-receptor blocker aglépristone for the induction of parturition in beagle bitches. The course of parturition was therefore investigated in six parturitions induced by aglépristone and in six spontaneous parturitions. In addition, data were collected on pup survival and growth rates. Aglépristone was administered twice with a 9h interval on day 58 of pregnancy. If parturition did not proceed a standard intervention protocol was applied. Expulsion of the first pup occurred between 32 and 56 h after the first treatment with aglépristone, at which time the plasma progesterone concentration was still elevated. Accordingly, the gestation length of the bitches in the induced group (59.5+/-0.2 days) was significantly shorter than that of the spontaneously whelping bitches (62.2+/-0.5 days). The expulsion phase length, the inter-pup interval, the number of puppies born dead, and the number of clinical interventions needed during parturition did not significantly differ between the spontaneously whelping and the induced group. Pup survival and mean birth weights in the two groups did not differ significantly and aglépristone treatment had no significant influence on the growth rates. The results of this study show that aglépristone is an effective drug which can be used safely for the induction of parturition in the dog.

Published

2005

28. Exact stationary state for an asymmetric exclusion process with fully parallel dynamics.

Author

de Gier J and Nienhuis B

Abstract

The exact stationary state of an asymmetric exclusion process with fully parallel dynamics is obtained using the matrix product ansatz. We give a simple derivation for the deterministic case by a physical interpretation of the dimension of the matrices. We prove the stationarity via a cancellation mechanism, and by making use of an explicit representation of the matrix algebra we easily find closed expressions for the correlation functions in the general probabilistic case. Asymptotic expressions, obtained by making use of earlier results, allow us to derive the exact phase diagram.

Published

1999

29. Recovery of storage and emptying functions of the urinary bladder after spinal anesthesia with lidocaine and with bupivacaine in men.

Author

Kamphuis ET, Ionescu TI, Kuipers PW, de Gier J, van Venrooij GE, and Boon TA

Subjects

Adult, Humans, Male, Middle Aged, Pressure, Urinary Bladder physiology, Urinary Tract anatomy & histology, Urinary Tract innervation, Anesthesia, Spinal, Anesthetics, Local pharmacology, Bupivacaine pharmacology, Lidocaine pharmacology, Urinary Bladder drug effects, Urination drug effects

Abstract

Background: The aim of this study was to evaluate and compare the effects of spinal anesthesia with lidocaine and with bupivacaine on urinary bladder function in healthy men who were scheduled for minor orthopaedic surgical procedures., Methods: Twenty men were randomly allocated to receive either bupivacaine or lidocaine. Before spinal anesthesia, filling cystometry was performed with the patient in the supine position and a pressure flow study was done with the patient in the standing position. After operation, cystometric measurements were continued until the patient could void urine spontaneously. The levels of analgesia and of motor blockade were recorded., Results: The urge to void disappeared immediately after injection of the local anesthetics. There was no difference in the duration of lower extremity motor blockade between bupivacaine and lidocaine. Detrusor blockade lasted significantly longer in the bupivacaine group (means +/- SD, 460 +/- 60 min) than in the lidocaine group (235 +/- 30 min). Total fluid intake and urine volume accumulated during the detrusor blockade were significantly higher in the bupivacaine group than in the lidocaine group. In the bupivacaine group, the total volume of accumulated urine (875 +/- 385 ml) was also significantly higher than cystometric bladder capacity (505 +/- 120 ml) with the risk of over distension of the bladder. Spontaneous voiding of urine did not occur until segmental sensory analgesia had regressed to the third sacral segment., Conclusions: Spinal anesthesia with lidocaine and with bupivacaine causes a clinically significant disturbance of bladder function due to interruption of the micturition reflex. The urge to void disappears quickly and bladder function remains impaired until the block has regressed to the third sacral segment in all patients. With long-acting local anesthetics, the volume of accumulated urine may exceed the cystometric bladder capacity. With respect to recovery of urinary bladder function, the use of short-acting local anesthetics for spinal anesthesia seems to be preferable.

Published

1998

30. Abnormal lipoprotein in cholestasis.

Author

Werre JM and De Gier J

Subjects

Humans, Cholestasis blood, Erythrocytes metabolism, Lipoprotein-X blood

Published

1995

31. The full length of a mitochondrial presequence is required for efficient monolayer insertion and interbilayer contact formation.

