Your search keyword '"Nestor JJ Jr"' showing total 31 results

1. The medicinal chemistry of peptides.

Author

Nestor JJ Jr

Subjects

Chemistry, Pharmaceutical, Cyclization, Drug Design, Hydrophobic and Hydrophilic Interactions, Peptides chemical synthesis, Peptides pharmacokinetics, Polyethylene Glycols chemistry, Peptides chemistry

Abstract

The shortcomings of native peptides as pharmaceuticals have been long known: short duration of action, lack of receptor selectivity, lack of oral bioavailability. However medicinal chemistry offers solutions to the first two limitations and oral bioavailability issues have been addressed with novel routes of administration (e.g. intranasal, inhalation) and injectable depot formulations. The principal issue for peptide drugs has been a short duration of action, widely assumed to be due to proteolysis. While proteolysis is a problem for native peptide structures, modification of the peptide structure by acylation, PEGylation, unnatural amino acids or restricted conformation can largely remove this issue. However rapid clearance from the blood into the urine remains an issue for even proteolytically stable molecules. Medicinal chemistry approaches here have been peptide modifications to slow release from the injection site (hydrophobic, hydrophilic, self-associating depots), PEGylation, fatty acid acylation, and the like. Medicinal chemistry approaches used in successful peptide pharmaceuticals using unnatural amino acids to achieve depot formation are highlighted in this review.

Published

2009

2. A new gonadotropin-releasing hormone (GnRH) superagonist in goldfish: influence of dialkyl-D-homoarginine at position 6 on gonadotropin-II and growth hormone release.

Author

Murthy CK, Turner RJ, Nestor JJ Jr, Rivier JE, and Peter RE

Subjects

Amino Acid Sequence, Animals, Dose-Response Relationship, Drug, Female, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone pharmacology, Male, Molecular Sequence Data, Pituitary Gland chemistry, Structure-Activity Relationship, Goldfish, Gonadotropin-Releasing Hormone agonists, Gonadotropin-Releasing Hormone chemistry, Gonadotropins metabolism, Growth Hormone metabolism, Homoarginine chemistry

Abstract

The two native forms of gonadotropin-releasing hormones (GnRH) present in goldfish, salmon GnRH (sGnRH) and chicken GnRH-II (cGnRH-II), stimulate gonadotropin-II (GTH-II) and growth hormone (GH) release both in vivo and in vitro. In our previous study using perifused goldfish pituitary fragments, many mammalian GnRH antagonists, especially those with D-Arg6, showed weak to strong stimulation of GTH-II and GH release. In the present study, the dose-related stimulation of GTH-II and GH release by [Ac-D(2)-Nal1, 4Cl-D-Phe2, D-Trp3, D-Arg6, Trp7, D-Ala10] mGnRH (analog J) and [Ac-D(2)-Nal1, 4Cl-D-Phe2, D-Trp3, D-hArg(Et2)6, D-Ala10] mGnRH (analog K) was demonstrated; the stimulatory potency of both analogs was significantly lower than that of native sGnRH. In the presence of analogs J and K, cGnRH-II stimulated GTH-II release was significantly suppressed. Further, GTH-II and GH stimulation by 2 microM of analog K was significantly suppressed by a 'true' GnRH antagonist, [Ac-delta 3-Pro1, 4FD-Phe2, D-Trp3,6] mGnRH (analog E). These results indicate that analogs J and K increase GTH-II and GH release in goldfish by acting on GnRH receptors on gonadotrophs and somatotrophs. Since analog K, having [D-hArg(Et2)6], strongly stimulated GTH-II release, the potency of [D-hArg(Et2)6] or [D-hArg(CH2CF3)2(6)] substituted analogs to stimulate GTH-II and GH release from the perifused goldfish pituitary fragments was tested. Among the peptides tested, [D-hArg(Et2)6, Pro9-NHEt] sGnRH had a higher potency in stimulating GTH-II release than any other analog tested in the present or in previous studies. For stimulation of GH release, [D-hArg(Et2)6, Pro9-NHEt] sGnRH and [D-Arg6, Pro9-NHEt] sGnRH were the most potent analogs tested; analogs of mGnRH were less potent than sGnRH, indicating the importance of Trp7, Leu8 residues in the native peptide. These results suggest the importance of [D-Arg6] or alkylated [D-Arg6] in determining the intrinsic activity and potency of GnRH peptides in goldfish.

Published

1994

3. Therapeutic effects of a synthetic peptide of C-reactive protein in pre-clinical tumor models.

Author

Barna BP, Eppstein DA, Thomassen MJ, Nestor JJ Jr, Ho T, Medendorp SV, and Deodhar SD

Subjects

Adenocarcinoma therapy, Animals, Carcinoma, Renal Cell therapy, Colonic Neoplasms therapy, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Carriers, Fibrosarcoma therapy, Humans, Immunotherapy, Kidney Neoplasms therapy, Lung Neoplasms secondary, Lung Neoplasms therapy, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Neoplasm Transplantation, Regulatory Sequences, Nucleic Acid, C-Reactive Protein pharmacology, Neoplasms, Experimental therapy, Peptide Fragments pharmacology

Abstract

Previous studies have shown that multilamellar vesicles (MLV) or other carriers containing purified human C-reactive protein (CRP) have therapeutic activity in preclinical tumor models. Here we evaluated the therapeutic effects of MLV containing novel synthetic peptides, derived from the structure of CRP, on the extent of (a) established lung metastases of fibrosarcoma T241 in C57Bl/6 mice, (b) survival of C57Bl/6 mice bearing established liver metastases of colon carcinoma MCA-38, and (c) primary tumor growth of Renca renal carcinoma in Balb/c mice. In all cases, a single synthetic CRP peptide, RS-83277, demonstrated significant antitumor effects comparable to that seen with intact CRP. Two other synthetic CRP peptides, RS-83287 and RS-83147, showed no therapeutic activity and were comparable to control MLV containing only buffer. None of the peptides contained sequences homologous with that of the phagocyte stimulant, tuftsin. Activity of MLV-encapsulated RS-83277 was dose-dependent, and a comparable dose of the soluble peptide, given either alone or following injection of buffer-MLV, was ineffective. These results demonstrate immunotherapeutic potential for a novel synthetic peptide derived from CRP, and endogenous acute-phase protein.

