Your search keyword '"Karyagina, A."' showing total 15 results

1. Comparative Characteristics of the Effectiveness of Tyrosine Kinase Inhibitors Vs Allogeneic Hematopoietic Stem Cell Transplantation in the Chronic Phase of Chronic Myeloid Leukemia

Author

Lomaia, Elza, primary, Chitanava, Tamara, additional, Vlasova, Yulia, additional, Motorin, Dmitry, additional, Voloshin, Sergey, additional, Zammoeva, Darina, additional, Badaev, Renat, additional, Matvienko, Yulia, additional, Efremova, Elizaveta, additional, Mileeva, Ekaterina, additional, Siordia, Nadia, additional, Kulemina, Olga, additional, Sbityakova, Eugenia, additional, Lazorko, Natalia, additional, Alexeeva, Julia, additional, Martynkevich, Irina, additional, Karyagina, Elena, additional, Ilyina, Natalia, additional, Medvedeva, Nadezhda, additional, Dorofeeva, Natalia, additional, Shneider, Tatiana, additional, Stepanova, Svetlana, additional, Shuvaev, Vasily, additional, and Morozova, Elena, additional

Published

2022

2. Comparative Characteristics of the Effectiveness of Tyrosine Kinase Inhibitors Vs Allogeneic Hematopoietic Stem Cell Transplantation in the Chronic Phase of Chronic Myeloid Leukemia

Author

Elza Lomaia, Tamara Chitanava, Yulia Vlasova, Dmitry Motorin, Sergey Voloshin, Darina Zammoeva, Renat Badaev, Yulia Matvienko, Elizaveta Efremova, Ekaterina Mileeva, Nadia Siordia, Olga Kulemina, Eugenia Sbityakova, Natalia Lazorko, Julia Alexeeva, Irina Martynkevich, Elena Karyagina, Natalia Ilyina, Nadezhda Medvedeva, Natalia Dorofeeva, Tatiana Shneider, Svetlana Stepanova, Vasily Shuvaev, and Elena Morozova

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

3. Rozrolimupab, a mixture of 25 recombinant human monoclonal RhD antibodies, in the treatment of primary immune thrombocytopenia

Author

Robak, Tadeusz, Windyga, Jerzy, Trelinski, Jacek, von Depka Prondzinski, Mario, Giagounidis, Aristoteles, Doyen, Chantal, Janssens, Ann, Álvarez-Román, María Teresa, Jarque, Isidro, Loscertales, Javier, Rus, Gloria Pérez, Hellmann, Andrzej, Jêdrzejczak, Wiesław Wiktor, Kuliczkowski, Kazimierz, Golubovic, Lana M., Celeketic, Dusica, Cucuianu, Andrei, Gheorghita, Emanuil, Lazaroiu, Mihaela, Shpilberg, Ofer, Attias, Dina, Karyagina, Elena, Svetlana, Kalinina, Vilchevska, Kateryna, Cooper, Nichola, Talks, Kate, Prabhu, Mukhyaprana, Sripada, Prasad, Bharadwaj, T.P.R., Næsted, Henrik, Skartved, Niels J.Ø., Frandsen, Torben P., Flensburg, Mimi F., Andersen, Peter S., and Petersen, Jørgen

Published

2012

4. Final Results from the Phase 3 Traial Areta Comparing a Novel, Extended-Release Anagrelide Formulation to Placebo in Essential Thrombocythemia Patients with Defined Risk Status

Author

Gisslinger, Heinz, primary, Klade, Christoph, additional, Abdulkadyrov, Kudrat, additional, Kyrcz-Krzemien, Slawomira, additional, Karyagina, Elena, additional, Melikyan, Anait L., additional, Warzocha, Krzysztof, additional, Grohmann-Izay, Barbara, additional, Hodisch, Juri, additional, Widmann, Rudolf S., additional, Kralovics, Robert, additional, Petrides, Petro E., additional, Schwarz, Jiri, additional, and Kiladjian, Jean-Jacques, additional

