Your search keyword '"Pruunsild K"' showing total 31 results

1. Value of flow cytometry for MRD-based relapse prediction in B-cell precursor ALL in a multicenter setting

Author

Modvig, S., Hallböök, H., Madsen, H. O., Siitonen, S., Rosthøj, S., Tierens, A., Juvonen, V., Osnes, L. T. N., Vålerhaugen, H., Hultdin, M., Matuzeviciene, R., Stoskus, M., Marincevic, M., Lilleorg, A., Ehinger, M., Norén-Nystrøm, U., Toft, N., Taskinen, M., Jónsson, O. G., Pruunsild, K., Vaitkeviciene, G., Vettenranta, K., Lund, B., Abrahamsson, J., Porwit, A., Schmiegelow, K., and Marquart, H. V.

Published

2021

2. Minimal residual disease quantification by flow cytometry provides reliable risk stratification in T-cell acute lymphoblastic leukemia

Author

Modvig, S., Madsen, H. O., Siitonen, S. M., Rosthøj, S., Tierens, A., Juvonen, V., Osnes, L.T.N., Vålerhaugen, H., Hultdin, M., Thörn, I., Matuzeviciene, R., Stoskus, M., Marincevic, M., Fogelstrand, L., Lilleorg, A., Toft, N., Jónsson, O. G., Pruunsild, K., Vaitkeviciene, G., Vettenranta, K., Lund, B., Abrahamsson, J., Schmiegelow, K., and Marquart, H. V.

Published

2019

3. Prospective study of thromboembolism in 1038 children with acute lymphoblastic leukemia: a Nordic Society of Pediatric Hematology and Oncology (NOPHO) study

Author

Tuckuviene, R., Ranta, S., Albertsen, B.K., Andersson, N.G., Bendtsen, M.D., Frisk, T., Gunnes, M.W., Helgestad, J., Heyman, M.M., Jonsson, O.G., Mäkipernaa, A., Pruunsild, K., Tedgård, U., Trakymiene, S.S., and Ruud, E.

Published

2016

4. Correction: Minimal residual disease quantification by flow cytometry provides reliable risk stratification in T-cell acute lymphoblastic leukemia

Author

Modvig, S., Madsen, H. O., Siitonen, S. M., Rosthøj, S., Tierens, A., Juvonen, V., Osnes, L. T. N., Vålerhaugen, H., Hultdin, M., Thörn, I., Matuzeviciene, R., Stoskus, M., Marincevic, M., Fogelstrand, L., Lilleorg, A., Toft, N., Jónsson, O. G., Pruunsild, K., Vaitkeviciene, G., Vettenranta, K., Lund, B., Abrahamsson, J., Schmiegelow, K., and Marquart, H. V.

Published

2020

5. Value of flow cytometry for MRD-based relapse prediction in B-cell precursor ALL in a multicenter setting

Author

Modvig, S, Hallböök, H, Madsen, H.O., Siitonen, S, Rosthøj, S, Tierens, A, Juvonen, V, Osnes, L T N, Vålerhaugen, H, Hultdin, M, Matuzeviciene, R, Stoskus, M, Marincevic, M, Lilleorg, A, Ehinger, M, Norén-Nystrøm, U, Toft, N., Taskinen, M, Jónsson, O G, Pruunsild, K, Vaitkeviciene, G, Vettenranta, K, Lund, B., Abrahamsson, J, Porwit, A, Schmiegelow, K., Marquart, H. V., Modvig, S, Hallböök, H, Madsen, H.O., Siitonen, S, Rosthøj, S, Tierens, A, Juvonen, V, Osnes, L T N, Vålerhaugen, H, Hultdin, M, Matuzeviciene, R, Stoskus, M, Marincevic, M, Lilleorg, A, Ehinger, M, Norén-Nystrøm, U, Toft, N., Taskinen, M, Jónsson, O G, Pruunsild, K, Vaitkeviciene, G, Vettenranta, K, Lund, B., Abrahamsson, J, Porwit, A, Schmiegelow, K., and Marquart, H. V.

Abstract

PCR of TCR/Ig gene rearrangements is considered the method of choice for minimal residual disease (MRD) quantification in BCP-ALL, but flow cytometry analysis of leukemia-associated immunophenotypes (FCM-MRD) is faster and biologically more informative. FCM-MRD performed in 18 laboratories across seven countries was used for risk stratification of 1487 patients with BCP-ALL enrolled in the NOPHO ALL2008 protocol. When no informative FCM-marker was available, risk stratification was based on real-time quantitative PCR. An informative FCM-marker was found in 96.2% and only two patients (0.14%) had non-informative FCM and non-informative PCR-markers. The overall 5-year event-free survival was 86.1% with a cumulative incidence of relapse (CIR5y) of 9.5%. FCM-MRD levels on days 15 (HzR 4.0, p < 0.0001), 29 (HzR 2.7, p < 0.0001), and 79 (HzR 3.5, p < 0.0001) associated with hazard of relapse adjusted for age, cytogenetics, and WBC. The early (day 15) response associated with CIR5y adjusted for day 29 FCM-MRD, with higher levels in adults (median 2.4 × 10-2 versus 5.2 × 10-3, p < 0.0001). Undetectable FCM- and/or PCR-MRD on day 29 identified patients with a very good outcome (CIR5y = 3.2%). For patients who did not undergo transplantation, day 79 FCM-MRD > 10-4 associated with a CIR5y = 22.1%. In conclusion, FCM-MRD performed in a multicenter setting is a clinically useful method for MRD-based treatment stratification in BCP-ALL.

Published

2021

6. Value of flow cytometry for MRD-based relapse prediction in B-cell precursor ALL in a multicenter setting

Author

Modvig, S., Hallböök, H., Madsen, H. O., Siitonen, S., Rosthøj, S., Tierens, A., Juvonen, V., Osnes, L. T. N., Vålerhaugen, H., Hultdin, Magnus, Matuzeviciene, R., Stoskus, M., Marincevic, M., Lilleorg, A., Ehinger, M., Norén-Nyström, Ulrika, Toft, N., Taskinen, M., Jónsson, O. G., Pruunsild, K., Vaitkeviciene, G., Vettenranta, K., Lund, B., Abrahamsson, J., Porwit, A., Schmiegelow, K., Marquart, H. V., Modvig, S., Hallböök, H., Madsen, H. O., Siitonen, S., Rosthøj, S., Tierens, A., Juvonen, V., Osnes, L. T. N., Vålerhaugen, H., Hultdin, Magnus, Matuzeviciene, R., Stoskus, M., Marincevic, M., Lilleorg, A., Ehinger, M., Norén-Nyström, Ulrika, Toft, N., Taskinen, M., Jónsson, O. G., Pruunsild, K., Vaitkeviciene, G., Vettenranta, K., Lund, B., Abrahamsson, J., Porwit, A., Schmiegelow, K., and Marquart, H. V.