Published

1993

4. Potent gonadotropin releasing hormone antagonists with low histamine-releasing activity.

Author

Nestor JJ Jr, Tahilramani R, Ho TL, Goodpasture JC, Vickery BH, and Ferrandon P

Subjects

Amino Acid Sequence, Amino Acids analysis, Animals, Female, Gonadotropin-Releasing Hormone analogs & derivatives, Male, Molecular Sequence Data, Ovulation drug effects, Rats, Rats, Sprague-Dawley, Gonadotropin-Releasing Hormone antagonists & inhibitors, Histamine Release drug effects

Abstract

The incorporation of Arg residues into position 6 of gonadotropin releasing hormone antagonists had resulted in compounds with increased in vivo potency but also made these analogues potent mast cell degranulators. We have focused on the substitution of position 8 by hArg(R)2 (NG,NG'-dialkylhomoarginine) substitutions, based on the hypotheses that the Arg-Pro sequence is of major importance for this side effect and that shielding of the charge may be an effective way to block degranulation. Analogues in four series were evaluated: (A) [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal-(3)3,6,Arg5,hArg(R)2(8),D-+ ++Ala10]GnRH, (B) [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal(3)3,6,hArg(R)2(5,8),D-Ala10 ]-GnRH, (C) [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal(3)3,6,hArg(R)2(8),D-Ala10]G nRH, (D) [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal(3)3,D-hArg(R)2(6),hArg(R)2( 8),D-Ala10]GnRH. Although substitution by hArg(Et)2, hArg(Bu), hArg(CH2)3, and hArg(CH2CF3)2 was tested, in each series the hArg(Et)2 residue was superior. Two compounds were considered for clinical evaluation: [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal(3)3,6,hArg(Et)2(8),D-Ala10] GnRH and [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Pal(3)3,D-hArg(Et)2(6),hArg(Et) 2(8),D- Ala10]GnRH (ganirelix acetate). These compounds had high potency for ovulation suppression and low histamine-releasing potency in vitro (ED50 = 0.6, 0.29 microgram/rat and EC50 = 196, 13 micrograms/mL, respectively). Ganirelix is currently in Phase II clinical trials and appears to be the most potent GnRH antagonist tested in humans (based upon ED50 for 24-h suppression of testosterone levels).

Published

1992

5. Disposition of RS-26306, a potent luteinizing hormone-releasing hormone antagonist, in monkeys and rats after single intravenous and subcutaneous administration.

Author

Chan RL, Hsieh SC, Haroldsen PE, Ho W, and Nestor JJ Jr

Subjects

Animals, Bile metabolism, Blood Proteins metabolism, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone pharmacokinetics, Injections, Intravenous, Injections, Subcutaneous, Macaca fascicularis, Male, Protein Binding, Rats, Rats, Inbred Strains, Scintillation Counting, Species Specificity, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors

Abstract

The metabolic disposition of RS-26306, a new potent luteinizing hormone-releasing hormone antagonist, was studied in rats and monkeys after single i.v. and sc administration with the 3H-labeled compound. Plasma pharmacokinetics after iv administration were: CLs = 2.5 ml/min/kg, Vd beta = 0.29 liter/kg, t1/2 = 1.4 hr (rats), and CLs = 0.8 ml/min/kg, Vd beta = 0.32 liter/kg, t1/2 = 5.1 hr (monkeys). Cmax and Tmax in rats were 0.53 micrograms/ml and 4 hr after the 1 mg/kg sc dose, and were 1.07 micrograms/ml and 12 hr after the 10 mg/kg sc dose. AUC0-infinity after the 10 mg/kg sc dose in rats was seven times that after the 1 mg/kg sc dose. Apparent plasma disappearance t1/2 in rats were 3.6 and 15.2 hr, respectively, after the 1 and 10 mg/kg sc doses. An average of 12 and 4% of dose radioactivity remained at the injection site in rats 3 and 10 days, respectively, after a 10 mg/kg sc dose. In monkeys, Tmax after a 1 mg/kg sc dose was 0.5 hr for three animals but was 24 hr for the fourth animal, although plasma of this monkey contained substantial levels of RS-26306 between 15 min and 24 hr. Apparent plasma t1/2 in monkeys after a 1 mg/kg sc dose was at least 19 hr. Our data suggest depot formation after sc doses. In vitro plasma binding amounted to 82-84%. Excretion was mainly biliary: 12-25 and 55-84% of dose radioactivity was recovered in urine and feces, respectively, in both species. The biological samples contained only traces of 3H2O. Three metabolites, which were truncated peptides of the parent decapeptide, were identified in the rat bile. One of these was also present in the monkey plasma. The restricted enzymatic degradation of RS-26306, extensive plasma binding, and long circulating t1/2 of RS-26306 contribute to its prolonged activity in animal models and in humans.

Published

1991

6. Effects of an LH-releasing hormone antagonist on the secretion of LH, FSH, prolactin and ovarian steroids at different stages of the luteal phase in the stumptailed macaque (Macaca arctoides).

Author

Fraser HM, Abbott M, Laird NC, McNeilly AS, Nestor JJ Jr, and Vickery BH

Subjects

Animals, Corpus Luteum drug effects, Estradiol blood, Female, Follicle Stimulating Hormone blood, Gonadotropin-Releasing Hormone pharmacology, Luteal Phase, Luteinizing Hormone blood, Macaca, Progesterone blood, Prolactin blood, Corpus Luteum physiology, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors, Gonadotropins, Pituitary blood

Abstract

The role of the pituitary gonadotrophins in controlling luteal function in the stumptailed macaque has been investigated by examining profiles of serum concentrations of LH, FSH, progesterone and oestradiol in daily blood samples from 13 monkeys during the menstrual cycle, and in blood samples taken at hourly intervals between 09.00 and 21.00 h on different days of the luteal phase in 13 cycles. The effects of acute withdrawal of gonadotrophins was investigated by administering a single injection of 300 micrograms LHRH antagonist/kg body weight at different stages of the luteal phase during 28 cycles. Although there were high basal values and marked fluctuations of bioactive LH during the first 4 days after the LH peak, progesterone profiles showed no corresponding short-term changes, there being a slow and steady rise in progesterone concentrations during the sampling periods. After day 5, basal LH secretion decreased, but high amplitude LH pulses were identified which were associated with episodes of progesterone secretion. Administration of the LHRH antagonist caused a suppression of bioactive LH and progesterone concentrations at all stages of the luteal phase, although some basal secretion of progesterone was maintained through the 24-h period of effective antagonist gonadotroph blockade. Luteal function recovered apparently normally in all monkeys treated in the early-mid-luteal phase. Serum concentrations of FSH and oestradiol fluctuated comparatively less during the 12-h sampling periods, and the antagonist had less suppressive effects on the concentrations of these hormones. The LHRH antagonist had no apparent effect on prolactin release.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1986

7. Gestational age-related inhibition of placental hCG, alpha hCG and steroid hormone release in vitro by a GnRH antagonist.

