Development and standardization of lozenges containing furosemide

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Introduction. Increasing the bioavailability and speed of onset of the diuretic effect of furosemide are necessary for accelerated elimination of toxins in acute and chronic diseases associated with swelling, as well as in acute and chronic poisoning. In conditions where oral or parenteral administration of furosemide is difficult or impossible due to the presence of restrictions in a number of diseases, the use of dosage forms of furosemide with local resorptive action, in particular lozenges, is relevant.

Purpose of the study: Experimental substantiation of quality standards and methods of analysis of lozenges containing furosemide.

Material and methods. The objects of the study are furosemide and lozenges manufactured at the production site of a pharmaceutical company. Research methods: spectrophotometric, chromatographic (HPLC).

Results. The basic physicochemical and technological properties of furosemide have been studied. It has been established that furosemide, as a practically insoluble substance in water, is advisable to introduce into the composition of a drug with local resorptive action in the form of a water-soluble derivative. Methods have been developed for the determination of furosemide in lozenges using two methods, spectrophotometry and HPLC, which meet the main validation criteria, are characterized by accuracy, reproducibility, relative ease of execution, and allow for quality control of the drug at all stages of production.

Conclusion. The physicochemical properties of furosemide make it possible to obtain water-soluble derivatives that can be included in dosage forms with local resorptive action. We have obtained furosemide in the form of a potassium salt, which is the active ingredient of lozenges, the composition of the tablets has been selected and tested, and pilot series have been developed. Methods for the detection and quantitative determination of furosemide have been developed, tested and certified.

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作者简介

Ifrat Zilfikarov

Maikop State Technological University of the Ministry of Science and Higher Education of the Russian Federation; ZAO “VIFITEH”, State Scientific Center for Medical and Biology; All-Russian Scientific Research Institute of Medicinal and Aromatic Plants (VILAR) of the Ministry of Science and Higher Education of the Russian Federation

编辑信件的主要联系方式.
Email: dagfarm@mail.ru
ORCID iD: 0000-0002-8638-9963

Doctor of Pharmaceutical Sciences, Professor of the Russian Academy of Sciences, Leading Researcher at the Department of Pharmacy of Maikop State Technological University; Deputy General Director of JSC "VIFITECH" for Science; Head of the Laboratory of the Quality Control Department of the All-Russian Research Institute of Medicinal and Aromatic Plants (VILAR)

俄罗斯联邦, st. Pervomaiskaya, 191, Maykop, Republic of Adygea, 385000; room 84, Obolensk village, Serpukhov district, Moscow region, 142279; st. Grina, 7, building 1, Moscow, 117216

Artur Arutyunov

Maikop State Technological University of the Ministry of Science and Higher Education of the Russian Federation

Email: ak.arut17@mail.ru
ORCID iD: 0000-0003-3883-6631

Candidate of Medical Sciences, Associate Professor, Dean of the Faculty of Pharmacy, Head of the Department of Pharmacy

俄罗斯联邦, st. Pervomaiskaya, 191, Maykop, Republic of Adygea, 385000

Anastasia Lebedeva

ZAO “VIFITEH”, State Scientific Center for Medical and Biology

Email: nastya-kot777@mail.ru
ORCID iD: 0000-0003-0701-1290

Senior Chromatography Engineer of the Laboratory 

俄罗斯联邦, room 84, Obolensk village, Serpukhov district, Moscow region, 142279

Inna Bochkareva

Maikop State Technological University of the Ministry of Science and Higher Education of the Russian Federation

Email: bochkarevainna@gmail.com
ORCID iD: 0000-0002-7898-4404

Candidate of Pharmaceutical Sciences, Associate Professor of the Department of Pharmacy, Dean of the Faculty of Postgraduate Education 

俄罗斯联邦, st. Pervomaiskaya, 191, Maykop, Republic of Adygea, 385000

Vera Artemyeva

Maikop State Technological University of the Ministry of Science and Higher Education of the Russian Federation

Email: kaf_farm@mkgtu.ru
ORCID iD: 0000-0001-8467-2899

Senior Lecturer at the Department of Pharmacy

俄罗斯联邦, st. Pervomaiskaya, 191, Maykop, Republic of Adygea, 385000

参考

  1. Beresneva O.N., Penchul N.A. The effect of furosemide on the cardiovascular system in experimental CRF. Nefrologiya. 2000; 4 (2): 97 (in Russian).
  2. Goryunova T.V., Osmolovskaya Yu.F., Zhirov I.V., Tereshchenko S.N. The choice of loop diuretic in patients with chronic heart failure. RMJ. 2017; 11: 771–4 (in Russian).
  3. Gosudarstvennaya farmakopeya Rossijskoj Federacii: v 4 t. XIV izd. M., 2018 [E`lektronny`j resurs]. Available at: https://femb.ru/record/pharmacopea14 [Accessed 12 January, 2023] (in Russian).
  4. Mareev V.Yu., Fomin I.V., Ageev F.T., Begrambekova Yu.L. et al. Russian Heart Failure Society, Russian Society of Cardiology. Russian Scientific Medical Society of Internal Medicine Guidelines for Heart failure: chronic (CHF) and acute decompensated (ADHF). Diagnosis, prevention and treatment. Kardiologiia. 2018; 58 (6S): 8–164. doi: 10.18087/cardio.2475 (in Russian).
  5. Preobrazhensky D.V., Nekrasova N.I., Khoseva N.I. et al. Torasemide is the Effective Loop Diuretic for Long-Term Therapy of Arterial Hypertension. Kardiologiia. 2011; 4: 67–73 (in Russian).
  6. Buggey J., Mentz R.J., Pitt B. et al. A reappraisal of loop diuretic choice in heart failure patients. Am. Heart J. 2015; 169: 323–33.
  7. Felker G.M., Menz R.J. Acute Decompensated Heart Failure. JACC. 2012; 59 (24): 2145–53.
  8. Hammarlund-Udenaes M., Benet L.Z. Furosemide pharmacokinetics and pharmacodynamics in health and disease – an update. M. J. Pharmacokinet Biopharm. 1989; 17: 1–46.

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2. Fig. 1. UV absorption spectrum of a solution of furosemide in 0.01 M sodium hydroxide solution

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3. Fig. 2. Chemistry of the reaction for producing potassium salt of furosemide

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4. Fig. 3. HPLC chromatogram of the standard solution and UV absorption spectrum of the CO peak of furosemide, measured in a stopped flow

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5. Fig 4. HPLC chromatogram of the test solution and UV absorption spectrum of the furosemide peak measured in stopped flow

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