Author

Leenhouts JM, Török Z, Demel RA, de Gier J, and de Kruijff B

Subjects

Adrenodoxin metabolism, Aldehyde Dehydrogenase metabolism, Amino Acid Sequence, Animals, Anions chemistry, Biological Transport, Cattle, Cytochrome P-450 Enzyme System metabolism, Electron Transport Complex IV metabolism, Intracellular Membranes metabolism, Lipids chemistry, Mitochondria chemistry, Molecular Sequence Data, Phosphatidylcholines metabolism, Phosphatidylethanolamines chemistry, Phosphatidylethanolamines metabolism, Lipid Bilayers metabolism, Mitochondria metabolism, Protein Precursors chemistry, Protein Precursors metabolism, Protein Sorting Signals chemistry, Protein Sorting Signals metabolism

Abstract

The peptide specificity of both presequence-monolayer interactions and the ability of presequences to induce interbilayer contacts between large unilamellar vesicles was investigated. A range of different synthetic peptides that are documented for their mitochondrial protein import abilities were used for this purpose. Both monolayer insertion and vesicle aggregation were found to be strongly dependent on the primary structure of the studied presequence peptides. The combination of monolayer data and results of vesicle aggregation experiments leads to the overall suggestion that monolayer insertion and interbilayer contact formation are mechanistically related. For maximal effects the full length of a presequence peptide is required. The cardiolipin specificity of presequence-induced interbilayer contact formation previously reported was found to be a more general property among presequence peptides. The peptide's ability to induce vesicle-vesicle contacts seems to parallel the efficiency of its import ability into mitochondria. These results lead to an extended hypothesis on the role of presequence-induced contact site formation during the mitochondrial protein import process.

Published

1994

32. The cryoprotectant trehalose destabilises the bilayer organisation of Escherichia coli-derived membrane systems at elevated temperatures as determined by 2H and 31P-NMR.

Author

Fabrie CH, Smeets JM, de Kruijff B, and de Gier J

Subjects

Cell Membrane chemistry, Cell Membrane drug effects, Chemical Phenomena, Chemistry, Physical, Cold Temperature, Deuterium, Fatty Acids chemistry, Glycerol pharmacology, Heating, Lipids chemistry, Magnetic Resonance Spectroscopy methods, Membranes, Artificial, Models, Biological, Phospholipids chemistry, Phosphorus, Escherichia coli drug effects, Escherichia coli ultrastructure, Lipid Bilayers chemistry, Trehalose pharmacology

Abstract

In this study, 2H and 31P-NMR techniques were used to study the effects of trehalose and glycerol on phase transitions and lipid acyl chain order of membrane systems derived from cells of E. coli unsaturated fatty acid auxotroph strain K1059, which was grown in the presence of [11,11-2H2]-oleic acid or [11,11-2H2]-elaidic acid. From an analysis of the temperature dependence of the quadrupolar splitting it could be concluded that neither 1 M trehalose or glycerol generally had any significant effect on the temperature of the lamellar gel to liquid-crystalline phase transition. In the case of the oleate-containing hydrated total lipid extract, glycerol but not trehalose caused a 5 degrees C increase of this transition temperature. In general, both cryoprotectants induced an ordering of the acyl chains in the liquid-crystalline state. Trehalose and glycerol both decrease the bilayer to non-bilayer transition temperature of the hydrated lipid extract of oleate-grown cells by about 5 degrees C, but only trehalose in addition induces an isotropic to hexagonal (HII) phase transition. In the biological membranes, trehalose and not glycerol destabilised the lipid bilayer, and in the case of the E. coli spheroplasts, part of the induced non-bilayer structures is ascribed to a hexagonal (HII) phase in analogy with the total lipids. Interestingly, 1 mM Mg2+ was a prerequisite for the destabilisation of the lipid bilayer. In the hydrated total lipid extract of E. coli grown on the more ordered elaidic acid, both transition temperatures were shifted about 20 degrees C upwards compared with the oleate-containing lipid, but the effect of trehalose on the lipid phase behaviour was similar. The bilayer destabilising ability of trehalose might have implications for the possible protection of biological systems by (cryo-)protectants during dehydration, in that protection is unlikely to be caused by preventing the occurrence of polymorphic phase transitions.

Published

1994

33. The membrane potential has no detectable effect on the phosphocholine headgroup conformation in large unilamellar phosphatidylcholine vesicles as determined by 2H-NMR.

Author

Leenhouts JM, Chupin V, de Gier J, and de Kruijff B

Subjects

Benzothiazoles, Carbocyanines, Coloring Agents, Deuterium, Lipid Bilayers, Magnetic Resonance Spectroscopy methods, Molecular Conformation, Onium Compounds, Organophosphorus Compounds, Phosphatidylglycerols, Tetraphenylborate, Liposomes, Membrane Potentials, Phosphatidylcholines chemistry, Phosphorylcholine chemistry

Abstract

In this study the effect of a transmembrane electrical potential on the phospholipid headgroup conformation was investigated using the 2H-NMR technique. Large unilamellar vesicles were prepared of dioleoylphosphatidylcholine, specifically 2H-labeled at the alpha- or beta-position of the choline group. No conformational change of the phosphocholine headgroup could be detected after induction of a valinomycin-induced K(+)-diffusion potential across the bilayer. However, this method could be used to measure the redistribution of tetraphenylphosphonium across the bilayer in response to delta psi, which reorients the phosphocholine headgroups in the opposite bilayer-water interfaces.