Author

Siler-Khodr TM, Khodr GS, Rhode J, Vickery BH, and Nestor JJ Jr

Subjects

Culture Techniques, Estradiol metabolism, Estrone metabolism, Female, Glycoprotein Hormones, alpha Subunit, Humans, Placental Lactogen metabolism, Pregnancy, Progesterone metabolism, Radioimmunoassay, Time Factors, Chorionic Gonadotropin metabolism, Gestational Age, Peptide Fragments metabolism, Pituitary Hormone Release Inhibiting Hormones pharmacology, Pituitary Hormones, Anterior metabolism, Placenta drug effects, Placental Hormones metabolism

Abstract

Human placental tissues have been shown to contain gonadotrophin-releasing hormone-(GnRH)-like activity. Thus, the effect of a potent GnRH antagonist (N-Ac-Pro1,D-p-Cl-Phe2,D-Nal(2)3,6-GnRH, obtained from Syntex Laboratories) on placental hormonal release was studied. Explant cultures of placentae of 6 to 15 weeks' gestation were studied. This GnRH antagonist did not inhibit the alpha human chorionic gonadotrophin (alpha hCG), human chorionic gonadotrophin (hCG), oestrone or oestradiol release from the six- and nine-week placental cultures, but greatly suppressed the release of these hormones in the placental cultures from 13- and 15-week gestations. Synthetic GnRH partially reversed the action of this antagonist on the hormonal releases in the 15-week placental cultures. These data demonstrate a gestational age-related action of this antagonist on placental hormonal release. Thus, a role for the endogenous GnRH-like activity of the placenta in the control of placental hormonogenesis is indicated.

Published

1987

8. (4-Phenylalanine)oxytocin, an inhibitor of the antidiuretic effect of 8-arginine-vasopressin.

Author

Nestor JJ Jr, Ferger MF, and Chan WY

Subjects

Animals, Blood Pressure drug effects, Chickens, Depression, Chemical, Diuresis drug effects, Female, In Vitro Techniques, Male, Natriuresis drug effects, Oxytocin chemical synthesis, Oxytocin pharmacology, Phenylalanine chemical synthesis, Phenylalanine pharmacology, Rats, Uterine Contraction drug effects, Arginine Vasopressin analogs & derivatives, Oxytocin analogs & derivatives, Vasopressins analogs & derivatives

Abstract

[4-Phenylalanine]oxytocin was prepared from Z-Cys(Bzl)-Tyr(Bzl)-Ile-Phe-Asn-Cys(Bzl)-Pro-Leu-Gly-NG2 (4) by deprotection with Na in NH3 followed by cyclization of the resulting disulfhydryl compound with ICH2CH2I. The protected peptide 4 was prepared from Boc-Asn-Cys(Bzl)-Pro-Leu-Gly-NH2 by the stepwise solution method. Coupling was effected by a modification of the dicyclohexylcarbodiimide-1-hydroxybenzotriazole preactivation method wherein the precipitate of dicyclohexylurea is removed by filtration prior to mixing of the amino and carboxyl components. The analog was found to be an effective inhibitor of the antidiuretic (ADH) response to exogenous arginine-vasopressin. It produced marked diuresis in the anti-ADH assay at approximately the same dose level as does [Leu4]oxytocin but, in contrast to [Leu4]oxytocin, showed natriuretic activity only at relatively high dose levels. In addition, [Phe4]oxytocin exhibited 0.15% of the oxytocic potency of oxytocin, weak antiavian vasodepressor activity (pA2 = 6.93), and no measurable rat pressor activity.

Published

1975

9. Inhibition of oxytocic responses to oxytocin in pregnant rats by (1-L-penicillamine)oxytocin and (1-beta-mercapto-beta, beta-diethylpropionic acid)oxytocin.

Author

Chan WY, Nestor JJ Jr, Ferger MF, and Du Vigneaud V

Subjects

Animals, Female, Pregnancy, Rats, Transducers, Diethylpropion pharmacology, Oxytocin antagonists & inhibitors, Penicillamine pharmacology, Pregnancy, Animal, Uterus drug effects

Published

1974

10. Luteinizing hormone-releasing hormone antagonists containing very hydrophobic amino acids.

Author

Nestor JJ Jr, Tahilramani R, Ho TL, McRae GI, and Vickery BH

Subjects

Amino Acid Sequence, Animals, Female, Gonadotropin-Releasing Hormone analogs & derivatives, Ovulation drug effects, Rats, Solubility, Structure-Activity Relationship, Gonadotropin-Releasing Hormone antagonists & inhibitors, Hormones chemical synthesis

Abstract

In a continuation of our studies on the effects of hydrophobic substitutions in analogues of luteinizing hormone-releasing hormone (LH-RH), we have synthesized LH-RH antagonists containing the very hydrophobic amino acid 3-(2-naphthyl)-D-alanine (D-Nal(2)). The D-Nal(2) substitution was found to be effective when incorporated in positions 3 and 6. The most potent analogue containing two D-Nal(2) residues was [N-Ac-Pro,D-pF-Phe,D-Nal(2)]LH-RH (ED50 = 2.2 micrograms, rat antiovulatory assay, propylene glycol-saline vehicle). This analogue also demonstrates that the N-Ac-Pro substitution is as effective as the more costly N-Ac-delta-Pro modification. Analogues containing D-Nal(2) in combination with the hydrophilic D-Arg residue in position 6 were prepared. Neither N-Ac-Pro at position 1 nor D-Nal(2) at position 3 was effective in combination with D-Arg. N-Ac-D-Nal(2) at position 1 gave a highly potent antagonist ([N-Ac-D-Nal(2),D-pF-Phe,D-Trp,D-Arg]LH-RH; ED50 = 2.4 micrograms) that exhibited a prolonged duration of action (ED50 = 9.0 micrograms, corn oil vehicle, dosing on diestrus II).

