Your search keyword '"LEUKEMIA etiology"' showing total 121 results

1. Expression pattern and prognostic implication of SALL4 gene in myeloid leukemias: a case-control study.

Author

Farawela, Hala M., Zawam, Hamdy M., Al-Wakeel, Hanan A., El-Nagdy, Mona H., El-Refaey, Fatma A., and Abdel-Rahman, Hala A.

Subjects

*MYELOID leukemia, *LEUKEMIA etiology, *STEM cells, *ACUTE myeloid leukemia, *GENE expression

Abstract

SALL4 is a transcription factor that retains stem cells in an undifferentiated state and promotes its self-renewal. In addition, it is implicated in leukemogenesis via its effect on leukemic stem cells. This study aimed to characterize the expression pattern of SALL4 gene in acute myeloid leukemia (AML) and chronic myeloid leukemia (CML) at different progression phases of the leukemic process and to assess its prognostic significance. Real-time PCR was used in 106 patients: 54 AML patients; 43 de novo and 11 in complete remission (CR), 52 CML patients; 31 in chronic phase (CP), 11 in deep molecular response (MR4) and 10 in accelerated/blastic phase (AP/BP); and in 21 nonmalignant bone marrow samples. SALL4 gene expression was elevated in AML, AML-CR and CML-CP (median = 5.180, 4.604 and 14.125 fold changes, respectively). Elevated SALL4 gene expression among AML de novo patient was associated with poor disease-free survival (DFS) rates (p = .022). Among CML patients, the highest percentage of patients with a high SALL4 (p = .033) was among CML-CP. SALL4 has a role in leukemogenesis; high SALL4 expression was associated with poor DFS among AML patients. [ABSTRACT FROM AUTHOR]

Published

2019

2. ASXL1 mutations in AML are associated with specific clinical and cytogenetic characteristics.

Author

Kakosaiou, Katerina, Panitsas, Fotios, Daraki, Aggeliki, Pagoni, Maria, Apostolou, Paraskevi, Ioannidou, Agapi, Vlachadami, Ioanna, Marinakis, Theodoros, Giatra, Chara, Vasilatou, Diamantina, Sambani, Constantina, Pappa, Vassiliki, and Manola, Kalliopi N.

Subjects

*GENETIC mutation, *ACUTE myeloid leukemia, *LEUKEMIA etiology, *PROGNOSIS, *COHORT analysis, *CYTOGENETICS

Abstract

Mutations of ASXL1 are early events in acute myeloid leukemia (AML) leukemogenesis and have been associated with unfavorable prognosis. In this study, we investigated the type and frequency of ASXL1 mutations in a large cohort of patients with de novo or secondary AML (s-AML) and looked for correlations with cytogenetic findings and disease features. ASXL1 mutations were associated with older age, s-AML and higher peripheral leukocytosis. We observed more frequent co-occurrence of ASXL1 mutations with trisomy 8 and chromosome 11 aberrations but a negative correlation with myelodysplastic syndromes (MDS)-related cytogenetic abnormalities, especially −5/del(5q) and −7/del(7q). ASXL1 mutations were also found in other genetically defined AML subgroups such as those with t(9;22), inv(3)/t(3;3), t(8;21) or t(15;17); however, none of our inv(16) cases carried ASXL1 mutations. We detected two previously unreported ASXL1 mutations, p.IIe593Val and p.Cys688Tyr. Our findings suggest that ASXL1 mutations tend to cluster with specific clinical and cytogenetic profiles of AML patients. [ABSTRACT FROM AUTHOR]

Published

2018

3. Gestational age and childhood leukemia: A meta-analysis of epidemiologic studies.

Author

Wang, Yang-Feng, Wu, Li-Qun, Liu, Yi-Ni, Bi, Yong-Yi, and Wang, Hong

Subjects

*LEUKEMIA in children, *GESTATIONAL age, *EPIDEMIOLOGY, *LEUKEMIA etiology, *ACUTE myeloid leukemia, *PREMATURE labor