Published

1993

34. Osmotic behaviour and permeability properties of liposomes.

Author

de Gier J

Subjects

Cell Membrane metabolism, Mathematics, Membrane Lipids chemistry, Membrane Lipids metabolism, Models, Theoretical, Osmolar Concentration, Permeability, Phosphatidic Acids chemistry, Lipid Bilayers chemistry, Liposomes chemistry, Phosphatidylcholines chemistry

Abstract

In this overview liposomes are described as bilayer-bounded vesicles which under defined conditions act as ideal osmometers according to the Boyle van't Hoff law. Investigations on osmotic volume changes, directly or indirectly by taking advantage of changes in light scattering, are considered and applications in permeability measurements are discussed. Solute-solvent interactions occurring in isotonic swelling experiments are analysed in view of an irreversible thermodynamic description. In a second part liquid crystalline lipid bilayers are characterized as highly selective permeability bilayers and the physical principles underlying this selectivity are considered. Attention is given to special physical and chemical conditions that may cause structural defects in the bilayer organization and can affect the selective permeability properties of the bilayer or completely deteriorate its barrier function. Finally an evaluation is given of intrinsic ionophoretic activity in lipid bilayers containing negatively charged lipids.

Published

1993

35. A novel property of a mitochondrial presequence. Its ability to induce cardiolipin-specific interbilayer contacts which are dissociated by a transmembrane potential.

Author

Leenhouts JM, de Gier J, and de Kruijff B

Subjects

Amino Acid Sequence, Animals, Membrane Potentials, Microspheres, Molecular Sequence Data, Cardiolipins metabolism, Electron Transport Complex IV metabolism, Intracellular Membranes metabolism, Mitochondria enzymology, Phosphatidylcholines metabolism, Protein Precursors metabolism, Protein Sorting Signals metabolism

Abstract

A new property of the presequence of the mitochondrial precursor protein cytochrome oxidase subunit IV is presented. This mitochondrial presequence induces interbilayer contacts between large unilamellar vesicles consisting of phosphatidylcholine and cardiolipin. The presequence-vesicle aggregates can be dissociated by applying a membrane potential across the bilayers (negative inside). These effects require the presence of cardiolipin and are not observed for other negatively charged phospholipids. We propose a role for the presequence in the formation and dissociation of mitochondrial contact sites.

Published

1993

36. The effect of a membrane potential on the interaction of mastoparan X, a mitochondrial presequence, and several regulatory peptides with phospholipid vesicles.

Author

de Kroon AI, de Gier J, and de Kruijff B

Subjects

Amino Acid Sequence, Cardiolipins chemistry, Circular Dichroism, Hydrogen-Ion Concentration, Intercellular Signaling Peptides and Proteins, Membrane Potentials, Mitochondria chemistry, Molecular Sequence Data, Spectrometry, Fluorescence, Tryptophan, Cosyntropin chemistry, Dynorphins chemistry, Electron Transport Complex IV chemistry, Enzyme Precursors chemistry, Peptides chemistry, Phospholipids chemistry, Protein Sorting Signals chemistry

Abstract

Recently the pH gradient evoked by a K+ diffusion potential was shown to translocate a synthetic monobasic amphipathic hexapeptide across the bilayer of lipid vesicles (De Kroon, A.I.P.M., Vogt, B., Van 't Hof, R., De Kruijff, B. and De Gier, J. (1991) Biophys. J. 60, in press). Here this observation is extended by studying the effect of a membrane potential on a set of bioactive peptides. The panel of peptides comprises the toxin mastoparan X, a tryptophan-containing analogue of the presequence of the mitochondrial protein cytochrome oxidase subunit IV (preCoxIV(1-25)W18), and the regulatory peptides ACTH(1-24), alpha-MSH, ACTH(1-10), dynorphin A, bombesin, and LHRH. The interaction of these peptides with phospholipid vesicles has been measured using the intrinsic tryptophan residue as fluorescent probe. In the absence of a K+ diffusion potential only mastoparan X and the presequence show considerable binding to vesicles consisting of phosphatidylcholine (PC). In contrast, under these conditions all peptides display affinity for vesicles consisting of the acidic phospholipid cardiolipin (CL), the extent of which depends on the net positive charge of the peptide. Application of a K+ diffusion potential to large unilamellar vesicles (LUV) consisting of PC results in a time dependent tryptophan fluorescence increase for mastoparan X, which is accelerated upon incorporating increasing amounts of CL into the LUV. A similar fluorescence increase in response to a K+ diffusion potential was observed for the above model peptide. Yet the mechanism resulting in the fluorescence increase of mastoparan X is completely different from that of the hexapeptide. Binding experiments indicate that a membrane potential-induced enhanced binding of the peptide to the outer surface of the vesicles contributes to the fluorescence increase. PreCoxIV(1-25)W18, dynorphin A, and ACTH(1-24) show fluorescence responses upon applying a membrane potential that are consistent with that of mastoparan X, whereas the other peptides tested do not respond up to a LUV CL content of 50%. The results tentatively suggest that the membrane potential only affects a peptide when it has the ability to adopt a stable membrane bound conformation.

