Histaprodifens:  Synthesis, Pharmacological in Vitro Evaluation, and Molecular Modeling of a New Class of Highly Active and Selective Histamine H<sub>1</sub>-Receptor Agonists

Elz, Sigurd; Krämer, Kai; Pertz, Heinz H.; Detert, M.; Laak, Antonius ter; Kuehne, Ronald; Schunack, Walter

doi:10.1021/jm991056a

Cited by 77 publications

(107 citation statements)

References 53 publications

(127 reference statements)

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“…H 1 R agonists are divided into three classes ( Fig. 1): 1) small agonists (2-4) derived from histamine (1), 2) histamine derivatives with bulkier aromatic substituents at position 2 of the imidazole ring (5-18), and 3) histaprodifens, e.g., compounds 19 to 23 Zingel et al, 1995;Elz et al, 2000). H 1 R agonists are important experimental tools to analyze H 1 R function in cellular and organ systems (Zingel et al, 1995;Hill et al, 1997).…”

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confidence: 99%

“…In fact, the K d values of [ 3 H]mepyramine for H 1 Rs from various species differ by ϳ2 to 6-fold (Chang et al, 1979). Moreover, histaprodifens exhibit different potencies and efficacies in the guinea pig ileum and rat aorta (Elz et al, 2000). Furthermore, 2-(3-chlorophenyl)histamine (12) is a potent H 1 R agonist in the guinea pig ileum but failed to exhibit agonistic activity in H 1 R-expressing dibutyryl cAMP-differentiated human HL-60 leukemia cells (Seifert et al, 1994).…”

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confidence: 99%

“…3). Mutagenesis data (Leurs et al, , 1995Ohta et al, 1994;Nonaka et al, 1998) and modeling approaches (Elz et al, 2000) indicated that histamine and histaprodifens interact with amino acid residues in TMs III, IV, V, and VII. Considering the alignment of H 1 Rs with bovine rhodopsin (Palczewski et al, 2000) and results of the substituted-cysteine accessibility method with the dopamine D 2 -receptor (Ballesteros et al, 2001), there are no amino acid differences in the ligand binding pocket of gpH 1 R and hH 1 R. The two lipid-directed residues, Phe-153 in TM IV of hH 1 R versus Leu in gpH 1 R and Ile-433 in TM VI of hH 1 R versus Val in gpH 1 R, represent the only differences near the binding site.…”

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Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Seifert¹,

Wenzel-Seifert²,

Bürckstümmer³

et al. 2003

J Pharmacol Exp Ther

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Species isoforms of histamine H 2 -, H 3 -, and H 4 -receptors differ in their pharmacological properties. The study aim was to dissect differences between the human H 1 R (hH 1 R) and guinea pig H 1 R (ghH 1 R). We coexpressed hH 1 R and gpH 1 R with regulators of G-protein signaling in Sf9 insect cells and analyzed the GTPase activity of G q -proteins. Small H 1 R agonists showed similar effects at hH 1 R and gpH 1 R, whereas bulkier 2-phenylhistamines and histaprodifens were up to ϳ10-fold more potent at gpH 1 R than at hH 1 R. Most 2-phenylhistamines and histaprodifens were more efficacious at gpH 1 R than at hH 1 R. Several first-generation H 1 R antagonists were ϳ2-fold, and arpromidine-type H 1 R antagonists up to ϳ10-fold more potent at gpH 1 R than at hH 1 R. [ The Phe-1533 Leu-153/Ile-4333 Val-433 double mutant expressed excellently but only partially changed the pharmacological properties of hH 1 R. Small H 1 R agonists and 2-phenylhistamines interacted differentially with human and guinea pig H 2 R in terms of potency and efficacy, respectively. Our data show the following: 1) there are differences in agonist-and antagonistpharmacology of hH 1 R and gpH 1 R encompassing diverse classes of bulky ligands. These differences may be explained by higher conformational flexibility of gpH 1 R relative to hH 1 R; 2) Phe-153 and Ile-433 are critical for proper folding and expression of hH 1 R; and 3) H 2 R species isoforms distinguish between H 1 R agonists.Histamine serves as a neurotransmitter and autacoid and acts through specific H x Rs designated as H 1 R, H 2 R, H 3 R, and H 4 R, respectively (Hill et al., 1997;Hough, 2001). The H 1 R couples to G q -proteins. Numerous H 1 R agonists and antagonists are known. H 1 R agonists are divided into three classes ( Fig. 1): 1) small agonists (2-4) derived from histamine (1), 2) histamine derivatives with bulkier aromatic substituents at position 2 of the imidazole ring (5-18), and 3) histaprodifens, e.g., compounds 19 to 23 Zingel et al., 1995;Elz et al., 2000). H 1 R agonists are important experimental tools to analyze H 1 R function in cellular and organ systems (Zingel et al., 1995;Hill et al., 1997). H 1 R antagonists are commonly divided into sedating (first-generation, 24-32) and nonsedating (second-generation, 41-45) antagonists (Fig. 2). Today, especially the second-generation H 1 R antagonists are of great importance for the treatment of allergic diseases (Hill et al., 1997). Guanidines 33, 34, and 36 to 39 derived from arpromidine (35) are dual H 2 R agonists/ H 1 R antagonists (Buschauer, 1989).The availability of H x R cDNAs allowed for the comparison of the pharmacological properties of H x R species isoforms in recombinant systems under identical experimental conditions. Such expression studies uncovered species differences This work was supported by the National Institutes of Health COBRE Award 1 P20 RR15563 and matching support from the State of Kansas and the University of Kansas (R.S.), a grant from the Army Research Office (DAAD 19-00-...