Abstract

Objective: An increasing amount of evidence shows that childhood leukemia is initiated in utero. Birth characteristics initiated in utero, such as gestational age, may play a role in leukemogenesis. The purpose of our meta-analysis is to explore the association between gestational age and childhood leukemia. Methods: Relevant studies up to 21 April 2017 were collected by searching PubMed and EMBASE databases. Subgroup analysis, sensitivity analysis and publication bias assessment were conducted. Results: A total of 13 studies were included. Pooled odds ratios (ORs) with 95% confidence intervals (CIs) for preterm birth and postterm birth were 1.06 (0.98, 1.13) and 1.01 (0.90, 1.13) for childhood leukemia, 1.04 (0.97, 1.11) and 1.03 (0.95, 1.12) for acute lymphocytic leukemia (ALL), 1.20 (1.00, 1.44) and 1.20 (1.00, 1.43) for acute myeloid leukemia (AML), compared with full-term birth. Study type and study region were the reasons behind the heterogeneity. In subgroup analyses, the summary ORs with 95% CI for childhood leukemia and ALL were 1.23 (1.07, 1.41) and 1.21 (1.06, 1.39) for postterm birth in cohort studies. No significant changes in sensitivity analyses and no publication bias were observed in our analysis. Conclusion: Our results suggest that both preterm and postterm infants have an elevated risk of developing AML. In addition, postterm birth increased the risk of childhood leukemia and ALL in cohort studies. However, more studies are warranted to validate these results and explore the biologic mechanisms underlying these relationships. [ABSTRACT FROM AUTHOR]

Published

2018

4. Eya2, a Target Activated by Plzf, Is Critical for PLZF-RARA-Induced Leukemogenesis.

Author

Ryoichi Ono, Masahiro Masuya, Satomi Ishii, Naoyuki Katayama, and Tetsuya Nosakaa

Subjects

*LEUKEMIA, *LEUKEMIA etiology, *TRANSCRIPTION factors, *GENE expression, *LABORATORY mice

Abstract

PLZF is a transcription factor that confers aberrant self-renewal in leukemogenesis, and the PLZF-RARA fusion gene causes acute promyelocytic leukemia (APL) through differentiation block. However, the molecular mechanisms of aberrant self-renewal underlying PLZF-mediated leukemogenesis are poorly understood. To investigate these mechanisms, comprehensive expression profiling of mouse hematopoietic stem/progenitor cells transduced with Plzf was performed, which revealed the involvement of a key transcriptional coactivator, Eya2, a target molecule shared by Plzf and PLZF-RARA, in the aberrant self-renewal. Indeed, PLZF-RARA as well as Plzf rendered those cells immortalized through upregulation of Eya2. Eya2 also led to immortalization without differentiation block, while depletion of Eya2 suppressed clonogenicity in cells immortalized by PLZF-RARA without influence on differentiation and apoptosis. Interestingly, cancer outlier profile analysis of human samples of acute myeloid leukemia (AML) in The Cancer Genome Atlas (TCGA) revealed a subtype of AML that strongly expressed EYA2. In addition, gene set enrichment analysis of human AML samples, including TCGA data, showed that this subtype of AML was more closely associated with the properties of leukemic stem cells in its gene expression signature than other AMLs. Therefore, EYA2 may be a target for molecular therapy in this subtype of AML, including PLZF-RARA APL. [ABSTRACT FROM AUTHOR]

Published

2017

5. Single nucleotide polymorphism array analysis of clonal evolution in younger adult acute lymphoblastic leukemia.

Author

Dirse, Vaidas, Gineikiene, Egle, Zvirblis, Tadas, Bertasiute, Ruta, Paulsson, Kajsa, and Griskevicius, Laimonas

Subjects

*GENETIC polymorphisms, *LYMPHOBLASTIC leukemia, *PATIENTS, *GENES, *LEUKEMIA etiology

Abstract

The article presents a study on single nucleotide polymorphism array analysis of clonal evolution in younger adult acute lymphoblastic leukemia. Topics include three patients stated to have displayed identical genetic changes at diagnosis and relapse, and 44 percent of the cases stated to have deletions in genes known to be associated with leukemogenesis.