Published

1984

11. Differential inhibition of human placental prostaglandin release in vitro by a GnRH antagonist.

Author

Siler-Khodr TM, Khodr GS, Harper MJ, Rhode J, Vickery BH, and Nestor JJ Jr

Subjects

Culture Techniques, Female, Gonadotropin-Releasing Hormone pharmacology, Humans, Pregnancy, Pregnancy Trimester, First, Pregnancy Trimester, Second, Prostaglandins E metabolism, Prostaglandins F metabolism, Dinoprost analogs & derivatives, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors, Placenta drug effects, Prostaglandins metabolism

Abstract

Previously, we have demonstrated that the production of prostaglandins by human placental tissue varied with gestational age. In addition, we have shown that placental prostaglandin release was affected by GnRH, and that its response was also dependent on the gestational age of the placenta. Thus, we have studied the effect of a GnRH antagonist ([N-Ac-Pro1,D-p-Cl-Phe2,D-Nal(2)3,6-LHRH, Syntex Research, Palo Alto, CA) on basal prostaglandin release from placentas of 6 to 15 weeks' gestation and found that this antagonist (1 microgram/ml) effects an inhibition of the release of prostaglandin E, prostaglandin F, and 13,14-dihydro-15-keto-prostaglandin from placentas of 13 and 15 weeks of gestation. This effect was not overridden by GnRH at 10 times the antagonist concentration in the 13-week placental cultures, but was totally reversed by GnRH (10 micrograms/ml) in the 15-week placental cultures. These data demonstrate that this GnRH antagonist can affect human placental prostaglandin production at 13 to 15 weeks of gestation and indicate that endogenous placental GnRH-like activity may exert a control over placental prostaglandin release at this gestational stage.

Published

1986

12. Hydrophobic, aza-glycine analogues of luteinizing hormone-releasing hormone.

Author

Ho TL, Nestor JJ Jr, McCrae GI, and Vickery BH

Subjects

Animals, Biological Assay, Chromatography, High Pressure Liquid, Estrus drug effects, Female, Glycine pharmacology, Gonadotropin-Releasing Hormone pharmacology, Indicators and Reagents, Pregnancy, Rats, Structure-Activity Relationship, Glycine analogs & derivatives, Gonadotropin-Releasing Hormone analogs & derivatives, Hydrazines

Abstract

The effect of combination of the hydrophilic aza-Gly substitution (NHNHCO) at position 10 with hydrophobic, unnatural D-amino acids in position 6 on the potency of luteinizing hormone-releasing hormone (LH-RH) analogues has been investigated. Previously the aza-Gly residue was shown to provide protection from enzymatic cleavage and lead to potency increases in a less hydrophobic series. The compounds were prepared by coupling of the corresponding nonapeptide acids with semicarbazide hydrochloride by the N,N'-dicyclohexylcarbodiimide/1-hydroxybenzotriazole procedure. The required nonapeptide acids were prepared by the solid phase method on chloromethyl-polystyrene resin using HF/anisole deprotection. The products were purified by preparative reversed-phase high-performance liquid chromatography. The analogues were tested in a rat estrous cyclicity suppression assay designed to show the paradoxical antifertility effects of these compounds. The potencies of [6-(3-benzimidazol-2-yl)-D-alanine), 10-aza-glycine] LH-RH and [6-(3-(5,6-dimethylbenzimidazol-2-yl)-D-alanine), 10-aza-glycine] LH-RH are 40 and 190 times that of LH-RH respectively. The most active compound in this series is [6-(3-(2-naphthyl)-D-alanine), 10-aza-glycine] LH-RH with a potency 230 times that of LH-RH. This compound is 2.3 times as potent as the standard ([D-Trp6, Pro9-NHEt] LH-RH) and appears to be the most potent LH-RH agonist reported.

Published

1984

13. Regression of tumors in guinea pigs after treatment with synthetic muramyl dipeptides and trehalose dimycolate.

Author

McLaughlin CA, Schwartzman SM, Horner BL, Jones GH, Moffatt JG, Nestor JJ Jr, and Tegg D

Subjects

Acetylmuramyl-Alanyl-Isoglutamine administration & dosage, Animals, Cord Factors administration & dosage, Drug Combinations, Emulsions, Immunotherapy, Lymphatic Metastasis, Structure-Activity Relationship, Acetylmuramyl-Alanyl-Isoglutamine therapeutic use, Cord Factors therapeutic use, Glycolipids therapeutic use, Glycopeptides therapeutic use, Liver Neoplasms, Experimental therapy

Abstract

A high incidence of tumor regression was observed in guinea pigs bearing transplantable, line-10 hepatocellular carcinomas when synthetic muramyl dipeptides combined with trehalose dimycolate in oil-in-water emulsions were injected directly into the tumors. These compounds are promising candidates to replace viable bacillus Calmette-Guérin in cancer immunotherapy in humans and animals.

Published

1980

14. [1-Beta-mercapto-beta,beta-pentamethylenepropionic acid]oxytocin, a potent inhibitor of oxytocin.

Author

Nestor JJ Jr, Ferger MF, and du Vigneaud V

Subjects

Animals, Blood Pressure drug effects, Chickens, Chromatography, Thin Layer, Female, Male, Muscle Contraction drug effects, Oxytocin chemical synthesis, Oxytocin pharmacology, Propionates chemical synthesis, Propionates pharmacology, Rats, Sulfhydryl Compounds chemical synthesis, Sulfhydryl Compounds pharmacology, Uterus drug effects, Oxytocin analogs & derivatives, Oxytocin antagonists & inhibitors

Abstract

[1-Beta-mercapto-beta,beta-pentamethylenepropionic acid]oxytocin was prepared from beta-Mpa(beta-(CH2)5)(Bzl)-Tyr(Bzl)-Ile-Gln-Asn-Cys(Bzl)-Pro-Leu-Gly-NH2 by removal of the Bzl-protecting groups with Na-NH3 followed by cyclization of the resulting disulfhydryl compound with K3Fe(CN)6.The analog was purified by desalting on Sephadex G-15 in 50% HOAc and gel filtration on Sephadex G-25 and LH-20. The protected intermediate above was synthesized from Z-Cys(Bzl)-Pro-Leu-Gly-NH2 by the stepwose p-nitrophenyl ester method using Nalpha-Boc protection at the penta-, hexa-, and octapeptide stages. The analog was found to be a potent inhibitor of the oxytocic and avian vasodepressor effects of oxytocin (pA2 values of 7.43 and 8.30, respectively) but was only a weak inhibitor of the rat pressor effect of 8-lysine-vasopressin. The rat antipressor potency of [1-deaminopenicillamine]oxytocin was also determined in this study: pA2 = 6.27. Of the alkyl-substituted 1-position analogs of oxytocin studied so far, [1-beta-mercapto-beta,beta-pentamethylenepropionic acid]oxytocin is the most potent antioxytocic agent.

Published

1975

15. Potent, long-acting luteinizing hormone-releasing hormone antagonists containing new synthetic amino acids: N,N'-dialkyl-D-homoarginines.

