Aldosterone synthase inhibition: cardiorenal protection in animal disease models and translation of hormonal effects to human subjects

Ménard, Joël; Rigel, Dean F.; Watson, Catherine E.; Jeng, Arco Y.; Fu, Fumin; Beil, Michael E.; Liu, Jing; Chen, Wei; Hu, Chii-Whei; Leung-Chu, Jennifer; LaSala, Daniel; Liang, Guiqing; Rebello, Sam; Zhang, Yiming; Dole, William P.

doi:10.1186/s12967-014-0340-9

Cited by 44 publications

(39 citation statements)

References 49 publications

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“…FAD286 (the R-enantiomer of fadrozole; 4-(5,6,7,8-tetrahydroimidazo[1,5-a]pyridin-5-yl)benzonitrile) (Santen et al, 1991;Ménard and Pascoe, 2006) and LCI699 (4-[(5R)-6,7-dihydro-5H-pyrrolo[1,2-c]imidazol-5-yl]-3-fluorobenzonitrile) (Amar et al, 2010;Calhoun et al, 2011) are examples of ASIs that have been evaluated in preclinical models (Fiebeler et al, 2005;Ménard et al, 2014) as well as in patients (Santen et al, 1991;Ménard and Pascoe, 2006;Amar et al, 2010;Calhoun et al, 2011). However, these molecules exhibit only modest selectivity for inhibition of human AS over CS, and have resulted in blunted cortisol responses when evaluated in patients (Santen et al, 1991;Amar et al, 2010), a likely reason for their clinical failure as selective AS inhibitors.…”

Section: Introductionmentioning

confidence: 99%

Selectivity of BI 689648, a Novel, Highly Selective Aldosterone Synthase Inhibitor: Comparison with FAD286 and LCI699 in Nonhuman Primates

Weldon

Cerny

Gueneva-Boucheva

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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The mineralocorticoid aldosterone is an important regulator of blood pressure, volume, and electrolyte balance. However, excess aldosterone can be deleterious as a driver of vascular remodeling and tissue fibrosis associated with cardiometabolic diseases. Aldosterone synthase (AS) inhibitors (ASI) attenuate the production of aldosterone directly and have been proposed as an alternative to mineralocorticoid receptor antagonists for blocking the pathologic effects of excess aldosterone. Discovery of selective ASIs has been challenging because of the high sequence identity (93%) AS shares with cortisol synthase (CS), and the low identity of rodent AS compared with human (63%). Using cynomolgus (cyno) monkey-based models, we identified BI 689648 [6-(5-methoxymethyl-pyridin-3-yl)-3,4-dihydro-2H-[1,8]naphthyridine-1-carboxylic acid amide], a novel, highly selective ASI that exhibits an in vitro IC 50 of 2 nM against AS and 300 nm against CS (150-fold selectivity) compared with the recently described ASIs FAD286 [4-(5,6,7,8-tetrahydroimidazo[1,5-a]pyridin-5-yl)benzonitrile] (3 nM AS; 90 nM CS; 40-fold) and LCI699 (4-[(5R)-6,7-dihydro-5H-pyrrolo[1,2-c]imidazol-5-yl]-3-fluorobenzonitrile) (10 nM AS; 80 nM CS; 8-fold). After oral administration in cyno monkeys, BI 689648 (5 mg/kg) exhibits a peak plasma concentration of ∼500 nM. For in vivo profiling we used an adrenocorticotropin-challenge model in which BI 689648 was .20-fold more selective compared with FAD286 and LCI699. Because both FAD286 and LCI699 failed to provide adequate selectivity for CS when tested in patients, the desire for more selective molecules to test the ASI hypothesis remains high. Therefore, highly selective aldosterone synthase inhibitors such as BI 689648 represent an important step forward toward developing ASIs with greater potential for clinical success in cardiometabolic diseases.

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Section: Introductionmentioning

confidence: 99%

Selectivity of BI 689648, a Novel, Highly Selective Aldosterone Synthase Inhibitor: Comparison with FAD286 and LCI699 in Nonhuman Primates

Weldon

Cerny

Gueneva-Boucheva

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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“…In addition to these cortisol-lowering actions, pasireotide and osilodrostat have been shown to exert a number of other pharmacological effects, including pasireotide-mediated suppression of GH secretion from the pituitary gland (Colao et al, 2012(Colao et al, , 2014 and osilodrostat-mediated inhibition of aldosterone synthase (Menard et al, 2010). The doses of osilodrostat and pasireotide studied in current combination are biologically relevant as similar or lower doses were shown to be pharmacologically active in previous rat studies (Silva et al, 2005;Menard et al, 2014).…”

Section: Discussionmentioning

confidence: 86%

Osilodrostat (LCI699), a potent 11β-hydroxylase inhibitor, administered in combination with the multireceptor-targeted somatostatin analog pasireotide: A 13-week study in rats

