Compared pharmacology of human histamine H<sub>3</sub> and H<sub>4</sub> receptors: structure–activity relationships of histamine derivatives

Gbahou, Florence; Vincent, Ludwig; Humbert-Claude, Marie; Tardivel-Lacombe, J.; Chabret, Claude; Arrang, Jean‐Michel

doi:10.1038/sj.bjp.0706666

Cited by 59 publications

(41 citation statements)

References 57 publications

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“…[51][52][53] Studies comparing the receptor pharmacology of hH 3 R and hH 4 R show remarkable differences in SAR of imidazole-containing ligands concerning affinity and efficacy 49,54) (Figs. 3, 4).…”

Section: Molecular Aspectsmentioning

confidence: 99%

“…50) The hH 4 R possesses a higher similarity to hH 3 R with a sequence homology ranging from 38% up to 58% within the transmembrane domains. [51][52][53] Studies comparing the receptor pharmacology of hH 3 R and hH 4 R show remarkable differences in SAR of imidazole-containing ligands concerning affinity and efficacy 49,54) (Figs. 3, 4).…”

Section: Molecular Aspectsmentioning

confidence: 99%

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Histamine H3 Receptor Antagonists Go to Clinics

Sander

Kottke

Stark

2008

Biological & Pharmaceutical Bulletin

184

116

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INTRODUCTIONThe biogenic amine histamine, 2-(1H-imidazol-4-yl)-ethanamine, is produced by decarboxylation of L-histidine and is implicated in a wide range of physiological and pathophysiological functions. It is metabolised by histamine N tmethyltransferase (HMT) and mono-or diaminoxidase. Histamine is mainly acting via four distinct metabotropic histamine receptor subtypes (H 1 R-H 4 R), which have meanwhile all been cloned. Whereas antagonists for H 1 R and H 2 R subtypes have been blockbusters in therapy of allergy and ulcer, respectively, antagonists for H 3 R and H 4 R subtypes are not on the market. The recently described H 4 R seems to be involved in inflammatory and immunomodulatory processes. H 3 Rs play a central role in neurotransmission of histamine and in control of many other neurotransmitters. Several antagonists are in preclinical and some in clinical stage of development. PHARMACOLOGICAL BACKGROUND Auto-and HeteroreceptorThe H 3 R was first described in 1983 as a presynaptic autoreceptor, which mediates synthesis of histamine and inhibition of its release from histaminergic neurons in slices of rat cerebral cortex. 1) Localisation studies in rodents show a predominance in distinct regions of the central nervous system (CNS) as the H 3 R is mainly located in cerebral cortex, hippocampus, amygdala, nucleus accumbens, globus pallidus, striatum, and hypothalamus 2-5) ( Fig. 1). In addition, it is expressed in the peripheral nervous system, e.g. in gastrointestinal tract, airways and cardiovascular system. 6) Molecular aspects of the receptor, [7][8][9][10] structure-activity relationships (SAR) of ligands, [11][12][13][14][15][16][17][18][19] and pharmacology [20][21][22][23][24][25][26] have recently been resumed in many excellent reviews. This contribution focuses on the development of clinical candidates and the multifaceted potential indications targeted.In mammalian brain histaminergic neurons originate in the tuberomammillary nucleus (TMN) spreading into above mentioned brain regions, where they control histamine levels by regulation of synthesis and liberation rates 27) and modulate different neuronal systems. 28) H 3 R expression is not solely restricted to histaminergic neurons: due to its function as a heteroreceptor it can be found on colocalised neurons, and H 3 R activation modulates the release of various important neurotransmitters, i.e. dopamine, [29][30][31][32][33] acetylcholine, [34][35][36][37] norepinephrine, 38,39) serotonin, 40,41) GABA, [42][43][44] glutamate, 45) and substance P. [46][47][48] Therefore, histaminergic neurons and the cross-linkage between major neurotransmitter systems are involved in many (patho)physiological brain functions, including vigilance, memory processes, feeding behaviour and locomotor activity (Fig. 2). Interneuron cross-talk and adaptive processes seem to be important factors in H 3 Rmediated signalling. Molecular AspectsThe human histamine H 3 receptor (hH 3 R) cDNA firstly described 1999 encodes a 445 amino acid protein and belongs to the his...

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Section: Molecular Aspectsmentioning

confidence: 99%

Section: Molecular Aspectsmentioning

confidence: 99%

Histamine H3 Receptor Antagonists Go to Clinics

Sander

Kottke

Stark

2008

Biological & Pharmaceutical Bulletin

184

116

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“…Различная экспрессия и эффекторная функ-ция участков и структур этого сигнального пути зависит от стадии созревания/дифференциров-ки, тканевой принадлежности и активности кле-ток-мишеней, на основании чего развиваются многообразные реакции в биологических систе-мах [2,4,12,18,21,23]. В настоящее время нако-плено значительное количество данных, свиде-тельствующих об экспрессии на поверхности мононуклеаров периферической крови (МПК) и дендритных клеток (ДК) всех 4-х известных ти-пов Н-рецепторов [3,7,8,9,10,11,13,22,23].…”

Section: Introductionunclassified

Chemokine Secretion Patterns in Mononuclear and Dendritic Cells: Role of Histamine Type H3/H4 Receptors

Евстратова¹,

Ригер²,

Никитюк³

et al. 2016

Med. immunol.