Abstract

PCR of TCR/Ig gene rearrangements is considered the method of choice for minimal residual disease (MRD) quantification in BCP-ALL, but flow cytometry analysis of leukemia-associated immunophenotypes (FCM-MRD) is faster and biologically more informative. FCM-MRD performed in 18 laboratories across seven countries was used for risk stratification of 1487 patients with BCP-ALL enrolled in the NOPHO ALL2008 protocol. When no informative FCM-marker was available, risk stratification was based on real-time quantitative PCR. An informative FCM-marker was found in 96.2% and only two patients (0.14%) had non-informative FCM and non-informative PCR-markers. The overall 5-year event-free survival was 86.1% with a cumulative incidence of relapse (CIR5y) of 9.5%. FCM-MRD levels on days 15 (HzR 4.0, p < 0.0001), 29 (HzR 2.7, p < 0.0001), and 79 (HzR 3.5, p < 0.0001) associated with hazard of relapse adjusted for age, cytogenetics, and WBC. The early (day 15) response associated with CIR5y adjusted for day 29 FCM-MRD, with higher levels in adults (median 2.4 x 10(-2) versus 5.2 x 10(-3), p < 0.0001). Undetectable FCM- and/or PCR-MRD on day 29 identified patients with a very good outcome (CIR5y = 3.2%). For patients who did not undergo transplantation, day 79 FCM-MRD > 10(-4) associated with a CIR5y = 22.1%. In conclusion, FCM-MRD performed in a multicenter setting is a clinically useful method for MRD-based treatment stratification in BCP-ALL.

Published

2020

7. Value of flow cytometry for MRD-based relapse prediction in B-cell precursor ALL in a multicenter setting

Author

Modvig, S., primary, Hallböök, H., additional, Madsen, H. O., additional, Siitonen, S., additional, Rosthøj, S., additional, Tierens, A., additional, Juvonen, V., additional, Osnes, L. T. N., additional, Vålerhaugen, H., additional, Hultdin, M., additional, Matuzeviciene, R., additional, Stoskus, M., additional, Marincevic, M., additional, Lilleorg, A., additional, Ehinger, M., additional, Norén-Nystrøm, U., additional, Toft, N., additional, Taskinen, M., additional, Jónsson, O. G., additional, Pruunsild, K., additional, Vaitkeviciene, G., additional, Vettenranta, K., additional, Lund, B., additional, Abrahamsson, J., additional, Porwit, A., additional, Schmiegelow, K., additional, and Marquart, H. V., additional

Published

2020

8. Correction: Minimal residual disease quantification by flow cytometry provides reliable risk stratification in T-cell acute lymphoblastic leukemia

Author

Modvig, S., primary, Madsen, H. O., additional, Siitonen, S. M., additional, Rosthøj, S., additional, Tierens, A., additional, Juvonen, V., additional, Osnes, L. T. N., additional, Vålerhaugen, H., additional, Hultdin, M., additional, Thörn, I., additional, Matuzeviciene, R., additional, Stoskus, M., additional, Marincevic, M., additional, Fogelstrand, L., additional, Lilleorg, A., additional, Toft, N., additional, Jónsson, O. G., additional, Pruunsild, K., additional, Vaitkeviciene, G., additional, Vettenranta, K., additional, Lund, B., additional, Abrahamsson, J., additional, Schmiegelow, K., additional, and Marquart, H. V., additional

Published

2019

9. Diagnostics and treatment of diffuse intrinsic pontine glioma: where do we stand?

Author

El-Khouly, F.E. Veldhuijzen van Zanten, S.E.M. Santa-Maria Lopez, V. Hendrikse, N.H. Kaspers, G.J.L. Loizos, G. Sumerauer, D. Nysom, K. Pruunsild, K. Pentikainen, V. Thorarinsdottir, H.K. Rutkauskiene, G. Calvagna, V. Drogosiewicz, M. Dragomir, M. Deak, L. Kitanovski, L. von Bueren, A.O. Kebudi, R. Slavc, I. Jacobs, S. Jadrijevic-Cvrlje, F. Entz-Werle, N. Grill, J. Kattamis, A. Hauser, P. Pears, J. Biassoni, V. Massimino, M. Lopez Aguilar, E. Torsvik, I.K. Joao Gil-da-Costa, M. Kumirova, E. Cruz-Martinez, O. Holm, S. Bailey, S. Hayden, T. Thomale, U.W. Janssens, G.O.R. Kramm, C.M. van Vuurden, D.G.

Abstract

Introduction: Diffuse intrinsic pontine glioma (DIPG) is a rare clinically, neuro-radiologically, and molecularly defined malignancy of the brainstem with a median overall survival of approximately 11 months. Our aim is to evaluate the current tendency for its treatment in Europe in order to develop (inter)national consensus guidelines. Methods: Healthcare professionals specialized in DIPG were asked to fill in an online survey with questions regarding usual treatment strategies at diagnosis and at disease progression in their countries and/or their centers, respectively. Results: Seventy-four healthcare professionals responded to the survey, of which 87.8% were pediatric oncologists. Only 13.5% of the respondents biopsy all of their patients, 41.9% biopsy their patients infrequently. More than half of the respondents (54.1%) treated their patients with radiotherapy only at diagnosis, whereas 44.6% preferred radiotherapy combined with chemotherapy. When the disease progresses, treatment strategies became even more diverse, and the tendency for no treatment increased from 1.4% at diagnosis to 77.0% after second progression. 36.5% of the healthcare professionals treat children younger than 3 years differently than older children at diagnosis. This percentage decreased, when the disease progresses. Most of the participants (51.4%) included less than 25% of their patients in clinical trials. Conclusion: This survey demonstrates a large heterogeneity of treatment regimens, especially at disease progression. We emphasize the need for international consensus guidelines for the treatment of DIPG, possible by more collaborative clinical trials. © 2019, The Author(s).

Published

2019

10. Minimal residual disease quantification by flow cytometry provides reliable risk stratification in T-cell acute lymphoblastic leukemia

Author

Modvig, S, Madsen, H O, Siitonen, S M, Rosthøj, S, Tierens, A, Juvonen, V, Osnes, L T N, Vålerhaugen, H, Hultdin, M, Thörn, Ingrid, Matuzeviciene, R, Stoskus, M, Marincevic, Millaray, Fogelstrand, L, Lilleorg, A, Toft, N, Jónsson, O G, Pruunsild, K, Vaitkeviciene, G, Vettenranta, K, Lund, B, Abrahamsson, J, Schmiegelow, K, Marquart, H V, Modvig, S, Madsen, H O, Siitonen, S M, Rosthøj, S, Tierens, A, Juvonen, V, Osnes, L T N, Vålerhaugen, H, Hultdin, M, Thörn, Ingrid, Matuzeviciene, R, Stoskus, M, Marincevic, Millaray, Fogelstrand, L, Lilleorg, A, Toft, N, Jónsson, O G, Pruunsild, K, Vaitkeviciene, G, Vettenranta, K, Lund, B, Abrahamsson, J, Schmiegelow, K, and Marquart, H V

Abstract

Minimal residual disease (MRD) measured by PCR of clonal IgH/TCR rearrangements predicts relapse in T-cell acute lymphoblastic leukemia (T-ALL) and serves as risk stratification tool. Since 10% of patients have no suitable PCR-marker, we evaluated flowcytometry (FCM)-based MRD for risk stratification. We included 274 T-ALL patients treated in the NOPHO-ALL2008 protocol. MRD was measured by six-color FCM and real-time quantitative PCR. Day 29 PCR-MRD (cut-off 10-3) was used for risk stratification. At diagnosis, 93% had an FCM-marker for MRD monitoring, 84% a PCR-marker, and 99.3% (272/274) had a marker when combining the two. Adjusted for age and WBC, the hazard ratio for relapse was 3.55 (95% CI 1.4-9.0, p = 0.008) for day 29 FCM-MRD ≥ 10-3 and 5.6 (95% CI 2.0-16, p = 0.001) for PCR-MRD ≥ 10-3 compared with MRD < 10-3. Patients stratified to intermediate-risk therapy on day 29 with MRD 10-4-<10-3 had a 5-year event-free survival similar to intermediate-risk patients with MRD < 10-4 or undetectable, regardless of method for monitoring. Patients with day 15 FCM-MRD < 10-4 had a cumulative incidence of relapse of 2.3% (95% CI 0-6.8, n = 59). Thus, FCM-MRD allows early identification of patients eligible for reduced intensity therapy, but this needs further studies. In conclusion, FCM-MRD provides reliable risk prediction for T-ALL and can be used for stratification when no PCR-marker is available.