Published

2016

5. Final Results from the Phase 3 Traial Areta Comparing a Novel, Extended-Release Anagrelide Formulation to Placebo in Essential Thrombocythemia Patients with Defined Risk Status

Author

Jiri Schwarz, Petro E. Petrides, Barbara Grohmann-Izay, Elena Karyagina, Anait L. Melikyan, Rudolf Widmann, Kudrat Abdulkadyrov, Christoph Klade, Robert Kralovics, Juri Hodisch, Slawomira Kyrcz-Krzemien, Heinz Gisslinger, Krzysztof Warzocha, and Jean-Jacques Kiladjian

Subjects

medicine.medical_specialty, Thrombocytosis, Essential thrombocythemia, business.industry, Immunology, Area under the curve, Cell Biology, Hematology, Anagrelide, medicine.disease, Placebo, 030226 pharmacology & pharmacy, Biochemistry, Crossover study, Anagrelide Hydrochloride, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, medicine, Clinical endpoint, business, medicine.drug

Abstract

Background : Anagrelide hydrochloride (ana), is a well-known compound used to selectively normalize platelet counts (plc) by inhibiting megakaryocyte development and maturation. Common side-effects of licensed formulations may be largely due to peak plasma concentrations of ana and its 3OH-metabolite, whereas efficacy is proportional to the Area under the curve (AUC). A novel extended-release formulation (ana retard, AR) has superior pharmacokinetics (Petrides 2015) and has been demonstrated to be equally effective as the licensed formulation (Gisslinger 2016). Here, we investigate a "treat-early" concept in non-high risk ET patients. Study design:AR was compared to placebo in a phase 3, randomized, parallel group, multicenter, subject- and sponsor-blinded trial in patients diagnosed with ET according WHO 2008 and a defined risk status including JAK2 mutation, protein C/S or antithrombin III deficiency, factor V Leiden or prothrombin mutation, cardiovascular risk factors. The primary endpoint was time to first ET-related event adjudicated by a blinded expert panel, or progressive thrombocytosis (plc≥1000G/L or plc increase >300G/L within 3 months) requiring medical intervention. Secondary endpoints included plc response and change of risk status. Results : 146 patients were randomized and dosed (all Caucasian, mean age 43 years, 74% females), and 112 completed the first year with drop-out rates of 22% in AR and 25% in placebo. Only 49% of placebo patients vs. 74% of AR patients consented to enter the extension phase. Consequently, over the entire study duration, median exposure times differed significantly with 123 weeks for AR and 62 weeks for placebo. The primary endpoint was met in all analysis sets, with p Conclusions: Long term treatment of ET patients with defined risk status, using this novel modified-release anagrelide formulation proofed well tolerable, normalized plc in a vast majority, significantly reduced progression to high-risk status and most importantly was associated with significantly less clinical ET related events. These data have important implications for the optimal management of ET and support a "treat-early" approach. References Results of a phase I, single dose, randomized, 3-way crossover study, to assess the bioavailability of a novel anagrelide extended release (ER) formulation in comparison to a commercially available anagrelide reference product (CARP) in healthy volunteers, Petrides P, Zagrijtschuk O, Klade C, DGHO, 2015 Phase 3 trial TEAM-ET in 106 high-risk Essential Thrombocythemia patients, demonstrating non-inferiority of Anagrelide Retard, a novel, extended-release anagrelide formulation, to the licensed comparator Gisslinger H, Radinoff A, Karyagina E,Kyrcz-Krzemień S, Abdulkadyrov K, Gerbutavicius R,Melikyan A, Burgstaller S, Hus M, Kłoczko J, Yablokova V, Tzvetkov N, Całbecka M, Shneyder T, Warzocha K, Jurgutis M, Kaplanov K, Hodisch J, Klade C, Buxhofer-Ausch V, European School of Hematology EHA 21st Congress, 2016 Disclosures Gisslinger: AOP Orphan Pharmaceuticals AG, Novartis, Celgene, Baxalta: Consultancy, Honoraria, Research Funding. Klade:AOP Orphan: Employment. Kyrcz-Krzemien:AOP Orphan Pharmaceuticals AG, Novartis, BMS, Medac: Honoraria. Warzocha:BMS: Consultancy, Honoraria; Novartis: Consultancy, Honoraria. Grohmann-Izay:AOP Orphan Pharmaceuticals AG: Employment. Hodisch:AOP Orphan Pharmaceuticals: Employment. Widmann:AOP Orphan Pharmaceuticals: Employment. Kralovics:Qiagen: Membership on an entity's Board of Directors or advisory committees; AOP Orphan: Research Funding. Schwarz:AOP Orphan Pharmaceuticals: Consultancy. Kiladjian:Novartis: Research Funding; AOP Orphan: Research Funding.

