Your search keyword '"Ezan E"' showing total 129 results

101. Erythromycin increases plasma concentrations of alpha-dihydroergocryptine in humans.

Author

de Mey C, Althaus M, Ezan E, and Retzow A

Subjects

Administration, Oral, Adult, Analysis of Variance, Anti-Bacterial Agents pharmacology, Area Under Curve, Cross-Over Studies, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System metabolism, Drug Administration Schedule, Enzyme Inhibitors administration & dosage, Erythromycin administration & dosage, Humans, Male, Mixed Function Oxygenases metabolism, Radioimmunoassay, Cytochrome P-450 Enzyme Inhibitors, Dihydroergotoxine urine, Dopamine Agonists urine, Enzyme Inhibitors pharmacology, Erythromycin pharmacology, Mixed Function Oxygenases antagonists & inhibitors

Abstract

Objective: Our objective was to investigate the potential for relevant pharmacotherapeutic interaction between cytochrome P4503A4 (CYP3A4)-inhibiting agents such as erythromycin and the dopamine agonist alpha-dihydroergocryptine (DHEC)., Methods: The study was carried out as a single-center, controlled, nonblinded, 2-way crossover clinical trial with randomly allocated period-balanced sequences, investigating two treatments of a single oral dose of 10 mg DHEC (on the morning of day 1), once administered alone (reference), once along with a 4-day treatment (days -2 to 1) of 500 mg erythromycin 3 times daily. Periods were separated by a washout of at least 14 days. Nine healthy white male volunteers, 22 to 42 years old, with a body weight range of 58 to 90 kg (body mass index, 20.2-25.1 kg x m(-2)) began the study. One subject discontinued prematurely, and 8 concluded the study in accordance with the study protocol., Results: The plasma and urinary pharmacokinetics of DHEC and its metabolites were characterized by a large variability. Concomitant treatment with erythromycin led to respective increases of 9.5 (95% confidence interval [CI], 6.5 to 13.9) and 16.5 (95% CI, 8.7 to 31.5) times the maximum observed plasma drug concentration and the area under the time course of the plasma concentrations up to the last quantifiable concentration after dosing of unchanged DHEC (determined by radioimmunoassay). The 24-hour urinary excretion was on average 11 times larger (95% CI, 5.9 to 20.7). Qualitatively similar findings were recorded for the total of DHEC plus metabolites (as determined by enzyme immunoassay)., Conclusions: The concomitant use of erythromycin or similarly CYP3A4-inhibiting agents along with direct dopaminergic agonists such as the ergoline DHEC may cause a clinically relevant increase in pharmacokinetic exposure, which may induce exaggerated dopaminergic effects.

Published

2001

102. Long-term effect of N-acetyl-seryl-aspartyl-lysyl-proline on left ventricular collagen deposition in rats with 2-kidney, 1-clip hypertension.

Author

Rhaleb NE, Peng H, Yang XP, Liu YH, Mehta D, Ezan E, and Carretero OA

Subjects

Animals, Blood Pressure drug effects, Cell Division drug effects, Collagen metabolism, Dose-Response Relationship, Drug, Heart drug effects, Heart Rate drug effects, Heart Ventricles metabolism, Hypertension, Renovascular physiopathology, Hypertrophy, Left Ventricular pathology, Macrophages drug effects, Macrophages pathology, Male, Monocytes drug effects, Monocytes pathology, Myocardium pathology, Oligopeptides blood, Rats, Rats, Sprague-Dawley, Time Factors, Collagen drug effects, Heart Ventricles drug effects, Hypertension, Renovascular metabolism, Oligopeptides pharmacology

Abstract

Background: N-acetyl-seryl-aspartyl-lysyl-proline (Ac-SDKP) is a natural inhibitor of pluripotent hematopoietic stem cell proliferation. Ac-SDKP plasma concentration is increased 5-fold after angiotensin-converting enzyme inhibition. Here we studied the effect of Ac-SDKP on monocyte/macrophage infiltration, fibroblast proliferation, and collagen deposition in the rat heart in renovascular hypertension., Methods and Results: We investigated whether long-term Ac-SDKP administration would prevent left ventricular (LV) hypertrophy and interstitial collagen deposition in rats with 2-kidney, 1-clip (2K-1C) hypertension. Ac-SDKP (400 microgram. kg(-1). d(-1)) did not affect development of hypertension. Mean blood pressure was similar in rats with 2K-1C hypertension whether they were given vehicle or Ac-SDKP and was higher than in controls. Both LV weight and cardiomyocyte size were significantly increased in rats with 2K-1C hypertension compared with controls and were unaffected by Ac-SDKP. Proliferating cell nuclear antigen- and monocyte/macrophage-positive cells were increased in the LV of 2K-1C hypertensive rats; this increase was significantly blunted by Ac-SDKP (P<0.001). LV interstitial collagen fraction was also increased in 2K-1C hypertensive rats given vehicle (10.1+/-0.8%) compared with sham (5.3+/-0.1%, P<0.0001), and this increase was prevented by Ac-SDKP (5.4+/-0.4%, P<0.001)., Conclusions: Ac-SDKP inhibited monocyte/macrophage infiltration, cell proliferation, and collagen deposition in the LV of hypertensive rats without affecting blood pressure or cardiac hypertrophy, suggesting that it may be partly responsible for the cardioprotective effect of angiotensin-converting enzyme inhibitors.

Published

2001

103. RXP 407, a selective inhibitor of the N-domain of angiotensin I-converting enzyme, blocks in vivo the degradation of hemoregulatory peptide acetyl-Ser-Asp-Lys-Pro with no effect on angiotensin I hydrolysis.

Author

Junot C, Gonzales MF, Ezan E, Cotton J, Vazeux G, Michaud A, Azizi M, Vassiliou S, Yiotakis A, Corvol P, and Dive V

Subjects

Animals, Blood Pressure drug effects, Dose-Response Relationship, Drug, Hydrolysis, Indicators and Reagents, Lisinopril pharmacology, Male, Mice, Oligopeptides blood, Peptidyl-Dipeptidase A blood, Peptidyl-Dipeptidase A drug effects, Time Factors, Angiotensin I metabolism, Angiotensin-Converting Enzyme Inhibitors pharmacology, Oligopeptides antagonists & inhibitors, Oligopeptides pharmacology, Peptidyl-Dipeptidase A chemistry, Phosphinic Acids pharmacology

Abstract

The phosphinic peptide RXP 407 has recently been identified as the first potent selective inhibitor of the N-active site (domain) of angiotensin-converting enzyme (ACE) in vitro. The aim of this study was to probe the in vivo efficacy of this new ACE inhibitor and to assess its effect on the metabolism of AcSDKP and angiotensin I. In mice infused with increasing doses of RXP 407 (0.1--30 mg/kg/30 min), plasma concentrations of AcSDKP, a physiological substrate of the N-domain, increased significantly and dose dependently toward a plateau 4 to 6 times the basal levels. RXP 407 significantly and dose dependently inhibited ex vivo plasma ACE N-domain activity, whereas it had no inhibitory activity toward the ACE C-domain. RXP 407 (10 mg/kg) did not inhibit the pressor response to an i.v. angiotensin I bolus injection in mice. In contrast, lisinopril infusion (5 and 10 mg/kg/30 min) affected the metabolism of both AcSDKP and angiotensin I. Thus, RXP 407 is the first ACE inhibitor that might be used to control selectively AcSDKP metabolism with no effect on blood pressure regulation.