Author

Nestor JJ Jr, Tahilramani R, Ho TL, McRae GI, and Vickery BH

Subjects

Alkylation, Animals, Gonadotropin-Releasing Hormone antagonists & inhibitors, Gonadotropin-Releasing Hormone pharmacology, Indicators and Reagents, Luteinizing Hormone blood, Male, Orchiectomy, Rats, Rats, Inbred Strains, Structure-Activity Relationship, Arginine analogs & derivatives, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone chemical synthesis, Homoarginine analogs & derivatives, Homoarginine chemical synthesis

Abstract

A new series of unnatural amino acids has been prepared and incorporated into antagonistic analogues of luteinizing hormone-releasing hormone (LH-RH), on the basis of the hypothesis that stabilization of a proposed phospholipid membrane interaction might yield analogues with high potency and a prolonged duration of action. Thus a series of NG,NG'-dialkyl-D-homoarginine analogues [H-D-hArg(R2)-OH; R = Me, Et, Pr, i-Pr, Bu, hexyl, cyclohexyl, (Et, Me2NPr)] was conveniently prepared by semisynthesis from D-Lys using the appropriate dialkylcarbodiimide. A number of the analogues that were prepared by using these new amino acid analogues exhibited very high potency and a prolonged duration of action. One of the most potent members of the series, [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Trp3,D-hArg(Et2)6,D-Ala10 ]LH-RH (detirelix), had an ED50 of 0.7 microgram in the rat antiovulatory assay when administered at noon on proestrus and only 2.5 micrograms when administered 24 h earlier, at noon on diestrus II. This antagonist is undergoing detailed biological and clinical evaluation.

Published

1988

16. Studies of the biological activity of LHRH analogs in the rainbow trout, landlocked salmon, and the winter flounder.

Author

Crim LW, Nestor JJ Jr, and Wilson CE

Subjects

Animals, Gonadotropin-Releasing Hormone metabolism, Gonadotropin-Releasing Hormone pharmacology, Gonadotropins, Pituitary metabolism, In Vitro Techniques, Male, Radioligand Assay, Receptors, LHRH metabolism, Testosterone pharmacology, Flatfishes metabolism, Flounder metabolism, Gonadotropin-Releasing Hormone analogs & derivatives, Salmon metabolism, Salmonidae metabolism, Trout metabolism

Abstract

Studies of gonadotropic hormone (GtH) release bioactivity by mammalian and submammalian varieties of LHRH and LHRH analog were primarily conducted in vivo in testosterone-primed yearling (TPY) rainbow trout, a convenient test animal for LHRH bioassays in fish. Validation of these results, using sexually mature fish, was accomplished by examining LHRH agonist activities on release of GtH in vivo in spermiating landlocked salmon and by studying LHRH peptide hormone binding affinities using a flounder pituitary LHRH radioreceptor assay. Our surveys of LHRH analog bioactivity in vivo in TPY trout and salmon demonstrated that all types of fish, bird, and mammalian LHRH agonists possess superactive properties on the fish pituitary. The most active group of LHRH analogs, based upon both LHRH receptor binding affinity and in vivo release of gonadotropin, was judged to include [D-Nal(2)6,Pro9-NHEt]LHRH, [D-Nal(2)6-AzaGly10]LHRH, [D-Ala6,Pro9-NHEt]-LHRH, and the fish LHRH analogs, [D-Arg6,Trp7,Leu8,Pro9-NHEt]LHRH, [D-hArg(Et2(6),Trp7,Leu8,Pro9-NHEt]LHRH.

Published

1988

17. Epidermal growth factor receptor occupancy inhibits vaccinia virus infection.

Author

Eppstein DA, Marsh YV, Schreiber AB, Newman SR, Todaro GJ, and Nestor JJ Jr

Subjects

Animals, Cytopathogenic Effect, Viral, Epidermal Growth Factor metabolism, ErbB Receptors, Fibroblasts, Mice, Molecular Weight, Peptides metabolism, Transforming Growth Factors, Virus Replication, Receptors, Cell Surface metabolism, Vaccinia virus pathogenicity

Abstract

Vaccinia virus encodes VGF, an early protein of relative molecular mass 19,000 (19K) which, from amino-acid residues 45 to 85, is homologous in 19 residues to epidermal growth factor (EGF), and transforming growth factor-alpha (TGF-alpha). The conserved sequence includes a region of high homology (6 out of 10 amino acids) from residues 71 to 80, corresponding to the third disulphide loop of both EGF and TGF-alpha. This region has recently been shown to contain a binding region of TGF-alpha for the EGF receptor, and this raises the question of whether vaccinia virus utilizes the EGF receptor in order to bind to and infect cells. We now show that occupancy of the EGF receptor inhibits vaccinia virus infection. Inhibition is observed in a dose-dependent fashion by pre-treatment with either EGF or synthetic decapeptide antagonists of EGF's mitogenic activity which correspond to the sequence of the third disulphide loop of VGF or TGF-alpha. The relative ability of the peptides to inhibit vaccinia virus infection parallels their binding affinity to the EGF receptor.

Published

1985

18. Phosphorylation substrates for protein kinase C in intact pituitary cells: characterization of a receptor-mediated event using novel gonadotropin-releasing hormone analogues.

Author

Strulovici B, Tahilramani R, and Nestor JJ Jr

Subjects

Animals, Carrier Proteins, In Vitro Techniques, Kinetics, Male, Phorbol Esters metabolism, Phosphates metabolism, Phosphorus Radioisotopes, Phosphorylation, Pituitary Gland, Anterior drug effects, Rats, Rats, Inbred Strains, Substrate Specificity, Caenorhabditis elegans Proteins, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone pharmacology, Pituitary Gland, Anterior metabolism, Protein Kinase C metabolism, Proteins metabolism, Receptors, Drug

Abstract

The involvement of protein kinase C in the signal transduction of gonadotropin-releasing hormone (GnRH) action was investigated with a GnRH superagonist, partial agonists, and antagonists in intact rat pituitary cells. Exposure of 32P-labeled cells to GnRH or to the superagonist [D-Nal(2)6]GnRH (200 times GnRH potency in vivo) induced the enhanced phosphorylation of 42-, 34-, 11-, and 10-kDa proteins and the dephosphorylation of a 15-kDa protein as assessed by sodium dodecyl sulfate-polyacrylamide gel electrophoresis/autoradiography. This effect was blocked in a dose-dependent manner by potent GnRH antagonists. At its maximally effective concentration of 10(-9) M, [D-Nal(2)6]GnRH induced an up to 2 times more pronounced phosphorylation of endogenous substrates than GnRH at 10(-7) M. This was in accord with its ability to cause an 8-fold increase in the translocation of protein kinase C to the particulate fraction vs. 3.4-fold for GnRH. This effect correlated with potency for a series of GnRH agonists ( [D-Nal(2)6]GnRH greater than GnRH greater than [Gly2]LH-RH) and was prevented by GnRH antagonists, as assessed by a novel phorbol ester receptor binding assay and by a standard kinase assay. Downregulation of protein kinase C by prolonged incubation of the pituitary cells with high concentrations of active phorbol esters abolished protein kinase C activity and also prevented the phosphorylation induced by GnRH, or [D-Nal(2)6]GnRH. The same effect was obtained by preincubating the cells with the protein kinase C inhibitor H-7. In this study we identify for the first time physiological substrates for protein kinase C in intact pituitary cells.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1987

19. (1-Beta-mercapto-beta,beta-diethylpropionic acid)-8-lysine-vasopressin, a potent inhibitor of 8-lysine-vasopressin and of oxytocin.