Published

2016

6. The Results of the Russian Registry of Primary Immune Thrombocytopenia (ITP) in Adults

Author

Lisukov, Igor, primary, Maschan, Alexey, additional, Shamardina, Anastasia, additional, Chagorova, Tatyana, additional, Davydkin, Igor, additional, Sycheva, Tatyana, additional, Zagoskina, Tamara, additional, Karyagina, Elena, additional, Salogub, Galina, additional, Savinova, Marina, additional, Schelekhova, Tatyana, additional, Kovaleva, Lidiya, additional, Schneider, Tatyana, additional, Unzhekova, Anna, additional, Kuznetsova, Elena, additional, Schatochin, Yuriy, additional, Ivanova, Maria, additional, Vinogradova, Elena, additional, Kaplanov, Kamil, additional, Markova, Inna, additional, Kanjukova, Olimpiada, additional, Abdulkadyrov, Kudrat, additional, Sedlova, Julia, additional, Osynikhina, Svetlana, additional, Tsvetaeva, Nina, additional, Volodicheva, Elena, additional, Akhmadeev, Aryslan, additional, Maschan, Michael A, additional, Kulagin, Alexandr, additional, Rumyantsev, Alexander, additional, and Afanasyev, Boris V, additional

Published

2015

7. The Impact of Genetic Abnormalities (GA) and Other Factors on Survival in Patients after 65 Years with Multiple Myeloma (MM)

Author

Garifullin, Andrei, primary, Martynkevich, Irina, additional, Voloshin, Sergei, additional, Kuvshinov, Alexei, additional, Martynenko, Ludmila, additional, Kleina, Elizaveta, additional, Salogub, Galina, additional, Karyagina, Elena, additional, Schmidt, Alexander, additional, and Abdulkadyrov, Kudrat, additional

Published

2015

8. The Results of the Russian Registry of Primary Immune Thrombocytopenia (ITP) in Adults

Author

Inna V. Markova, Igor A. Lisukov, Elena Vinogradova, Tatyana Chagorova, T P Zagoskina, AD Kulagin, Anna Unzhekova, Alexey Maschan, Yuriy Schatochin, Boris V. Afanasyev, Michael Maschan, Elena Kuznetsova, Kudrat Abdulkadyrov, Julia Sedlova, Alexander Rumyantsev, I.L. Davydkin, K D Kaplanov, Galina Salogub, Aryslan Akhmadeev, Shamardina Av, Tatyana Schelekhova, Nina Tsvetaeva, Tatyana Schneider, Lidiya Kovaleva, Elena Volodicheva, Tatyana Sycheva, Olimpiada Kanjukova, Marina Savinova, Maria Ivanova, Svetlana Osynikhina, and Elena Karyagina

Subjects

medicine.medical_specialty, Gastrointestinal bleeding, Pediatrics, Romiplostim, business.industry, medicine.medical_treatment, Immunology, Splenectomy, Eltrombopag, macromolecular substances, Cell Biology, Hematology, medicine.disease, Biochemistry, chemistry.chemical_compound, chemistry, Internal medicine, Cohort, medicine, Rituximab, business, Prospective cohort study, medicine.drug, Cohort study