Published

2016

6. Clearance of donor cell leukemia by means of graft versus leukemia effect: A case report.

Author

Ruiz-Delgado, Guillermo J., León Peña, Andrés A., Gómez-de-León, Andrés, and Ruiz-Argüelles, Guillermo J.

Subjects

*LEUKEMIA, *HEMATOPOIETIC stem cell transplantation, *DISEASE incidence, *LEUKEMIA etiology, *GENE expression

Abstract

Donor cell leukemia (DCL) is a rare complication of hematopoietic stem cell transplantation (HSCT). Its incidence has been reported between 0.12 and 5%, although the majority of cases are anecdotal. The mechanisms of leukemogenesis in DCL may be distinct from other types of leukemia. Here we describe a case of a 27-year-old woman with a diagnosis of biphenotypic acute leukemia who received a HSCT and developed a DCL. We briefly discuss the possible pathogenesis, diagnosis, and treatment of DCL. [ABSTRACT FROM AUTHOR]

Published

2016

7. Investigation of the inhibitors of histone-lysine N -methyltransferase SETD2 for acute lymphoblastic leukaemia from traditional Chinese medicine.

Author

Chang, Y.-L., Chen, H.-Y., Chen, K.-B., Chen, K.-C., Chang, K.-L., Chang, P.-C., Chang, T.-T., and Chen, Y.-C.

Subjects

*LYMPHOBLASTIC leukemia treatment, *HISTONE methyltransferases, *LYSINE, *CHINESE medicine, *LEUKEMIA etiology

Abstract

Leukaemia is the leading cause of childhood malignancies. Recent research indicates that theSETD2gene is associated with acute lymphoblastic leukaemia. This study aims to identify potential lead compounds from traditional Chinese medicine (TCM) using virtual screening for SET domain containing 2 (SETD2) protein against acute lymphoblastic leukaemia. Docking simulation was performed to determine potential candidates which obtain suitable docking poses in the binding domain of the SETD2 protein. We also performed molecular dynamics (MD) simulation to investigate the stability of docking poses of SETD2 protein complexes with the top three TCM candidates and a control. According to the results of docking and MD simulation, coniselin and coniferyl ferulate have high binding affinity and stable interactions with the SETD2 protein. Coniselin is isolated from the alcoholic extract ofComiselinum vaginatumThell. Coniferyl ferulate can be isolated fromAngelica sinensis,Poria cocos(Schw.) Wolf, andNotopterygium forbesii. Although S-adenosyl-L-homocysteine has more stable interactions with key residues in the binding domain than coniselin and coniferyl ferulate during MD simulation, the TCM compounds coniselin and coniferyl ferulate are still potential candidates as lead compounds for further study in the drug development process with the SETD2 protein against acute lymphoblastic leukaemia. [ABSTRACT FROM PUBLISHER]

Published

2016

8. Preferential occurrence of spliceosome mutations in acute myeloid leukemia with preceding myelodysplastic syndrome and/or myelodysplasia morphology.

Author

Cho, Young-Uk, Jang, Seongsoo, Seo, Eul-Ju, Park, Chan-Jeoung, Chi, Hyun-Sook, Kim, Dae-Young, Lee, Jung-Hee, Lee, Je-Hwan, Lee, Kyoo-Hyung, Koh, Kyung-Nam, Im, Ho-Joon, Seo, Jong Jin, Park, Sang Hyuk, Park, Young-Mi, and Lee, Jong-Keuk

Subjects

*ACUTE myeloid leukemia, *SPLICEOSOMES, *MYELODYSPLASTIC syndromes, *GENETIC mutation, *LEUKEMIA etiology