Author

Dyckes DF, Nestor JJ Jr, Ferger MF, and Du Vigneaud V

Subjects

Animals, Blood Pressure drug effects, Blood Volume drug effects, Chickens, Chromatography, Gel, Chromatography, Ion Exchange, Chromatography, Thin Layer, Female, Lysine antagonists & inhibitors, Lysine chemical synthesis, Lysine pharmacology, Propionates chemical synthesis, Propionates pharmacology, Rats, Structure-Activity Relationship, Sulfides chemical synthesis, Sulfides pharmacology, Uterus drug effects, Vasopressins antagonists & inhibitors, Vasopressins pharmacology, Oxytocin antagonists & inhibitors, Vasopressins chemical synthesis

Published

1974

20. "DAKLI": a multipurpose ligand with high affinity and selectivity for dynorphin (kappa opioid) binding sites.

Author

Goldstein A, Nestor JJ Jr, Naidu A, and Newman SR

Subjects

Animals, Avidin metabolism, Binding Sites, Biotin, Brain metabolism, Dynorphins metabolism, Fluorescein-5-isothiocyanate, Fluoresceins, Guinea Pigs, Receptors, Opioid, kappa, Succinimides, Thiocyanates, Peptides metabolism, Receptors, Opioid metabolism

Abstract

We describe a synthetic ligand, "DAKLI" (Dynorphin A-analogue Kappa LIgand), related to the opioid peptide dynorphin A. A single reactive amino group at the extended carboxyl terminus permits various reporter groups to be attached, such as 125I-labeled Bolton-Hunter reagent, fluorescein isothiocyanate, or biotin. These derivatives have high affinity and selectivity for the dynorphin (kappa opioid) receptor. An incidental finding is that untreated guinea pig brain membranes have saturable avidin binding sites.

Published

1988

21. A synthetic fragment of rat transforming growth factor alpha with receptor binding and antigenic properties.

Author

Nestor JJ Jr, Newman SR, DeLustro B, Todaro GJ, and Schreiber AB

Subjects

Amino Acid Sequence, Animals, Chromatography, High Pressure Liquid, Cross Reactions, Epidermal Growth Factor metabolism, ErbB Receptors, Mice, Peptide Fragments chemical synthesis, Peptides immunology, Submandibular Gland analysis, Transforming Growth Factors, Epitopes immunology, Peptide Fragments metabolism, Peptides chemical synthesis, Receptors, Cell Surface metabolism

Abstract

A fragment of rat transforming growth factor alpha (TGF alpha) comprising the third disulfide loop (residues 34-43) was selected as a potential antigenic and receptor binding region. Immunization of rabbits with a peptide conjugate resulted in antibodies which were specific for both the peptide and rat TGF alpha, but not for the homologous epidermal growth factor (EGF). The synthetic decapeptide exhibited low affinity for EGF receptors on human cells. Affinity was increased 100x to 0.2% of EGF or TGF alpha binding by blocking the peptide ends. The blocked decapeptide had no mitogenic activity but prevented the mitogenic effect of EGF and TGF alpha on fibroblasts. This decapeptide is an antagonist and contains an important receptor binding region of TGF alpha.

Published

1985

22. Immuno-enhancing activity of the amino-terminal domain of human prealbumin: isolation, characterization and synthesis.

Author

Burton PM, Horner BL, Jones GH, Lin T, Nestor JJ Jr, Newman SR, Parks TL, Smith AJ, and White A

Subjects

Amino Acid Sequence, Animals, Azathioprine pharmacology, Chromatography, High Pressure Liquid, Humans, In Vitro Techniques, Mice, Mice, Inbred C57BL, Peptide Fragments chemical synthesis, Peptide Fragments pharmacology, Prealbumin chemical synthesis, Prealbumin pharmacology, Rosette Formation, Spleen drug effects, Peptide Fragments isolation & purification, Prealbumin analogs & derivatives, Spleen immunology

Abstract

A decapeptide isolated from highly purified preparations of human prealbumin was able to restore azathioprine (Az) sensitivity, a property of a sub-class of T-lymphocytes, to the spleen rosette-forming cells (RFC) of adult thymectomized (ATx) mice in vitro. The peptide was sequenced by the Edman method and shown to correspond to the ten amino-terminal residues of prealbumin, Gly-Pro-Thr-Gly-Thr-Gly-Glu-Ser-Lys-Cys. Synthesis of this peptide by solid phase methodology confirmed its activity both in vitro and in vivo. Synthesis of a number of structural analogues indicated that the amino-terminal deca, undeca and dodecapeptides of prealbumin as well as some of their derivatives were also able to restore Az sensitivity to RFC in vitro and in vivo. The Cys10 residue and the Glu7 residues both contributed significantly to potency in vitro. Removal of up to three amino acids from the N-terminus of the decapeptide led to a progressive loss of activity. The data indicates that the ability of human prealbumin to restore the Az sensitivity to the RFC of adult Tx mice is intrinsic to the protein and resides in the amino-terminal domain of the molecule.

Published

1987

23. Inhibition of hCG, alpha hCG and progesterone release from human placental tissue in vitro by a GnRH antagonist.

Author

Siler-Khodr TM, Khodr GS, Vickery BH, and Nestor JJ Jr

Subjects

Cells, Cultured, Female, Glycoprotein Hormones, alpha Subunit, Gonadotropin-Releasing Hormone pharmacology, Humans, Placenta drug effects, Pregnancy, Pregnancy Trimester, Second, Chorionic Gonadotropin metabolism, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors, Peptide Fragments metabolism, Placenta metabolism, Progesterone metabolism

Abstract

A dramatic suppression of hCG, alpha hCG and progesterone release from midgestation, human placentas in vitro was effected when incubated with 1 microgram/ml of an antagonist to GnRH. This inhibition of hormonal release occurred rapidly and was partially restored by the addition of GnRH. Human chorionic somatomammotropin was also suppressed, but only two days following the decline of the other hormones. These data demonstrate that an antagonist to GnRH can rapidly inhibit human placental hormone release.

Published

1983

24. Synthesis of a novel class of heteroaromatic amino acids and their use in the preparation of analogues of luteinizing hormone-releasing hormone.

