Your search keyword '"Haviv, F."' showing total 8 results

1. Elimination of antibacterial activities of non-peptide luteinizing hormone-releasing hormone (LHRH) antagonists derived from erythromycin A.

Author

Randolph JT, Sauer DR, Haviv F, Nilius AM, and Greer J

Subjects

Animals, CHO Cells, Cricetinae, Humans, Microbial Sensitivity Tests, Protein Binding physiology, Staphylococcus drug effects, Staphylococcus growth & development, Streptococcus drug effects, Streptococcus growth & development, Structure-Activity Relationship, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents metabolism, Erythromycin chemistry, Erythromycin metabolism, Gonadotropin-Releasing Hormone antagonists & inhibitors, Gonadotropin-Releasing Hormone metabolism

Abstract

Antibacterial SAR for a series of macrolides derived from erythromycin A that are potent LHRH antagonists was developed in an attempt to eliminate the antibiotic activities of these compounds. Increasing the size of the alkyl substituents on the desosamine 3'-amine resulted in potent LHRH antagonists that were inactive against staphylococcal bacteria strains, and were significantly (>10-fold) less active against streptococcal bacteria strains. Complete elimination of antibacterial activities could be achieved by replacement of one or both methyl groups on the 3'-amine with a large alkyl substituent.

Published

2004

2. Nonpeptide luteinizing hormone-releasing hormone antagonists derived from erythromycin A: design, synthesis, and biological activity of cladinose replacement analogues.

Author

Randolph JT, Waid P, Nichols C, Sauer D, Haviv F, Diaz G, Bammert G, Besecke LM, Segreti JA, Mohning KM, Bush EN, Wegner CD, and Greer J

Subjects

Administration, Oral, Animals, Cells, Cultured, Cricetinae, Drug Design, Erythromycin pharmacology, Gonadotropin-Releasing Hormone blood, Gonadotropin-Releasing Hormone metabolism, Hexoses pharmacology, Humans, Injections, Intravenous, Male, Models, Molecular, Orchiectomy, Pituitary Gland cytology, Pituitary Gland metabolism, Rats, Structure-Activity Relationship, Erythromycin analogs & derivatives, Erythromycin chemical synthesis, Gonadotropin-Releasing Hormone antagonists & inhibitors, Hexoses chemical synthesis

Abstract

The design and synthesis of a series of 11,12-cyclic carbamate derivatives of 6-O-methylerythromycin A that are novel, nonpeptide LHRH antagonists, is described. The macrolide antagonist 1, discovered during a screen of our chemical repository, was compared to a macrocyclic peptide antagonist 2 using molecular modeling, thus providing a model for the design of more potent antagonists. Medicinal chemistry efforts to find a replacement for cladinose at position 3 of the erythronolide core provided a series of oxazolidinone carbamates that were equally as active as the cladinose-containing parent macrolides. The descladinose LHRH antagonist 14 has 1-2 nM affinity for both rat and human LHRH receptors and is a potent inhibitor of LH release (pA2 = 8.76) in vitro. In vivo, 14 was found to produce a dose-dependent suppression of LH in male castrate rats via both i.v. and p.o. dosing.

Published

2004

3. LHRH antagonists.

Author

Haviv F, Bush EN, Knittle J, and Greer J

Subjects

Animals, Gonadotropin-Releasing Hormone agonists, Humans, Oligopeptides pharmacokinetics, Solubility, Structure-Activity Relationship, Gonadotropin-Releasing Hormone antagonists & inhibitors, Hormone Antagonists pharmacology, Oligopeptides pharmacology

Abstract

After almost two decades, the research on LHRH antagonists has produced a number of decapeptides that are currently in clinical studies. The structures of these antagonists, unlike the agonists, differ substantially from that of LHRH. Five of the ten amino acids are unnatural and of D configuration. The structural combination of a hydrophobic N-terminus (residues 1, 2, and 3) and a basic/hydrophilic C-terminus (residues 6 and 8) was thought to be responsible for some HR reactions encountered with the second generation of LHRH antagonists. This side effect was greatly reduced by substituting the appropriate combination of amino acids at positions 5, 6, and 8. The next hurdle in the drug development of LHRH antagonists was solubility and aggregation. In the case of A-75998, water solubility was improved by 12- to 25-fold via substitution of NMeTyr at position 5. However, based on DLS analysis, the aqueous solutions still contained some large aggregates that were not visible to the naked eye. This formation of aggregates was eliminated on formulating A-75998 in Encapsin. In men, a single s.c. dose of 2 mg of A-75998 suppressed T to the castrate levels for over 30 hr. Other LHRH antagonists including ganirelix and cetrorelix are also in phase I/II clinical studies. Clinical studies with cetrorelix in prostate cancer; in vitro fertilization, and benign prostate hypotrophy have been reported.