Abstract

Spliceosome mutations are associated with myelodysplasia. Here, we aimed to evaluate the frequency and clinical associations of these mutations in 204 patients with acute myeloid leukemia with myelodysplasia-related changes (AML with MRC) and 37 with therapy-related AML (t-AML). The frequency of mutation-positive patients was 17.0%, includingU2AF1(8.3%),SRSF2(5.8%) andSF3B1(2.9%). Mutations were detected almost exclusively in patients with AML with MRC, especially in cases with a preceding myelodysplastic syndrome (MDS) history or myelodysplastic morphology. By contrast, mutations were rare in patients with only MDS-related cytogenetics or t-AML. The presence of a mutation had no impact on survival. In a paired analysis, 16.7% of mutation-negative patients in the MDS phase acquired mutations during leukemogenesis. Our observations highlight the preponderance of spliceosome mutations within a specific AML subgroup with myelodysplasia, and suggest that these mutations might contribute pathologically to leukemogenesis in such patients. [ABSTRACT FROM PUBLISHER]

Published

2015

9. G-protein coupled receptor 34 activates Erk and phosphatidylinositol 3-kinase/Akt pathways and functions as alternative pathway to mediate p185Bcr-Abl-induced transformation and leukemogenesis.

Author

Zuo, Bo, Li, Mei, Liu, Yulan, Li, Kun, Ma, Shuyun, Cui, Meihua, Qin, Yazhen, Zhu, Honghu, Pan, Xiuying, Guo, Jingzhu, Dai, Zonghan, and Yu, Weidong

Subjects

*G proteins, *MEMBRANE proteins, *CELL growth, *LEUKEMIA etiology, *GENE expression

Abstract

Tyrosine 177 and the Src homology 2 (SH2) domain play important roles in linking p185Bcr-Abl to downstream pathways critical for cell growth and survival. However, a mutant p185Y177FR552L (p185YR), in which tyrosine 177 and arginine 552 in the SH2 domain are mutated, is still capable of transforming hematopoietic cells in vitro. Transplant of these cells into syngeneic mice also leads to leukemogenesis, albeit with a phenotype distinct from that produced by wild-type p185Bcr-Abl (p185wt)-transformed cells. Here we show that G-protein coupled receptor 34 (Gpr34) expression is markedly up-regulated in p185YR-transformed cells compared to those transformed by p185wt. Knockdown of Gpr34 in p185YR cells is sufficient to suppress growth factor-independent proliferation and survival in vitro and attenuate leukemogenesis in vivo. The Erk and phosphatidylinositol 3-kinase/Akt pathways are activated in p185YR cells and the activation is dependent on Gpr34 expression. These studies identify Gpr34 as an alternative pathway that may mediate p185Bcr-Abl-induced transformation and leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2015

10. Src family kinases and their role in hematological malignancies.

Author

Ku, Matthew, Wall, Meaghan, MacKinnon, Ruth N., Walkley, Carl R., Purton, Louise E., Tam, Constantine, Izon, David, Campbell, Lynda, Cheng, Heung-Chin, and Nandurkar, Harshal

Subjects

*SRC gene, *PROTEIN-tyrosine kinases, *HEMATOLOGIC malignancies, *HEMATOPOIESIS, *LEUKEMIA etiology, *GENE expression, *DISEASE progression, *DRUG resistance

Abstract

The Src family protein tyrosine kinases (SFKs) are non-receptor intracellular kinases that have important roles in both hematopoiesis and leukemogenesis. The derangement of their expression or activation has been demonstrated to contribute to hematological malignancies. This review first examines the mechanisms of SFK overexpression and hyperactivation, emphasizing the dysregulation of the upstream modulators. Subsequently, the role of SFK up-regulation in the initiation, progression and therapy resistance of many hematological malignancies is also analyzed. The presented evidence endeavors to highlight the influence of SFK up-regulation on an extensive number of hematological malignancies and the need to consider them as candidates in targeted anticancer therapy. [ABSTRACT FROM AUTHOR]