Published

2019

11. Minimal residual disease quantification by flow cytometry provides reliable risk stratification in T-cell acute lymphoblastic leukemia

Author

Modvig, S., primary, Madsen, H. O., additional, Siitonen, S. M., additional, Rosthøj, S., additional, Tierens, A., additional, Juvonen, V., additional, Osnes, L.T.N., additional, Vålerhaugen, H., additional, Hultdin, M., additional, Thörn, I., additional, Matuzeviciene, R., additional, Stoskus, M., additional, Marincevic, M., additional, Fogelstrand, L., additional, Lilleorg, A., additional, Toft, N., additional, Jónsson, O. G., additional, Pruunsild, K., additional, Vaitkeviciene, G., additional, Vettenranta, K., additional, Lund, B., additional, Abrahamsson, J., additional, Schmiegelow, K., additional, and Marquart, H. V., additional

Published

2018

12. Results of NOPHO ALL2008 treatment for patients aged 1-45 years with acute lymphoblastic leukemia.

Author

Toft, N, Birgens, H, Abrahamsson, J, Griškevičius, L, Hallböök, Helene, Heyman, M, Klausen, T W, Jónsson, Ó G, Palk, K, Pruunsild, K, Quist-Paulsen, P, Vaitkeviciene, G, Vettenranta, K, Åsberg, A, Frandsen, T L, Marquart, H V, Madsen, H O, Norén-Nyström, U, Schmiegelow, K, Toft, N, Birgens, H, Abrahamsson, J, Griškevičius, L, Hallböök, Helene, Heyman, M, Klausen, T W, Jónsson, Ó G, Palk, K, Pruunsild, K, Quist-Paulsen, P, Vaitkeviciene, G, Vettenranta, K, Åsberg, A, Frandsen, T L, Marquart, H V, Madsen, H O, Norén-Nyström, U, and Schmiegelow, K

Abstract

Adults with acute lymphoblastic leukemia (ALL) do worse than children. From 7/2008 to 12/2014, Nordic and Baltic centers treated 1509 consecutive patients aged 1-45 years with Philadelphia chromosome-negative ALL according to the NOPHO ALL2008 without cranial irradiation. Overall, 1022 patients were of age 1-9 years (A), 266 were 10-17 years (B) and 221 were 18-45 years (C). Sixteen patients (three adults) died during induction. All others achieved remission after induction or 1-3 intensive blocks. Subsequently, 45 patients (12 adults) died, 122 patients relapsed (32 adults) with a median time to relapse of 1.6 years and 13 (no adult) developed a second malignancy. Median follow-up time was 4.6 years. Among the three age groups, older patients more often had higher risk ALL due to T-ALL (32%/25%/9%, P<0.001), KMT2A rearrangements (6%/5%/3%, P<0.001) and higher day 29 residual leukemia for B-lineage (P<0.001), but not T-ALL (P = 0.53). Event-free survival rates (pEFS(5y)) were 89 +/- 1% (A), 80 +/- 3% (B) and 74 +/- 4% (C) with significant differences only for non-high risk groups. Except for thrombosis, pancreatitis and osteonecrosis, the risk of 19 specified toxicities was not enhanced by age above 10 years. In conclusion, a pediatric-based protocol is tolerable and effective for young adults, despite their increased frequency of higher risk features.

Published

2018

13. Results of NOPHO ALL2008 treatment for patients aged 1–45 years with acute lymphoblastic leukemia

Author

Toft, N, primary, Birgens, H, additional, Abrahamsson, J, additional, Griškevičius, L, additional, Hallböök, H, additional, Heyman, M, additional, Klausen, T W, additional, Jónsson, ÓG, additional, Palk, K, additional, Pruunsild, K, additional, Quist-Paulsen, P, additional, Vaitkeviciene, G, additional, Vettenranta, K, additional, Åsberg, A, additional, Frandsen, T L, additional, Marquart, H V, additional, Madsen, H O, additional, Norén-Nyström, U, additional, and Schmiegelow, K, additional

Published

2017

14. ADULTS AND CHILDREN (1-45 YEARS) WITH PH-NEGATIVE ALL HAVE ALMOST IDENTICAL OUTCOME IN RISK-STRATIFIED ANALYSIS OF NOPHO ALL2008

Author

Toft, N., Birgens, H., Abrahamsson, J., Griskevicius, L., Hallbook, H., Heyman, M., Klausen, T. W., Jonsson, O. G., Palk, K., Pruunsild, K., Quist-Paulsen, P., Vaitkeviciene, G., Vettenranta, K., Asberg, A., Frandsen, T. Leth, Marquart, H. V., Madsen, H. O., Norén-Nyström, Ulrika, Schmiegelow, K., Toft, N., Birgens, H., Abrahamsson, J., Griskevicius, L., Hallbook, H., Heyman, M., Klausen, T. W., Jonsson, O. G., Palk, K., Pruunsild, K., Quist-Paulsen, P., Vaitkeviciene, G., Vettenranta, K., Asberg, A., Frandsen, T. Leth, Marquart, H. V., Madsen, H. O., Norén-Nyström, Ulrika, and Schmiegelow, K.

Published

2016

15. P.466 Genetic characterization of hepatitis C virus strains from Estonia

Author

Tallo, T., primary, Norder, H., additional, Tefanova, V., additional, Krispin, T., additional, Schmidt, J., additional, Ilmoja, M., additional, Orgulas, K., additional, Pruunsild, K., additional, Priimägi, L., additional, and Magnius, L.O., additional

Published

2006

16. ADULTS AND CHILDREN (1-45 YEARS) WITH PH-NEGATIVE ALL HAVE ALMOST IDENTICAL OUTCOME IN RISK-STRATIFIED ANALYSIS OF NOPHO ALL2008

Author

Toft, N., Birgens, H., Abrahamsson, J., Griskevicius, L., Hallbook, H., Heyman, M., Klausen, T. W., Jonsson, O. G., Palk, K., Pruunsild, K., Quist-Paulsen, P., Vaitkeviciene, G., Vettenranta, K., Asberg, A., Thomas Frandsen, Marquart, H. V., Madsen, H. O., Noren-Nystrom, U., and Schmiegelow, K.

17. No association between relapse hazard and thiopurine methyltransferase geno- or phenotypes in non-high risk acute lymphoblastic leukemia: a NOPHO ALL2008 sub-study.

