Pharmacokinetics, Safety, and Tolerability of Metformin in Healthy Elderly Subjects

Jang, Kyungho; Chung, Hyewon; Yoon, Jang soo; Moon, Seol Joo; Yoon, Seo Hyun; Yu, Kyung‐Sang; Kim, Kwang Il; Chung, Jae Yong

doi:10.1002/jcph.699

Cited by 15 publications

(11 citation statements)

References 24 publications

(45 reference statements)

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“…Beyond some gastrointestinal symptoms, its most serious side effect, lactic acidosis, is observed only when GFR is below 30 ml/min [ 20 ], far below the cut-off value accepted for a patient to enter the ongoing trials (eGFR> 60 ml/min). This profile will be hopefully maintained also in non-diabetic patients and the fearsome risk of hypoglycemia should remain negligible: clinical trials using metformin in diabetes prevention, in fact, have shown no case of hypoglycemia occurring as serious adverse effect during nearly 18.000 subjects/year of follow-up [ 21 ], nor hypoglycemia is described in obese non-diabetic children assuming the drug [ 22 ], nor in normal subjects after an acute load of metformin [ 23 ]. Such tolerability is a crucial point in a long lasting treatment.…”

Section: Discussionmentioning

confidence: 99%

Metformin in autosomal dominant polycystic kidney disease: experimental hypothesis or clinical fact?

Pisani¹,

Riccio²,

Bruzzese³

et al. 2018

BMC Nephrol

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BackgroundAutosomal dominant polycystic kidney disease (ADPKD) accounts for 8–10% of end-stage chronic kidney disease (CKD) patients worldwide. In the last decade, the advanced knowledge in genetics and molecular pathobiology of ADPKD focused some aberrant molecular pathways involved in the pathogenesis of the disease leading to controlled clinical trials aimed to delay its progression with the use of mTOR inhibitors, somatostatin or tolvaptan. Preclinical studies suggests an effective role of metformin in ADPKD treatment by activating AMPK sensor. Clinical trials are currently recruiting participants to test the metformin use in ADPKD patients.MethodsWe retrospectively examined the records of our ADPKD patients, selecting 7 diabetic ADPKD patients under metformin treatment and 7 matched non-diabetic ADPKD controls, to test the effect of metformin on renal progression during a 3 year follow-up.ResultsDuring the first year, the GFR decreased by 2.5% in Metformin Group and by 16% in Controls; thereafter, renal function remained stable in Metformin Group and further decreased in Controls, reaching a 50% difference after 3 years of observation. Accordingly, the overall crude loss of GFR, estimated by a linear mixed model, resulted slower in the Metformin than in Control Group (− 0.9; 95% C.I.: -2.7 to 0.9 vs - 5.0; 95% C.I.: -6.8 to − 3.2 mL/min/1.73 m2 per year, p = 0.002).ConclusionsOur data are suggestive of a beneficial effect of metformin on progression of ADPKD. Large, randomized, prospective trials are needed to confirm this hypothesis.

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Section: Discussionmentioning

confidence: 99%

Metformin in autosomal dominant polycystic kidney disease: experimental hypothesis or clinical fact?

Pisani¹,

Riccio²,

Bruzzese³

et al. 2018

BMC Nephrol

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“…During expansion, cells were exposed (or not) to 25 μmol/L metformin (Merck, Sigma Aldrich, St. Quentin Fallavier, France). The metformin concentration chosen in our study is close to Cmax observed in ederly subjects, which exhibited higher average Cmax than younger subjects (Jang, Chung et al 2016). At a late passage (P11), cells were exposed (or not) to 0.1 μmol/L compound C (Merck, Sigma Aldrich).…”

Section: Methodsmentioning

confidence: 70%

Metformin alleviates aging-associated cellular senescence of human adipose stem cells and derived adipocytes