Published

2015

11. MicroRNA-26a-5p and microRNA-23b-3p up-regulate peroxiredoxin III in acute myeloid leukemia.

Author

Jiang, Wenjie, Min, Jie, Sui, Xiaohui, Qian, Yanyan, Liu, Ying, Liu, Zhaojian, Zhou, Haibin, Li, Xi, and Gong, Yaoqin

Subjects

*MICRORNA, *PEROXIREDOXINS, *ACUTE myeloid leukemia, *MICRORNA genetics, *GENE expression, *GRANULOCYTES, *LEUKEMIA etiology

Abstract

MicroRNAs (miRNAs) are small RNAs that regulate target gene expression. Using microarray-based miRNA expression profiling, we compared the miRNA expression in granulocytes from four patients with acute myeloid leukemia and four healthy controls. Thirty-four miRNAs were found to be differentially expressed, including 20 miRNAs that were up-regulated and 14 miRNAs that were down-regulated. The expression of selected miRNAs (miR-26a-5p and miR-23b-3p) was independently validated in 20 patients and 12 healthy controls. Notably, we demonstrated that peroxiredoxin III ( PrxIII) is a common direct target of both miR-26a-5p and miR-23b-3p. Furthermore, these results indicate that the two decreased miRNAs could scavenge cellular reactive oxygen species (ROS) by targeting the PrxIII gene. These findings are discussed with regard to the known function of PrxIII as a ROS scavenger and the high endogenous ROS levels required for hematopoietic stem cell differentiation. These findings may potentially offer insights into the pathological relationships between miR-26a-5p, miR-23b-3p and leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2015

12. A Review and Meta-Analysis of Outdoor Air Pollution and Risk of Childhood Leukemia.

Author

Filippini, Tommaso, Heck, Julia E., Malagoli, Carlotta, Giovane, Cinzia Del, and Vinceti, Marco

Subjects

*PHYSIOLOGICAL effects of air pollution, *LEUKEMIA in children, *LEUKEMIA etiology, *LYMPHOBLASTIC leukemia, *ACUTE myeloid leukemia, *BENZENE, *ONCOLOGY, *CANCER risk factors

Abstract

Leukemia is the most frequent malignant disease affecting children. To date, the etiology of childhood leukemia remains largely unknown. Few risk factors (genetic susceptibility, infections, ionizing radiation, etc.) have been clearly identified, but they appear to explain only a small proportion of cases. Considerably more uncertain is the role of other environmental risk factors, such as indoor and outdoor air pollution. We sought to summarize and quantify the association between traffic-related air pollution and risk of childhood leukemia, and further examined results according to method of exposure assessment, study quality, leukemia subtype, time period, and continent where studies took place. After a literature search yielded 6 ecologic and 20 case-control studies, we scored the studies based on the Newcastle-Ottawa Scale. The studies assessed residential exposure to pollutants from motorized traffic by computing traffic density in the neighboring roads or vicinity to petrol stations, or by using measured or modeled nitrogen dioxide and benzene outdoor air levels. Because heterogeneity across studies was observed, random-effects summary odds ratios (OR) and 95% confidence intervals (CI) were reported. Whenever possible we additionally conducted stratified analyses comparing acute lymphoblastic leukemia (ALL) and acute myeloid leukemia (AML). Limiting the analysis to high-quality studies (Newcastle-Ottawa Scale ≥ 7), those using traffic density as the exposure assessment metric showed an increase in childhood leukemia risk in the highest exposure category (OR = 1.07, 95% CI 0.93–1.24). However, we observed evidence of publication bias. Results for NO2exposure and benzene showed an OR of 1.21 (95% CI 0.97–1.52) and 1.64 (95% CI 0.91–2.95) respectively. When stratifying by leukemia type, the results based upon NO2were 1.21 (95% CI 1.04–1.41) for ALL and 1.06 (95% CI 0.51–2.21) for AML; based upon benzene were 1.09 (95% CI 0.67–1.77) for ALL and 2.28 (95% CI 1.09–4.75) for AML. Estimates were generally higher for exposures in the postnatal period compared to the prenatal period, and for European studies compared to North American studies. Overall, our results support a link between ambient exposure to traffic pollution and childhood leukemia risk, particularly due to benzene. [ABSTRACT FROM AUTHOR]