Published

2001

104. Development of an enzyme immunoassay for a stable amidated analog of the hemoregulatory peptide acetyl-Ser-Asp-Lys-Pro.

Author

Junot C, Theodoro F, Thierry J, Clement G, Wdzieczak-Bakala J, and Ezan E

Subjects

Animals, Humans, Immune Sera, Mice, Mice, Inbred CBA, Oligopeptides chemistry, Oligopeptides pharmacokinetics, Protein Conformation, Reproducibility of Results, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Amides chemistry, Immunoenzyme Techniques methods, Oligopeptides analysis

Abstract

The tetrapeptide Acetyl-Ser-Asp-Lys-Pro (AcSDKP) has been shown to protect hematopoietic stem cells from the toxicity of anticancer chemotherapies. Since its pharmacological efficacy is limited by a rapid degradation by Angiotensin-I Converting Enzyme (ACE), AcSDKP analogs resistant to ACE have been synthesized. One of these compounds (AcSDKP-NH,) differs from the native AcSDKP by amidation of the C-terminus. Further evaluations of this molecule require an analytical method in order to characterize its pharmacokinetic profile. We report, here, the development of a highly specific and sensitive enzyme immunoassay (EIA) for AcSDKP-NH, thatdoes not cross-react with endogenous or exogenous AcSDKP. Using AcSDKP-NH2-acetylcholinesterase conjugate as a tracer, rabbit specific antiserum and microtiter plates coated with goat anti-rabbit immunoglobulins, this EIA allows the determination of AcSDKP-NH2 with limits of quantitation of 1 nM in mouse plasma and 100 pmol/g in tissues. Intra-day and inter-day coefficients of variations were less than 20%. The method was successfully applied to a pharmacokinetic study in order to compare plasma and tissue profiles of AcSDKP-NH2 and AcSDKP. Plasma AcSDKP-NH2 levels were found higher than those of AcSDKP, with AUCinf and Cmax values, respectively, 26- and 10-fold higher than that of AcSDKP.

Published

2001

105. Lack of angiotensin II-facilitated erythropoiesis causes anemia in angiotensin-converting enzyme-deficient mice.

Author

Cole J, Ertoy D, Lin H, Sutliff RL, Ezan E, Guyene TT, Capecchi M, Corvol P, and Bernstein KE

Subjects

Angiotensin II blood, Animals, Blood Pressure drug effects, Erythrocyte Indices, Female, Genotype, Hematocrit, Kidney physiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Peptidyl-Dipeptidase A blood, Peptidyl-Dipeptidase A genetics, Systole, Anemia blood, Angiotensin II pharmacology, Erythropoiesis drug effects, Peptidyl-Dipeptidase A deficiency

Abstract

While nephrologists often observe reduced hematocrit associated with inhibitors of angiotensin-converting enzyme (ACE), the basis for this effect is not well understood. We now report that two strains of ACE knockout mice have a normocytic anemia associated with elevated plasma erythropoietin levels. (51)Cr labeling of red cells showed that the knockout mice have a normal total blood volume but a reduced red cell mass. ACE knockout mice, which lack tissue ACE, are anemic despite having normal renal function. These mice have increased plasma levels of the peptide acetyl-SDKP, a possible stem cell suppressor. However, they also show low plasma levels of angiotensin II. Infusion of angiotensin II for 2 weeks increased hematocrit to near normal levels. These data suggest that angiotensin II facilitates erythropoiesis, a conclusion with implications for the management of chronically ill patients on inhibitors of the renin-angiotensin system.

Published

2000

106. Captopril inhibits in vitro and in vivo the proliferation of primitive haematopoietic cells induced into cell cycle by cytotoxic drug administration or irradiation but has no effect on myeloid leukaemia cell proliferation.

Author

Chisi JE, Briscoe CV, Ezan E, Genet R, Riches AC, and Wdzieczak-Bakala J

Subjects

Animals, Antimetabolites, Antineoplastic pharmacology, Cell Division drug effects, Cell Line, Cells, Cultured, Cytarabine pharmacology, Interleukin-3 pharmacology, Leukemia, Myeloid immunology, Leukemia, Myeloid metabolism, Macrophage Colony-Stimulating Factor pharmacology, Mice, Mice, Inbred Strains, Oligopeptides metabolism, Peptidyl-Dipeptidase A blood, Recombinant Proteins pharmacology, S Phase, Angiotensin-Converting Enzyme Inhibitors pharmacology, Captopril pharmacology, Hematopoietic Stem Cells drug effects

Abstract

Angiotensin I-converting enzyme (ACE) has been shown to be involved in the catabolism of the tetrapeptide acetyl-Ser-Asp-Lys-Pro (AcSDKP). As AcSDKP is a physiological inhibitor of haematopoietic stem cell proliferation, we investigated the in vitro and in vivo effects of captopril, one of the specific inhibitors of ACE, on the proliferation of primitive haematopoietic cells. Regenerating bone marrow cells obtained from mice given one injection of cytosine arabinoside (100 mg/kg) as well as SA2 myeloid leukaemia cells were incubated in vitro for 24 h with 10-6 M captopril. Captopril significantly reduced the proportion of high proliferative potential colony-forming cells (HPP-CFC-1) in S-phase, whereas it had no effect on the proportion of SA2 leukaemic colony-forming cells in S-phase. When given in vivo to mice 1 h after 2 Gy gamma-irradiation or cytosine arabinoside (AraC) injection, captopril (100 mg/kg) was shown to prevent HPP-CFC-1 entry into S-phase induced by these cytotoxic treatments. The observed effects correlated with a reduction in ACE degradative activity and an increase in the level of endogenous AcSDKP both in the supernatants of captopril-treated bone marrow cells and in plasma of treated animals. The present findings suggest that AcSDKP might mediate the observed in vitro and in vivo inhibitory effects of captopril on primitive haematopoietic cell proliferation.