Mantecon

Pelletier

Gorwood

et al. 2020

Preprint

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SUMMARYAging is associated with central fat redistribution, and insulin resistance. To identify age-related adipose features, we evaluated the senescence and adipogenic potential of adipose-derived-stemcells (ASCs) from abdominal subcutaneous fat obtained from healthy normal-weight young (<25y) or older women (>60y).Aged-donor ASCs showed more intense features of aging (senescence, mitochondrial dysfunction, and oxidative stress) than young-donor ASCs. Oxidative stress and mitochondrial dysfunction occurred earlier in adipocytes derived from aged-donor than from young-donor ASCs, leading to insulin resistance and impaired adipogenesis.When aged-donor ASCs were treated with metformin, senescence, oxidative stress and mitochondrial dysfunction returned to the levels observed in young-donor ASCs. Furthermore, metformin’s prevention of senescence and dysfunction during ASC proliferation restored the cells’ adipogenic capacity and insulin sensitivity. This effect was mediated by the activation of AMP-activated-protein-kinase.We show here that targeting senescent ASCs from aged women with metformin may alleviate age-related dysfunction, insulin resistance, and impaired adipogenesis.

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“…A report showed that gender and race (Caucasians, Blacks, and Hispanics) little affected AUC of metformin [ 120 ]. The elderly subjects (68 ± 2 years) were reported to exhibit 1.7 and 2.0 times higher average C max and AUC than the younger subjects (23 ± 3 years) [ 93 ]. Subjects used in the prediction were young and healthy, excluding effects of both ages and disease on metformin disposition.…”

Section: Resultsmentioning

confidence: 99%

A Whole-Body Physiologically Based Pharmacokinetic Model Characterizing Interplay of OCTs and MATEs in Intestine, Liver and Kidney to Predict Drug-Drug Interactions of Metformin with Perpetrators

Yang

Zhang

et al. 2021

Pharmaceutics

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Transmembrane transport of metformin is highly controlled by transporters including organic cation transporters (OCTs), plasma membrane monoamine transporter (PMAT), and multidrug/toxin extrusions (MATEs). Hepatic OCT1, intestinal OCT3, renal OCT2 on tubule basolateral membrane, and MATE1/2-K on tubule apical membrane coordinately work to control metformin disposition. Drug–drug interactions (DDIs) of metformin occur when co-administrated with perpetrators via inhibiting OCTs or MATEs. We aimed to develop a whole-body physiologically based pharmacokinetic (PBPK) model characterizing interplay of OCTs and MATEs in the intestine, liver, and kidney to predict metformin DDIs with cimetidine, pyrimethamine, trimethoprim, ondansetron, rabeprazole, and verapamil. Simulations showed that co-administration of perpetrators increased plasma exposures to metformin, which were consistent with clinic observations. Sensitivity analysis demonstrated that contributions of the tested factors to metformin DDI with cimetidine are gastrointestinal transit rate > inhibition of renal OCT2 ≈ inhibition of renal MATEs > inhibition of intestinal OCT3 > intestinal pH > inhibition of hepatic OCT1. Individual contributions of transporters to metformin disposition are renal OCT2 ≈ renal MATEs > intestinal OCT3 > hepatic OCT1 > intestinal PMAT. In conclusion, DDIs of metformin with perpetrators are attributed to integrated effects of inhibitions of these transporters.

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Pharmacokinetics, Safety, and Tolerability of Metformin in Healthy Elderly Subjects

Cited by 15 publications

References 24 publications

Metformin in autosomal dominant polycystic kidney disease: experimental hypothesis or clinical fact?

Metformin in autosomal dominant polycystic kidney disease: experimental hypothesis or clinical fact?

Metformin alleviates aging-associated cellular senescence of human adipose stem cells and derived adipocytes

A Whole-Body Physiologically Based Pharmacokinetic Model Characterizing Interplay of OCTs and MATEs in Intestine, Liver and Kidney to Predict Drug-Drug Interactions of Metformin with Perpetrators

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