Published

1991

37. Ion gradient-induced membrane translocation of model peptides.

Author

de Kroon AI, Vogt B, van't Hof R, de Kruijff B, and de Gier J

Subjects

Amino Acid Sequence, Hydrogen-Ion Concentration, Kinetics, Membrane Potentials, Membranes, Molecular Sequence Data, Osmolar Concentration, Peptides chemical synthesis, Protein Conformation, Liposomes, Models, Biological, Peptides chemistry, Phosphatidylcholines

Abstract

The K+ diffusion potential-induced association of synthetic model peptides carrying a single positive charge originating from the NH2-terminal amino function with large unilamellar vesicles (LUV) consisting of phosphatidylcholine (PC) has been reported previously (de Kroon, A. I. P. M., J. de Gier, and B. de Kruijff. 1989. Biochim. Biophys. Acta. 981:371-373). To determine the vesicle localization of the associated peptides, fluorescence measurements utilizing the peptides' tryptophan residue as intrinsic fluorescent probe were performed. The application in these measurements, of vesicles that exhibit an asymmetric transbilayer distribution of brominated PC which is a quencher of tryptophan fluorescence, unequivocally demonstrated that the peptide H3N(+)-AIMLWA-Ome (AIXme+) is accumulated in the interface of the inner leaflet of the vesicle membrane in response to the valinomycin-induced K+ diffusion potential (negative inside). The relative contributions of the membrane potential (delta psi) and the pH gradient (delta pH, acidic inside) induced by the K+ diffusion potential, to the process have been assessed. An analysis of the pH and delta pH dependencies of the process demonstrated that the K+ diffusion potential-induced peptide accumulation is largely determined by a redistribution of peptide according to the transbilayer pH gradient, in agreement with a translocation across the vesicle membrane of the neutral, deprotonated form of the peptide. The general validity of the mechanism proposed for the vesicle-uptake of AIXme+ has been examined by extending the experiments to peptide analogues with a single negative charge and to peptides with two positive charges, and by investigating the effect of incorporating the acidic phospholipid cardiolipin (CL) into the LUV. The incorporation of CL appeared not to affect the K+ diffusion, potential-induced vesicle uptake of AIXme+. The peptide H3N(+)-RMLWA-Ome (RXme2+) showed a small delta pH independent fluorescence response to the delta psi upon raising the CL content of the vesicles to 25%.

Published

1991

38. The membrane interaction of amphiphilic model peptides affects phosphatidylserine headgroup and acyl chain order and dynamics. Application of the "phospholipid headgroup electrometer" concept to phosphatidylserine.

Author

de Kroon AI, Killian JA, de Gier J, and de Kruijff B

Subjects

Amino Acid Sequence, Biological Transport, Deuterium, Freezing, Lipid Bilayers chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Phosphatidylserines chemistry, Solubility, Thermodynamics, Lipid Bilayers metabolism, Phosphatidylserines metabolism

Abstract

Deuterium nuclear magnetic resonance (2H NMR) was used to study the interaction of amphiphilic model peptides with model membranes consisting of 1,2-dioleoyl-sn-glycero-3-phospho-L-serine deuterated either at the beta-position of the serine moiety ([2-2H]DOPS) or at the 11-position of the acyl chains ([11,11-2H2]DOPS). The peptides are derived from the sequences H-Ala-Met-Leu-Trp-Ala-OH (AX, one-letter code with X = MLWA) and H-Arg-Met-Leu-Trp-Ala-OH (RX+) and contain a positive charge of +1 (AXme+) or +2 (RXme2+) at the amino terminus or one positive charge at each end of the molecule (AXetN2+). Upon titration of dispersions of DOPS with the peptides, the divalent peptides show a similar extent of binding to the DOPS bilayers, which is larger than that of the single charged peptide. Under these conditions the values of the quadrupolar splitting (delta vq) of both [2-2H]DOPS and [11,11-2H2]DOPS are decreased, indicating that the peptides reduce the order of both the DOPS headgroup and the acyl chains. The extent of the decrease depends on the amount of peptide bound and on the position of the charged moieties in the peptide molecule. The effects exerted by the peptides on the delta vq value of [2-2H]DOPS are consistent with the PS headgroup responding as a molecular electrometer to the surface charge resulting from the presence of the peptides in the lipid-water interface. The effects on the acyl chain deuterons are in agreement with a localization of the peptides intercalated in between the lipid headgrouops.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1991