Published

2000

107. A sensitive amphotericin B immunoassay for pharmacokinetic and distribution studies.

Author

Machard S, Theodoro F, Benech H, Grognet JM, and Ezan E

Subjects

Amphotericin B administration & dosage, Amphotericin B blood, Animals, Biological Assay, Humans, Mice, Rabbits, Reproducibility of Results, Sensitivity and Specificity, Tissue Distribution, Amphotericin B pharmacokinetics, Immunoenzyme Techniques

Abstract

Since currently used assays of amphotericin B (AMB) lack sensitivity or are not easily adaptable in all laboratories, we have developed an enzyme immunoassay for AMB in biological fluids and tissues. Antibodies to AMB were raised in rabbits after administration of an AMB-bovine serum albumin conjugate. The enzymatic tracer was obtained by coupling AMB via its amino group to acetylcholinesterase (EC 3.1.1.7). These reagents were used for the development of a competitive immunoassay performed on microtitration plates. The limit of quantification was 100 pg/ml in plasma and 1 ng/g in tissues. The plasma assay was performed directly without extraction on a minimal volume of 0.1 ml. The intra- and interassay coefficients of variation were in the range of 5 to 17%, and the recoveries were 92 to 111% for AMB added to human plasma. The assay was applied to a pharmacokinetic study with mice given AMB intraperitoneally at the dose of 1 mg/kg. The drug distribution in selected compartments (plasma, liver, spleen, lung, and brain) was monitored until 72 h after administration. In conclusion, our assay is at least 100-fold more sensitive than previously described bioassays or chromatographic determinations of AMB and may be useful in studying the tissue pharmacokinetics of new AMB formulations and in drug monitoring in clinical situations.

Published

2000

108. Nonadherence with angiotensin-converting enzyme inhibitor therapy: a comparison of different ways of measuring it in patients with chronic heart failure.

Author

Struthers AD, MacFadyen R, Fraser C, Robson J, Morton JJ, Junot C, and Ezan E

Subjects

Aged, Angiotensin I blood, Angiotensin II blood, Biomarkers blood, Biomarkers urine, Chronic Disease, Diuretics therapeutic use, Drug Therapy, Combination, Echocardiography, Furosemide therapeutic use, Heart Failure diagnosis, Heart Failure metabolism, Humans, Oligopeptides blood, Oligopeptides urine, Peptidyl-Dipeptidase A blood, Radionuclide Ventriculography, Treatment Outcome, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Heart Failure drug therapy, Lisinopril therapeutic use, Treatment Refusal statistics & numerical data

Abstract

Objectives: This study was designed to compare different proposed methods of assessing adherence with angiotensin-converting enzyme (ACE) inhibitor (ACEI) therapy in chronic heart failure., Background: The use of ACEIs in chronic heart failure gives us a unique opportunity to assess a patient's adherence by measuring whether the expected biochemical effect of an ACEI is present in the patient's bloodstream. In fact, there are several different ways of assessing ACE in vivo: these are serum ACE activity itself, plasma N-acetyl-seryl-aspartyl-lysyl-proline (AcSDKP), urine AcSDKP, plasma angiotensin I (AI), plasma angiotensin II (AII), or the AII/AI ratio., Methods: Patients with chronic heart failure (n = 39) were randomized to regimens of ACEI nonadherence for one week, ACEI adherence for one week or two versions of partial adherence for one week, after which the above six tests were performed., Results: All six tests significantly distinguished between full nonadherence for one week and full or partial adherence. Only plasma AcSDKP produced a significantly different result between partial adherence and either full adherence or full nonadherence for one week. In terms of their ability to distinguish full nonadherence from full adherence, plasma AcSDKP was 89% sensitive and 100% specific with an area under its ROC of 0.95. Corresponding figures for urine AcSDKP were 92%, 97% and 0.95 and for serum ACE they were 86%, 95% and 0.90., Conclusions: All six tests distinguished full nonadherence from all other forms of adherence. The rank order of performance was plasma AcSDKP, urine AcSDKP, serum ACE, AII/AI ratio and plasma AII followed by plasma AI.

Published

1999

109. Effect of angiotensin-converting enzyme inhibition on plasma, urine, and tissue concentrations of hemoregulatory peptide acetyl-Ser-Asp-Lys-Pro in rats.

Author

Junot C, Nicolet L, Ezan E, Gonzales MF, Menard J, and Azizi M

Subjects

Animals, Bone Marrow drug effects, Bone Marrow metabolism, Dose-Response Relationship, Drug, Growth Inhibitors blood, Growth Inhibitors urine, Kidney drug effects, Kidney metabolism, Lung drug effects, Lung metabolism, Male, Oligopeptides blood, Oligopeptides urine, Proteins metabolism, Rats, Rats, Wistar, Tissue Distribution, Angiotensin-Converting Enzyme Inhibitors pharmacology, Captopril pharmacology, Growth Inhibitors metabolism, Oligopeptides metabolism

Abstract

The hemoregulatory peptide Acetyl-Ser-Asp-Lys-Pro (AcSDKP) has been reported to accumulate in plasma and urine after the oral administration of angiotensin-converting enzyme (ACE) inhibitors in humans. It is unknown whether such an accumulation also occurs in tissues. We administered captopril (3, 10, or 30 mg/kg) orally for 2 weeks to Wistar rats. In a second experiment, captopril (10 mg/kg) was administered for 9 days and was followed by a 1-h i.v. infusion of either AcSDKP (0.1 or 2 mg/kg) or saline on day 9. Captopril alone dose-dependently increased plasma AcSDKP by a factor of 3 to 5 and urine AcSDKP by a factor of 3. It slightly increased renal and pulmonary AcSDKP concentrations but did not affect AcSDKP concentrations in bone marrow and spleen. The combination of AcSDKP (2 mg/kg) and captopril gave very high AcSDKP concentrations in plasma and urine and increases in AcSDKP concentration by factors of 27 in kidney, 5.5 in lung, and 6.9 in the extracellular fraction of bone marrow. In contrast, no change was observed in the AcSDKP concentration in spleen and in the intracellular fraction of bone marrow. In conclusion, during chronic ACE inhibition in rats, AcSDKP levels slightly increased in organs with high ACE contents. No such increase occurred in hematopoietic organs. AcSDKP had to be combined with captopril to significantly increase its concentration in tissues other than the spleen. The possibility of pharmacologically increasing AcSDKP levels in the extracellular fraction of bone marrow may be of value for protecting hematopoietic cells from the toxicity of cancer chemotherapy.