Author

Nielsen SN, Toksvang LN, Grell K, Nersting J, Abrahamsson J, Lund B, Kanerva J, Jónsson ÓG, Vaitkeviciene G, Pruunsild K, Appell ML, Hjalgrim LL, and Schmiegelow K

Subjects

Adolescent, Antimetabolites, Antineoplastic therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Child, Child, Preschool, DNA genetics, Female, Genotype, Humans, Infant, Male, Mercaptopurine therapeutic use, Methotrexate therapeutic use, Phenotype, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Recurrence, Methyltransferases genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics

Abstract

Purpose: 6-mercaptopurine(6MP)/methotrexate maintenance therapy is essential to reduce relapse of childhood acute lymphoblastic leukemia (ALL). Common germline variants in TPMT cause low activity of thiopurine methyltransferase (TPMT) and higher 6MP metabolite (TGN) levels. Higher levels of TGNs incorporated into DNA (DNA-TG) and low TPMT activity have previously been associated with a lower relapse risk. We explored if TPMT geno- or phenotype was associated with DNA-TG levels and relapse rate in NOPHO ALL2008., Methods: TPMT genotype, repeated phenotyping, and DNA-TG measurements were collected in 918 children with non-high risk ALL (NOPHO ALL2008 maintenance therapy study). Maintenance therapy started with 6MP at 50 and 75 mg/m 2 for TPMT heterozygous and wildtype patients and was adjusted to a target WBC of 1.5 - 3.0 × 10 9 /L., Results: Of 918 patients, 78 (8.5%) were TPMT heterozygous and 903 had at least one TPMT measurement (total 3063). Mean TPMT activities were higher with wildtype than heterozygous TPMT (N = 752, 16.6 versus 9.6 U/mL ery., p < 0.001). The 5-year cumulative incidence of relapse was 6.4% and 6.0% for TPMT heterozygous and wildtype patients, and there was no association between genotype and relapse rate (N = 918, hazard ratio = 1.01, 95% confidence interval [CI] 0.40 - 2.54, p = 0.98). Although TPMT heterozygous patients had higher DNA-TG (N = 548, median 760.9 [interquartile range (IQR) 568.7 - 890.3] versus 492.7 [IQR 382.1 - 634.6] fmol/µg, p < 0.001), TPMT activity was not associated with relapse rate (N = 813; hazard ratio = 0.98 per one U/mL ery. increase in TPMT activity, 95% CI 0.91 - 1.06, p = 0.67)., Conclusion: TPMT geno- and phenotype were not associated with relapse in non-high risk NOPHO ALL2008.

Published

2021

18. Effects of germline DHFR and FPGS variants on methotrexate metabolism and relapse of leukemia.

Author

Tulstrup M, Moriyama T, Jiang C, Grosjean M, Nersting J, Abrahamsson J, Grell K, Hjalgrim LL, Jónsson ÓG, Kanerva J, Lund B, Nielsen SN, Nielsen RL, Overgaard U, Quist-Paulsen P, Pruunsild K, Vaitkeviciene G, Wolthers BO, Zhang H, Gupta R, Yang JJ, and Schmiegelow K

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Genome-Wide Association Study, Humans, Infant, Infant, Newborn, Male, Methotrexate administration & dosage, Methotrexate metabolism, Middle Aged, Neoplasm Recurrence, Local drug therapy, Neoplasm Recurrence, Local genetics, Neoplasm Recurrence, Local metabolism, Polyglutamic Acid administration & dosage, Polyglutamic Acid metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Prognosis, Young Adult, Methotrexate analogs & derivatives, Neoplasm Recurrence, Local pathology, Peptide Synthases genetics, Polyglutamic Acid analogs & derivatives, Polymorphism, Single Nucleotide, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology, Tetrahydrofolate Dehydrogenase genetics

Abstract

Methotrexate (MTX) during maintenance therapy is essential for curing acute lymphoblastic leukemia (ALL), but dosing strategies aiming at adequate treatment intensity are challenged by interindividual differences in drug disposition. To evaluate genetic factors associated with MTX metabolism, we performed a genome-wide association study in 447 ALL cases from the Nordic Society for Pediatric Haematology and Oncology ALL2008 study, validating results in an independent set of 196 patients. The intergenic single-nucleotide polymorphism rs1382539, located in a regulatory element of DHFR, was associated with increased levels of short-chain MTX polyglutamates (P = 1.1 × 10-8) related to suppression of enhancer activity, whereas rs35789560 in FPGS (p.R466C, P = 5.6 × 10-9) was associated with decreased levels of long-chain MTX polyglutamates through reduced catalytic activity. Furthermore, the FPGS variant was linked with increased relapse risk (P = .044). These findings show a genetic basis for interpatient variability in MTX response and could be used to improve future dosing algorithms., (© 2020 by The American Society of Hematology.)

Published

2020

19. Diagnostics and treatment of diffuse intrinsic pontine glioma: where do we stand?

Author

El-Khouly FE, Veldhuijzen van Zanten SEM, Santa-Maria Lopez V, Hendrikse NH, Kaspers GJL, Loizos G, Sumerauer D, Nysom K, Pruunsild K, Pentikainen V, Thorarinsdottir HK, Rutkauskiene G, Calvagna V, Drogosiewicz M, Dragomir M, Deak L, Kitanovski L, von Bueren AO, Kebudi R, Slavc I, Jacobs S, Jadrijevic-Cvrlje F, Entz-Werle N, Grill J, Kattamis A, Hauser P, Pears J, Biassoni V, Massimino M, Lopez Aguilar E, Torsvik IK, Joao Gil-da-Costa M, Kumirova E, Cruz-Martinez O, Holm S, Bailey S, Hayden T, Thomale UW, Janssens GOR, Kramm CM, and van Vuurden DG

Subjects

Biopsy, Combined Modality Therapy, Disease Progression, Humans, Prognosis, Brain Stem Neoplasms diagnosis, Brain Stem Neoplasms therapy, Diffuse Intrinsic Pontine Glioma diagnosis, Diffuse Intrinsic Pontine Glioma therapy

Abstract

Introduction: Diffuse intrinsic pontine glioma (DIPG) is a rare clinically, neuro-radiologically, and molecularly defined malignancy of the brainstem with a median overall survival of approximately 11 months. Our aim is to evaluate the current tendency for its treatment in Europe in order to develop (inter)national consensus guidelines., Methods: Healthcare professionals specialized in DIPG were asked to fill in an online survey with questions regarding usual treatment strategies at diagnosis and at disease progression in their countries and/or their centers, respectively., Results: Seventy-four healthcare professionals responded to the survey, of which 87.8% were pediatric oncologists. Only 13.5% of the respondents biopsy all of their patients, 41.9% biopsy their patients infrequently. More than half of the respondents (54.1%) treated their patients with radiotherapy only at diagnosis, whereas 44.6% preferred radiotherapy combined with chemotherapy. When the disease progresses, treatment strategies became even more diverse, and the tendency for no treatment increased from 1.4% at diagnosis to 77.0% after second progression. 36.5% of the healthcare professionals treat children younger than 3 years differently than older children at diagnosis. This percentage decreased, when the disease progresses. Most of the participants (51.4%) included less than 25% of their patients in clinical trials., Conclusion: This survey demonstrates a large heterogeneity of treatment regimens, especially at disease progression. We emphasize the need for international consensus guidelines for the treatment of DIPG, possible by more collaborative clinical trials.

Published

2019

20. Genetic predisposition to PEG-asparaginase hypersensitivity in children treated according to NOPHO ALL2008.

Author

Højfeldt SG, Wolthers BO, Tulstrup M, Abrahamsson J, Gupta R, Harila-Saari A, Heyman M, Henriksen LT, Jónsson ÒG, Lähteenmäki PM, Lund B, Pruunsild K, Vaitkeviciene G, Schmiegelow K, and Albertsen BK

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 3 genetics, Adolescent, Asparaginase administration & dosage, Child, Child, Preschool, Chromosomes, Human, Pair 19 genetics, Chromosomes, Human, Pair 6 genetics, Female, Genome-Wide Association Study, HLA-DQ Antigens genetics, Humans, Infant, Male, Polyethylene Glycols administration & dosage, Transcription Factors genetics, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Drug Hypersensitivity genetics, Genetic Predisposition to Disease, Genetic Variation, Neoplasm Proteins genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology

Abstract

Asparaginase is essential in childhood acute lymphoblastic leukaemia (ALL) treatment, however hypersensitivity reactions to pegylated asparaginase (PEG-asparaginase) hampers anti-neoplastic efficacy. Patients with PEG-asparaginase hypersensitivity have been shown to possess zero asparaginase enzyme activity. Using this measurement to define the phenotype, we investigated genetic predisposition to PEG-asparaginase hypersensitivity in a genome-wide association study (GWAS). From July 2008 to March 2016, 1494 children were treated on the Nordic Society of Paediatric Haematology and Oncology ALL2008 protocol. Cases were defined by clinical hypersensitivity and no enzyme activity, controls had enzyme activity ≥ 100 iu/l and no hypersensitivity symptoms. PEG-asparaginase hypersensitivity was reported in 13·8% (206/1494) of patients. Fifty-nine cases and 772 controls fulfilled GWAS inclusion criteria. The CNOT3 variant rs73062673 on 19q13.42, was associated with PEG-asparaginase allergy (P = 4·68 × 10 -8 ). We further identified two signals on chromosome 6 in relation to HLA-DQA1 (P = 9·37 × 10 -6 ) and TAP2 (P = 1·59 × 10 -5 ). This study associated variants in CNOT3 and in the human leucocyte antigen (HLA) region with PEG-asparaginase hypersensitivity, suggesting that not only genetic variations in the HLA region, but also regulation of these genes are of importance in the biology of this toxicity. Furthermore, our study emphasizes the importance of using asparaginase enzyme activity measurements to identify PEG-asparaginase hypersensitivity., (© 2018 British Society for Haematology and John Wiley & Sons Ltd.)

Published

2019

21. Methotrexate polyglutamate levels and co-distributions in childhood acute lymphoblastic leukemia maintenance therapy.

Author

Nersting J, Nielsen SN, Grell K, Paerregaard M, Abrahamsson J, Lund B, Jonsson OG, Pruunsild K, Vaitkeviciene G, Kanerva J, and Schmiegelow K

Subjects

Adolescent, Antimetabolites, Antineoplastic administration & dosage, Child, Child, Preschool, Female, Follow-Up Studies, Humans, Infant, Male, Methotrexate administration & dosage, Polyglutamic Acid metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology, Prognosis, Antimetabolites, Antineoplastic metabolism, Erythrocytes metabolism, Methotrexate analogs & derivatives, Methotrexate metabolism, Polyglutamic Acid analogs & derivatives, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism

Abstract

Purpose: Methotrexate polyglutamates (MTXpg) facilitate incorporation of thioguanine nucleotides into DNA (DNA-TG, the primary cytotoxic thiopurine metabolite and outcome determinant in MTX/6-mercaptopurine treatment of childhood ALL). We hypothesized that mapping erythrocyte levels of MTXpg with 1-6 glutamates and their associations with DNA-TG formation would facilitate future guidelines for maintenance therapy dosing., Methods and Results: Summed MTX with 1-6 glutamates resolved by LCMS [median (interquartile): 5.47 (3.58-7.69) nmol/mmol hemoglobin] was in agreement with total MTX by radio ligand assay. In 16,389 blood samples from 1426 ALL maintenance therapy patients, MTXpg3 21.0 (15.2-27.4)% was the predominant metabolite, and MTXpg1 (the maternal drug) constituted 38.6 (27.2-50.2)% of MTXpg1-6. All subsets correlated; the strongest associations were between metabolites with similar polyglutamate lengths. Correlations of MTXpg1 with MTXpg2 and MTXpg3,4,5,6 were r s  = 0.68 and r s  = 0.25-0.42, respectively. Intercorrelations of MTXpg3,4,5,6 were all r s  ≥ 0.51. MTXpg4 accounted for 29.8 (24.7-33.3)% of MTXpg3-6, yet explained 96% of the summed MTXpg3-6 variation. MTXpg1-4, MTXpg1-6, MTXpg2-6 and MTXpg3 were all associated with DNA-TG levels (p < 0.00001), but collinearity precluded identification of the most informative subset., Conclusions: Measuring erythrocyte MTXpg4 simplifies and can replace longer chain MTXpg monitoring. Resolving individual MTXpg identifies samples that are unsuitable for dose guidance due to high levels of MTXpg1 remaining in the plasma fraction because of recent MTX intake. All tested MTXpg subsets correlated with DNA-TG and may be used for ALL maintenance therapy dose adjustments, but the most informative subset remains to be identified.

Published

2019

22. NT5C2 germline variants alter thiopurine metabolism and are associated with acquired NT5C2 relapse mutations in childhood acute lymphoblastic leukaemia.

Author

Tulstrup M, Grosjean M, Nielsen SN, Grell K, Wolthers BO, Wegener PS, Jonsson OG, Lund B, Harila-Saari A, Abrahamsson J, Vaitkeviciene G, Pruunsild K, Toft N, Holm M, Hulegårdh E, Liestøl S, Griskevicius L, Punab M, Wang J, Carroll WL, Zhang Z, Dalgaard MD, Gupta R, Nersting J, and Schmiegelow K

Subjects

Adolescent, Antimetabolites, Antineoplastic therapeutic use, Child, Child, Preschool, DNA metabolism, Female, Gene Frequency drug effects, Gene Frequency genetics, Genome-Wide Association Study methods, Genotype, Humans, Infant, Male, Mercaptopurine therapeutic use, Neoplasm Recurrence, Local genetics, Neoplasm Recurrence, Local metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Recurrence, Thioguanine metabolism, 5'-Nucleotidase genetics, Germ Cells metabolism, Polymorphism, Single Nucleotide genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism

Abstract

The antileukaemic drug 6-mercaptopurine is converted into thioguanine nucleotides (TGN) and incorporated into DNA (DNA-TG), the active end metabolite. In a series of genome-wide association studies, we analysed time-weighted means ( wm ) of erythrocyte concentrations of TGN (Ery-TGN) and DNA-TG in 1009 patients undergoing maintenance therapy for acute lymphoblastic leukaemia (ALL). In discovery analyses (454 patients), the propensity for DNA-TG incorporation ( wm DNA-TG/ wm Ery-TGN ratio) was significantly associated with three intronic SNPs in NT5C2 (top hit: rs72846714; P = 2.09 × 10 -10 , minor allele frequency 15%). In validation analyses (555 patients), this association remained significant during both early and late maintenance therapy (P = 8.4 × 10 -6 and 1.3 × 10 -3 , respectively). The association was mostly driven by differences in wm Ery-TGN, but in regression analyses adjusted for wm Ery-TGN (P < 0.0001), rs72846714-A genotype was also associated with a higher wm DNA-TG (P = 0.029). Targeted sequencing of NT5C2 did not identify any missense variants associated with rs72846714 or wm Ery-TGN/ wm DNA-TG. rs72846714 was not associated with relapse risk, but in a separate cohort of 180 children with relapsed ALL, rs72846714-A genotype was associated with increased occurrence of relapse-specific NT5C2 gain-of-function mutations that reduce cytosol TGN levels (P = 0.03). These observations highlight the impact of both germline and acquired mutations in drug metabolism and disease trajectory.