Published

1998

4. In vitro and in vivo activities of reduced-size antagonists of luteinizing hormone-releasing hormone.

Author

Haviv F, Fitzpatrick TD, Nichols CJ, Bush EN, Diaz G, Bammert G, Nguyen AT, Johnson ES, Knittle J, and Greer J

Subjects

Amino Acid Sequence, Animals, Castration, Drug Design, Gonadotropin-Releasing Hormone chemical synthesis, Gonadotropin-Releasing Hormone chemistry, Gonadotropin-Releasing Hormone pharmacokinetics, Gonadotropin-Releasing Hormone pharmacology, Histamine Release drug effects, Luteinizing Hormone metabolism, Mast Cells drug effects, Mast Cells physiology, Molecular Sequence Data, Oligopeptides pharmacokinetics, Oligopeptides pharmacology, Peptide Fragments pharmacokinetics, Peptide Fragments pharmacology, Pituitary Gland drug effects, Pituitary Gland metabolism, Rats, Structure-Activity Relationship, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone antagonists & inhibitors, Oligopeptides chemical synthesis, Peptide Fragments chemical synthesis

Abstract

A novel series of octapeptide LHRH antagonists was designed on the basis of the structure of the (2-9) fragment of a LHRH agonist. By adopting a systematic SAR study, we were able to improve first the in vitro activity and then the in vivo LH suppression, raising them up to the range of the decapeptide antagonists NalGlu (51) and A-75998 (50), resulting in A-76154 (49). The octapeptide antagonist A-76154 is the most potent reduced-size LHRH antagonist reported. It suppresses LH in the castrated rat by over 80% for a period of 4 h following sc bolus administration of 30 micrograms/kg.

Published

1994

5. Differential orientation of a GnRH agonist and antagonist in the pituitary GnRH receptor.

Author

Janovick JA, Haviv F, Fitzpatrick TD, and Conn PM

Subjects

Affinity Labels, Amino Acid Sequence, Animals, Cell Membrane metabolism, Female, Gonadotropin-Releasing Hormone antagonists & inhibitors, Gonadotropin-Releasing Hormone chemistry, Molecular Sequence Data, Molecular Weight, Oligopeptides chemistry, Photochemistry, Pyrrolidonecarboxylic Acid analogs & derivatives, Rats, Gonadotropin-Releasing Hormone analogs & derivatives, Oligopeptides metabolism, Pituitary Gland metabolism, Receptors, LHRH metabolism

Abstract

In the present study we have used a high affinity photoaffinity label (PAL) agonist (pGlu-His-Trp-Ser-125I-iodoTyr-D-Lys(para-N3-Benzoyl)-Leu-Arg-P roNHEt) and a PAL antagonist (NAcD2Nal-D4ClPhe-D3Pal-Ser-125I-iodo-NMeTyr-D-L ys(para-N3-Benzoyl)Leu-Lys(Isp) - Pro-D-Ala-NH2) to covalently label the GnRH receptor. Rat pituitary membranes were incubated 3 h with either the radioiodinated agonist or antagonist in the dark, exposed to UV light, then electrophoresed in SDS. The PAL agonist and antagonist labeled broad bands (estimated molecular weight [M(r)] 46K-60K). Labeling by either PAL agonist or antagonist was displaced by unlabeled agonist or antagonist, indicating that the agonist and antagonist bind to the same molecule. The broad band, believed to reflect differential glycosylation, was divided into six sections corresponding M(r) to 60K, 56K, 52K, 48K, 46K and 44K for the agonist and 62K, 58K, 54K, 52K, 48K and 45K for the antagonist; these were electroeluted with recovery > 80% based on radioactivity. Each could be re-electrophoresed to the same location from which it was eluted. Other eluted samples were treated with trypsin. The M(r) of the samples labeled with the agonist PAL were shifted to M(r) 48K, 42K, 40K, 37K, 35K and 33K by proteolysis. The observation that each section shifted approximately the same M(r) after trypsin treatment suggests that the backbone of the labeled proteins in each gel section is identical. Samples labeled with the antagonist PAL were shifted to M(r) < 10,000 in all cases. These data indicate that the agonist and antagonist PALs bind to different regions of the GnRH receptor and, therefore, are likely oriented differently with respect to the receptor and support the view that different strategies should be used for the design of agonists and antagonists.