Published

1999

110. In vivo assessment of captopril selectivity of angiotensin I-converting enzyme inhibition: differential inhibition of acetyl-ser-asp-lys-pro and angiotensin I hydrolysis.

Author

Junot C, Menard J, Gonzales MF, Michaud A, Corvol P, and Ezan E

Subjects

Animals, Captopril administration & dosage, Hydrolysis, Injections, Intravenous, Kinetics, Male, Rats, Rats, Inbred SHR, Renin blood, Substrate Specificity, Time Factors, Angiotensin I metabolism, Angiotensin-Converting Enzyme Inhibitors pharmacology, Captopril pharmacology, Oligopeptides pharmacokinetics, Peptidyl-Dipeptidase A blood

Abstract

Angiotensin I-converting enzyme (ACE) is a zinc metallopeptidase that plays a major role in blood pressure regulation. The demonstration that the hemoregulatory peptide acetyl-Ser-Asp-Lys-Pro (AcSDKP) is a natural and specific substrate of the N-active site of ACE suggests that this enzyme may have a new physiological role such as the modulation of hematopoietic stem cells. In vitro studies have shown that ACE inhibitors displayed various potencies in inhibiting the degradation of different natural or synthetic substrates of ACE, among which captopril inhibits AcSDKP hydrolysis more potently than angiotensin I hydrolysis. To look for this selectivity in vivo, we investigated the pharmacodynamic effect of increasing doses of captopril (0.01-10 mg/kg) during the 90 min after i.v. administration to spontaneously hypertensive rats. Plasma and urinary AcSDKP levels were measured. The renin-angiotensin system was evaluated by measurements of ACE activity in plasma samples, using the synthetic substrate Hip-His-Leu, by determinations of plasma renin concentrations and measurements of arterial blood pressure. The results showed that captopril (0.01-0.3 mg/kg) selectively inhibited AcSDKP hydrolysis, with limited effects on the renin-angiotensin system. AcSDKP levels in plasma and urine rose to a plateau 4 times the basal level for doses more than 0.3 mg/kg. All of the parameters reflecting the renin-angiotensin system were significantly affected at doses of 1 and 10 mg/kg. The present study therefore confirms that captopril can be used to protect hematopoietic stem cells during antitumor chemotherapy while having only a limited effect on cardiovascular homeostasis.

Published

1999

111. Lisinopril, an angiotensin I-converting enzyme inhibitor, prevents entry of murine hematopoietic stem cells into the cell cycle after irradiation in vivo.

Author

Rousseau-Plasse A, Wdzieczak-Bakala J, Lenfant M, Ezan E, Genet R, Robinson S, Briscoe T, Melville J, and Riches A

Subjects

Animals, Cell Cycle radiation effects, Cell Division drug effects, Cell Division radiation effects, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells radiation effects, Mice, Mice, Inbred BALB C, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Cell Cycle drug effects, Gamma Rays, Hematopoietic Stem Cells drug effects, Lisinopril therapeutic use

Abstract

The hemoregulatory peptide N-Acetyl-Ser-Asp-Lys-Pro (AcSDKP) has been shown in vivo to inhibit the cycling of murine hematopoietic stem cells triggered into S-phase by either cytotoxic drug administration or irradiation. This property, further confirmed using in vitro models, demonstrates that the peptide has an in vivo protective effect on the hematopoietic system. AcSDKP has been shown to be a physiological substrate of angiotensin I-converting enzyme (ACE), which catabolizes the peptide through a dipeptidasic activity. Thus, oral administration of ACE inhibitor to humans has led to an increase in the plasma AcSDKP concentration. In the present paper, we report on the in vivo effect of lisinopril, an ACE inhibitor, on the proliferative status of murine hematopoietic stem cells triggered into S-phase by irradiation. Administration of lisinopril (10 mg/kg) 1 hour after irradiation led to a 90 to 100% inhibition of murine plasma ACE activity as observed during the first 4 hours postirradiation. This inhibition was correlated with a 600% increase in the endogenous plasma AcSDKP level and a total suppression at 24 hours of entry of the hematopoietic stem cell into the cell cycle. We discuss the possible role of ACE in the regulation of hematopoietic stem cell proliferation through control of the AcSDKP concentration.

Published

1998

112. Bromocriptine modulates P-glycoprotein function.

Author

Orlowski S, Valente D, Garrigos M, and Ezan E

Subjects

Animals, Biological Transport, Active, Bromocriptine metabolism, Bromocriptine pharmacokinetics, Ca(2+) Mg(2+)-ATPase antagonists & inhibitors, Cell Line, Transformed, Cricetinae, Dopamine Agonists pharmacology, Drug Resistance, Drug Resistance, Multiple, Hydroxylation, Kinetics, Progesterone pharmacology, Vincristine pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Bromocriptine pharmacology

Abstract

The multidrug resistance (MDR)-associated P-glycoprotein (P-gp) is a membrane transporter which carries, at the expense of MgATP hydrolysis, many amphiphilic molecules, such as the MDR-related cytotoxic drugs vincristine and vinblastine, and the MDR-reversing agents verapamil and progesterone. We have tested the effects on P-gp function of bromocriptine (BCT), an ergot alkaloid known as a D2 dopaminergic receptor agonist. BCT (at 4 microM) partially reverses the P-gp-mediated vincristine resistance of the Chinese hamster lung fibroblasts DC-3F/ADX, a MDR cell line. P-gp containing membrane vesicles prepared from the DC-3F/ADX cells exhibit, in the absence of any added drug, a basal MgATPase activity due to P-gp. BCT inhibits this basal ATPase activity, with a half-inhibiting concentration of 0.30 +/- 0.15 microM. BCT also inhibits the verapamil-induced P-gp ATPase stimulation competitively (Ki approximately 0.2 microM), and the progesterone-induced P-gp ATPase stimulation non-competitively (Ki approximately 0.07-0.10 microM). BCT also non-competitively inhibits the vinblastine-dependent P-gp ATPase activity within the same concentration range. Hydroxylated metabolites of BCT have different effects on P-gp ATPase, only the monohydroxylated being able to modulate both the basal and the drug-stimulated ATPase activities. In conclusion, these effects of BCT on P-gp function can be linked to a specific interaction with P-gp, probably involving inhibition of P-gp-mediated drug transport.

Published

1998

113. High plasma level of N-acetyl-seryl-aspartyl-lysyl-proline: a new marker of chronic angiotensin-converting enzyme inhibition.