Abstract

Study objectives The aim of the study was to evaluate disease characteristics and treatment practices of ITP in Russia. Materials and methods The ITP Registry was a multicenter, prospective, observational cohort study. The observation period for each patient in the Registry was not less than 12 months. Inclusion criteria: diagnosis of primary ITP, informed consent of the patient. Exclusion criteria: secondary thrombocytopenia. Data from medical records were registered in the e-CRF in average every 3 months. Descriptive statistics was used. Patients were registered since June 2011 till June 2014. Results Five hundred and seven adult 394female (77.7%)/113 male(22.3%) pts from 26 hematology centers in various regions of the Russian Federation were included. Observation period ranged from 1.4 to 29.8 months with an average of 18.6 ± 6.2 mo. Median age was 50.2 years (range 18.6-89.1). Median disease duration was 1.83 years (range 0-56.07). History of ITP of lasting < 1 year was reported in 186 (36.7%) pts, 1-5 years - in 142 (28%), 5-10 years - in 56 (11%), over 10 years - in 87 (17.2%), and was considered as unknown - in 36 (7.1%). Newly diagnosed ITP was reported in 19.5% of adult pts; persistent - in 16.6% and chronic ITP - in 63.9% of pts, respectively. Median platelets count was 14,0 x 109/L (range 0.0- 119.0 x 109/L). Hemorrhagic manifestations in the history of ITP were reported in 92.5% of pts: skin hemorrhages - in 89.5% of pts, oral bleeding - in 50.3% , epistaxis - in 37.3% , gastrointestinal bleeding - in 7.7%, intracranial bleeding - in 0.4%, hematuria - in 4.5%, and other hemorrhages - in 20.9% of pts. Severe ITP at the time of enrollment was observed in 158 (31.2%) pts (104 pts (20.5%) had a clinically significant bleeding at the disease onset, and 54 (10.7%) pts developed new clinically significant hemorrhages during the treatment. Refractory ITP at the time of enrollment was reported in 100 (19.7%) pts (resistance to the first, second and subsequent lines of therapy in 62 (12.2%) pts); 38 (7.5%) pts did not respond to splenectomy. At the time of enrollment, 250 (49.3%) pts received medical treatment for ITP. Severe ITP after enrollment was observed in 124 (24.8%) adult pts. Throughout the study, various hemorrhagic manifestations of ITP were reported in 48.0% of pts, severe hemorrhagic syndrome was reported in 10.0% of pts; Before enrollment, splenectomy was reported in 94 pts (18.5%); complete response (CR) was maintained in 34 (36.2%) pts, partial response - in 20 (21.3%), and no response - in 7 (7.4%). Thirty-two (34.0%) pts had lost the response after initial success. During the study, splenectomy was performed in 44 (10.8%) pts, of those - in 7 pts (15.9%) with newly diagnosed ITP; in 6 pts (13.6%) - with persistent ITP, and in 31 pts (70.5%) - with chronic ITP. The duration of the disease at the time of splenectomy varied from 0 to 21 yrs; with a median of 1.03 year. CR to splenectomy was observed in 31 (70.5%) pts, partial response - in 10 (22.7%), and no response in 1 (2.3%), while 2 (4.5%) pts lost response. Since the response to splenectomy might change during the observation in the study, the best response was registered. Table 1. Distribution of the best response to splenectomy variable (before study entry and in the course of the study). Number of Pts (n) % Best response to splenectomy Missing data 1 0.7% Complete response 65 47.1% A response 30 21.7% No response 8 5.8% Loss of response 34 24.6% Total 138 100% Two hundred and forty-three (47.9%) pts received their first-line treatment during the study; glucocorticosteroids (GCS) - 222 (91.3%) pts, immunoglobulins (IVIG) - 2 pts (0.8%), other drugs - 26 (10.7 %) pts. A second-line therapy was administered to 133 pts (26.23%), of which 27 (20.3%) received GCS, IVIG - 23 (17.3%), alfa-interferons - 6 (4.5%), immunosuppressants - 8 (6%), rituximab - 18 (13.53%), romiplostim - 39 (29.3%), eltrombopag - 37 (27.8%), other drugs - 2 (1.5%) pts. Conclusion For the first time in Russia, information regarding the clinical presentation and the "real life" management practice of adults with primary ITP was obtained in a large cohort of pts in a prospective study. The Registry showed a variability of ITP clinical course. One fifth of pts were refractory to therapy. The main therapy options for the ≥ 2nd line in a cohort of adult pts were splenectomy and TPO receptor agonists. However, large proportion of pts still received GCSs in the 2nd and even 3rd line of therapy. Disclosures No relevant conflicts of interest to declare.