Vashisht

Boisclair

et al. 2015

Toxicology and Applied Pharmacology

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The somatostatin analog pasireotide and the 11β-hydroxylase inhibitor osilodrostat (LCI699) reduce cortisol levels by distinct mechanisms of action. There exists a scientific rationale to investigate the clinical efficacy of these two agents in combination. This manuscript reports the results of a toxicology study in rats, evaluating different doses of osilodrostat and pasireotide alone and in combination. Sixty male and 60 female rats were randomized into single-sex groups to receive daily doses of pasireotide (0.3mg/kg/day, subcutaneously), osilodrostat (20mg/kg/day, orally), osilodrostat/pasireotide in combination (low dose, 1.5/0.03mg/kg/day; mid-dose, 5/0.1mg/kg/day; or high dose, 20/0.3mg/kg/day), or vehicle for 13weeks. Mean body-weight gains from baseline to Week 13 were significantly lower in the pasireotide-alone and combined-treatment groups compared to controls, and were significantly higher in female rats receiving osilodrostat monotherapy. Osilodrostat and pasireotide monotherapies were associated with significant changes in the histology and mean weights of the pituitary and adrenal glands, liver, and ovary/oviduct. Osilodrostat alone was associated with adrenocortical hypertrophy and hepatocellular hypertrophy. In combination, osilodrostat/pasireotide did not exacerbate any target organ changes and ameliorated the liver and adrenal gland changes observed with monotherapy. Cmax and AUC0-24h of osilodrostat and pasireotide increased in an approximately dose-proportional manner. In conclusion, the pasireotide and osilodrostat combination did not exacerbate changes in target organ weight or toxicity compared with either monotherapy, and had an acceptable safety profile; addition of pasireotide to the osilodrostat regimen may attenuate potential adrenal gland hyperactivation and hepatocellular hypertrophy, which are potential side effects of osilodrostat monotherapy.

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“…Во избежание таких побочных эффектов и для снижения сывороточной концентрации АЛ и со-зданы ингибиторы альдостеронсинтазы (ИАС), представляющие собой новую терапевтическую опцию по предотвращению неблагоприятных эф-фектов антагонистов АЛ [67][68][69][70][71]. С учетом боль-шой значимости проблемы разработаны новые препараты -ингибиторы АСFAD286 и LCI699, но и они также недостаточно специфичны в отно-шении CYP11B2 в сравнении с 11β-гидроксилазой (CYP11B1).…”

Section: терапевтические возможности использования полиморфизма гена асunclassified

“…С учетом боль-шой значимости проблемы разработаны новые препараты -ингибиторы АСFAD286 и LCI699, но и они также недостаточно специфичны в отно-шении CYP11B2 в сравнении с 11β-гидроксилазой (CYP11B1). Позитивный эффект ИАС доказан в эксперименте [67,71].…”

Section: терапевтические возможности использования полиморфизма гена асunclassified

“…Следующее поколение ИАС должно снижать уровень АЛ в крови, подавляя фермент, отвечающий за его синтез, -АС. Новые инги-биторы АС будут не только эффективно снижать АД, но и предотвращать развитие неблагопри-ятных последствий, продлевая жизнь пациентов и способствуя снижению высокого уровня общей смерт ности от данной патологии [70,71].…”

Section: терапевтические возможности использования полиморфизма гена асunclassified

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Поліморфізм Гена Альдостеронсинтази При Аліментарному Ожирінні, Компонентах Метаболічного Синдрому, Деяких Формах Вторинних Артеріальних Гіпертензій І патології Кори Надниркових Залоз (Огляд Літератури)

Koval¹,

Miloslavsky²,

Snegurskaya³

et al. 2021

Mìžnarodnij endokrinologìčnij žurnal

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В огляді подано дані літератури про патогенетичну роль альдостерону, рівнів альдостеронсинтази і поліморфізмів гена даного ферменту при аліментарному ожирінні, наявності компонентів метаболічного синдрому, у хворих на вторинні форми артеріальної гіпертензії, при патології кори надниркових залоз й інших ендокринних порушеннях. Ген альдостеронсинтази становить собою перспективний кандидатний ген у європейській і азіатській популяції при метаболічному синдромі, цукровому діабеті, аліментарному ожирінні, деяких вторинних формах артеріальної гіпертензії, патології кори наднирників, діабетичній нефропатії, гестаційній гіпертензії. Генотипування поліморфізмів гена альдостеронсинтази може допомогти в диференціально-діагностичних алгоритмах у хворих зі вторинними формами артеріальної гіпертензії, пухлинами наднирників, первинним і вторинним гіперальдостеронізмом. Розглядаються перспективи терапевтичного використання інгібіторів альдостеронсинтази серед різних категорій хворих з ознаками артеріальної гіпертензії, ожиріння й ендокринними порушеннями.

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Aldosterone synthase inhibition: cardiorenal protection in animal disease models and translation of hormonal effects to human subjects

Cited by 44 publications

References 49 publications

Selectivity of BI 689648, a Novel, Highly Selective Aldosterone Synthase Inhibitor: Comparison with FAD286 and LCI699 in Nonhuman Primates

Selectivity of BI 689648, a Novel, Highly Selective Aldosterone Synthase Inhibitor: Comparison with FAD286 and LCI699 in Nonhuman Primates

Osilodrostat (LCI699), a potent 11β-hydroxylase inhibitor, administered in combination with the multireceptor-targeted somatostatin analog pasireotide: A 13-week study in rats

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