Literature DB >> 25435722

Assessment of interleukin 1β serum level in different responder groups and stages of chronic myeloid leukemia patients on imatinb mesylate therapy.

Bassam Francis Matti1, Maysoon Ali Saleem2, Shahla'a Fadhil Sabir3.   

Abstract

Chronic myeloid leukemia (CML) is a myeloproliferative disorder characterized by the presence of an acquired mutation which affects the hematopoietic stem cell, leading to a striking overproduction of immature granulocytes. The first important clue to its pathogenesis the Philadelphia chromosome created by a reciprocal translocation between chromosomes 9 and 22 (t [9; 22] [q34; q11]). The development of the BCR-ABL-targeted imatinib mesylate represents a paradigm shift in the treatment of CML. Imatinib displays inhibitory activity against other kinase(s) that play a role in monocyte/macrophage development. Accordingly many studies revealed the role of cytokines in pathophysiology of myeloid neoplasia including participation of IL-1β in the pathogenesis of CML. This study designed to assess the behavior of IL-1β through newly diagnosed patients, different responders groups (optimal, suboptimal and failure cytogenetic response) and advanced stages (acceleration and crisis groups) of CML Iraqi patients whom receiving Imatinib mesylate (tyrosine kinase inhibitor), trying to elucidate the role of immunity in pathophysiology of CML disease development and treatments. In this study 96 Iraqi CML patients under imatinib mesylate treatment categorized by complete blood picture and fluorescent in situ hybridization analysis into different response groups and stages, then used an enzyme linked immunosorbent assay technique to assess serum level of IL-1β in each response group and advance stage (acceleration and transformed) of CML patients, in comparison to level in 32 healthy control subjects and 32 newly diagnosed CML. Out of 128 patients the mean serum of interleukin 1β level (pg/ml) for the newly diagnosed, optimal responded, suboptimal responded, failure cytogenetic and advance stage of CML were 6.53 ± 3.81, 18.47 ± 4.29, 18.69 ± 3.03, 5.73 ± 2.44, and 18.10 ± 3.10, respectively. While healthy was 12.17 ± 3.44. The measurement of IL-1β before and during treatment of CML patients may contribute to the early identification of responder and non responder patients, and help in the earlier choice and/or design of alternative therapeutic strategies.

Entities:  

Keywords:  Chronic myeloid leukemia; Imatinib mesylate; Interleukin-1β

Year:  2014        PMID: 25435722      PMCID: PMC4243414          DOI: 10.1007/s12288-014-0339-7

Source DB:  PubMed          Journal:  Indian J Hematol Blood Transfus        ISSN: 0971-4502            Impact factor:   0.900


  22 in total

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Journal:  N Engl J Med       Date:  1999-04-29       Impact factor: 91.245

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Authors:  Ayda Bennour; Hatem Bellâaj; Yosra Ben Youssef; Moez Elloumi; Abderrahim Khelif; Ali Saad; Halima Sennana
Journal:  J Cancer Res Clin Oncol       Date:  2011-07-08       Impact factor: 4.553

Review 3.  How I treat newly diagnosed chronic phase CML.

Authors:  Jorge Cortes; Hagop Kantarjian
Journal:  Blood       Date:  2012-05-21       Impact factor: 22.113

4.  Clinical value of assessing the response to imatinib monitored by interphase FISH and RQ-PCR for BCR-ABL in peripheral blood for long-term survival of chronic phase CML patients: results of the Niigata CML-multi-institutional co-operative clinical study.

Authors:  Tatsuo Furukawa; Miwako Narita; Tadashi Koike; Kazue Takai; Koichi Nagai; Masashi Kobayashi; Satoru Koyama; Yoshinobu Seki; Hoyu Takahashi; Masahiro Fujiwara; Kenji Kishi; Koji Nikkuni; Noriatsu Isahai; Wataru Higuchi; Nobuhiko Nomoto; Souichi Maruyama; Masayoshi Masuko; Takashi Kuroha; Takashi Abe; Ken Toba; Masuhiro Takahashi; Yoshifusa Aizawa; Akira Shibata
Journal:  Int J Hematol       Date:  2011-02-05       Impact factor: 2.490

5.  The poor response to imatinib observed in CML patients with low OCT-1 activity is not attributable to lower uptake of imatinib into their CD34+ cells.

Authors:  Jane R Engler; Amity Frede; Verity Saunders; Andrew Zannettino; Deborah L White; Timothy P Hughes
Journal:  Blood       Date:  2010-07-15       Impact factor: 22.113

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Journal:  Blood       Date:  1994-11-01       Impact factor: 22.113

7.  Abnormal function of the bone marrow microenvironment in chronic myelogenous leukemia: role of malignant stromal macrophages.

Authors:  R Bhatia; P B McGlave; G W Dewald; B R Blazar; C M Verfaillie
Journal:  Blood       Date:  1995-06-15       Impact factor: 22.113

8.  BCR-ABL independence and LYN kinase overexpression in chronic myelogenous leukemia cells selected for resistance to STI571.

Authors:  Nicholas J Donato; Ji Yuan Wu; Jonathan Stapley; Gary Gallick; Hui Lin; Ralph Arlinghaus; Moshe Talpaz
Journal:  Blood       Date:  2003-01-15       Impact factor: 22.113

Review 9.  Chronic myeloid leukemia: an update of concepts and management recommendations of European LeukemiaNet.

Authors:  Michele Baccarani; Jorge Cortes; Fabrizio Pane; Dietger Niederwieser; Giuseppe Saglio; Jane Apperley; Francisco Cervantes; Michael Deininger; Alois Gratwohl; François Guilhot; Andreas Hochhaus; Mary Horowitz; Timothy Hughes; Hagop Kantarjian; Richard Larson; Jerald Radich; Bengt Simonsson; Richard T Silver; John Goldman; Rudiger Hehlmann
Journal:  J Clin Oncol       Date:  2009-11-02       Impact factor: 44.544

10.  Dynamics and potential impact of the immune response to chronic myelogenous leukemia.

Authors:  Peter S Kim; Peter P Lee; Doron Levy
Journal:  PLoS Comput Biol       Date:  2008-06-20       Impact factor: 4.475

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  1 in total

1.  Hepcidin Gene Cloning and Expression Pattern in Turbot (Scophthalmus maximus) after Vibrio. anguillarum Infection.

Authors:  Ai-Fang Deng; Zhi-Hui Jiang; Bai-Lin Cong
Journal:  Iran J Biotechnol       Date:  2020-10-01       Impact factor: 1.671

  1 in total

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