Published

1993

6. The effect of NMeTyr5 substitution in luteinizing hormone-releasing hormone antagonists.

Author

Haviv F, Fitzpatrick TD, Nichols CJ, Swenson RE, Mort NA, Bush EN, Diaz G, Nguyen AT, Holst MR, and Cybulski VA

Subjects

Amino Acid Sequence, Animals, Methyltyrosines metabolism, Methyltyrosines pharmacology, Molecular Sequence Data, Peptides metabolism, Peptides pharmacology, Rats, Receptors, LHRH metabolism, Structure-Activity Relationship, Gonadotropin-Releasing Hormone antagonists & inhibitors, Methyltyrosines chemical synthesis, Peptides chemical synthesis

Published

1993

7. Effect of N-methyl substitution of the peptide bonds in luteinizing hormone-releasing hormone agonists.

Author

Haviv F, Fitzpatrick TD, Swenson RE, Nichols CJ, Mort NA, Bush EN, Diaz G, Bammert G, Nguyen A, and Rhutasel NS

Subjects

Amino Acid Sequence, Animals, Chymotrypsin metabolism, Gonadotropin-Releasing Hormone chemical synthesis, Gonadotropin-Releasing Hormone metabolism, Gonadotropin-Releasing Hormone pharmacology, In Vitro Techniques, Intestinal Mucosa metabolism, Leuprolide analogs & derivatives, Leuprolide pharmacology, Luteinizing Hormone metabolism, Male, Methylation, Models, Molecular, Molecular Sequence Data, Nafarelin analogs & derivatives, Nafarelin pharmacology, Peptides chemical synthesis, Peptides pharmacology, Pituitary Gland metabolism, Rats, Receptors, LHRH metabolism, Structure-Activity Relationship, Triptorelin Pamoate analogs & derivatives, Gonadotropin-Releasing Hormone analogs & derivatives

Abstract

Each peptide bond in leuprolide (1), deslorelin (13), and nafarelin (24) was separately substituted with N-methyl. The synthesized compounds were tested for in vitro receptor binding, LH release, and stability against chymotrypsin and intestinal degradation. The NMe-Ser4 (30), NMe-Leu7 (33), and Sar10 (35) analogues of nafarelin had pD2 values 2-, 20-, 9-fold higher than their respective parent. All the other N-methyl agonists were less active. For the first time, conversion of LHRH agonists to antagonists was observed as a result of N-methyl substitution in the peptide backbone. [NMe-Phe2,DLeu6,Pro9NHEt]LHRH (4), [NMe-1Nal3,DLeu6,Pro9NHEt]LHRH (6), [NMe-His2,DTrp6,Pro9NHEt]LHRH (14), [NMe-Phe2,DNal6]LHRH (27), and [D2Nal6,NMe-Arg8]LHRH (34) exhibited antagonist responses. Substitutions of NMe-1Nal3, NMe-Ser4, or NMe-Tyr5 in leuprolide rendered the 3-4 peptide bond in these compounds completely stable to chymotrypsin. Examination of the three-dimensional structure of leuprolide when bound to the active site of chymotrypsin, reveals the NH's of residues 3 and 5 are involved in hydrogen bond interactions with the enzyme. N-Methylation at these positions is not only disrupting the hydrogen bond interactions, but is also sterically preventing the substrate from fitting in the enzyme's active site. All the compounds in the leuprolide series were also tested against intestinal degradation using an in vitro rat jejunum sac assay. In this model the pattern of stabilization was similar, but not identical, to that against chymotrypsin. The pharmacokinetics of all the analogues in the leuprolide series and of several others in the deslorelin and nafarelin series were determined. The clearance values of all the three NMe-Tyr5 analogues, 8, 20, and 31 were lower than their respective parents. These slower clearances suggest lower rates of metabolism.

Published

1993

8. Active reduced-size hexapeptide analogues of luteinizing hormone-releasing hormone.

Author

Haviv F, Palabrica CA, Bush EN, Diaz G, Johnson ES, Love S, and Greer J

Subjects

Animals, Cells, Cultured, Gonadotropin-Releasing Hormone pharmacology, Kinetics, Male, Orchiectomy, Peptide Fragments pharmacology, Pituitary Gland metabolism, Rats, Receptors, LHRH metabolism, Structure-Activity Relationship, Gonadotropin-Releasing Hormone analogs & derivatives, Gonadotropin-Releasing Hormone chemical synthesis, Luteinizing Hormone metabolism, Peptide Fragments chemical synthesis, Pituitary Gland drug effects, Receptors, LHRH drug effects

Abstract

A series of reduced-size hexapeptide analogues of LH-RH were synthesized that contain the residues corresponding to amino acid positions 4-9 and are linked to various carboxylic acids in place of residue 3. These compounds were tested in vitro in the rat pituitary receptor binding and LH release assays. A wide range of binding affinities was obtained up to and exceeding that of LH-RH. Both agonists and antagonists were obtained. From the SAR studies, it appears that a very precise size, length, and shape of the substituent at position 3 is required to achieve agonist activity, whereas the structural requirements for antagonist activity appear to be much less stringent. Depending on the nature of the substituent at positions 6 and 4, the biological response switches from antagonist to agonist or vice versa. The results suggest that conformational changes at position 6 or 4 feed back to the substituent at position 3, which induces the change from agonist to antagonist. The most potent compounds in the series were tested in vivo and found to be active.

Published

1989