Author

Azizi M, Ezan E, Nicolet L, Grognet JM, and Ménard J

Subjects

Adolescent, Adult, Aged, Aldosterone blood, Angiotensin-Converting Enzyme Inhibitors administration & dosage, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Angiotensins blood, Biomarkers blood, Female, Humans, Male, Middle Aged, Peptidyl-Dipeptidase A blood, Renin blood, Renin-Angiotensin System physiology, Sensitivity and Specificity, Time Factors, Angiotensin-Converting Enzyme Inhibitors pharmacology, Oligopeptides blood

Abstract

The acute administration of the angiotensin-converting enzyme (ACE) inhibitor captopril to healthy subjects transiently increases 5.5-fold the plasma levels of a natural stem-cell regulator, N-acetyl-seryl-aspartyl-lysyl-proline (Ac-SDKP). The aim of this study was to measure plasma Ac-SDKP levels during chronic treatment with all types of ACE inhibitors and to assess its relevance as a marker of ACE inhibition. Plasma levels of Ac-SDKP were blindly determined in age- and sex-matched hypertensive patients either treated (ACEI group, n=27) or not (non-ACEI group, n=23) with an ACE inhibitor for more than 1 month. Geometric mean [range] of plasma Ac-SDKP levels were significantly higher in the ACEI group (3.78 [1.48 to 14.5] pmol/mL) than in the non-ACEI group, with no overlap between the groups (0.75 [0.36 to 1.22] pmol/mL, P<.0001). The measurement of Ac-SDKP in plasma discriminated all the patients of the ACEI group, whereas the simultaneous determination of either in vitro (using hippuryl-histidine-leucine as substrate) or in vivo (angiotensin II/angiotensin I ratio) ACE activity failed to identify nine and five cases, respectively. We conclude that Ac-SDKP accumulates in plasma during chronic ACE inhibitor treatment. The long-term consequences of Ac-SDKP accumulation are unknown. The reliability of plasma Ac-SDKP measurement makes it the best marker of chronic ACE inhibition, which can help to verify patients' compliance to ACE inhibitor treatment.

Published

1997

114. An enzyme immunoassay for rat growth hormone: validation and application to the determination of plasma levels and in vitro release.

Author

Ezan E, Laplante E, Bluet-Pajot MT, Mounier F, Mamas S, Grouselle D, Grognet JM, and Kordon C

Subjects

Acetylcholinesterase metabolism, Animals, Binding, Competitive, Cross Reactions, Culture Media chemistry, Growth Hormone blood, Growth Hormone immunology, Human Growth Hormone analysis, Human Growth Hormone immunology, Humans, Molecular Weight, Pituitary Gland, Anterior chemistry, Rabbits, Rats, Recombinant Proteins analysis, Sensitivity and Specificity, Growth Hormone analysis, Immunoenzyme Techniques

Abstract

A competitive enzyme immunoassay for rat growth hormone (rGH) has been developed using polyclonal anti-rGH antibodies and an acetylcholinesterase (EC 3.1.1.7.) enzymatic tracer coupled covalently with rGH. The assay was performed in 96-well microtiter plates coated with rabbit polyclonal anti-goat immunoglobulin antibodies. Molecular sieve filtration and Western blot analysis revealed a single immunoreactive peak for rat plasma or pituitary extracts. Cross-reactivity with other rat pituitary hormones or human GH was less than 1%. Assay of samples in a concentration range of 0.7 to 69 ng/ml by enzyme immunoassay and radioimmunoassay were well correlated (r = 0.87 and 0.85 respectively for plasma and culture medium samples). Intra- and inter-assay variations in plasma were 4 (n = 24) and 14% (n = 9) respectively. Minimal detectable amounts of rGH were 0.6 ng/ml. A two-site immunometric assay also developed with the same antibodies allowed a detection threshold of 0.25 ng/ml.

Published

1997

115. Metabolite involvement in bromocriptine-induced prolactin inhibition in rats.

Author

Valente D, Delaforge M, Urien S, Guivarc'h D, Vienet R, Grognet JM, and Ezan E

Subjects

Animals, Bromocriptine metabolism, Male, Prolactin metabolism, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Bromocriptine pharmacology, Dopamine Agonists pharmacology, Prolactin antagonists & inhibitors

Abstract

Bromocriptine (BCT) is a dopamine D2 receptor agonist used for the treatment of Parkinson's disease and hyperprolactinemic disorders. After oral administration, BCT is metabolized into mono- or dihydroxylated metabolites. To study how these metabolites influence parent drug pharmacodynamics, we administered BCT to rats intravenously (1 mg/kg i.v.) and orally (10 mg/kg p.o.) and measured the inhibition of prolactin secretion. Despite similar areas under the curve for BCT, the duration of the effect was 36 h after oral and only 18 h after intravenous administration. Pharmacokinetic/pharmacodynamic models were used to correlate the concentration of BCT in the effect compartment with the lowering of prolactin. One of these models (effect compartment model) showed that the effective concentration (EC50) at the site of action was much lower after oral (0.56 nM) than after intravenous administration (3.68 nM). In contrast, the EC50 values based on BCT metabolite data were in the same range for both administrations. These observations suggested the activity of one or more BCT metabolites. To confirm this hypothesis, hydroxylated metabolites of BCT (produced in vitro by rat liver microsomes) were administered i.v. (100 microg/kg) in rats. We found that monohydroxylated BCT was able to lower prolactin secretion like BCT. Dihydroxylated metabolites, as well as monohydroxylated metabolites, were effective in reducing in vitro prolactin secretion. Because we demonstrated that the concentration of hydroxylated metabolites after oral administration is 55-fold that of BCT, it can be concluded that BCT activity in the pituitary after oral administration is mediated by its metabolites.

Published

1997

116. Effect of variability of plasma interferences on the accuracy of drug immunoassays.

Author

Ezan E, Emmanuel A, Valente D, and Grognet JM

Subjects

Drug Monitoring, Humans, Immunoassay methods, Plasma immunology

Abstract

Most immunoassays applied to drugs in human plasma do not use an extraction of analyte. To compensate for interferences due to plasma proteins or salts, standards are prepared in drug-free plasma. Because the concentration of plasma components varies from one subject to another, it is likely that the drug-free plasma is not representative of the potential interference in each plasma. Using two immunoassays, for a steroid (nomegestrol acetate) and a heptapeptide (BN 52080), the authors have shown that tracer binding to the antibody may vary significantly between plasma from different subjects. Intersubject variability of tracer-antibody binding was 21.6% (coefficient of variation for 25 subjects) for nomegestrol acetate. When the same plasma were spiked with the steroid at a concentration corresponding to the central part of the standard curve, the recovery was between 39 and 215%. Intersubject variability in tracer binding was lower (7.7%) for the peptide immunoassay, but still affected accuracy. The authors show that this problem is common to direct immunoassays for other drugs and must be solved in assay development.