Published

2015

9. The Impact of Genetic Abnormalities (GA) and Other Factors on Survival in Patients after 65 Years with Multiple Myeloma (MM)

Author

Irina Martynkevich, Andrei Garifullin, Galina Salogub, Sergei Voloshin, Elena Karyagina, Alexander Schmidt, Alexei Kuvshinov, Ludmila Martynenko, Kudrat Abdulkadyrov, and Elizaveta Kleina

Subjects

Old patients, medicine.medical_specialty, Bortezomib, business.industry, Immunology, Fish analysis, Cell Biology, Hematology, medicine.disease, Biochemistry, Gastroenterology, Surgery, Regimen, Standard Risk, Internal medicine, medicine, Overall survival, In patient, business, Multiple myeloma, medicine.drug

Abstract

Background. The increase of life expectancy in patients after 65 years with MM is the main aim of treatment. Lack of carrying out aggressive anti-multiple myeloma therapy increase influence of different factors on OS. Aims. To compare influence GA and other different factors on overall survival in 65 and more years old patients with MM. Methods. We retrospectively analyzed 40 patients 65 and more years (median age 71 years, range 65-86; male/female - 1:1.35). The incidences of genetic abnormalities were determined in all cases. Cytogenetic analysis was performed on bone marrow samples using standard GTG-method. Metaphase FISH analysis was performed according to the manufacturer's protocol using DNA probes: LSI 13(RB1)13q14, IGH/CCND1, IGH/FGFR3, LSI TP53 (17q13.1). Stratification of patients was carried in groups of risk according to the modified molecular classification mSMARTmod 1.0 and mSMARTmod 2.0. Patients with 2 and more chromosomal aberrations were additionally entered in high-risk group of both systems. Results. GA in multiple myeloma after 65 years old patients were detected in 22.8% (9/40). The occurrence frequency of t(11;14) was 26.0% (6/23), del(13q) - 20.8% (5/24), t(4;14) - 4.3% (n=1/23), del(17p) - 0% (n=0/11). 33/40 (82.5%) patients entered into standard risk group, 4/40 (10%) - into intermediate risk, 3/40 (7,5%) - into high-risk. Median OS (MOS) according to mSMARTmod 1.0 in standard risk group (33/40) was 78 months, in high-risk (7/40) - 54 months. Median OS according to mSMARTmod 2.0 in standard risk group (33/40) was 78 months, in intermediate-risk (4/40) - 56 months, in high-risk (3/40) - 49 months. In patients groups without renal failure (35/40) MOS was 78 vs. 46 months with renal failure (5/40). MOS isn't reached in patients with ISS I (4/27), but MOS in patients with ISS II (13/27) and ISS III (10/27) were 50 and 54 months, respectively. MOS in patients group (10/40), who have both (bortezomib and lenolidomide) anti-myeloma agents was 110 months vs. 57 months in group (30/40) only with bortezomib-based regimen of treatment. Conclusions. Many factors influence on OS in 65 and more years old patients with MM. However, patients, who had treatment with bortezomib and lenelidomide had the best results of OS. Disclosures No relevant conflicts of interest to declare.