39. The role of charge and hydrophobicity in peptide-lipid interaction: a comparative study based on tryptophan fluorescence measurements combined with the use of aqueous and hydrophobic quenchers.

Author

De Kroon AI, Soekarjo MW, De Gier J, and De Kruijff B

Subjects

Amino Acid Sequence, Cardiolipins metabolism, Chemical Phenomena, Chemistry, Physical, Fluorescence, Fluorescent Dyes, Membrane Lipids chemistry, Molecular Sequence Data, Peptides chemical synthesis, Peptides chemistry, Phosphatidylcholines metabolism, Solubility, Lipid Bilayers, Liposomes metabolism, Membrane Lipids metabolism, Peptides metabolism, Tryptophan chemistry

Abstract

The interaction of interrelated model peptides with model membranes has been studied by techniques based on tryptophan fluorescence. The peptides used are derivatives of the sequence H-Ala-Met-Leu-Trp-Ala-OH, which was designed for this purpose. Several modifications yielded a set of 13 penta- and hexapeptides varying in net charge, hydrophobicity, charge distribution, and the intramolecular position of the tryptophan residue with respect to the charge(s). The affinity of these peptides for small unilamellar vesicles (SUV) consisting of zwitterionic egg phosphatidylcholine (eggPC) and negatively charged beef heart cardiolipin (bhCL) has been investigated in a comparative way. The criteria for affinity comprise (1) intrinsic fluorescence changes upon titration of the peptides with the lipid vesicles, (2) reduced accessibility of the peptides to aqueous quenchers of tryptophan fluorescence (I- and acrylamide) in the presence of lipid, and (3) exposure to membrane-incorporated fluorescence quenchers, brominated phosphatidylcholines (BrPC). Application of BrPC brominated at different positions along the acyl chains provided information on the membrane topology of the peptides. With respect to the extent of affinity for zwitterionic membranes, the overall hydrophobicity of the peptides is the main determinant. A comparison of the affinity for PC of equally hydrophobic peptides carrying either a single positive or negative charge reveals preferential interaction of the cationic peptide. Both hydrophobic and electrostatic interactions determine the affinity of positively charged mono- and divalent peptides for CL vesicles. The distribution of the charged moieties in divalent positively charged peptides, either both at one end of the molecule or one at each end, has little influence on the affinity of these peptides for CL but does affect the extent of exposure to BrPC. Upon decreasing the surface charge density of the vesicles by diluting CL with increasing amounts of PC, both types of peptides show different behavior. The position of the tryptophan relative to the charged moiety in the peptide molecule is shown to affect the fluorescent properties upon interaction with vesicles. Concerning the membrane topology, all peptides adopt a localization near the membrane surface, with the neutral peptides inserting slightly deeper into the bilayer than the charged peptides. The results allow a comparative analysis of the factors determining the extents and modes of lipid-model peptide interaction; in addition, the validity of the methods applied is discussed.

Published

1990

40. Gramicidin A induced fusion of large unilamellar dioleoylphosphatidylcholine vesicles and its relation to the induction of type II nonbilayer structures.

Author

Tournois H, Fabrie CH, Burger KN, Mandersloot J, Hilgers P, van Dalen H, de Gier J, and de Kruijff B

Subjects

Freeze Fracturing, Microscopy, Electron, Molecular Conformation, Permeability, Phosphatidylcholines, Structure-Activity Relationship, Gramicidin pharmacology, Liposomes, Membrane Fusion drug effects, Membrane Lipids