Published

1997

117. Enzyme immunoassays for bromocriptine and its metabolites.

Author

Valente D, Ezan E, Créminon C, Delaforge M, Benech H, Pradelles P, and Grognet JM

Subjects

Administration, Oral, Animals, Antibody Specificity, Bromocriptine administration & dosage, Bromocriptine immunology, Cross Reactions, Injections, Intravenous, Male, Rabbits, Rats, Rats, Sprague-Dawley, Reproducibility of Results, Bromocriptine analysis, Bromocriptine metabolism, Immunoenzyme Techniques standards

Abstract

We have developed two bromocriptine enzyme immunoassays with different specificities for applications in human and animal pharmacokinetic studies. The first assay uses antibodies directed against the cyclopeptide structure of bromocriptine, and is specific for untransformed bromocriptine. The second assay uses antibodies directed against the bromolysergic part of the molecule and allows the measurement of both bromocriptine and its metabolites. Enzymatic tracers were obtained by covalent coupling of bromocriptine analogs to acetylcholinesterase from the electric eel Electrophorus electricus. Both assays have a limit of detection of 10 pg/ml and a limit of quantification of 50 pg/ml. The specificity of the assays was determined following fractionation by high-performance liquid chromatography of rat samples obtained after administration of bromocriptine.

Published

1996

118. Bioequivalence study of alpha-dihydroergocryptine: utility of metabolite evaluation.

Author

Ezan E, Ardouin T, Delhotal Landes B, Flouvat B, Hanslik T, Legeai JM, and Grognet JM

Subjects

Adrenergic alpha-Antagonists blood, Adrenergic alpha-Antagonists chemistry, Adrenergic alpha-Antagonists metabolism, Adult, Caffeine blood, Caffeine metabolism, Central Nervous System Stimulants blood, Central Nervous System Stimulants metabolism, Cross-Over Studies, Dihydroergotoxine blood, Dihydroergotoxine chemistry, Dihydroergotoxine metabolism, Humans, Male, Therapeutic Equivalency, Adrenergic alpha-Antagonists pharmacokinetics, Dihydroergotoxine pharmacokinetics

Abstract

Metabolite assessment is an open question in bioequivalence studies. In situations of low absorption, high first-pass metabolism, and intrasubject variability, metabolites may reflect absorption more adequately than the parent drug, and their determination may help decision-making in bioequivalence issues. Treating alpha-dihydroergocryptine (DHECT) as a model, we used both unchanged DHECT and a pool of DHECT metabolites to evaluate the bioequivalence of 2 oral DHECT formulations (reference-R and test-T) in 12 subjects. DHECT and its metabolites were immunoassayed. There was no difference between the 2 formulations in terms of the AUC0-infinity (area under the curve) values determined from unchanged DHECT or DHECT with metabolites profiles: 572 +/- 490 pg/ml.h (R) and 442 +/- 276 pg/ml.h (T) for unchanged DHECT, and 7,141 +/- 2,936 pg/ml.h (R) and 6,941 +/- 1,462 pg/ml.h (R) for DHECT with metabolites. Confidence intervals were within the ranges 0.8-1.25 (AUC0-infinity) and 0.7-1.43 (Cmax) for DHECT with metabolites but not for unchanged DHECT. This study describes a particular case where only measurements on the basis of the metabolites can justify the assumption of bioequivalence.

Published

1996

119. Pharmcokinetics in healthy volunteers and patients of NAc-SDKP (seraspenide), a negative regulator of hematopoiesis.

Author

Ezan E, Carde P, Le Kerneau J, Ardouin T, Thomas F, Isnard F, Deschamps de Paillette E, and Grognet JM

Subjects

Adult, Aged, Humans, Injections, Intramuscular, Injections, Subcutaneous, Male, Metabolic Clearance Rate, Middle Aged, Oligopeptides administration & dosage, Hematopoiesis drug effects, Neoplasms metabolism, Oligopeptides pharmacokinetics

Abstract

NAc-SDKP is a peptide being tested as a bone marrow hematopoiesis protector in chemotherapy trials in cancer patients. We studied the pharmacokinetics of NAc-SDKP in six healthy human volunteers and in five patients undergoing chemotherapy. Plasma concentrations of NAc-SDKP were monitored using a specific enzyme immunoassay. Because NAc-SDKP is an endogenous compound, a preliminary study was undertaken to determine intra- and interday baseline variations in healthy subjects. The baseline value (range 1.7-3.2 nM) differed between subjects, but was constant over time. The influence of the route of administration was studied in six healthy volunteers with 128 nmol/kg given as a 12-hr intravenous infusion or as a single subcutaneous or intramuscular injection. After cessation of intravenous infusion in healthy volunteers, NAc-SDKP was characterized by a quick elimination phase, with a mean half-life of 4.5 min. The volume distribution was 117 ml/kg and the area under the curve was 117 nM hr. After subcutaneous and intramuscular administrations, peak plasma drug concentrations occurred at 0.26 and 0.28 hr, with Cmax values of 156 and 110 nM, respectively. The bioavailabilities determined after subcutaneous and intramuscular administrations were 100 and 81%, respectively. NAc-SDKP pharmacokinetics was studied in patients after intravenous infusion over 48 hr of a dose of between 51.3 and 513 nmol/kg. Area under the curve values increased proportionately with the dose. Mean clearance was lower in patients than in healthy volunteers: 524 vs. 1120 ml/hr/kg, respectively.

Published

1994

120. Enzyme immunometric assay for leukotriene C4.

Author

Volland H, Vulliez Le Normand B, Mamas S, Grassi J, Créminon C, Ezan E, and Pradelles P

Subjects

Acetylcholinesterase, Antibodies, Monoclonal, Blood Platelets metabolism, Cells, Cultured, Chromatography, High Pressure Liquid, Haptens immunology, Humans, Leukotriene A4 blood, Leukotriene C4 immunology, Sensitivity and Specificity, Immunoenzyme Techniques, Leukotriene C4 analysis

Abstract

An enzyme immunometric assay of LTC4 named SPIE-IA is described. The assay involves different sequential steps: (1) immunocapture of LTC4 by monoclonal anti-LTC4 antibodies coated on 96-well microtiter plates; (2) cross-linking of LTC4 via its amino group to the wells using glutaraldehyde; (3) treatment with HCl; (4) measurement of linked LTC4 using the same monoclonal anti-LTC4 antibodies labeled with acetylcholinesterase. A minimal detectable concentration of 2 pg/ml after 60 min of enzymatic reaction was obtained. Cross-reactivity was less than 15% with LTD4 or LTE4. The coefficient of variation was less than 6% in the 20-1000 pg/ml range. Good correlation was observed between SPIE-IA and a competitive enzyme immunoassay for biological samples. The different sequential steps of the assay are investigated.