Published

2015

10. Importance of DNMT3A Gene mutations detection in Prognostic Analyses of Patients with Acute Myeloid Leukemia

Author

Petrova, Ekaterina, primary, Martynkevich, Irina, additional, Polushkina, Lyubov, additional, Martynenko, Lyudmila, additional, Ivanova, Marina, additional, Cybakova, Natalya, additional, Shabanova, Elena, additional, Zyuzgin, Ilya, additional, Karyagina, Elena, additional, Gritsaev, Sergey, additional, and Abdulkadyrov, Kudrat, additional

Published

2014

11. Importance of DNMT3A Gene mutations detection in Prognostic Analyses of Patients with Acute Myeloid Leukemia

Author

Gritsaev Sv, Elena Shabanova, Elena Karyagina, Lyudmila Martynenko, Ekaterina Petrova, Ilya Zyuzgin, Lyubov Polushkina, Natalya Cybakova, Irina Martynkevich, Marina Ivanova, and Kudrat Abdulkadyrov

Subjects

Neuroblastoma RAS viral oncogene homolog, Oncology, medicine.medical_specialty, Mutation, NPM1, Immunology, Wild type, Myeloid leukemia, Cell Biology, Hematology, Biology, medicine.disease_cause, Bioinformatics, Biochemistry, Exon, Internal medicine, embryonic structures, medicine, Missense mutation, Allele

Abstract

Objectives and background: Normal karyotype (NK) in AML patients accounts for nearly 45% of all cases and were assigned into intermediate risk group. The identification of new molecular markers in this group is the focus of most of researches. The application of the next-generation sequence techniques led to detect molecular markers with valuable prognostic significance. F.e., identification of DNMT3A mutations has gained the tremendous attention in recent times, because of its essential role in cell development, high frequency in AML patients and association of poor clinical outcome. Objects: to analyse character and frequency of DNMT3A mutations in AML patients; to study their associations with clinical and laboratory parameters and other molecular markers; to investigate their prognostic value. Methods: The screening of DNMT3A mutations was performed by the high-resolution melting curve analysis. Mutations in FLT3, CKIT and NPM1 were analysed by polymerase chain reaction and in NRAS by sequencing. Standard GTG-method was used for patients karyotyping. The investigation group included 98 AML patients. Missense mutations of DNMT3A exon 23 (R882) were identified in 16 (16,3%) de novo AML patients. The most common mutation in DNMT3A was R882H (n=9;56.3%), followed by R882C (n=6;37.5%), and R882S (n=1;6.2%). All but one patients (with mutation R882S) were heterozygous and retained a wild-type allele. Patients with isolated DNMT3A mutations were seen in 3 cases; 3 pts with R882C had also mutations in NRAS; 3 pts had DNMT3Amut/FLT3-ITDmut; 1 pt - DNMT3Amut/FLT3-ITDmut/ FLT3-TKDmut; 4 pts - DNMT3Amut/FLT3-ITDmut/ NPM1mut and 3 pts - DNMT3Amut/ NPM1mut. Results: Patients who harbored a mutation in DNMT3A had higher white blood cells count (p=0.039) at diagnosis and more frequently belonged to FAB group M4 (p=0.033), as compared with DNMT3A wild-type. Of the 16 patients who had AML with DNMT3A mutation, 13 (26.5%) had tumors with normal cytogenetic profiles (of a total of 49 cytogenetically normal samples) (p=0.006). There was no statistical correlation with other parameters, including sex, age, hemoglobin, and platelet count between patients with and without DNMT3A mutations (p>0.05). DNTM3A mutations were significantly more prevalent in NPM1 positive cases when compared to NPM1 wild type cases (p=0.000). DNTM3A mutations were also more dominant in FLT3-ITD positive pts than wild type (p=0.000). In contrast, DNMT3A mutations were not observed in cases with CKIT mutations indicating that these mutations can be mutually exclusive in nature. There was a statistical significance between overall survival (OS) of NK-AML pts with DNMT3A mutations and DNMT3Awt (p=0.032). Figure 1 Figure 1. Conclusions: AML with DNMT3A mutations represent the group, homogeneous on a number of clinical and laboratory parameters. DNMT3A mutations are highly recurrent in patients with de novo AML with an intermediate-risk cytogenetic profile. FLT3-ITD and NPM1 mutations appear as a major significant coexisting genetic mutations in DNMT3Amut pts. The presence of DNMT3A mutations can be considered as independent adverse prognostic factor for OS, suggesting that testing of DNMT3A mutations can help further improve risk stratification in NK-AML. References: Ley T.J., Ding L., Walter M.J., McLellan M.D. et al. DNMT3A mutations in acute myeloid leukemia. N Engl J Med 2010;363:2424-2433. Disclosures No relevant conflicts of interest to declare.