Published

2015

13. Acute myeloid leukemia with DNMT3A mutations.

Author

Li, Yunlong and Zhu, Baosheng

Subjects

*ACUTE myeloid leukemia, *GENETIC mutation, *DNA methyltransferases, *CYTOSINE, *SOMATIC mutation, *EPIGENETICS, *GENE expression, *LEUKEMIA etiology

Abstract

Acute myeloid leukemia (AML), a type of blood cancer, is characterized by an increase in the number of abnormal white blood cells in the bone marrow, frequently causing hematopoietic insufficiency. It is a heterogeneous disease featuring cytogenetic aberrations, recurrent somatic mutations and alterations in gene expression. DNA (cytosine-5-)-methyltransferase 3 alpha (DNMT3A) is closely associated with epigenetic modifications in mammalian development and disease. More recent studies have identified recurrent somatic mutations in DNMT3A in AML, most of which are heterozygous. The DNMT3A R882 codon is a mutational hotspot. The frequency of DNMT3A mutations varies among different countries, but mutations have been found to be associated with cytogenetics, age, white blood cell (WBC) count, prognosis and response of patients to chemotherapy. The normal function of DNMT3A can be disrupted by these mutations, which subsequently results in an abnormality of epigenetic modification. These data suggest that mutations in the DNMT3A gene represent a novel class of mutations in AML with distinct biological and clinical features. Further studies are needed to elucidate the exact molecular mechanism and function of DNMT3A mutations in leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2014

14. Baseline low immunoglobulin A predicts inferior disease-free survival in pediatric acute myeloid leukemia and serial evaluation suggests role of immunoglobulin A in leukemogenesis.

Author

Bansal, Anuj Kumar, Vishnubhatla, Sreenivas, Kumar, Uma, and Bakhshi, Sameer

Subjects

*HEALTH outcome assessment, *ACUTE myeloid leukemia in children, *LEUKEMIA in children, *IMMUNOGLOBULIN A, *FOLLOW-up studies (Medicine), *DISEASE relapse, *LEUKEMIA etiology

Abstract

Data on serial evaluation of immunoglobulins (Ig) in pediatric AML is lacking. From April 2010 to May 2011, 45 consecutive patients with AML aged 1-18 years were prospectively enrolled along with nine healthy controls. Ig were assessed at diagnosis, post-induction, post-consolidation, 3 and 6 months follow-up and relapse. At diagnosis, Ig levels were significantly higher in patients than in healthy controls. Patienths with gum hypertrophy had low Ig levels (IgG, p = 0.007; IgA, p = 0.003; IgM, p = 0.06). Baseline Ig did not correlate with complete remission (CR). Patients who relapsed had a lower baseline IgA level than those in continuous CR (169 ± 94 g/dL vs. 310 ± 177 g/dL, p = 0.019). Patients with a low baseline IgA level (less than median) had inferior disease-free-survival (DFS) on multivariate analysis ( p = 0.048). Post-induction, IgM ( p < 0.001) and IgA ( p = 0.048) were significantly reduced as compared to their baseline values. On serial follow-up in patients who were in continuous CR, there was a significant decrease in IgA from post-induction until 6 months after treatment completion. This is the first study to evaluate the trend of humoral immunity in sequential pediatric patients with AML. Our study demonstrates that in pediatric AML, baseline Ig were higher than in controls. Gum hypertrophy was observed in patients with low Ig (IgA and IgG) levels. Relatively lower baseline IgA predicted disease relapse and inferior DFS. On serial follow-up, IgA significantly decreased in those who continued to stay in CR but not in patients who relapsed, suggesting an association of IgA with leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2014

