Identification of Highly Efficacious Glucocorticoid Receptor Agonists with a Potential for Reduced Clinical Bone Side Effects

Harcken, Christian; Riether, Doris; Kuzmich, Daniel; Liu, Pingrong; Betageri, Raj; Ralph, Mark; Emmanuel, Michel J.; Reeves, Jonathan T.; Berry, Angela; Souza, Donald; Nelson, Richard M.; Kukulka, Alison; Fadra, Tazmeen; Zuvela-Jelaska, Ljiljana; Dinallo, Roger M.; Bentzien, Jörg; Nabozny, Gerald H.; Thomson, D. S.

doi:10.1021/jm4019178

Cited by 29 publications

(22 citation statements)

References 40 publications

(67 reference statements)

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“…However, Compound 14 demonstrated a dose-dependent increase in the triglycerides and the serum insulin levels that suggested a lack of dissociation based on these biomarkers. A further advance was the realization that, at least apparently, compounds that contain 'diazaindole' moieties and display different transcriptional regulatory profiles in vitro and are considered 'dissociated' between gene transrepression and transactivation seem to be more interesting [50]. These compounds maintained anti-inflammatory activity in vivo in collageninduced arthritis studies in mouse but had reduced effects on bone relevant parameters compared to the widely used synthetic glucocorticoid prednisolone in vivo [50].…”

Section: Other Potential Boehringer Ingelheim Gr Agonistsmentioning

confidence: 99%

“…A further advance was the realization that, at least apparently, compounds that contain 'diazaindole' moieties and display different transcriptional regulatory profiles in vitro and are considered 'dissociated' between gene transrepression and transactivation seem to be more interesting [50]. These compounds maintained anti-inflammatory activity in vivo in collageninduced arthritis studies in mouse but had reduced effects on bone relevant parameters compared to the widely used synthetic glucocorticoid prednisolone in vivo [50]. Furthermore, a series of non-steroidal 'dissociated' GR agonists was optimized for drug-like properties such as cytochrome P450 inhibition, metabolic stability, aqueous solubility and human ether-a-go-go-related gene (hERG) ion-channel inhibition.…”

Section: Other Potential Boehringer Ingelheim Gr Agonistsmentioning

confidence: 99%

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Novel glucocorticoid receptor agonists in the treatment of asthma

Cazzola

Coppola

Rogliani

et al. 2015

Expert Opinion on Investigational Drugs

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Several agents have been synthesized, but few have been tested in experimental models of asthma. Furthermore, only three (BI-54903, GW870086X and AZD5423) have entered clinical development, although the development of at least one of them (BI-54903) was discontinued. The reason for the limited success so far obtained is that the model of transactivation versus transrepression is a too simplistic representation of GR activity. It is difficult to uncouple the therapeutic and harmful effects mediated by GR, but some useful information that might change the current perspective is appearing in the literature. The generation of gene expression 'fingerprints' produced by different GR agonists in target and off-target human tissues could be useful in identifying drug candidates with an improved therapeutic ratio.

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Section: Other Potential Boehringer Ingelheim Gr Agonistsmentioning

confidence: 99%

Section: Other Potential Boehringer Ingelheim Gr Agonistsmentioning

confidence: 99%

Novel glucocorticoid receptor agonists in the treatment of asthma

Cazzola

Coppola

Rogliani

et al. 2015

Expert Opinion on Investigational Drugs

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“…PF‐04171327 (fosdagrocorat) is a phosphate ester prodrug of PF‐00251802 (dagrocorat), a selective high‐affinity partial agonist of the glucocorticoid receptor (Figure ). Previous preclinical, phase 1, and phase 2 studies have demonstrated the anti‐inflammatory effects of PF‐04171327 …”

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confidence: 99%

In Vitro and In Vivo Investigation of Potential for Complex CYP3A Interaction for PF‐00251802 (Dagrocorat), a Novel Dissociated Agonist of the Glucocorticoid Receptor

Ripp

Mukherjee

Eng

et al. 2017

Clinical Pharm in Drug Dev

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The dissociated agonists of the glucocorticoid receptor are a novel class of agents in clinical development for rheumatoid arthritis. PF‐04171327 (fosdagrocorat) is a phosphate ester prodrug of PF‐00251802 (dagrocorat), a selective high‐affinity partial agonist of the glucocorticoid receptor, which is further metabolized to PF‐04015475. This study evaluated the cytochrome P450 (CYP)–mediated drug–drug interaction (DDI) potential of PF‐00251802 and PF‐04015475 in vitro and used model‐based prediction approaches to estimate clinical impact. PF‐00251802 is a reversible inhibitor of several CYPs, but modeling has suggested no clinically relevant interaction. PF‐00251802 and PF‐04015475 are time‐dependent inhibitors and inducers of CYP3A in vitro; PF‐00251802 is also a time‐dependent inhibitor of CYP2D6. Model‐based prediction suggested the potential for weak inhibition of CYP3A in vivo. A clinical DDI study was conducted with midazolam, a sensitive CYP3A substrate. A phase 1 open‐label, multiple‐dose study evaluated the effect of PF‐04171327 on midazolam pharmacokinetics and safety in 12 healthy volunteers. Administration of midazolam alone or concomitantly with PF‐04171327 resulted in equivalent pharmacokinetic profiles (AUCinf, 21.17 vs 20.28 ng·h/mL, respectively), indicating that PF‐04171327 had no net effect on CYP3A activity in vivo. These findings support the further development of PF‐00251802 and PF‐04171327 as potential treatments for patients with rheumatoid arthritis (NCT00987038).

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“…However, the translation of in vitro dissociation markers to preclinical in vivo parameters in mouse models had been previously established with tool compounds from this series and was expected to apply to these ■ EXPERIMENTAL PROCEDURES Synthesis. All compounds (except 9) described herein have been synthesized following the general scheme outlined in previous publications and summarized in Scheme 1: 16,18 A substituted halogenated aminopyridine 5 undergoes a Sonogashira coupling with the alkyne 6, and the coupling product is cyclized under basic conditions to the azaindoles 7. 20 The majority of the synthetic effort was spent on generating the required substituted alkynes and substituted pyridines, where required, compounds were modified further after the key coupling/cyclization sequence.…”

mentioning

confidence: 99%

“…b Maximum efficacy at the highest tested concentration compared to dexamethasone, defined at 100%; maximum concentration tested is 2 μM. optimized compounds 18. (R)-39 was tested in a 9-day type II collagen-induced arthritis model in rats at 3, 10, and 30 mg/kg qd po in 30% cremophor to guide human efficacious concentration projections.…”

mentioning

confidence: 99%