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Адрес для переписки:Ханферьян Роман Авакович ФГБУН «Федеральный исследовательский центр питания, биотехнологии и безопасности пищи» 109240, Россия, Москва, Устьинский проезд, 2/14. Тел.: 8 (495) 698-53-45. Е-mail: khanferyan@ion иммунология, 2016. Т. 18, № 5. С. 437-442. doi: 10.15789/1563-0625-2016-5-437-442 © Евстратова В.С. и соавт., 2016 Immunologiya, 2016, Vol. 18, no. 5, pp. 437-442. doi: 10.15789/1563-0625-2016 Federal Research Center of Nutrition and Biotechnology, Moscow, Russian FederationAbstract. The study presents results concerning effects of H 3 /H 4 histamine receptors antagonist (Ciproxifan) upon in vitro chemokine secretion by dendritic cells (DC) and peripheral blood mononuclear cells (PBMC). We have been shown that in vitro inhibition of type H 3 /H 4 histamine receptor affects in different ways production of major chemokines by PBMC and DC, including eotaxin, RANTES, MCP-1, MIP-1α, MIP-1β, GRO-α, and IL-8. E.g., RANTES and GRO-α secretion in DC cultures was reduced, respectively, by 20% and 40%. Meanwhile, MIP-1β secretion was virtually unchanged, whereas MCP-1 secretion exhibited a four-fold increase. In PBMC cultures, the H 3 /H 4 receptor antagonist induced a significant increase in eotaxin, RANTES, MIP-1α, MIP-1β, GRO-α, and IL-8 secretion (p < 0.05).

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“…This is due to the current infeasibility of regularly crystallizing the GPCR-fragment complexes that are required for further fragment expansion. Recently, there has been several lines of evidence suggesting that FADD might be useful for GPCR hit identification [5]. These publications encouraged us to try this approach in the discovery of GPCR antagonists.…”

Section: Introductionmentioning

confidence: 99%

“…The histamine GPCRs signal through Gi/o proteins leading to inhibition of cAMP formation, mobilisation of calcium from intracellular stores and stimulation of MAP kinase in both heterologous expression systems and native immune cells [5,6]. H3 and H4 receptors remain highly attractive targets for drug discovery and medicinal chemistry development programs [7][8][9][10].…”

Section: Introductionmentioning

confidence: 99%

From Receptors to Ligands: Fragment-assisted Drug Design for GPCRs Applied to the Discovery of H3 and H4 Receptor Antagonists

Àlex¹,

Heifetz²,

Mazanetz³

et al. 2013

Med chem

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G-Protein Coupled Receptors (GPCRs) have enormous physiological and biomedical importance, being the primary target of a large number of modern drugs. The availability of structural information of the binding site of the targeted GPCR plays a key role in rationalization, efficiency and cost-effectiveness of the drug discovery process. However, obtaining structural information on GPCRs using X-ray crystallography or NMR requires a large investment of time and is technically very challenging. This situation significantly limits the ability of these methods to have an impact in drug discovery for GPCR targets in the short term and hence there is an urgent need for other effective and cost-efficient alternatives. We present here a practical approach that integrates GPCR modelling with fragment based screening to provide structural insights on the H3 and H4 histamine receptor binding sites. This approach creates a cost-efficient new avenue for structure-based drug design (SBDD) against GPCR targets. We report here a success of using this protocol for the discovery of selective and dual H3 and H4 antagonists. Our fragment screen yielded 44 H3, 21 H4 selective and 20 dual fragment hits. These fragments were used to construct high-quality H3 and H4 models followed by binding site exploration and structure based virtual screening (VS). Overall, 172 compounds were purchased for testing based on the virtual screening results. Of the 74 compounds predicted to have dual activity, 33 had activity against one or other of the two receptors (44%), of which 17 had activity against both. Of the 19 compounds predicted to be H3 selective, 13 were active against H3 (68%) and 10 of these also had selectivity over H4. Of the 79 compounds predicted to be H4 selective, 36 were active against H4 (45%) and 2 of these also had selectivity over H3.

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Compared pharmacology of human histamine H₃ and H₄ receptors: structure–activity relationships of histamine derivatives

Cited by 59 publications

References 57 publications

Histamine H3 Receptor Antagonists Go to Clinics

Histamine H3 Receptor Antagonists Go to Clinics

Chemokine Secretion Patterns in Mononuclear and Dendritic Cells: Role of Histamine Type H3/H4 Receptors

From Receptors to Ligands: Fragment-assisted Drug Design for GPCRs Applied to the Discovery of H3 and H4 Receptor Antagonists

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Compared pharmacology of human histamine H3 and H4 receptors: structure–activity relationships of histamine derivatives

Cited by 59 publications

References 57 publications

Histamine H3 Receptor Antagonists Go to Clinics

Histamine H3 Receptor Antagonists Go to Clinics

Chemokine Secretion Patterns in Mononuclear and Dendritic Cells: Role of Histamine Type H3/H4 Receptors

From Receptors to Ligands: Fragment-assisted Drug Design for GPCRs Applied to the Discovery of H3 and H4 Receptor Antagonists

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Compared pharmacology of human histamine H₃ and H₄ receptors: structure–activity relationships of histamine derivatives