15. Inactivation of the Cdkn2a locus cooperates with HMGA1 to drive T-cell leukemogenesis.

Author

Di Cello, Francescopaolo, Dhara, Surajit, Hristov, Alexandra C., Kowalski, Jeanne, Elbahloul, Ossama, Hillion, Joelle, Roy, Sujayita, Meijerink, Jules P. P., Winter, Stuart S., Larson, Richard S., Huso, David L., and Resar, Linda

Subjects

*CYCLIN-dependent kinases, *HIGH mobility group proteins, *LEUKEMIA etiology, *LYMPHOBLASTIC leukemia, *DISEASE relapse, *TRANSGENIC mice, *EMBRYONIC stem cells, *HEMATOPOIETIC stem cells, *GENETICS

Abstract

T-cell acute lymphoblastic leukemia (T-ALL) is an aggressive leukemia with high relapse rates compared to B-lineage ALL. We previously showed that HMGA1a transgenic mice develop aggressive T-ALL, indicating that HMGA1 causes leukemic transformation in vivo. HMGA1 is also highly expressed in embryonic stem cells, hematopoietic stem cells and diverse, refractory human cancers. Disruption of the CDKN2A tumor suppressor locus occurs in most cases of T-ALL and is thought to contribute to leukemic transformation. To determine whether loss of function of CDKN2A cooperates with HMGA1 in T-ALL, we crossed HMGA1a transgenics onto a Cdkn2a null background. We discovered that T-ALL is markedly accelerated in HMGA1a transgenic Cdkn2a null mice. In addition, these mice recapitulate salient clinical and pathologic features of human T-ALL. HMGA1 is also highly overexpressed in human T-ALL. These findings suggest that HMGA1 plays a causative role in T-ALL and could represent a rational therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2013

16. DNA damage response in CD133 + stem/progenitor cells from umbilical cord blood: Low level of endogenous foci and high recruitment of 53BP1.

Author

Vasilyev, Stanislav A., Kubes, Miroslav, Markova, Eva, and Belyaev, Igor

Subjects

*HEMATOPOIETIC stem cells, *RADIATION-induced abnormalities, *LEUKEMIA etiology, *P53 protein, *CD34 antigen

Abstract

Purpose: Human hematopoietic stem cells (HSC) are thought to be a major target of radiation-induced leukemogenesis and also provide a relevant cellular model for assessing cancer risk. Cluster of designation 133+ (CD133+) is a marker found in human progenitor and hematopoietic stem cells. Our study examined the repair of radiation-induced DNA double-strand breaks (DSB) in CD133 + umbilical cord blood cells (UCBC). Materials and methods: After γ-irradiation, endogenous and induced DSB were evaluated in CD133 + UCBC, CD133 − UCBC and peripheral blood lymphocytes (PBL) in terms of phosphorylated histone 2A family member X (γH2AX) and tumor suppressor p53 binding protein 1 (53BP1) foci. Results: We found that repair signaling in CD133 + UCBC is different from CD133 − UCBC and PBL. These differences include lower endogenous DSB levels and higher 53BP1 recruitment. Conclusions: Our data, together with a recent report on radiation-induced γH2AX and 53BP1 foci in CD34 + cells, indicate enhanced DNA repair capacity in HSC as compared to mature lymphocytes. [ABSTRACT FROM AUTHOR]

Published

2013

17. Systemic mastocytosis is uncommon in KIT D816V mutation positive core-binding factor acute myeloid leukemia.

Author

Kristensen, Thomas, Preiss, Birgitte, Broesby-Olsen, Sigurd, Vestergaard, Hanne, Friis, Lone, and Møller, Michael Boe

