Differences in the binding of quinine and quinidine to plasma proteins.

Mihaly, G W; Ching, Michael S.; Klejn, Margaret B.; Paull, John; Smallwood, Richard A.

doi:10.1111/j.1365-2125.1987.tb03244.x

Cited by 51 publications

(39 citation statements)

References 18 publications

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“…This is supported by the observations in the present study; there was no relationship between serum albumin concentration and quinine binding, but a significant log linear correlation between AAG concentration and the fraction of quinine bound. However we and others (Mihaly et al, 1987) have found that plasma protein binding of quinidine (circa 70-80%) is significantly lower than quinine plasma protein binding (85-95%), and AAG affinity is correspondingly less, and so as with other isomers, findings concerning one diastereoisomer cannot necessarily be extrapolated to the other. In this study the Hill plot gave mean (s.e.…”

Section: Patientscontrasting

confidence: 53%

Alpha 1‐acid glycoprotein (orosomucoid) and plasma protein binding of quinine in falciparum malaria.

Silamut

Molunto

et al. 1991

Brit J Clinical Pharma

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Section: Patientscontrasting

confidence: 53%

Alpha 1‐acid glycoprotein (orosomucoid) and plasma protein binding of quinine in falciparum malaria.

Silamut

Molunto

et al. 1991

Brit J Clinical Pharma

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“…This may be compounded further by differences in distribution and plasma protein binding which have not been assessed in this study. It is known that quinine is highly protein bound (92%) and that the percentage binding varies directly with plasma protein concentration (Mihaly et al, 1987). Patients with kwashiorkor and malaria treated with quinine should be carefully monitored to see whether there are any clinical correlates with the pharmacokinetic changes.…”

Section: Discussionmentioning

confidence: 99%

Pharmacokinetics of quinine in African children suffering from kwashiorkor.

Salako

Sowunmi

Akinbami

1989

Brit J Clinical Pharma

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The pharmacokinetics of quinine were studied in seven normal African children and in six African children suffering from kwashiorkor, after an oral dose of 10 mg kg-1 of quinine hydrochloride. The two groups were similar in age but the children with kwashiorkor weighed significantly less than the control children (P < 0.001). The children with kwashiorkor further differed from the control children in having significantly lower packed cell volume (P < 0.001), total plasma protein and plasma albumin (P < 0.001), and higher serum SGOT (P < 0.05). The apparent absorption half-life was significantly longer in kwashiorkor than in controls (P < 0.05). Similarly, the Cmax was significantly lower (P < 0.01) in kwashiorkor than in controls. Quinine was eliminated more slowly in children with kwashiorkor, the elimination half-life being significantly longer (P < 0.001) and the oral clearance significantly less (P < 0.001) than in controls. It is concluded that kwashiorkor significantly affects the pharmacokinetics of quinine, and that the effect may be due to the pathological changes in the intestine and liver in this condition.

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“…This has important implications since, theoretically, the shift from high-affinity to lowaffinity binding may influence the ability of compounds to cross biological membranes. Indeed, differences in orosomucoid binding have been shown to alter hepatic extraction ratio of quinidine (Mansor et al, 1991), a drug that is bound to both orosomucoid and albumin (Mihaly et al, 1987).…”

Section: Discussionmentioning

confidence: 99%

In Vitro Synergy and Enhanced Murine Brain Penetration of Saquinavir Coadministered with Mefloquine

Owen

Janneh²,

Hartkoorn³

et al. 2005

J Pharmacol Exp Ther

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Highly active antiretroviral therapy has substantially improved prognosis in human immunodeficiency virus (HIV). However, the integration of proviral DNA, development of viral resistance, and lack of permeability of drugs into sanctuary sites (e.g., brain and lymphocyte) are major limitations to current regimens. Previous studies have indicated that the antimalarial drug chloroquine (CQ) has antiviral efficacy and a synergism with HIV protease inhibitors. We have screened a panel of antimalarial compounds for activity against HIV-1 in vitro. A limited efficacy was observed for CQ, mefloquine (MQ), and mepacrine (MC). However, marked synergy was observed between MQ and saquinavir (SQV), but not CQ in U937 cells.Furthermore, enhancement of the antiviral activity of SQV and four other protease inhibitors (PIs) by MQ was observed in MT4 cells, indicating a class specific rather than a drug-specific phenomenon. We demonstrate that these observations are a result of inhibition of multiple drug efflux proteins by MQ and that MQ also displaces SQV from orosomucoid in vitro. Finally, coadministration of MQ and SQV in CD-1 mice dramatically altered the tissue distribution of SQV, resulting in a Ͼ3-fold and Ͼ2-fold increase in the tissue/blood ratio for brain and testis, respectively. This pharmacological enhancement of in vitro antiviral activity of PIs by MQ now warrants further examination in vivo.

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Differences in the binding of quinine and quinidine to plasma proteins.

Cited by 51 publications

References 18 publications

Alpha 1‐acid glycoprotein (orosomucoid) and plasma protein binding of quinine in falciparum malaria.

Alpha 1‐acid glycoprotein (orosomucoid) and plasma protein binding of quinine in falciparum malaria.

Pharmacokinetics of quinine in African children suffering from kwashiorkor.

In Vitro Synergy and Enhanced Murine Brain Penetration of Saquinavir Coadministered with Mefloquine

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