Published

1994

121. Effect of chronic converting-enzyme inhibition on kidney function of senescent hypertensive rats.

Author

Vienet R, Grognet JM, Ezan E, Lecaque D, Hamon G, and Corman B

Subjects

Aging pathology, Animals, Hypertension pathology, Indoles pharmacology, Kidney pathology, Kidney physiopathology, Male, Rats, Rats, Inbred SHR, Aging physiology, Angiotensin-Converting Enzyme Inhibitors pharmacology, Hypertension physiopathology, Kidney drug effects

Abstract

The age-related changes in the structure and the function of the kidney and the effect of chronic inhibition of angiotensin-converting enzyme (ACE) activity on these alterations were assessed in senescent, genetically hypertensive rats. Mean blood pressure was unchanged between 6 and 21 months, being 136 +/- 10 and 135 +/- 21 mm Hg, respectively. Hypertrophy of the glomeruli with a high incidence of glomerulosclerosis was reported in the 21-month-old animals. Renal blood flow, glomerular filtration rate, and filtration fraction were reduced between 6 and 21 months, whereas albuminuria and cGMP excretion were markedly enhanced with aging. Chronic ACE inhibition by administration of 0.3 mg/kg/day trandolapril from 18-21 months increased the life expectancy of the animals without affecting their mean blood pressure. The incidence of glomerular lesions and the excretion of enzymes that reflected the integrity of tubular and glomerular cells were not altered by ACE inhibition. On the other hand, the filtration fraction was restored in the 21-month-old treated animals, and the age-related albuminuria and rise in cGMP excretion were prevented by ACE inhibition. These results indicated that ACE inhibitor administered at the end of the life of senescent hypertensive rats was able to prevent some of the age-related changes in kidney function when glomerulosclerosis was already present.

Published

1994

122. Enzyme immunoassays for a new angiotensin-converting enzyme inhibitor, zabicipril, and its active metabolite in human plasma: application to pharmacokinetic studies.

Author

Ezan E, Morge X, Lelièvre E, Créminon C, Piraube C, and Grognet JM

Subjects

Acetylcholinesterase, Adult, Angiotensin-Converting Enzyme Inhibitors pharmacokinetics, Antibody Specificity, Bridged Bicyclo Compounds pharmacokinetics, Chromatography, High Pressure Liquid, Humans, Immunoenzyme Techniques, Male, Reference Standards, Reproducibility of Results, Sensitivity and Specificity, Angiotensin-Converting Enzyme Inhibitors blood, Bridged Bicyclo Compounds blood, Bridged Bicyclo Compounds, Heterocyclic

Abstract

Zabicipril (S 9650) is a new angiotensin-converting enzyme inhibitor whose hydrolysis in vivo produces the pharmacologically active metabolite zabiciprilat (S 10211). Two competitive enzyme immunoassays specific for either zabicipril or zabiciprilat have been developed using acetylcholinesterase (E.C. 3.1.1.7) as label. Antibodies were raised in rabbits after immunization with lysil derivatives of zabicipril or zabiciprilat coupled with bovine serum albumin. Assays were performed in 96-well microtiter plates coated with a monoclonal antibody raised against rabbit immunoglobulin G, thus ensuring rapid separation of free and bound fractions of the tracer. The analysis does not require any extraction step. In the case of the assay of zabiciprilat, interference generated by endogenous angiotensin-converting enzyme (ACE) was eliminated by the addition of perindoprilat, another ACE inhibitor. Perindoprilat was not recognized by the antibodies (cross-reactivity < 0.01%) and did not affect assay efficiency. The specificity of the assays was checked by high-performance liquid chromatography of human plasma samples obtained after oral administration of 2 mg of zabicipril. No metabolites or endogenous substances were detected. The mean reproducibility was 15% for the assay of zabicipril and 19% for the assay of zabiciprilat. The quantification limits were 1.2 ng/ml for the zabicipril assay and 0.8 ng/ml for the zabiciprilat assay. These assays are therefore suitable for pharmacokinetic studies and drug monitoring in clinical studies.

Published

1993

123. Enzyme immunoassay using a rat prolactin-alkaline phosphatase recombinant tracer.

Author

Gillet D, Ezan E, Ducancel F, Gaillard C, Ardouin T, Istin M, Ménez A, Boulain JC, and Grognet JM

Subjects

Alkaline Phosphatase chemistry, Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, DNA chemistry, Escherichia coli enzymology, Female, Male, Molecular Sequence Data, Prolactin chemistry, Prolactin genetics, Rats, Rats, Sprague-Dawley, Recombinant Proteins chemistry, Sensitivity and Specificity, Immunoenzyme Techniques, Prolactin blood

Abstract

This paper describes a competitive enzyme immunoassay of rat prolactin (rPrl) using a recombinant conjugate as a colorimetric tracer. rPrl was inserted into the N-terminal end of Escherichia coli alkaline phosphatase (AP), using an expression vector which allows insertion of foreign DNA sequences between codons +6 and +7 of the phoA gene. The assay was performed in 96-well microtiter plates coated with a mouse monoclonal antibody raised against rabbit immunoglobulin G. Each component (recombinant tracer, rabbit antiserum against rPrl, and rPrl standard) was added in a volume of 50 microL. The sensitivity of the assay was sufficiently high to allow titration of rPrl in plasma. The detection threshold was 15 pg (0.3 ng/mL) and the B/B0 50% value was 150 pg (3 ng/mL). The intraassay coefficient of variation was less than 10% over a wide range of rPrl concentrations (2.9-50 ng/mL). The interassay coefficient of variation was less than 15% for rat plasma samples in the concentration range of 4-40 ng/mL. The good parallelism observed between the standard curve and sample dilution curves showed that the immunoreactivity in rat plasma behaves like standard rPrl. Together with recovery experiments, these results indicated that assay without extraction is possible. A single immunoreactive peak that comigrates with standard rPrl is observed after molecular sieve fractionation of plasma samples. The reliability of the assay was confirmed by good correlation with conventional radioimmunoassay (r = 0.996, slope 0.978).

