Altered intravenous pharmacokinetics of topotecan in rats with acute renal failure (ARF) induced by uranyl nitrate: Do adenosine A<sub>1</sub>antagonists (selective/non-selective) normalize the altered topotecan kinetics in ARF?

Mustafa, Sana; Paramesh, Venkatesh; Pasha, K; Mullangi, Ramesh; Srinivas, Nuggehally R.

doi:10.1080/00498250600839385

Cited by 7 publications

(7 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…A population pharmacokinetic analysis indicated that tubular secretion in addition to glomerular filtration is involved in topotecan renal clearance in humans (Mould et al, 2002). Prior studies in murine species demonstrated that the renal clearance of topotecan was significantly reduced by probenecid, a typical inhibitor of organic anion transporters, suggesting that topotecan undergoes renal tubular secretion via organic anion transporter(s) (Zamboni et al, 1998;Mustafa et al, 2006). However, the molecular mechanism of renal tubular secretion of topotecan has not been elucidated.…”

Section: Discussionmentioning

confidence: 99%

“…Many investigators have reported on the systemic and renal disposition of topotecan in various animals and humans (Herben et al, 1996(Herben et al, , 2002Zamboni et al, 1998;Hartmann and Lipp, 2006;Mustafa et al, 2006). Topotecan is primarily excreted into urine as both lactone and hydroxyl acid forms, accounting for approximately 49% of the dose administered i.v.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Matsumoto

Yoshida²,

Ishiguro³

et al. 2007

J Pharmacol Exp Ther

View full text Add to dashboard Cite

Topotecan [(S)-9-dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride] is primarily excreted into urine in humans, with approximately 49% of the dose recovered as total topotecan (topotecan lactone plus topotecan hydroxyl acid form). The renal elimination of topotecan involves tubular secretion in addition to glomerular filtration, but little is known about the molecular mechanism of the renal tubular secretion. In the present study, we investigated the transport characteristics of topotecan hydroxyl acid across the renal basolateral membrane using rat kidney slices and rat or human transporterexpressing Xenopus laevis oocytes. Pravastatin and probenecid significantly inhibited the uptake of topotecan hydroxyl acid by rat kidney slices with K i values of 10.6 and 8.1 M, respectively, and p-aminohippurate was weakly inhibitory at high concentrations, whereas excess tetraethylammonium had no effect. The uptake of topotecan hydroxyl acid by oocytes injected with complementary RNA of either rat or human organic anion transporter 3 (rOAT3 or hOAT3) was greater than that of waterinjected oocytes. Kinetic analysis showed that the K m values for rOAT3 and hOAT3 were 21.9 and 56.5 M, respectively. Neither rOAT1 nor hOAT1 stimulated topotecan hydroxyl acid transport. These results suggest that the urinary excretion of topotecan hydroxyl acid is accounted for by transport via OAT3, as well as glomerular filtration, in both rats and humans; therefore, drug-drug interactions involving OAT3 may cause a change in clearance of topotecan.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Matsumoto

Yoshida²,

Ishiguro³

et al. 2007

J Pharmacol Exp Ther

View full text Add to dashboard Cite

show abstract

“…Mustafa et al [26] Topotecan (123948-87-8) Uranyl nitrate induced ARF After i. v. dosing, the AUC values of topotecan was drastically reduced in ARF rats relative to control rats. The addition of probenecid further increased the exposure of topotecan in ARF rats.…”

Section: Absorption Related Changesmentioning

confidence: 96%

“…Renale xcretion:A sdocumented in all studiesane xpected outcome in ARF iss everereduction of renal clearanceapplicable tobothparentdrugand associated metabolites.Ifthe sole contributorand/ormajorpathwayfort he overall elimination isr enalclearance,then accumulation of the substrateisbound tohappen asexemplified bys ubstratess uchasetoposide (CAS 33419-42-0) [19], telithromycin (CAS 191114-48-4) [20], topotecan( CAS 123948-87-8) [26], adriamycin [45], etc.Inthe eventthatcertain CYP expressionsarealsoinduced during ARF, itispossible thatmetabolicc learanceo fthe drugafteroraldosing maygetmoreaffected thanintravenous dosing in ARF rats.Henced epending on the non-renalclearancep athways duetoe nhanced metabolism,the totalbodyclearancem aygets omewhat tempered asillustrated bys ubstratess uchasmycophenolica cid (CAS 24280-93-1) [22], DA-7867 [25], DA-125 [44]etc. Biliary excretion:A sillustrated byt wocasestudies bothp arentdrugand metabolite(s)canbep redominantlyexcreted viab iliary pathwayduring ARF.Since suchbiliary excretory pathways wereo fl imited applicability in control rats undernormalconditions,itappears thatARF conditionsmaypromptalternativee xcretory pathways forr educing the drugburden on the body.Asexemplified in the caseo fcyclosporine there maybed iminished bile secretion and pert he datagenerated from indocyanine green therem aybeasignificantdelayin the biliary excretion of the compound during ARF [68].Onthe contrary,the biliary excretion of 7-O-glucuronica cid conjugateo fm ycophenolica cid was significantlyincreased in ARF rats [22].Asaresultof rapid enterohepaticc ycling of the Phase2metabolite and poorr e-absorption from the lumen,therewasa suggestion of ani ncreased risko fg astrointestinald isorders [22].…”