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Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Seifert¹,

Wenzel-Seifert²,

Bürckstümmer³

et al. 2003

J Pharmacol Exp Ther

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“…A Rotiszint ecoplus (Roth, Karlsruhe, Germany) liquid scintillation cocktail was used. Histaprodifens were synthesized as described by Elz et al (2000), Menghin et al (2003), andStriegl (2006). Construction of pGEMh gpE2 H 1 R, pGEMh gpNgpE2 H 1 R, pVLh gpE2 H 1 R, and pVLh gpNgpE2 H 1 R. First, a pGEM-3Z-SFh gpN H 1 R plasmid was constructed.…”

Section: Methodsmentioning

confidence: 99%

“…1), identified as potent H 1 R agonists at the guinea pig (gp) ileum (Elz et al, 2000;Menghin et al, 2003), a 3,3-diphenylpropyl moiety is combined with a 2-substituted histamine. A pharmacological characterization of histaprodifens at the human H 1 R (hH 1 R) and guinea pig H 1 R (gpH 1 R) showed significant species differences Straßer et al, 2008).…”

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Ligand-Specific Contribution of the N Terminus and E2-Loop to Pharmacological Properties of the Histamine H₁-Receptor

Straßer¹,

Wittmann²,

Seifert³

2008

J Pharmacol Exp Ther

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There are species differences between human histamine H 1 receptor (hH 1 R) and guinea pig (gp) histamine H 1 receptor (gpH 1 R) for phenylhistamines and histaprodifens. Several studies showed participation of the second extracellular loop (E2-loop) in ligand binding for some G protein-coupled receptors (GPCRs). Because there are large species differences in the amino acid sequence between hH 1 R and gpH 1 R for the N terminus and E2-loop, we generated chimeric hH 1 Rs with gp E2-loop (h gpE2 H 1 R) and gp N terminus and gp E2-loop (h gpNgpE2 H 1 R). hH 1 R, gpH 1 R, and chimeras were expressed in Sf9 insect cells. [3 H]Mepyramine binding assays and steadystate GTPase assays were performed. In the series hH 1 R Ͼ h gpE2 H 1 R Ͼ h gpNgpE2 H 1 R, we observed a significant decrease in potency of histamine 1 in the GTPase assay. For phenoprodifen 5 and the chiral phenoprodifens 6R and 6S, a significant decrease in affinity and potency was found in the series hH 1 R Ͼ h gpE2 H 1 R Ͼ h gpNgpE2 H 1 R. In addition, we constructed new active-state H 1 R models based on the crystal structure of the human ␤ 2 -adrenergic receptor (h␤ 2 AR). Compared with the H 1 R active-state models based on the crystal structure of bovine rhodopsin, the E2-loop differs in its contact to the ligand bound in the binding pocket. In the bovine rhodopsin-based model, the backbone carbonyl of Lys187 (gpH 1 R) interacts with large histaprodifens in the binding pocket, but in the h␤ 2 ARbased model, Lys187 (gpH 1 R) is located distantly from the binding pocket. In conclusion, the differences in N terminus and E2-loop between hH 1 R and gpH 1 R exert an influence on affinity and/or potency for histamine and phenoprodifens 5, 6R, and 6S.

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Potassium‐Zincate‐Catalyzed Benzylic C−H Bond Addition of Diarylmethanes to Styrenes

et al. 2018

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Direct functionalization of the benzylic C À Hb ond of diarylmethanes is an important strategy for the synthesis of diarylmethine-containing compounds.H owever,t he methods developed to date for this purpose require as toichiometric amount (usually more) of either as trong base or an oxidant. Reported here is the first catalytic benzylic C À Hbond addition of diarylmethanes to styrenes and conjugated dienes.A potassium zincate complex, generated from potassium benzyl and zinc amide,acts as acatalyst and displays good activity and chemoselectivity.C onsidering the atom economy of the reaction and the ready availability of the catalyst, this reaction constitutes ap ractical, efficient method for diarylalkane synthesis.Supportinginformation and the ORCID identification number(s) for the author(s) of this article can be found under: https://doi.

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Histaprodifens: Synthesis, Pharmacological in Vitro Evaluation, and Molecular Modeling of a New Class of Highly Active and Selective Histamine H₁-Receptor Agonists

Cited by 77 publications

References 53 publications

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Ligand-Specific Contribution of the N Terminus and E2-Loop to Pharmacological Properties of the Histamine H₁-Receptor

Potassium‐Zincate‐Catalyzed Benzylic C−H Bond Addition of Diarylmethanes to Styrenes

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Histaprodifens: Synthesis, Pharmacological in Vitro Evaluation, and Molecular Modeling of a New Class of Highly Active and Selective Histamine H1-Receptor Agonists

Cited by 77 publications

References 53 publications

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H1-Receptor

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H1-Receptor

Ligand-Specific Contribution of the N Terminus and E2-Loop to Pharmacological Properties of the Histamine H1-Receptor

Potassium‐Zincate‐Catalyzed Benzylic C−H Bond Addition of Diarylmethanes to Styrenes

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Histaprodifens: Synthesis, Pharmacological in Vitro Evaluation, and Molecular Modeling of a New Class of Highly Active and Selective Histamine H₁-Receptor Agonists

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Multiple Differences in Agonist and Antagonist Pharmacology between Human and Guinea Pig Histamine H₁-Receptor

Ligand-Specific Contribution of the N Terminus and E2-Loop to Pharmacological Properties of the Histamine H₁-Receptor