Published

2014

12. Crude and Age-Adjusted Ph+/Bcr-Abl+ Chronic Myeloid Leukemia Incidence Rate in St. Petersburg and Leningrad Region Between 2006–2011

Author

Abdulkadyrov, Kudrat, primary, Lomaia, Elza, additional, Lazorko, Natalia, additional, Shuvaev, Vasiliy, additional, Abdulkadyrova, Alla, additional, Martinkevich, Irina, additional, Usacheva, Elena, additional, Udalieva, Vera, additional, Zotova, Irina, additional, Machulaitene, Elena, additional, Ilina, Natalia, additional, Karyagina, Elena, additional, Kholopova, Irina, additional, Romanova, Ekaterina, additional, Sbityakova, Eugenia, additional, Shneider, Tatiana, additional, and Zaritskey, Andrey, additional

Published

2012

13. Final Results From a Phase II Trial with the First in Class Recombinant Polyclonal Antibody Product Rozrolimupab in Primary Immune Thrombocytopenia

Author

Robak, Tadeusz, primary, Trelinski, Jacek, additional, von Depka Prondzinski, Mario, additional, Giagounidis, Aristoteles, additional, Doyen, Chantal, additional, Janssens, Ann, additional, Román, Mayte Álvarez, additional, Pueyo, Javier Loscertales, additional, Ramos, Isidro Jarque, additional, Loscertales, Javier, additional, Rus, Gloria Pérez, additional, Hellmann, Andrzej, additional, Wiktor-Jedrzejczak, Wieslaw, additional, Kuliczkowski, Kazimierz, additional, Golubovic, Lana, additional, Celeketic, Dusica, additional, Cucuianu, Andrei, additional, Gheorghita, Emanuil, additional, Mihaela, Lazaroiu, additional, Attias, Dina, additional, Shpilberg, Ofer, additional, Karyagina, Elena, additional, Vilchevska, Kateryna, additional, Svetlana, Kalinina, additional, Cooper, Nichola, additional, Talks, Kate, additional, Prabhu, Mukyaprana, additional, Prasad, Sripada V.S.S, additional, Bharadwaj, T. P. Raghava, additional, Flensburg, Mimi Folden, additional, Petersen, Jorgen, additional, and Windyga, Jerzy, additional

Published

2011

14. Crude and Age-Adjusted Ph+/Bcr-Abl+ Chronic Myeloid Leukemia Incidence Rate in St. Petersburg and Leningrad Region Between 2006–2011

Author

Irina Martinkevich, Natalia Ilina, Andrey Zaritskey, Elena Karyagina, Natalia Lazorko, Elza Lomaia, Elena Usacheva, Vera Udalieva, Ekaterina Romanova, Irina Zotova, Tatiana Shneider, Eugenia Sbityakova, Alla Abdulkadyrova, Vasiliy Shuvaev, Kudrat Abdulkadyrov, Elena Machulaitene, and Irina Kholopova

Subjects

medicine.medical_specialty, education.field_of_study, business.industry, Incidence (epidemiology), Mortality rate, Immunology, Population, Age adjustment, Cell Biology, Hematology, Biochemistry, Middle age, Transplantation, Imatinib mesylate, hemic and lymphatic diseases, Internal medicine, medicine, Sokal Score, education, business

