Sex difference in metabolism of simvastatin by rat hepatic microsomes

Ohtawa, Masakatsu; Uchiyama, Naotaka

doi:10.1007/bf03190142

Cited by 8 publications

(8 citation statements)

References 16 publications

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“…dose in male and female rats, respectively. These gender differences in the metabolism of SV are consistent with previously published in vitro data (Ohtawa and Uchiyama, 1992), which showed a higher rate of metabolism in males than in female rats. In vivo, a similar trend was observed, and the gender differences have been attributed to the different P450 isozymes responsible (CYP3A in female and CYP2C11 in male rats) for the metabolism of SV (Ishigami et al, 2001).…”

Section: Svasupporting

confidence: 92%

Structural Characterization of in Vivo Rat Glutathione Adducts and a Hydroxylated Metabolite of Simvastatin Hydroxy Acid

Subramanian

Fang²,

Prueksaritanont³

2002

Drug Metab Dispos

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ABSTRACT:Simvastatin hydroxy acid (SVA), the pharmacologically active form of simvastatin (SV), is a potent inhibitor of 3-hydroxy-3-methylglutaryl (HMG)-coenzyme A reductase and is formed on hydrolysis of the orally administered SV. In this article, we report the structural characterization of two new dihydroxy glutathione adducts and a trihydroxy derivative of SVA, all found in rat bile. Metabolite I is 5␤,6␤-dihydroxy-4a␣-glutathione-SVA, and metabolite II is a pentanoic acid derivative of metabolite I. The two identified GSH conjugates accounted for 16 and 9% in males and 11 and 5% in females of the total radioactivity (metabolites I and II, respectively). Metabolite III is 3,5␤,6␤-dihydrotriol-SVA and accounts for 2% (male) and 4% (female) of the total dose in rats. Of these three newly identified metabolites, only metabolite III was also observed in dog bile.

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Section: Svasupporting

confidence: 92%

Structural Characterization of in Vivo Rat Glutathione Adducts and a Hydroxylated Metabolite of Simvastatin Hydroxy Acid

Subramanian

Fang²,

Prueksaritanont³

2002

Drug Metab Dispos

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“…Second, pathophysiological differences between females and males could be a possible reason, since some studies had remarked on the sex differences in statin effects [39][40][41]. Moreover, in some animal studies, statins might have a greater clinical efficacy among males due to differences in the rate of metabolism, depending on sex [42,43]. Several epidemiological studies have reported greater cholesterol reductions by statins among women than men [44,45].…”

Section: Discussionmentioning

confidence: 99%

Impact of Statin Use on Dementia Incidence in Elderly Men and Women with Ischemic Heart Disease

et al. 2020

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This study aimed to determine the association between statins and the prevention of dementia according to sex differences in elderly patients with ischemic heart disease (IHD). We performed a nationwide retrospective cohort study using the Korean Health Insurance Review and Assessment Service database (2007)(2008)(2009)(2010)(2011)(2012)(2013)(2014)(2015). Among the 264,036 eligible patients aged ≥65 years with IHD, statin users were compared with non-users by propensity score matching at a 1:1 ratio (71,587 in each group). The primary outcome was dementia risk by estimating hazard ratios (HRs) and 95% confidence intervals (CIs). Differential risks of dementia were assessed by sex in the subgroups of statin types, exposure duration, and patient age, implying that sex is an influential factor for the link between statin use and dementia incidence. Among seven commonly prescribed statins, rosuvastatin was associated with the greatest preventive effect on dementia incidence, with an adjusted HR of 0.82 (95% CI = 0.78-0.87). In a subgroup analysis organized by sex, the differential risk of dementia incidence was assessed in each statin group, implying that sex is an influential factor for the link between statin and dementia. This study suggests that appropriate statin use considering sex differences may have beneficial effects on the development of dementia.

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“…Five metabolites 5-9 of SV were identified in rat plasma and urine using gas chromatography-mass spectrometry (GC-MS) [29]. In addition to that work, using HPLC-UV, six other metabolites 10-15 including metabolite 5 were detected in rat hepatic microsomes [30], and using NMR and mass spectroscopy [31] the same were detected in rat liver microsomes (RLMs). Later, Prueksaritanont et al [32] identified another two new metabolites 16 and 17, including three known metabolites 5, 10, and 11 using LC-MS/MS in HLMs.…”

Section: Introductionmentioning

confidence: 88%

“…In order to maximize its excellent cholesterol-lowering effect and minimize its serious side effects, an in-depth study of its metabolism becomes indispensable to understand the mechanisms underlying its pharmacological effects and its potential side effects. Metabolic profiling of SV has been reported in a number of articles using different analytical methods [29][30][31][32][33]. To date, thirteen metabolites of SV have been identified, which are depicted in Figure 2.…”

Section: Introductionmentioning

confidence: 99%

Simvastatin: In Vitro Metabolic Profiling of a Potent Competitive HMG-CoA Reductase Inhibitor

et al. 2022

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Simvastatin (SV) is a semisynthetic derivative of lovastatin (LV), which is biosynthetically produced from the fungus Aspergillus terreus and has a high log p value (log p = 4.39)and thus high hepatic extraction and high efficacy in controlling cholesterol synthesis. The current study was undertaken to investigate the metabolic profile of SV using various mass spectrometry (MS) platforms. Metabolic profiling was studied in in vitro models, rat liver microsomes (RLMs), and isolated perfused rat liver hepatocytes (RLHs) using both ion trap and triple quadruple LC–MS/MS systems. A total of 29 metabolites were identified. Among them, three types of SV-related phase-I metabolites, namely exomethylene simvastatin acid (exomethylene SVA), monohydroxy SVA, and dihydrodiol SVA, were identified as new in RLMs. No phase-II metabolites were identified while incubating with RLHs.

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Sex difference in metabolism of simvastatin by rat hepatic microsomes

Cited by 8 publications

References 16 publications

Structural Characterization of in Vivo Rat Glutathione Adducts and a Hydroxylated Metabolite of Simvastatin Hydroxy Acid

Structural Characterization of in Vivo Rat Glutathione Adducts and a Hydroxylated Metabolite of Simvastatin Hydroxy Acid

Impact of Statin Use on Dementia Incidence in Elderly Men and Women with Ischemic Heart Disease

Simvastatin: In Vitro Metabolic Profiling of a Potent Competitive HMG-CoA Reductase Inhibitor

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