Section: Changesr Elated Toe Xcretionmentioning

confidence: 99%

“…attempted tonormalizeARF induced byuranylnitrateusing aselectiveadenosine A1receptorantagonist 1,3-dipropyl-8-phenylxanthine (CAS 85872-53-3)( DPPX) [26].Interestingly,topotecanwasu sed asaprobetoi nvestigatethe role of DPPX in reversing ARF bymonitoring the pharmacokineticsof topotecani nARF rats and ARF rats thatw erep retreated differentdosesof DPPX [26].Asac onsequenceo fthe improvementof renal function byDPPX pretreatment,the pharmacokinetics of topotecanconsiderablyimproved in the ARF rats [26].Although the pharmacokineticsof topotecanwas notr estored tothe levelsobserved in control rats,there wasasuggestion thatadenosine A1receptorantagonist mayamelioratethe insultt othe kidney.Therefore,this proposed pharmacokineticstrategymayprovide ano pportunity forfuturep reclinicali nvestigationst om ake a productdecision on investigationald rug(s)i nd evelopment,if therei sasignificantconcernrelated toARF interactions.Previously,Clark etal. used avessel dilatorto improvethe conditionsof renali nsultincluding tubular necrosis [61].The datafrom thisexploratory worksuggested thatt he useo favessel dilatordecreased the serumcreatinine and blood ureanitrogen levelsconsiderablyascompared ton on treated ARF rats [61].Also, mortality wasdrasticallyreduced and therewasasignificantimprovementof the tubularnecrosisfindings.Unfortunately,thisinvestigation did notinclude anactive pharmacokineticstrategyt oconfirmthe reversibility of the system using pharmacokineticsast he surrogate (i. e. control rats versus ARF rats versus revived ARF rats) [61].…”

Section: Reviewmentioning

confidence: 99%

See 1 more Smart Citation

Altered disposition of drugs in acute renal failure rat models: drug development strategies and perspectives

Srinivas¹

2011

Arzneimittelforschung

View full text Add to dashboard Cite

In the evolving paradigm of drug development it is a reasonable strategy to avoid and/or anticipate potential risks in drug development for select drugs by performing in vitro and/or preclinical studies in appropriate animal models. The availability of acute renal failure (ARF) rat models provides an opportunity to explore the pharmacokinetic disposition of drugs and associated metabolites in conditions that mimic the pathophysiology of the disease in humans. Such studies may help in drug(s) selection for development, differentiating certain drug classes, and/or arriving at a dose strategy decision in the clinic. Scores of compounds, belonging to various therapeutic areas, have undergone pharmacokinetic investigations in ARF models induced by uranyl nitrate (CAS 10102-06-4), glycerol (CAS 56-81-5), cisplatin (CAS 15663-27-1) or gentamicin (CAS 1403-66-3) in rats. The published pharmacokinetic disposition data has unequivocally suggested that ARF conditions leads to decreased renal elimination of the drug and associated metabolites; however, the influence on the overall body clearance is dependent on the propensity of the contribution of renal versus non-renal mechanisms of elimination. In the case studies assembled for this review, 52.5% of the drugs showed an increased drug exposure, 35% of the drugs showed a decreased drug exposure and 12.5% of the drugs showed no altered exposure, in ARF rat models relative to control rats. Interestingly, ARF can have an overall impact on drug absorption, distribution, metabolism, local transport and biliary excretion. Hence, the overall pharmacokinetic disposition may have to be interpreted with caution during ARF since there is the potential for competiting pathways to co-exist. For instance, due to reduced renal elimination as a result of kidney insult caused by ARF, compensatory biliary excretion mechanism may occur. Alternatively, intestinal and/or hepatic enzymatic expression level may go up to facilitate enhanced metabolism. However, there may be instances where uraemic toxins floating in the circulation may block the metabolism and/ or may also retard the absorption process. This review covers: 1) an illustration of a number of case studies providing tabulated information on the key altered pharmacokinetic parameters observed in ARF and the hypothesized mechanistic explanation; 2) a comprehensive description of altered absorption, distribution, metabolism, excretion and efflux transport related changes observed during ARF; 3) a general framework for drug development strategies and 4) a succinct discussion on the overall perspectives of the applicability of ARF rat models.

show abstract

Examination of Urinary Excretion of Unchanged Drug in Humans and Preclinical Animal Models: Increasing the Predictability of Poor Metabolism in Humans

et al. 2021

View full text Add to dashboard Cite

Altered intravenous pharmacokinetics of topotecan in rats with acute renal failure (ARF) induced by uranyl nitrate: Do adenosine A₁antagonists (selective/non-selective) normalize the altered topotecan kinetics in ARF?

Cited by 7 publications

References 34 publications

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Altered disposition of drugs in acute renal failure rat models: drug development strategies and perspectives

Examination of Urinary Excretion of Unchanged Drug in Humans and Preclinical Animal Models: Increasing the Predictability of Poor Metabolism in Humans

Contact Info

Product

Resources

About

Altered intravenous pharmacokinetics of topotecan in rats with acute renal failure (ARF) induced by uranyl nitrate: Do adenosine A1antagonists (selective/non-selective) normalize the altered topotecan kinetics in ARF?

Cited by 7 publications

References 34 publications

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Involvement of Rat and Human Organic Anion Transporter 3 in the Renal Tubular Secretion of Topotecan [(S)-9-Dimethylaminomethyl-10-hydroxy-camptothecin hydrochloride]

Altered disposition of drugs in acute renal failure rat models: drug development strategies and perspectives

Examination of Urinary Excretion of Unchanged Drug in Humans and Preclinical Animal Models: Increasing the Predictability of Poor Metabolism in Humans

Contact Info

Product

Resources

About

Altered intravenous pharmacokinetics of topotecan in rats with acute renal failure (ARF) induced by uranyl nitrate: Do adenosine A₁antagonists (selective/non-selective) normalize the altered topotecan kinetics in ARF?