Abstract

The fusogenic properties of gramicidin were investigated by using large unilamellar dioleoylphosphatidylcholine vesicles. It is shown that gramicidin induces aggregation and fusion of these vesicles at peptide to lipid molar ratios exceeding 1/100. Both intervesicle lipid mixing and mixing of aqueous contents were demonstrated. Furthermore, increased static and dynamic light scattering and a broadening of 31P NMR signals occurred concomitant with lipid mixing. Freeze-fracture electron microscopy revealed a moderate vesicle size increase. Lipid mixing is paralleled by changes in membrane permeability: small solutes like carboxyfluorescein and smaller dextrans, FD-4(Mr approximately 4000), rapidly (1-2 min) leak out of the vesicles. However, larger molecules like FD-10 and FD-17 (Mr approximately 9400 and 17,200) are retained in the vesicles for greater than 10 min after addition of gramicidin, thereby making detection of contents mixing during lipid mixing possible. At low lipid concentrations (5 microM), lipid mixing and leakage are time resolved: leakage of CF shows a lag phase of 1-3 min, whereas lipid mixing is immediate and almost reaches completion during this lag phase. It is therefore concluded that leakage, just as contents mixing, occurs subsequent to aggregation and lipid mixing. Although addition of gramicidin at a peptide/lipid molar ratio exceeding 1/50 eventually leads to hexagonal HII phase formation and a loss of vesicle contents, it is concluded that leakage during fusion (1-2 min) is not the result of HII phase formation but is due to local changes in lipid structure caused by precursors of this phase. By making use of gramicidin derivatives and different solvent conformations, it is shown that there is a close parallel between the ability of the peptide to induce the HII phase and its ability to induce intervesicle lipid mixing and leakage. It is suggested that gramicidin-induced fusion and HII phase formation share common intermediates.

Published

1990

41. Protection by sugars against phase transition-induced leak in hydrated dimyristoylphosphatidylcholine liposomes.

Author

Fabrie CH, de Kruijff B, and de Gier J

Subjects

Biological Transport drug effects, Ethylene Glycols pharmacology, Lipid Bilayers metabolism, Sucrose pharmacology, Thermodynamics, Trehalose pharmacology, Carbohydrates pharmacology, Dimyristoylphosphatidylcholine metabolism, Liposomes metabolism

Abstract

The disaccharides trehalose and sucrose have small effects on temperature and enthalpy of the pre- and main phase transition in hydrated DMPC bilayers. In contrast, these sugars cause a considerable retention of carboxyfluorescein when large unilamellar vesicles of DMPC are heated through the main transition. This effect is sugar specific, as the monosaccharides glucose and fructose are less effective and ethyleneglycol has no effect at all.

Published

1990

42. The interaction of spectrin - actin and synthetic phospholipids.

Author

Mombers C, van Dijck PW, van Deenen LL, de Gier J, and Verkleij AJ

Subjects

Calcium pharmacology, Calorimetry, Differential Scanning, Freeze Fracturing, In Vitro Techniques, Magnesium pharmacology, Microscopy, Electron, Myristates metabolism, Phosphatidylcholines metabolism, Phosphatidylglycerols metabolism, Actins metabolism, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Liposomes, Membrane Proteins metabolism, Phospholipids metabolism, Spectrin metabolism

Abstract

Using differential scanning calorimetry and freeze fracture electron microscopy interactions were studied between lipids and a spectrin - actin complex isolated from human erythrocyte membranes. With dispersions of 1,2-dimyristoyl-sn-glycero-3-phosphocholine, 1,2-dimyristoyl-sn-glycero-3-phosphoglycerol and mixtures of these two compounds, which for experimental reasons were chosen as the lipid counterpart, such an interaction could clearly be deduced from changes in the temperature and the enthalpy of the phase transition. Furthermore it was demonstrated that the interaction with this membrane protein protects the bilayer against the action of Ca2+ and Mg2+ and prevents fusion of lipid vesicles which easily occurs in some of the systems when divalent ions were added to the pure lipid vesicles.

Published

1977

43. Membrane characteristics and osmotic fragility of red cells, fractionated with anglehead centrifugation and counterflow centrifugation.

Author

van der Vegt SG, Ruben AM, Werre JM, de Gier J, and Staal GE

Subjects

Cell Separation, Centrifugation methods, Centrifugation, Density Gradient, Erythrocyte Indices, Humans, Hypotonic Solutions, Male, Membrane Lipids analysis, Osmosis, Osmotic Fragility, Erythrocyte Aging, Erythrocyte Membrane metabolism

Abstract

Red cell populations were separated on the basis of differences in density using anglehead centrifugation and on the basis of differences in mean cell volume using counterflow centrifugation. In the different fractions, mean surface area was calculated, phospholipid and cholesterol content determined as well as the osmotic behaviour in hypotonic salt solutions. Older red cells appeared to be more resistant to hypotonic salt solutions, due to favourable surface area to volume ratio.