Published

2018

23. Results of NOPHO ALL2008 treatment for patients aged 1-45 years with acute lymphoblastic leukemia.

Author

Toft N, Birgens H, Abrahamsson J, Griškevičius L, Hallböök H, Heyman M, Klausen TW, Jónsson ÓG, Palk K, Pruunsild K, Quist-Paulsen P, Vaitkeviciene G, Vettenranta K, Åsberg A, Frandsen TL, Marquart HV, Madsen HO, Norén-Nyström U, and Schmiegelow K

Subjects

Adolescent, Adult, Antineoplastic Combined Chemotherapy Protocols adverse effects, Biomarkers, Tumor genetics, Child, Child, Preschool, Combined Modality Therapy, Female, Hematopoietic Stem Cell Transplantation, Humans, Infant, Male, Middle Aged, Mutation, Precursor Cell Lymphoblastic Leukemia-Lymphoma diagnosis, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Remission Induction, Treatment Outcome, Young Adult, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy

Abstract

Adults with acute lymphoblastic leukemia (ALL) do worse than children. From 7/2008 to 12/2014, Nordic and Baltic centers treated 1509 consecutive patients aged 1-45 years with Philadelphia chromosome-negative ALL according to the NOPHO ALL2008 without cranial irradiation. Overall, 1022 patients were of age 1-9 years (A), 266 were 10-17 years (B) and 221 were 18-45 years (C). Sixteen patients (three adults) died during induction. All others achieved remission after induction or 1-3 intensive blocks. Subsequently, 45 patients (12 adults) died, 122 patients relapsed (32 adults) with a median time to relapse of 1.6 years and 13 (no adult) developed a second malignancy. Median follow-up time was 4.6 years. Among the three age groups, older patients more often had higher risk ALL due to T-ALL (32%/25%/9%, P<0.001), KMT2A rearrangements (6%/5%/3%, P<0.001) and higher day 29 residual leukemia for B-lineage (P<0.001), but not T-ALL (P=0.53). Event-free survival rates (pEFS 5y ) were 89±1% (A), 80±3% (B) and 74±4% (C) with significant differences only for non-high risk groups. Except for thrombosis, pancreatitis and osteonecrosis, the risk of 19 specified toxicities was not enhanced by age above 10 years. In conclusion, a pediatric-based protocol is tolerable and effective for young adults, despite their increased frequency of higher risk features.

Published

2018

24. Children with low-risk acute lymphoblastic leukemia are at highest risk of second cancers.

Author

Nielsen SN, Eriksson F, Rosthoej S, Andersen MK, Forestier E, Hasle H, Hjalgrim LL, Aasberg A, Abrahamsson J, Heyman M, Jónsson ÓG, Pruunsild K, Vaitkeviciené GE, Vettenranta K, and Schmiegelow K

Subjects

Adolescent, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Antineoplastic Combined Chemotherapy Protocols adverse effects, Child, Chromosomes, Human, Pair 12 genetics, Chromosomes, Human, Pair 21 genetics, Female, Follow-Up Studies, Humans, Male, Methyltransferases genetics, Methyltransferases metabolism, Neoplasms, Second Primary blood, Neoplasms, Second Primary drug therapy, Neoplasms, Second Primary genetics, Ploidies, Precursor Cell Lymphoblastic Leukemia-Lymphoma blood, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Retrospective Studies, Risk Factors, Translocation, Genetic, Neoplasms, Second Primary epidemiology, Precursor Cell Lymphoblastic Leukemia-Lymphoma epidemiology

Abstract

Background: The improved survival rates for childhood acute lymphoblastic leukemia (ALL) may be jeopardized by the development of a second cancer, which has been associated with thiopurine therapy., Procedure: We retrospectively analyzed three sequential Nordic Society of Paediatric Haematology and Oncology's protocols characterized by increasing intensity of thiopurine-based maintenance therapy. We explored the risk of second cancer in relation to protocols, risk group, thiopurine methyltransferase (TPMT) activity, ALL high hyperdiploidy (HeH), and t(12;21)[ETV6/RUNX1]., Results: After median 9.5 years (interquartile range, 5.4-15.3 yrs) of follow-up, 40 of 3,591 patients had developed a second cancer, of whom 38 had non-high-risk B-cell precursor ALL. Patients with standard-risk ALL, who received the longest maintenance therapy, had the highest adjusted hazard of second cancer (hazard ratio [HR], intermediate vs. standard risk: 0.16, 95% CI: 0.06-0.43, P < 0.001; HR, high vs. standard risk: 0.09, 95% CI: 0.02-0.49, P = 0.006); no significant effects of protocol, age, or white blood cell count at diagnosis, ALL HeH, or t(12;21)[ETV6/RUNX1] were observed. A subset analysis on the patients with standard-risk ALL did not show an increased hazard of second cancer from either HeH or t(12;21) (adjusted HR 2.02, 95% CI: 0.69-5.96, P = 0.20). The effect of low TPMT low activity was explored in patients reaching maintenance therapy in clinical remission (n = 3,368); no association with second cancer was observed (adjusted HR 1.43, 95% CI: 0.54-3.76, P = 0.47)., Conclusions: The rate of second cancer was generally highest in patients with low-risk ALL, but we could not identify a subset at higher risk than others., (© 2017 Wiley Periodicals, Inc.)

Published

2017

25. DNA-thioguanine nucleotide concentration and relapse-free survival during maintenance therapy of childhood acute lymphoblastic leukaemia (NOPHO ALL2008): a prospective substudy of a phase 3 trial.

Author

Nielsen SN, Grell K, Nersting J, Abrahamsson J, Lund B, Kanerva J, Jónsson ÓG, Vaitkeviciene G, Pruunsild K, Hjalgrim LL, and Schmiegelow K

Subjects

Adolescent, Child, Child, Preschool, Female, Follow-Up Studies, Humans, Infant, Male, Mercaptopurine administration & dosage, Methotrexate administration & dosage, Methotrexate analogs & derivatives, Neoplasm Recurrence, Local blood, Neoplasm Recurrence, Local drug therapy, Neoplasm Staging, Polyglutamic Acid administration & dosage, Polyglutamic Acid analogs & derivatives, Precursor Cell Lymphoblastic Leukemia-Lymphoma blood, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Prognosis, Prospective Studies, Survival Rate, Thioguanine chemistry, Antineoplastic Combined Chemotherapy Protocols blood, Antineoplastic Combined Chemotherapy Protocols therapeutic use, DNA chemistry, Neoplasm Recurrence, Local mortality, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Thioguanine blood

Abstract

Background: Adjustment of mercaptopurine and methotrexate maintenance therapy of acute lymphoblastic leukaemia by leucocyte count is confounded by natural variations. Cytotoxicity is primarily mediated by DNA-incorporated thioguanine nucleotides (DNA-TGN). The aim of this study was to establish whether DNA-TGN concentrations in blood leucocytes during maintenance therapy are associated with relapse-free survival., Methods: In this substudy of the NOPHO ALL2008 phase 3 trial done in 23 hospitals in seven European countries (Denmark, Estonia, Finland, Iceland, Lithuania, Norway, and Sweden), we analysed data from centralised and blinded analyses of 6-mercaptopurine and methotrexate metabolites in blood samples from patients with non-high-risk childhood acute lymphoblastic leukaemia. Eligible patients were aged 1·0-17·9 years; had been diagnosed with non-high-risk precursor B-cell or T-cell leukaemia; had been treated according to the Nordic Society of Pediatric Hematology and Oncology ALL2008 protocol; and had reached maintenance therapy in first remission. Maintenance therapy was (mercaptopurine 75 mg/m 2 once per day and methotrexate 20 mg/m 2 once per week, targeted to a leucocyte count of 1·5-3·0 × 10 9 cells per L). We measured DNA-TGN and erythrocyte concentrations of TGN nucleotides, methylated mercaptopurine metabolites, and methotrexate polyglutamates. The primary objective was the association of DNA-TGN concentrations and 6-mercaptopurine and methotrexate metabolites with relapse-free survival. The secondary endpoint was the assessment of DNA-TGN concentration and 6-mercaptopurine and methotrexate metabolites during maintenance therapy phase 2., Findings: Between Nov 26, 2008 and June 14, 2016, 1509 patients from the NOPHO ALL2008 study were assessed for eligibility in the DNA-TGN substudy, of which 918 (89%) of 1026 eligible patients had at least one DNA-TGN measurement and were included in the analyses. Median follow-up was 4·6 years (IQR 3·1-6·1). Relapse-free survival was significantly associated with DNA-TGN concentration (adjusted hazard ratio 0·81 per 100 fmol/μg DNA increase, 95% CI 0·67-0·98; p=0·029). In patients with at least five blood samples, erythrocyte concentrations of TGN, methylated mercaptopurine metabolites, and methotrexate polyglutamates were associated with DNA-TGN concentration (all p<0·0001)., Interpretation: Our results suggest the need for intervention trials to identify clinically applicable strategies for individualised drug dosing to increase DNA-TGN concentration, and randomised studies to investigate whether such strategies improve cure rates compared with current dose adjustments based on white blood cell counts., Funding: Danish Cancer Society, Childhood Cancer Foundation (Denmark), Childhood Cancer Foundation (Sweden), Nordic Cancer Union, Otto Christensen Foundation, University Hospital Rigshospitalet, and Novo Nordic Foundation., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

