Abstract

Any drug is potentially associated with the risk of adverse drug reactions (ADRs), the incidence of which in developed and developing countries is estimated at 6.3 (3.3—11.0) and 5.5 % (1.1—16.9), respectively. Many ADRs increase mortality and / or morbidity and / or cause clinical manifestations that require a patient to seek medical help or hospitalization; a special term has been introduced — drug-induced diseases. Food can interact with drugs and increase the risk of ADRs, including serious ones. The simultaneous intake of food and drugs can affect the bioavailability, pharmacokinetics, pharmacodynamics and therapeutic efficacy of drugs due to changes in drug absorption and metabolism. A striking example of the effect of food on the pharmacokinetic profile of drugs is the change in the bioavailability of the tyrosine kinase inhibitor lapatinib: compared with taking on an empty stomach, the bioavailability of lapatinib in a single dose of 1 500 mg after taking it together with high-calorie standard food increases by an average of 325 % — 4.25 times. In other words, the concentration of the drug in the blood serum after taking one tablet at the same time with food is comparable to taking 4 tablets on an empty stomach. Currently, there are no recommendations for choosing a dosage regimen for drugs depending on the qualitative and quantitative composition of food, as well as taking into account potential interactions with food components, although these recommendations are extremely necessary for patients and healthcare professionals. In this regard, this article summarizes the data available at the time of writing in open sources concerning the effect of food on the absorption and metabolism of drugs, and also describes the possible mechanisms of interaction.

Highlights

  • Any drug is potentially associated with the risk of adverse drug reactions (ADRs), the incidence of which in developed and developing countries is estimated at 6.3 (3.3—11.0) and 5.5 % (1.1—16.9), respectively

  • Food can interact with drugs and increase the risk of ADRs, including serious ones

  • A striking example of the effect of food on the pharmacokinetic profile of drugs is the change in the bioavailability of the tyrosine kinase inhibitor lapatinib: compared with taking on an empty stomach, the bioavailability of lapatinib in a single dose of 1 500 mg after taking it together with high-calorie standard food increases by an average of 325 % — 4.25 times

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Summary

БЕЗОПАСНОСТЬ ЛЕКАРСТВ

Взаимодействие пищевых продуктов и лекарственных средств как фактор риска развития лекарственно индуцированных заболеваний: эпидемиология, факторы риска, потенциальные механизмы развития взаимодействий. There are no recommendations for choosing a dosage regimen for drugs depending on the qualitative and quantitative composition of food, as well as taking into account potential interactions with food components, these recommendations are extremely necessary for patients and healthcare professionals In this regard, this article summarizes the data available at the time of writing in open sources concerning the effect of food on the absorption and metabolism of drugs, and describes the possible mechanisms of interaction. [11], которые пришли к выводу, что полипрагмазия, одновременный приём ЛС и пищи, отсутствие консультирования по вопросам правильного приёма ЛС, а также наличие некоторых хронических заболеваний (сахарный диабет) повышают риски развития НР вследствие взаимодействия ЛС и продуктов питания [11]. Взаимодействие на уровне белков-переносчиков / drug-food interaction involving plasma proteins

Organic Anion Transporting Polypeptides
Oligopeptide transporter
Красное вино
Findings
Остроумова Ольга Дмитриевна

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