Published

1985

44. The effect of chain length and lipid phase transitions on the selective permeability properties of liposomes.

Author

Blok MC, van der Neut-Kok EC, van Deenen LL, and de Gier J

Subjects

Cations, Monovalent, Halogens, Osmolar Concentration, Osmosis, Permeability, Potassium, Temperature, Fatty Acids, Liposomes, Phosphatidylcholines

Abstract

This paper describes experiments showing the importance of the fatty acid chain length on the barrier properties of liposomal bilayers, prepared from saturated lecithins, under conditions of lateral phase separation. 1. Above the gel to liquid crystalline phase transition temperature, liposomes prepared from saturated lecithins with 14 or more carbon atoms per acyl chain exist as stable bilayers, which are practically impermeable to ions. 2. At temperatures well above the transition temperature dilauroyl phosphatidylcholine liposomes exhibited osmotic shrinkage, which was dependent on the ionic size of the solute used to bring about the osmotic gradient, indicating that the permeation through these less stable bilayers takes place mainly via individual diffusion of the permeating ions. 3. An enhanced release of trapped potassium from liposomes was demonstrated in the vicinity of the transition temperature. The extent of the increase, however, depended strongly on the length of the paraffin chain. 4. From measurements of the shrinkage behaviour of liposomes in the vicinity of the transition temperature it is concluded that the increased permeability decreases with increasing diameter of the permeating ion. This finding implies that the increased permeability at the transition temperature cannot be ascribed to "macroscopic" rupture of the liposomal membrane. The maximum permeability in the vicinity of the Tc is discussed in terms of probability and size distribution of statistical pore formation at the boundaries of liquid and solid domains.

Published

1975

45. Barrier properties of lecithin/lysolecithin mixtures.

Author

Mandersloot JG, Reman FC, Van Deenen LL, and De Gier J

Subjects

Binding Sites, Birefringence, Kinetics, Light, Liposomes, Models, Biological, Molecular Conformation, Permeability, Potassium, Scattering, Radiation, Surface Properties, Water, X-Ray Diffraction, Lysophosphatidylcholines, Membranes, Artificial, Phosphatidylcholines

Abstract

Light scattering, birefringence and X-ray studies showed that liposomes, with lipid molecules orientated in bilayers, are formed from egg licithin/lysolecithin mixtures up to 50 mol percent of lysolecithin; above this concentration much smaller mixed micelles are formed. Permeability studies demonstrated a dramatic increase in the permeability of the liposomes when the lyso concentration exceeds 22.5 mol percent. X-ray studies indicated a significant decrease in bilayer thickness with increasing lysolecithin concentration. It is suggested that decreased interaction energy between the lipid molecules in the bilayer is responsible for the inability of the thin bilayers to act as an effective permeability barrier.

Published

1975

46. Lipid-lipid and lipid-protein interaction in model systems and membranes.

Author

van Deenen LL, de Gier J, Demel RA, de Kruyff B, Blok MC, van der Neut-Kok EC, Haest CW, Ververgaert PH, and Verkleij AJ

Subjects

Acholeplasma laidlawii, Amphotericin B pharmacology, Cations, Divalent metabolism, Cations, Monovalent, Cell Membrane drug effects, Cell Membrane ultrastructure, Chemical Phenomena, Chemistry, Physical, Filipin pharmacology, Freeze Etching, Freeze Fracturing, Models, Biological, Structure-Activity Relationship, Anti-Bacterial Agents pharmacology, Cell Membrane metabolism, Cell Membrane Permeability drug effects, Lipid Metabolism, Membranes, Artificial, Proteins metabolism

Published

1975

47. Hydrolysis of phosphatidylcholine liposomes by pancreatic phospholipase A2 at the transition temperature.

Author

Op den Kamp JA, de Gier J, and van Deenen LL

Subjects

Animals, Bees, Binding Sites, Chromatography, Thin Layer, Lysophosphatidylcholines, Pancreas enzymology, Phosphatidylcholines, Swine, Temperature, Venoms, Water, Liposomes, Phospholipases

Published

1974

48. The effect of cholesterol incorporation on the temperature dependence of water permeation through liposomal membranes prepared from phosphatidylcholines.