26. Toxicity profile and treatment delays in NOPHO ALL2008-comparing adults and children with Philadelphia chromosome-negative acute lymphoblastic leukemia.

Author

Toft N, Birgens H, Abrahamsson J, Griškevičius L, Hallböök H, Heyman M, Klausen TW, Jónsson ÓG, Palk K, Pruunsild K, Quist-Paulsen P, Vaitkeviciene G, Vettenranta K, Asberg A, Helt LR, Frandsen T, and Schmiegelow K

Subjects

Adolescent, Adult, Antineoplastic Combined Chemotherapy Protocols toxicity, Child, Child, Preschool, Female, Humans, Infant, Male, Methotrexate administration & dosage, Methotrexate toxicity, Middle Aged, Osteonecrosis chemically induced, Osteonecrosis genetics, Osteonecrosis pathology, Philadelphia Chromosome, Precursor Cell Lymphoblastic Leukemia-Lymphoma diagnosis, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology, Prednisone administration & dosage, Prednisone toxicity, Prognosis, Remission Induction, Thrombosis chemically induced, Thrombosis genetics, Thrombosis pathology, Treatment Outcome, Vincristine administration & dosage, Vincristine toxicity, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Osteonecrosis diagnosis, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Thrombosis diagnosis

Abstract

Objectives: Cure rates improve when adolescents and young adults with acute lymphoblastic leukemia (ALL) are treated according to pediatric protocols. Assumed risks of toxicities and associated delays in treatment have played a role in setting upper age limits. The aim of this study was to examine the toxicity profile and treatment delays in NOPHO ALL2008 comparing children and adults., Methods: We collected information on 19 treatment-related toxicities, systematically captured at 3-month intervals throughout therapy, and time intervals between 12 consecutive treatment phases for 1076 patients aged 1-45 yrs treated according to the Nordic/Baltic ALL2008 protocol., Results: No adults died during induction. The duration of induction therapy and postinduction treatment phases did not differ between children and adults, except for patients 18-45 yrs being significantly delayed during two of nine high-risk blocks (median number of days for patients 1-9, 10-17, and 18-45 yrs; the glucocorticosteroid/antimetabolite-based block B1: 24, 26, and 29 d, respectively, P = 0.001, and Block 5 (in most cases also a B block): 29, 29, and 37 d, respectively, P = 0.02). A higher incidence of thrombosis with increasing age was found; highest odds ratio 5.4 (95% CI: (2.6;11.0)) for patients 15-17 yrs compared with children 1-9 yrs (P < 0.0001). Risk of avascular osteonecrosis was related to age with the highest OR for patients 10-14 yrs (OR = 10.4 (95% CI: (4.4;24.9)), P < 0.0001)., Conclusion: Adults followed and tolerated the NOPHO ALL2008 protocol virtually as well as children, although thrombosis and avascular osteonecrosis was most common among adolescents., (© 2015 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2016

27. PEG-asparaginase allergy in children with acute lymphoblastic leukemia in the NOPHO ALL2008 protocol.

Author

Henriksen LT, Harila-Saari A, Ruud E, Abrahamsson J, Pruunsild K, Vaitkeviciene G, Jónsson ÓG, Schmiegelow K, Heyman M, Schrøder H, and Albertsen BK

Subjects

Adolescent, Adult, Anaphylaxis chemically induced, Antineoplastic Agents adverse effects, Asparaginase adverse effects, Child, Child, Preschool, Drug Hypersensitivity etiology, Female, Follow-Up Studies, Humans, Infant, Male, Polyethylene Glycols adverse effects, Risk Factors, Antineoplastic Agents administration & dosage, Asparaginase administration & dosage, Polyethylene Glycols administration & dosage, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy

Abstract

Background: L-Asparaginase is an effective drug in the treatment of childhood acute lymphoblastic leukemia (ALL). The use of L-asparaginase may be limited by serious adverse events of which allergy is the most frequent. The objective of this study was to describe the clinical aspects of PEG-asparaginase allergy in children treated according to the Nordic Society of Paediatric Haematology and Oncology (NOPHO) ALL2008 protocol., Procedure: Children (1-17 years) enrolled in the NOPHO ALL2008 protocol between July 2008 and August 2011, who developed PEG-asparaginase allergy were identified through the NOPHO ALL2008 toxicity registry. In the NOPHO ALL2008 protocol, patients are randomized to 8 or 15 doses of intramuscular PEG-asparaginase (Oncaspar®) 1,000 IU/m(2) /dose administered at 2 or 6 weeks intervals during a total period of 30 weeks. (Clinical trials.gov no: NCT00819351)., Results: Of 615 evaluable patients, 79 patients developed clinical PEG-asparaginase allergy (cumulative risk; 13.2%) and discontinued PEG-asparaginase therapy for that reason. PEG-asparaginase allergy occurred after a median of two doses (75% range 2-4, max 14). In 58% of PEG-asparaginase hypersensitive patients, the clinical allergic reactions appeared within 2 hr after PEG-asparaginase administration and ranged from mild symptoms to systemic anaphylaxis. Nine patients experienced an anaphylactic reaction within 1 hr and 50 min from asparaginase administration; none were fatal. Four of 68 patients (6%) who subsequently received Erwinase therapy also reacted allergic to Erwinase., Conclusion: Clinical allergy to PEG-asparaginase occurred early in treatment, was in general moderate in severity, and mostly developed within 2 hr after PEG-asparaginase administration. The risk of subsequent Erwinase allergic reactions was low., (© 2014 Wiley Periodicals, Inc.)

Published

2015

28. Cerebral sinus venous thromboses in children with acute lymphoblastic leukaemia - a multicentre study from the Nordic Society of Paediatric Haematology and Oncology.