Author

Nestor JJ Jr, Horner BL, Ho TL, Jones GH, McRae GI, and Vickery BH

Subjects

Animals, Benzothiazoles, Chemical Phenomena, Chemistry, Estrus drug effects, Female, Gonadotropin-Releasing Hormone analogs & derivatives, Methods, Pregnancy, Rats, Tryptophan, Alanine analogs & derivatives, Gonadotropin-Releasing Hormone chemical synthesis

Abstract

A novel class of heterocyclic aromatic amino acids based on the 3-(2-benzimidazolyl)alanine system has been generated by chiral synthesis from D- or L-aspartic acid. The use of variously substituted o-phenylenediamines for condensation with the beta-carboxyl function of alpha-benzyl N-(benzyloxycarbonyl)-D-aspartate has led to a series of amino acids of graded hydrophobicity with a steric bulk similar to that of tryptophan. In a similar fashion, we have prepared 3-(2-benzothiazolyl)-D-alanine from o-aminothiophenol and 3-(2-benzoxazolyl)-D-alanine from o-aminophenol. Incorporation of these amino acids into the 6-position of luteinizing hormone-releasing hormone (LH-RH) led to a series of very potent agonist analogues (up to 160 times LH-RH potency), active in doses ranging from 0.1 to 0.5 microgram by twice daily injection in a rat estrus cyclicity suppression assay designed to show the paradoxical antifertility effects of these compounds.

Published

1984

25. (1-beta-mercapto-beta,beta-diethylpropionic acid,4-leucine)-8-lysine-vasopressin and (1-beta-mercapto-beta,beta-diethylpropionic acid,4-leucine)oxytocin, compounds possessing antihormonal properties.

Author

Dyckes DF, Nestor JJ Jr, Ferger MF, Du Vigneaud V, and Chan WY

Subjects

Animals, Blood Pressure drug effects, Chickens, Female, Leucine chemical synthesis, Lysine chemical synthesis, Male, Muscle Contraction drug effects, Muscle, Smooth drug effects, Natriuresis drug effects, Oxytocin antagonists & inhibitors, Oxytocin chemical synthesis, Oxytocin pharmacology, Propionates chemical synthesis, Rats, Structure-Activity Relationship, Uterus drug effects, Vasopressins antagonists & inhibitors, Vasopressins chemical synthesis, Vasopressins pharmacology, Oxytocin analogs & derivatives, Vasopressins analogs & derivatives

Published

1974

26. Design of LHRH agonist drug candidates.

Author

Nestor JJ Jr

Subjects

Biological Availability, Clinical Trials as Topic, Drug Evaluation, Preclinical, Gonadotropin-Releasing Hormone metabolism, Gonadotropin-Releasing Hormone therapeutic use, Kinetics, Metabolic Clearance Rate, Receptors, Cell Surface drug effects, Receptors, Cell Surface physiology, Gonadotropin-Releasing Hormone analogs & derivatives, Hormones chemical synthesis

Published

1987

27. Comparative studies on the hypotensive effect of LHRH antagonists in anesthetized rats.

Author

Lee CH, VanAntwerp D, Hedley L, Nestor JJ Jr, and Vickery BH

Subjects

Animals, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone toxicity, Heart Rate drug effects, Infusions, Intravenous, Male, Oligopeptides administration & dosage, Oligopeptides toxicity, Rats, Rats, Inbred Strains, Blood Pressure drug effects, Gonadotropin-Releasing Hormone antagonists & inhibitors

Abstract

Certain neuropeptides are known to cause a hypotensive response, thought to be due to mast cell degranulation. The effects of five antagonists of luteinizing hormone-releasing hormone on blood pressure and heart rate were compared in the anesthetized rat. When given intravenously, all five compounds induced hypotensive and bradycardiac effects. The order of potency for these effects was Nal-Arg Antagonist approximately detirelix [( N-Ac-D-Nal(2)1, D-pCl-Phe2,D-Trp3,D-hArg(Et2)6,D-Ala10]LHRH) greater than [N-Ac-D-Nal(2)1, D-pCl-Phe2,D-Pal(3)3,D-hArg(Et2)6,L-hArg (Et2)8,D-Ala10]LHRH (RS-26306) approximately antide greater than [N-Ac-D-Nal(2)1, D-pCl-Phe2,D-Pal(3)3,6, L-hArg(Et2)8,D-Ala10]LHRH (RS-15378) and did not parallel the order of antiovulatory potencies of these compounds. The hypotensive activity of LHRH antagonists, therefore, appeared dissociable from their antiovulatory activity. RS-26306 and RS-15378 appeared to have the greatest therapeutic ratios.

Published

1989

28. Suppression of luteal function by a luteinizing hormone-releasing hormone antagonist during the early luteal phase in the stumptailed macaque monkey and the effects of subsequent administration of human chorionic gonadotropin.

Author

Fraser HM, Nestor JJ Jr, and Vickery BH

Subjects

Animals, Corpus Luteum drug effects, Estradiol blood, Female, Follicle Stimulating Hormone blood, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone pharmacology, Luteinizing Hormone blood, Macaca, Progesterone blood, Chorionic Gonadotropin pharmacology, Corpus Luteum physiology, Gonadotropin-Releasing Hormone antagonists & inhibitors, Luteal Phase drug effects

Abstract

In previous studies a single sc injection of the LHRH antagonist [N-Ac-D-Nal(2)1,D-pCl-Phe2,D-Trp3,D-hArg(Et2)6,D-Ala10 ]LHRH during the luteal phase of the stumptailed macaque menstrual cycle caused a transient suppression of serum LH and progesterone concentrations. To investigate whether a more prolonged suppression of LH release during the early luteal phase could result in a sustained suppression of progesterone, 10 monkeys were treated with 3 consecutive daily injections of 300 micrograms LHRH antagonist/kg beginning on days 0 (n = 2), 1 (n = 1), 2 (n = 1), 3 (n = 2), 4 (n = 2), and 5 (n = 2) after the LH surge. When the antagonist was administered on the day of the LH surge, serum concentrations of bioactive LH were still elevated on the following day, but then fell to low levels. Serum progesterone concentrations were subnormal in these monkeys for the next 10 days, but recovered toward the late luteal phase. In the 8 monkeys receiving antagonist starting between days 1-5 after the LH surge, serum concentrations of bioactive LH were suppressed to near the detection limit of the assay for 4 days after the first injection. Seven of the 8 monkeys demonstrated a progressive decline in serum progesterone concentrations to undetectable values which remained for the duration of the luteal phase. In the remaining monkey the decline in progesterone was less marked; this animal presented a normal progesterone profile 3 days after the last antagonist injection. Premature menses occurred in all 8 monkeys; the next ovulation occurred 18.9 +/- 0.3 days after the last antagonist injection. To test luteal function after antagonist treatment during the early luteal phase and to mimic the rescue of the corpus luteum during a fertile cycle and assess the contraceptive effects of antagonist, hCG in daily doses of 30, 60, 90, 180, and 360 IU was administered starting on day 7 of the luteal phase to monkeys previously treated with three daily injections of 300 micrograms antagonist/kg during the early luteal phase. Control monkeys received hCG injections alone. In the controls, hCG administration elevated serum progesterone concentrations to 15-20 ng/ml. In three monkeys in which antagonist administration did not commence until day 5 or 6, hCG overcame the suppressive effect of the antagonist. However, in seven monkeys in which antagonist administration began on days 1-4, hCG caused only a small progesterone rise (maximal range, 1.8-4.9 ng/ml), about 20% of that observed in control monkeys receiving hCG.(ABSTRACT TRUNCATED AT 400 WORDS)