Author

Blok MC, Van Deenen LL, and De Gier J

Subjects

Biological Transport, Calorimetry, Kinetics, Models, Biological, Permeability, Temperature, Thermodynamics, Cholesterol, Liposomes, Membranes, Phosphatidylcholines, Water

Abstract

The permeation of water through liposomal membranes composed of phosphatidylcholine plus varying amounts of cholesterol was studied as a function of temperature. 1. Increasing amounts of cholesterol caused a gradual disappearance of the abrupt change in the rate of water permeation near the gel to liquid-crystalline phase transition temperature of dipalmitoylphosphatidylcholine and dimyristoylphosphatidylcholine liposomes. At cholesterol concentrations above about 30 mol % there was no longer a discontinuity in the rate of water permeation. 2. The incorporation of cholesterol produces a steep change in the activation energy of the water permeation above the transition temperature of the saturated lecithin occurring at about 15 mol % of cholesterol. Below the transition temperature there was a gradual decrease in the activation energy of the water permeation in the region of 0 to 33 mol % of cholesterol. 3. In systems containing unsaturated phosphatidylcholines cholesterol also enhanced the activation energy of the water permeation although to a lesser extent. The results indicate that the position of the cis-double bond in the fatty acid chain is very important in this respect. 4. In systems in which cholesterol increased the temperature dependence of the water permeation there is also an enhancement of the temperature dependence of the isotonic glycerol and erythritol swelling by the same number of kcal/mol.

Published

1977

49. Calcium-induced changes in permeability of dioleoylphosphatidylcholine model membranes containing bovine heart cardiolipin.

Author

Smaal EB, Schreuder C, van Baal JB, Tijburg PN, Mandersloot JG, de Kruijff B, and de Gier J

Subjects

Animals, Arsenazo III metabolism, Calcimycin pharmacology, Calcium metabolism, Cattle, Lipid Bilayers metabolism, Micelles, Permeability, Potassium metabolism, Calcium pharmacology, Cardiolipins metabolism, Membranes, Artificial, Phosphatidylcholines metabolism

Abstract

At calcium concentrations up to about 4 mM a selective permeability increase of cardiolipin/dioleoylphosphatidylcholine (50:50, mol%) membranes for calcium and its chelator arsenazo III is observed. Under these conditions calcium does not occupy all the binding sites of cardiolipin at the membrane interface and no vesicle-vesicle interactions are found. Lowering of the cardiolipin content of the vesicles to 20 mol% extends the calcium concentration range in which a selective permeability for calcium and arsenazo III is appearing up to about 12 mM. We suggest that the observed selective permeability increase is caused by transient formation of inverted micellar structures in the membrane with cardiolipin as translocating membrane component for calcium and arsenazo III. At calcium concentrations of 4 mM and higher for 50 mol% cardiolipin-containing vesicles a general permeability increase is found together with calcium-cardiolipin binding in a 1:1 stoichiometry, vesicles aggregation and, above 8 mM of calcium, vesicle fusion. The loss of barrier function of the membrane under these conditions is correlated with vesicle aggregation and may be explained by a transition from a bilayer into a hexagonal HII organization of the phospholipids.

Published

1987

50. Gramicidin-induced hexagonal HII phase formation in erythrocyte membranes.

Author

Tournois H, Leunissen-Bijvelt J, Haest CW, de Gier J, and de Kruijff B

Subjects

Erythrocyte Membrane drug effects, Erythrocyte Membrane ultrastructure, Freeze Fracturing, Humans, Magnetic Resonance Spectroscopy methods, Microscopy, Electron methods, Molecular Conformation, X-Ray Diffraction methods, Erythrocyte Membrane physiology, Gramicidin pharmacology, Liposomes, Membrane Lipids blood

Abstract

Using 31P nuclear magnetic resonance (NMR), small-angle X-ray scattering (SAXS), and freeze-fracture electron microscopic (FFEM) techniques, it is shown that gramicidin induces a hexagonal HII phase not only in liposomes prepared from total lipids extracted from human erythrocytes but also in isolated human erythrocyte membranes (white ghosts). A 37 degrees C, HII phase formation is detected at a gramicidin to phospholipid molar ratio exceeding 1:80. At a molar ratio of 1:5, about 30% of the phospholipid is organized in the HII phase. The gramicidin-induced HII phase exhibits a very small 31P chemical shift anisotropy [(CSA) approximately 10 +/- 1 ppm], indicating decreased head-group order, and it displays a temperature-dependent increase in tube diameter from 60.2 A at 4 degrees C to 64.2 A at 37 degrees C in ghosts and from 62.8 to 69.4 A at 37 degrees C in total lipid extracts, both in the presence of 1 mol of gramicidin/10 mol of phospholipid. This anomalous temperature-dependent behavior is probably due to the presence of cholesterol. 31P NMR data indicate that the HII phase formation by gramicidin is temperature dependent and show the gradual disappearance of the HII phase at low temperatures (less than 20 degrees C), resulting in a bilayer type of 31P NMR line shape at 4 degrees C, whereas SAXS and FFEM data suggest equal amounts of HII phases at all temperatures. This apparent discrepancy is probably the result of a decrease in the rate of lateral diffusion of the membrane phospholipids which leads to incomplete averaging of the 31P CSA in the HII phase.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1987