In silico prediction of acyl glucuronide reactivity

Potter, Timothy; Lewis, Richard J.; Luker, Tim; Bonnert, Roger V.; Bernstein, Michael A.; Birkinshaw, Timothy N.; Thom, Stephen; Wenlock, Mark C.; Paine, Stuart W.

doi:10.1007/s10822-011-9479-0

Cited by 12 publications

(7 citation statements)

References 25 publications

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“…Where pure reference standards of acyl glucuronides are available, NMR based methodologies to detect the disappearance of the anomeric resonance of 1-β-acyl glucuronide [25] or immunostimulation in human peripheral blood monocytes may also serve as a useful surrogate markers of reactivity [44]. In silico approaches such as the partial least squares model proposed by Potter and coworkers [45] can be broadened and qualified to support medicinal chemistry intervention strategies and synthesis of next generation analogs. Another aspect worthy of consideration is that observation of an acyl glucuronide as a ‘major’ metabolic pathway should not preclude progression of a new chemical entity into further development.…”

Section: Discussionmentioning

confidence: 99%

New Perspectives on Acyl Glucuronide Risk Assessment in Drug Discovery: Investigation of In vitro Stability, In situ Reactivity, and Bioactivation

Gunduz¹,

Argikar²,

Cirello³

et al. 2018

DML

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While the compounds tested from "withdrawn and warning category" all formed the glutathione adduct in buffer, none from "safe" category formed the glutathione adduct. In contrast, none of the compounds from any category formed methoxylamine conjugate, which reacts with putative aldehyde moiety formed via acyl migration. These results, highly favorite the nucleophilic displacement as a cause of the reactivity rather than the acyl migration via aldehyde formation. The workflow herein could also be applied in the discovery setting to triage new chemical entities of interest.

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Section: Discussionmentioning

confidence: 99%

New Perspectives on Acyl Glucuronide Risk Assessment in Drug Discovery: Investigation of In vitro Stability, In situ Reactivity, and Bioactivation

Gunduz¹,

Argikar²,

Cirello³

et al. 2018

DML

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“…A caveat is the relatively small number of No DILI acidic drugs (15); further data are needed to confirm the lack of a dose effect on the hepatotoxicity of acidic drugs. On the 44 Most DILI acidic drugs, 32 are carboxylic acids, which are prone to reactive metabolite formation via glucuronidation, where the chemical mechanism is well understood . With basic drugs, −p[MDD] and cLogP have the greatest impact, and Fsp3 is not different between the No DILI and Most DILI groups.…”

Section: Hepatotoxicitymentioning

confidence: 99%

Impact of Physicochemical Properties on Dose and Hepatotoxicity of Oral Drugs

Leeson

2018

Chem. Res. Toxicol.

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A database containing maximum daily doses of 1841 marketed oral drugs was used to examine the influence of physicochemical properties on dose and hepatotoxicity (drug induced liver injury, DILI). Drugs in the highest ∼20% dose range had significantly reduced mean lipophilicity and molecular weight, increased fractional surface area, increased % of acids, and decreased % of bases versus drugs in the lower ∼60% dose range. Drugs in the ∼20-40% dose range had intermediate mean properties, similar to the mean values for the full drug set. Drugs that are both large and highly lipophilic almost invariably do not have doses in the upper ∼20% range. The results show that oral druglike physicochemical properties are different according to these dose ranges, and this is consistent with maintenance of acceptable safety profiles as efficacious exposure increases. Verified DILI annotations from a compilation of >1000 approved drugs (Chen, M.; et al. Drug Discov. Today, 2016, 21, 648 ) were used. The drugs classified as "No DILI" ( n = 163) had significantly lower dose and lipophilicity, and higher Fsp3 (fraction of carbon atoms that are sp hybridized) versus the "Most DILI" ( n = 163) drugs. The percentages of acids were reduced and bases increased in the "No DILI" versus the "Most DILI" groups. Drugs classified as "Less DILI" or "Ambiguous DILI" had intermediate mean values of dose, lipophilicity, Fsp3, and % acids and bases. The impact of lipophilicity and Fsp3 on DILI increases in the upper 20% versus the lower 80% dose range, and a simple decision tree model predicted "No DILI" versus "Most DILI" outcomes with 82% accuracy. The model correctly classified 19 of 22 drugs (86%) that failed in development due to human hepatotoxicity. Because many oral drugs lacking DILI annotations are predicted to be "Most DILI", the model is best used preclinically in conjunction with experimental DILI mitigation.

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“…The prolonged use of most NSAIDs leads to gastrointestinal adverse reactions. This was the reason why SUP has been withdrawn from the pharmaceutical market; its use has led to acute renal failure in patients …”

Section: Introductionmentioning

confidence: 99%

Structural investigations of stereoselective profen binding by equine and leporine serum albumins

et al. 2020

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Serum albumin, the most abundant transport protein of mammalian blood, interacts with various nonsteroidal anti‐inflammatory drugs (NSAIDs) affecting their disposition, metabolism, and excretion. A big group of chiral NSAIDs transported by albumin, profens, is created by derivatives of 2‐arylpropionic acid. The chiral center in the structures of profens is adjacent to the carboxylate moiety and often determines different pharmacological properties of profen enantiomers. This study describes crystal structures of two albumins, isolated from equine and leporine serum, in complexes with three profens: ibuprofen, ketoprofen, and suprofen. Based on three‐dimensional structures, the stereoselectivity of albumin is discussed and referred to the previously published albumin complexes with drugs. Drug Site 2 (DS2) of albumin, the bulky hydrophobic pocket of subdomain IIIA with a patch of polar residues, preferentially binds (S)‐enantiomers of all investigated profens. Almost identical binding mode of all these drugs clearly indicates the stereoselectivity of DS2 towards (S)‐profens in different albumin species. Also, the affinity studies show that DS2 is the major site that presents high affinity towards investigated drugs. Additionally, crystallographic data reveal the secondary binding sites of ketoprofen in leporine serum albumin and ibuprofen in equine serum albumin, both overlapping with previously identified naproxen binding sites: the cleft formed between subdomains IIIA and IIIB close to the fatty acid binding site 5 and the niche created between subdomains IIA and IIIA, called fatty acid site 6.

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In silico prediction of acyl glucuronide reactivity

Cited by 12 publications

References 25 publications

New Perspectives on Acyl Glucuronide Risk Assessment in Drug Discovery: Investigation of In vitro Stability, In situ Reactivity, and Bioactivation

New Perspectives on Acyl Glucuronide Risk Assessment in Drug Discovery: Investigation of In vitro Stability, In situ Reactivity, and Bioactivation

Impact of Physicochemical Properties on Dose and Hepatotoxicity of Oral Drugs

Structural investigations of stereoselective profen binding by equine and leporine serum albumins

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