Author

Ranta S, Tuckuviene R, Mäkipernaa A, Albertsen BK, Frisk T, Tedgård U, Jónsson ÓG, Pruunsild K, Gretenkort Andersson N, Winther Gunnes M, Saulyte Trakymiene S, Frandsen T, Heyman M, Ruud E, and Helgestad J

Subjects

Adolescent, Adrenal Cortex Hormones adverse effects, Anticoagulants adverse effects, Anticoagulants therapeutic use, Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Asparaginase administration & dosage, Asparaginase adverse effects, Baltic States epidemiology, Child, Child, Preschool, Consolidation Chemotherapy, Female, Humans, Incidence, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Prospective Studies, Risk Factors, Scandinavian and Nordic Countries epidemiology, Sinus Thrombosis, Intracranial drug therapy, Sinus Thrombosis, Intracranial epidemiology, Treatment Outcome, Precursor Cell Lymphoblastic Leukemia-Lymphoma complications, Sinus Thrombosis, Intracranial etiology

Abstract

We present a prospective multicentre cohort of 20 children with acute lymphoblastic leukaemia (ALL) and cerebral sinus venous thrombosis (CSVT). The study covers a period of 5 years and comprises 1038 children treated according to the Nordic Society of Paediatric Haematology and Oncology (NOPHO) ALL 2008 protocol. The cumulative incidence of CSVT was 2%. Sixteen of the thromboses were related to asparaginase and 16 to steroids. Most CSVTs occurred in the consolidation phase. Nearly all were treated with low molecular weight heparin without bleeding complications. Mortality related to CSVT directly or indirectly was 10%, emphasizing the importance of this complication., (© 2014 John Wiley & Sons Ltd.)

Published

2015

29. Complying with the European Clinical Trials directive while surviving the administrative pressure - an alternative approach to toxicity registration in a cancer trial.

Author

Frandsen TL, Heyman M, Abrahamsson J, Vettenranta K, Åsberg A, Vaitkeviciene G, Pruunsild K, Toft N, Birgens H, Hallböök H, Quist-Paulsen P, Griškevičius L, Helt L, Hansen BV, and Schmiegelow K

Subjects

Adolescent, Child, Child, Preschool, Clinical Trials as Topic methods, European Union, Humans, Hypersensitivity etiology, Infant, Mycoses etiology, Outcome Assessment, Health Care methods, Pancreatitis etiology, Research Report standards, Risk Assessment methods, Risk Factors, Thrombosis etiology, Clinical Trials as Topic standards, Outcome Assessment, Health Care standards, Practice Guidelines as Topic standards, Risk Assessment standards

Abstract

The European Clinical Trials Directive of 2004 has increased the amount of paper work and reduced the number of initiated clinical trials. Particularly multinational trials have been delayed. To meet this challenge we developed a novel, simplified, fast and easy strategy for on-line toxicity registration for patients treated according to the Nordic/Baltic acute lymphoblastic leukaemia protocol, NOPHO ALL 2008, for children and young adults, including three randomisations. We used a risk-assessment based approach, avoiding reporting of expected adverse events and instead concentrating on 20 well-known serious, but rarer events with focus on changes in therapy introduced in the treatment protocol. This toxicity registration strategy was approved by the relevant regulatory authorities in all seven countries involved, as compliant within the EU directive of 2004. The centre compliance to registration was excellent with 98.9% of all patients being registered within 5weeks from the requested quarterly registration. Currently, four toxicities (thrombosis, fungal infections, pancreatitis and allergic reactions) have been chosen for further detailed exploration due to the cumulative fraction of patients with positive registrations exceeding 5%. This toxicity registration offers real-time toxicity profiles of the total study cohort and provides early warnings of specific toxicities that require further investigation., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2014

30. Group A rotavirus genotypes circulating prior to implementation of a National Immunization Program in Estonia.

Author

Soeorg H, Tamm E, Huik K, Pauskar M, Mägi D, Pruudel K, Vainomäe L, Moosar L, Kirss K, Torm S, Närska M, Pütsepp A, Nurm H, Pruunsild K, Jänes A, Zilmer K, and Lutsar I

Subjects

Child, Hospitalized, Child, Preschool, Estonia epidemiology, Feces virology, Female, Gastroenteritis pathology, Genotype, Humans, Infant, Male, Molecular Epidemiology, Polymerase Chain Reaction methods, Prevalence, Prospective Studies, Reverse Transcriptase Polymerase Chain Reaction methods, Rotavirus isolation & purification, Rotavirus Infections pathology, Severity of Illness Index, Gastroenteritis epidemiology, Gastroenteritis virology, Rotavirus classification, Rotavirus genetics, Rotavirus Infections epidemiology, Rotavirus Infections virology

Abstract

Group A rotaviruses (RVA) are a major cause of acute gastroenteritis in children ≤ 5 y worldwide which could be prevented with two recently introduced vaccines - monovalent Rotarix (live-attenuated G1P[8] strain) and pentavalent RotaTeq (human-bovine reassortant containing serotypes G1, G2, G3, G4 and P[8]). Prior to implementation of vaccines into national immunization program we aimed to describe RVA genotype distribution in hospitalized children aged < 5 y in Estonia during 2007-2008. A total of 671 children with confirmed RVA gastroenteritis from three major pediatric hospitals were prospectively enrolled. G- and P-genotypes were detected from 124 stool samples by semi-nested reverse transcription-PCR. Severity of disease was assessed using Clark scoring system. The majority of cases (65%) occurred in infants aged 7 to 24 mo and were of moderate severity (mean Clark score 12.1 (SD 3.2)). The prevailing strain was G2P[4] (34.7%), causing significantly more cases than G4P[8] (12.9%), G1P[8] or G9P[8] (both 4.0%), G3P[8] (1.6%). Yearly differences in genotype distribution occurred, as G2P[4] (52.8%) dominated in 2007, but G4P[8] (26.9%) in 2008. One third of strains remained non-typeable. The distribution of RVA genotypes in Estonia differs from that seen in other Central and Eastern European countries, although one should bear in mind the large proportion of P-untypeable strains and natural fluctuations of dominating RVA genotypes. Nevertheless, considering the high genotype-independent efficacy of the vaccines, introduction of national immunization should be considered.

Published

2012

31. Genetic characterization of hepatitis C virus strains in Estonia: fluctuations in the predominating subtype with time.

Author

Tallo T, Norder H, Tefanova V, Krispin T, Schmidt J, Ilmoja M, Orgulas K, Pruunsild K, Priimägi L, and Magnius LO

Subjects

5' Untranslated Regions genetics, Adolescent, Adult, Blood Donors, Estonia epidemiology, Female, Hepacivirus classification, Hospitals, Humans, Male, Molecular Sequence Data, Patients, Personnel, Hospital, RNA, Viral classification, Risk Factors, Species Specificity, Substance Abuse, Intravenous, Viral Core Proteins genetics, Viral Nonstructural Proteins genetics, Hepacivirus genetics, Hepatitis C epidemiology, Molecular Epidemiology

Abstract

During the last decade, there has been a dramatic increase in intravenous drug use in young adults in Estonia with an increased incidence of both hepatitis B and C as a consequence. Since genetic data are limited regarding hepatitis C virus (HCV) strains in Estonia, the aim of the study was to characterize HCV strains in different risk groups to determine their relatedness to strains from other geographical regions. Three hundred fifty-three anti-HCV positive sera collected during 1994-2004 from hospitalized patients, blood donors and health care workers were used as source of HCV RNA. Two hundred nine (59%) of the sera were positive for HCV RNA by PCR directed to the 5'-UTR region. For 174 strains the HCV subtype was determined by analyses of the NS5B and/or the 5'UTR-core regions. 1b (71%) was the most common subtype followed by 3a (24%), 2c (2%), 1a (1%), and 2a (1%). The 1b and 3a strains were similar to strains from other regions of the former USSR. Within genotype 1b there were several HCV lineages. However, for 3a there seemed to be two separate introductions into Estonia. There was a relative shift from subtype 1b to 3a in 1999-2000 with a further replacement of 3a with 1b in intravenous drug users in 2001 and onwards (P < 0.05). However, both subtypes were found to co-circulate in the community independent of risk factors. One patient was infected with the 2k/1b recombinant presumed to originate from St. Petersburg being the first isolate of this recombinant recovered outside Russia., ((c) 2007 Wiley-Liss, Inc.)

Published

2007