Published

1987

29. Synthesis and biological activity of some very hydrophobic superagonist analogues of luteinizing hormone-releasing hormone.

Author

Nestor JJ Jr, Ho TL, Simpson RA, Horner BL, Jones GH, McRae GI, and Vickery BH

Subjects

Amino Acids analysis, Animals, Chemical Phenomena, Chemistry, Chromatography, High Pressure Liquid, Contraceptives, Oral, Hormonal, Estrus drug effects, Female, Gonadotropin-Releasing Hormone chemical synthesis, Gonadotropin-Releasing Hormone pharmacology, Peptides chemical synthesis, Pregnancy, Rats, Rats, Inbred Strains, Solubility, Gonadotropin-Releasing Hormone analogs & derivatives

Abstract

The effect of increased hydrophobicity at position 6 of luteinizing hormone-releasing hormone (LH-RH) has been investigated by the incorporation of a series of 15 very hydrophobic, unnatural D-amino acids at this position. The unnatural amino acids studied can be considered analogues of phenylalanine with carbocyclic aromatic side chains consisting of substituted phenyl (e.g., 2,4,6-trimethylphenyl, p-biphenyl) or polycyclic aromatic (e.g., naphthalene, anthracene) units. When enzymatic resolution (subtilisin Carlsberg) of the most hydrophobic amino acids failed, the racemic amino acids were incorporated, and the diastereomeric LH-RH analogues were resolved by preparative high-performance liquid chromatography. The analogues were synthesized by the solid-phase technique. All of the synthetic compounds were very potent LH-RH superagonists, but [6-(3-(2-naphthyl)-D-alanine)]LH-RH, [6-(3-(2-naphthyl)-D-alanine), 7-(N alpha-methylleucine)]LH-RH and [6-(3-(2,4,6-trimethylphenyl)-D-alanine)]LH-RH appear to be among the most potent LH-RH agonist analogues yet reported when tested in a rat estrus cyclicity suppression assay designed to show the paradoxical antifertility effects of these compounds [ED50 approximately 7 x 10(-8) g; twice daily in saline]. These analogues are twice as potent as [D-Trp6,ProNHEt9]LH-RH in this assay system (i.e., approximately 200 times the potency of LH-RH).

Published

1982

30. Suppression of plasma gonadotropins and testosterone in adult male monkeys (Macaca fascicularis) by a potent inhibitory analog of gonadotropin-releasing hormone.

Author

Adams LA, Bremner WJ, Nestor JJ Jr, Vickery BH, and Steiner RA

Subjects

Animals, Gonadotropin-Releasing Hormone pharmacology, Kinetics, Macaca fascicularis, Male, Orchiectomy, Radioimmunoassay, Sexual Maturation, Time Factors, Follicle Stimulating Hormone blood, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors, Luteinizing Hormone blood, Testosterone blood

Abstract

The reduction of circulating levels of gonadotropins and testosterone is of value for the treatment of steroid-dependent neoplasms and the control of fertility. We tested the ability of single and multiple doses of the GnRH antagonist [N-Ac-D-Nal(2)1, D-pCl-Phe2, D-Trp3, D-hArg(Et2)6, D-Ala10]GnRH (GnRH-Ant) to suppress levels of these hormones in intact and castrate adult male cynomolgus monkeys. In Exp I, single injections of the antagonist at doses of 0 (vehicle), 5, 50, 250, and 500 micrograms/kg BW were given to castrate and intact animals. In Exp II, daily injections of antagonist at doses of 0, 50, 100, or 250 micrograms/kg BW were given to intact animals for 21 days. Plasma levels of testosterone, FSH, and LH were determined by RIA, and in intact animals, LH levels were measured by bioassay. In Exp 1, a single injection of 5 micrograms/kg BW or more of GnRH-Ant to castrate animals significantly reduced plasma LH and FSH by 4 h after injection (P less than or equal to 0.01). Nadir levels (40% of preinjection control values) of LH and FSH were reached 8 and 24 h, respectively, after administration of 250 or 500 micrograms/kg BW, and these hormones remained significantly lower than preinjection values over at least 48 h (P less than or equal to 0.05). A single injection of 50 micrograms/kg BW or more of antagonist to intact animals markedly reduced plasma LH and testosterone by 6 h after administration (P less than or equal to 0.05), while 250 or 500 micrograms/kg BW antagonist maintained LH and testosterone levels below 30% (P less than or equal to 0.05) of preinjection values for 24 h. In Exp II, daily injections of 250 micrograms/kg BW antagonist to intact animals resulted in near-castrate levels of plasma testosterone which were achieved by 24 h after the first injection of antagonist and persisted for the ensuing 20 days. Daily injections of 100 micrograms/kg BW or less of antagonist were ineffective in suppressing testosterone. Thus, this potent GnRH antagonist acutely and chronically lowers gonadotropin and testosterone levels in adult male cynomolgus monkeys. By virtue of its inhibitory effect, this antagonist is potentially useful as a therapeutic agent in clinical situations requiring long term suppression of testicular function, such as fertility control, the treatment of steroid-dependent neoplasms, and precocious puberty.

Published

1986

31. Synthesis and some pharmacological properties of (1-deamino,9-thioglycine)oxytocin.

Author

Jones WC Jr, Nestor JJ Jr, and Du Vigneaud V

Subjects

Animals, Chickens, Deamination, Female, Glycine chemical synthesis, Glycine pharmacology, Methods, Muscle Contraction drug effects, Oxytocin pharmacology, Rats, Structure-Activity Relationship, Thiones chemical synthesis, Thiones pharmacology, Uterus drug effects, Oxytocin chemical synthesis

Published

1973