Chronic Myeloid Leukemia Patient Registry in the Russian Federation: From Observational Studies to the Efficacy Evaluation in Clinical Practice

Туркина, А. Г.; Novitskaya, N. N.; Голенков, А. К.; Shuvaev, Vasiliy; Напсо, Л. И.; Krylova, IV; Savrilova, AM; Сафуанова, Г. Ш.; Av, Korobkin; Klitochenko, TYu; Бурнашева, Е. В.; Vasil’ev, E.V.; Сендерова, О. М.; Федорова, Е В; Yalunina, LM; Нехай, Е. В.; Кучма, Г. Б.; Lyamkina, A.S.; Щедрова, Н Г

doi:10.21320/2500-2139-2017-10-3-390-401

Клиническая онкогематология

2017

DOI: 10.21320/2500-2139-2017-10-3-390-401

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Chronic Myeloid Leukemia Patient Registry in the Russian Federation: From Observational Studies to the Efficacy Evaluation in Clinical Practice

А. Г. Туркина

N. N. Novitskaya

А. К. Голенков

et al.

Abstract: Background. Due to the significant increase in life expectancy and the quality of life in patients with chronic myeloid leukemia (CML) as well as the growing need for expensive tyrosine kinase inhibitors (TKI), the analysis of cost-effectiveness and lifelong monitoring of patients is especially important. Aim. We present the results of a multicenter observational study “The Russian Registry of Chronic Myeloid Leukemia in routine clinical practice (2011-2016)”. Materials & Methods. The study included Russia… Show more

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Cited by 12 publications

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“…The chronic myeloid leukemia (CML) represents the myeloproliferative new growth caused by activation of oncogene of BCR-ABL1 [6]. Frequency of CML increases with age and by estimates in the Russian Federation is 0,7 cases on 100 people [7]. TKI are basis of treatment of CML [8].…”

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confidence: 99%

Change of concentration of biochemical markers of dysfunction of endothelium at intake of inhibitors of tyrosinekinase of I and II generations at patients with a chronic myeloid leukemia as risk factor of development of cardiovascular complications

et al. 2021

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CML), the accepting inhibitors tyrosine of kinases (TKI) I and the II generations (TKI1 and TKI2 respectively), and development of arterial hypertension.Material and methods. Examination of 137 patients with CML in the chronic phase (CP) is conducted, the median of age — 47 years. 24 of them were with for the first time the verified diagnosis of CML and earlier did not accept TKI, they have made group of control. Other patients accepted TKI: 39 patients — imatinib 400 mg/day, 36 — dasatinib 100 mg/day, 38 — nilotinib 800 mg/day) more than 6 months. In biochemical analysis of blood indicators of lipidic range were defined. Level detection of ET-1 and VEGF was made by means of enzyme immunoassay. To all patients measurement of the heart rate (HR) and the arterial blood pressure (ABP) on both hands at an interval of 2 minutes from previous was once taken.Results. In group of patients from CML accepting nilotinib authentically significant increase in levels of systolic and diastolic ABP (р<0,001) in comparison with group of control, with group of the patients accepting imatinib and dasatinib is noted. The most serious changes of lipidic range are noted at the patients accepting nilotinib. In all groups statistically significant increase in level of C-reactive protein, fibrinogen, homocysteine, endothelin-1 and VEGF in comparison with group of control is revealed. The most expressed changes are found in group of the patients accepting nilotinib, values of parameters of C-reactive protein, fibrinogen, homocysteine, endothelin-1 and VEGF are changed authentically (р<0,001) and statistically significantly differ in comparison with group for the first time of the revealed patients with CML and groups of reception of imatinib and dazatinib.Conclusion. As a result of the conducted research endothelium variation of a function at patients from CML accepting TKI1 and TKI2 is revealed. The above-stated indicators can be used as additional diagnostic criteria for assessment of risk of development of arterial hypertension in patients with CML at reception of TKI.

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confidence: 99%

Change of concentration of biochemical markers of dysfunction of endothelium at intake of inhibitors of tyrosinekinase of I and II generations at patients with a chronic myeloid leukemia as risk factor of development of cardiovascular complications

et al. 2021

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Evolution of therapeutic approaches in patients with chronic myeloid leukemia and T315I mutation