Published

1993

124. Practical method for optimizing radioimmunoassay detection and precision limits.

Author

Ezan E, Tiberghien C, and Dray F

Subjects

Mathematics, Models, Biological, Sensitivity and Specificity, Antigen-Antibody Reactions, Radioimmunoassay

Abstract

A model of the competitive radioimmunoassay standard curve, based on the Law of Mass Action, has been developed and used in conjunction with experimental and counting errors to predict the assay detection limit and precision profiles. We verified the model with hapten radioimmunoassays performed in our laboratory. The resulting computer program can be used to determine the optimum antiserum concentration--depending on its affinity--and labeled-antigen concentration--according to its specific activity and nonspecific binding. The graphical representation of this model provides radioimmunologists with a practical tool for assay optimization.

Published

1991

125. Validation in rat plasma of a direct radioimmunoassay for a luteinizing hormone-releasing hormone antagonist (BIM 21009)

Author

Ezan E, Drieu K, Moreau JP, and Dray F

Subjects

Amino Acid Sequence, Animals, Antibody Specificity, Gonadotropin-Releasing Hormone blood, Molecular Sequence Data, Radioimmunoassay, Rats, Rats, Inbred Strains, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors

Abstract

Rabbits were immunized with [Ac-D-beta-Nal1-, D-p-Cl-Phe2, D-Phe3, D-Arg6, Phe7, D-Ala10]LHRH (BIM 21009) coupled to bovine serum albumin using bis-diazotized benzidine. The best antiserum had an affinity of 5. 10(-10) M and a specificity directed against the C-terminal part of the molecule. The antiserum was not affected by native LHRH but reacted to some extent with detergents. Assay of free-peptide plasma after gel filtration on Ultrogel AcA 34 showed apparent immunoreactivity associated with albumin and lipoproteins. The sensitivity of direct assay was 0.4 ng/ml. Measurements of BIM 21009 after s.c. injection in rats showed the resistance of the peptide to elimination. The specificity of the determinations in plasma were checked by High Performance Liquid Chromatography.

Published

1990

126. Pharmacokinetics of D-Trp6 LHRH in man: sustained release polymer microsphere study (I.M. route).

Author

Drieu K, Devissaguet JP, Duboistesselin R, Dray F, and Ezan E

Subjects

Antineoplastic Agents administration & dosage, Delayed-Action Preparations, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone pharmacokinetics, Humans, Injections, Intramuscular, Male, Triptorelin Pamoate, Antineoplastic Agents pharmacokinetics, Gonadotropin-Releasing Hormone analogs & derivatives

Published

1987

127. Triton X-100 eliminates plasma proteins interference in a radioimmunoassay for luteinizing hormone-releasing hormone (LHRH) and LHRH analogues.

Author

Ezan E, Drieu K, and Dray F

Subjects

Animals, Humans, Octoxynol, Radioimmunoassay methods, Rats, Triptorelin Pamoate, Blood Proteins analysis, Gonadotropin-Releasing Hormone blood, Polyethylene Glycols pharmacology

Abstract

A method is described for the radioimmunoassay of native LHRH and DTrp6-LHRH, an LHRH analogue which does not require extraction of plasma samples. Interference by binding proteins normally present in plasma is removed by addition of Triton X-100 to the binding buffer at a concentration of 1% for LHRH and 0.15% for the LHRH analogue. This approach permits a direct estimation of the peptide level in unextracted plasma with quantitative recoveries for concentrations ranging from 0.015 to 10 ng/ml. Although the antiserum titre is reduced, the affinity of the antibody does not change at the detergent concentrations used in this study. This procedure is recommended for peptide assays in which the non-specific effects of plasma prevent a direct assay.

Published

1989

128. ELISA for detection of human antibodies to Chlamydiae.

Author

Lema F, Everaere S, Rougeot C, Fuentes V, Ezan E, Dray F, and Bussard A

Subjects

Enzyme-Linked Immunosorbent Assay, Fluorescent Antibody Technique, Humans, Antibodies, Bacterial analysis, Chlamydia immunology

Abstract

An enzyme-linked immunosorbent assay for the detection of human antibodies to Chlamydiae is described which exploits the cross-react properties between the genus-specific antigen of Chlamydiae and the ReLPS constituent of the outer membrane of a Salmonella minnesota mutant. Of 100 random sera tested by ELISA-ReLPS and immunofluorescence 78% showed an absolute correlation, 15% were positive in immunofluorescence and negative in ELISA and 7% were positive in ELISA and negative in immunofluorescence. Furthermore results obtained by the ELISA-ReLPS on 55 sera from patients with clinical evidence of Chlamydiae infection correlated well with the values obtained by an ELISA using Chlamydia-coated microtitration plates and by two immunofluorescence tests using Chlamydia trachomatis and Chlamydia psittaci as antigens. The method described here is sensitive, simple, reproducible and may be employed for epidemiological and pathogenetic studies of chlamydial infections.

Published

1986

129. Radioimmunoassay of [D-Trp6]-luteinizing hormone-releasing hormone: its application to animal pharmacokinetic studies after single injection and long-acting formulation administration.

Author

Ezan E, Drieu K, Chapelat M, Rougeot C, and Dray F

Subjects

Animals, Cross Reactions, Delayed-Action Preparations, Dogs, Drug Compounding, Drug Evaluation, Preclinical, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone analysis, Gonadotropin-Releasing Hormone metabolism, Half-Life, Injections, Intravenous, Injections, Subcutaneous, Kinetics, Radioimmunoassay, Rats, Testosterone blood, Triptorelin Pamoate, Gonadotropin-Releasing Hormone analogs & derivatives

Abstract

A sensitive radioimmunoassay (RIA) for [D-Trp6]-luteinizing hormone-releasing hormone (LHRH) has been developed. This assay allowed measurement of the LHRH analog in unextracted plasma with a minimum detectable concentration of 10 pg/ml. Validation of plasma assays was performed through Sep-Pak and HPLC purification. The in vivo fate of the peptide was investigated in dogs after subcutaneous or intravenous injections. In both cases, the LHRH analog showed longer plasma half-life than native LHRH with an elimination half-life superior to 80 min. Long-acting formulations were tested in dogs and rats: the day following administration, [D-Trp6]-LHRH plasma level rose to 2.9-4.6 ng/ml in dogs and 0.8-3.8 ng/ml in rats. From day 4 to day 30, [D-Trp6]-LHRH plasma level followed a plateau with concentrations of 0.3-0.8 ng/ml in dogs and 0.2-0.4 ng/ml in rats. In parallel, testosterone plasma concentration was reduced to castrate level between day 4 and day 7 in dogs and was significantly lowered in rats. This sensitive [D-Trp6]-LHRH RIA will be particularly useful for the evaluation of long-acting formulations in patients with advanced prostate cancer.

Published

1986