Abstract

Abstract 4432 Background: The incidence of chronic myeloid leukemia (CML), reported from some population based registries, varies significantly. CML is known as age-dependent disease, so population age structure may strongly influent on the data. For international comparisons several systems for age-standardization are using in epidemiological studies. We conducted our retrospective study to reveal differences in CML incidence rates on the basis of calculation – crude or age-adjusted according to different population standards in St. Petersburg and Leningrad region. Methods: In 2005 the database of Ph- and/or bcr-abl- positive CML patients (pts) was conducted in St. Petersburg and Leningrad region. Since then the data from all newly diagnosed CML patients were included prospectively on population basis. The database was updated at least bi-annually. The data were obtained from hematologists, as general practitioners and private physicians are not licensed to treat oncohematological disorders. The data were double checked from the list of Imatinib distribution (the only drug reimbursed for first line treatment). To calculate crude CML incidence rate we use the data of the general census of the population in Russia in 2010 (the whole population of our region is 6596434 with population in age 15 and above 5821133). For age-adjusted CML incidence rate we use three of currently existing standards: The Segi (“World”), The Scandinavian (“European”) and the WHO standard (based on world average population between 2000–2025). Results: There are 258 (242 in chronic, 9 in accelerated and 7 in blastic phases) CML adult (15 years and above) pts, registered during 2006–2011. The median age is 53 years (48,5 and 55,5 years for men and women respectively). Sokal score was evaluable in 209 pts. It is low in 37%, intermediate in 35% and high in 28% pts. The crude CML incidence rate is slightly higher in men than in women with ratio 1,2:1. Mean annual crude CML incidence rate was 0,65 per 100 000 whole population of Saint Petersburg and Leningrad region, but it was 0,74 in adult population (15 years old and above). Mean annual CML incidence rates in the same age groups were slightly higher in all three standardized systems: 0,94 in Segi, 0,84 in Scandinavian and 0,88 in WHO standard populations. CML incidence rates in all age groups are presented in the table 1. CML incidence rate was lowest in young pts. It was unexpectedly very low in senior pts. CML incidence rates nearly for all age groups were slightly higher in St. Petersburg than in the Leningrad region. The majority of pts (98%) were treated with Imatinib (93% first or second line) or other tyrosine kinase inhibitors (5% first line-in international clinical trials, 18% after Imatinib failure or intolerance). Stem cell transplantation was performed only in 8/258 (3%) pts. Only 25235 (7,5%) evaluable pts progressed from chronic to advanced phases. Only 29/258 (11%) pts dead mostly due to CML (21 CML related deaths were reported). Estimated 5 years overall survival is 91,5%. Mean annual overall CML pts death rate was 1,9% (mean annual death rate between 2006–2010 in whole population of our region was 1,6%). Mean pts accumulated very fast - annual CML prevalence increasing rate between 2005–2011 was more than 14% (Picture 1). Conclusions: CML incidence both crude and age-adjusted in our population based registry is nearly the same in young and middle age, but much lower in senior (65 years and above) pts groups in comparison with published data from other registries which probably represents peculiarities of health system rather than real incidence. In the tyrosine kinase inhibitors era CML patients death rate is very low (nearly the same as in whole population) and CML pts is accumulated very fast in our region. Disclosures: No relevant conflicts of interest to declare.

Published

2012

15. Importance of DNMT3A Gene mutationsdetection in Prognostic Analyses of Patients with Acute Myeloid Leukemia

Author

Petrova, Ekaterina, Martynkevich, Irina, Polushkina, Lyubov, Martynenko, Lyudmila, Ivanova, Marina, Cybakova, Natalya, Shabanova, Elena, Zyuzgin, Ilya, Karyagina, Elena, Gritsaev, Sergey, and Abdulkadyrov, Kudrat

Abstract

Objectives and background:Normal karyotype (NK) in AML patients accounts for nearly 45% of all cases and were assigned into intermediate risk group. The identification of new molecular markers in this group is the focus of most of researches. The application of the next-generation sequence techniques led to detect molecular markers with valuable prognostic significance. F.e., identification of DNMT3Amutations has gained the tremendous attention in recent times, because of its essential role in cell development, high frequency in AML patients and association of poor clinical outcome. Objects: to analyse character and frequency of DNMT3Amutations in AML patients; to study their associations with clinical and laboratory parameters and other molecular markers; to investigate their prognostic value.

Published

2014