Turkina,

Lomaia,

Morozova

et al. 2024

Onkogematologiâ

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Background. The T315I mutation in BCR::ABL1 kinase domain determines the resistance of leukemia cells to tyrosine kinase inhibitors (TKIs) – imatinib and secondgeneration TKIs – in patients with chronic myeloid leukemia (CML). The impact of new T315Itargeted approaches on treatment outcomes is being actively studied.Aim. To evaluate the clinical characteristics and therapy approaches in chronicphase CML patients with T315I mutation in clinical practice. An additional objective is to evaluate overall survival (OS) by considering the therapy provided.Materials and methods. The noninterventional retrospective multicenter study included 88 adult patients with chronicphase CML and the T315I mutation identified between January 2015 and November 2023, with a followup period of ≥3 months from 6 hematology clinics in Russia. T315Itargeted therapy refers to TKIs registered in Russia with clinically proven efficacy against the T315I mutation – ponatinib and asciminib, as well as allogeneic hematopoietic stem cell transplantation.Results. The median time from diagnosis to T315I mutation detection was 47 (6–192) months. Patients with T315I received 1–6 lines of therapy; most often, the T315I mutation was detected after 2–3 lines of therapy. After T315I mutation detection, 68 (77 %) patients received T315Itargeted therapy. The probability of receiving T315Itargeted therapy was 51; 61; 74 and 84 % at 6; 12; 24 and 36 months after T315I mutation detection, respectively, and was statistically significantly higher in patients with a detected mutation in 2018–2019 and 2020–2023 compared to 2015–2017 (p = 0.0256). The time to the first T315Itargeted approach was significantly reduced by year of mutation detection (p = 0.0002); the median time to T315Itargeted therapy over these periods was reduced from 17.8 to 2 months. Allogeneic hematopoietic stem cell transplantation was performed in 22 (25 %) of 88 patients: in 9 (41 %) – as the 1st T315Itargeted therapy; in 13 (59 %) patients, asciminib or ponatinib were used as bridgetherapy before it. Overall survival in the total group (n = 88) was 95; 79 and 68 % at 12; 36 and 60 months, respectively. The OS of patients with identified T315I mutation after 2020 was higher than in 2015–2017 and 2018–2019 periods, but the differences were not statistically significant (p = 0.1625).Conclusion. Selection of resistant clones with the T315I mutation can occur after any line of 1st–2nd generation TKI therapy. Improved availability of T315Itargeted therapy in Russia has been demonstrated depending on the period of T315I mutation detection. When the time to T315Itargeted therapy was reduced, a trend towards improved OS was observed. The differences in OS estimates identified may be related to selection factors given the retrospective nature of the study. Detailed prospective studies are required to evaluate the efficacy of different T315Idirected therapy protocols.

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Key principles of drug therapy in patients with chronic myeloid leukemia

Журавлев

Knysh

2023

Farmakoèkonomika

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Objective: to summarize scientific information about the basic principles of modern drug therapy for patients with chronic myeloid leukemia (CML) considering their individual characteristics.Material and methods. The basis of the study included modern scientific articles and clinical guidelines on CML diagnosis and treatment (2021), State Register of Medicines (SRM) of the Russian Federation, instructions for the use of medicines. The following methods were used: structural analysis, analytical method, content analysis, retrospective analysis, systematic approach, situational-logical and graphical methods of analysis.Results. The analysis made it possible to summarize scientific information about the basic principles of drug therapy for patients suffering from CML. It was revealed that the problem of CML therapy today is relevant, since every year there is an increase in the incidence of this nosology. Currently, the most significant is the prescription of tyrosine kinase inhibitors (TKIs), since they have pronounced effects and are well tolerated by patients. Therapy for CML in TKIs prescription consists of several lines. Imatinib is the first line therapy because it has better safety profile. There are combinations with imatinib; for example, it is used together with interferon alfa, which allows, in some cases, to increase the response to treatment. The following drugs are used in the second line: nilotinib, dasatinib, bosutinib, ponatinib. If TKI therapy is ineffective, it is possible to prescribe standard chemotherapy, interferon therapy, or bone marrow transplantation in the absence of contraindications. Studies are underway on the possibility of using and including in clinical guidelines such drugs as arsenic trioxide, decitabine, omacetaxime, inhibitors of farnesyl transferases, granulocyte-macrophage factors, antitumor vaccines. The analysis of SRM identified 27 trade names for TKIs, the share of domestic drugs was 60%. There were no Russian analogues for bosutinib and ponatinib in SRM, which are recommended for use in case of ineffective TKI therapy of previous lines.Conclusion. The study of drug provision for CML patients is an urgent task for pharmaceutical practice and for the healthcare system as a whole. Currently, the acute issues are the individual approach to the treatment of each CML patient considering concomitant diseases, and the search for new, more effective drugs that can increase the life expectancy and quality of life of patients suffering from this disease.

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Chronic Myeloid Leukemia Patient Registry in the Russian Federation: From Observational Studies to the Efficacy Evaluation in Clinical Practice

Cited by 12 publications

References 12 publications

Change of concentration of biochemical markers of dysfunction of endothelium at intake of inhibitors of tyrosinekinase of I and II generations at patients with a chronic myeloid leukemia as risk factor of development of cardiovascular complications

Change of concentration of biochemical markers of dysfunction of endothelium at intake of inhibitors of tyrosinekinase of I and II generations at patients with a chronic myeloid leukemia as risk factor of development of cardiovascular complications

Evolution of therapeutic approaches in patients with chronic myeloid leukemia and T315I mutation

Key principles of drug therapy in patients with chronic myeloid leukemia

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