Subjects

*MAST cell disease, *ACUTE myeloid leukemia, *GENETIC mutation, *HUMAN chromosomes, *CELL fractionation, *LEUKEMIA etiology

Abstract

The KIT D816V mutation is detected in the vast majority of adult cases of systemic mastocytosis (SM). The mutation is also frequently detected in core-binding factor acute myeloid leukemia (CBF AML) defined by the presence of t(8;21)(q22;q22); RUNX1-RUNX1T1 or inv(16)(p13.1;q22)/t(16;16)(p13.1;q22); CBFB-MYH11 chromosomal rearrangements, but whether the mutation is indicative of associated SM is unclear. In the present study, patients with CBF AML were therefore analyzed for the KIT D816V mutation and mutation positive cases subsequently analyzed for the presence of SM. The KIT D816V mutation was detected in eight of 20 cases of CBF AML, with the frequency in t(8;21)(q22;q22) and inv(16)(p13.1;q22) positive cases being 31% and 57%, respectively. The fraction of KIT D816V mutation positive cells was highly variable among the eight mutation positive patients, with levels ranging from 0.04 to 98% in a pretreatment blood sample. Five of the eight cases carried the mutation in a cell fraction below one-tenth of the blast cell fraction, thus suggesting that KIT mutation is often a late event in leukemogenesis. None of the eight KIT D816V mutation positive cases fulfilled the World Health Organization diagnostic criteria of SM. The presence of the KIT D816V mutation in the CBF AML subgroup can therefore not be considered indicative of associated SM. [ABSTRACT FROM AUTHOR]

Published

2012

18. Targeted inhibition of VEGF-modulated survival and arsenic sensitivity in acute myeloid leukemia (AML).

Author

Ding, Yong, Zhu, Xuejiao, Li, Yumin, Fei, Jia, and Zhang, Yuan

Subjects

*VASCULAR endothelial growth factors, *ACUTE myeloid leukemia, *NEOVASCULARIZATION inhibitors, *LEUKEMIA etiology, *ANTISENSE DNA, *ARSENIC trioxide, *CANCER cell proliferation

Abstract

Vascular endothelial growth factor (VEGF) is a specific growth factor for tumor-associated angiogenesis, and is also involved in leukemogenesis; however, its exact role in leukemia development remains elusive. In this study we used antisense oligonucleotide (AS) to manipulate VEGF function in acute myeloid leukemia (AML). HL60 and primary AML cells were transfected with VEGF AS (0.3 µmol/l). Cell proliferation and survival were assessed using the trypan blue exclusion assay. The viability of cells was determined using MTT. The IC50 values of arsenic trioxide (ATO) in HL60 cell were calculated by ICp software. The results showed that VEGF AS effectively inhibited AML cell proliferation and survival 72 hours post-transfection and exhibited time dependence. The IC50 value of ATO was significantly down-regulated by VEGF AS in HL60. Meanwhile, VEGF AS alone induced cell apoptosis, and promoted ATO-induced apoptosis. There is synergistic inhibitory effects between AS and ATO. VEGF AS down-regulated VEGF protein level in the supernatants and cellular VEGF mRNA level by western blot and real-time PCR. Therefore, targeted inhibition of VEGF suppressed survival and increased arsenic sensitivity in AML. [ABSTRACT FROM AUTHOR]

Published

2012

19. Is exposure to formaldehyde in air causally associated with leukemia??--A hypothesis-based weight-of-evidence analysis.

Author

Rhomberg, Lorenz R., Bailey, Lisa A., Goodman, Julie E., Hamade, Ali K., and Mayfield, David

Subjects

*FORMALDEHYDE, *LEUKEMIA etiology, *CANCER risk factors, *EPIDEMIOLOGY, *DISINFECTION & disinfectants, *TOXICITY testing

Abstract

Recent scientific debate has focused on the potential for inhaled formaldehyde to cause lymphohematopoietic cancers, particularly leukemias, in humans. The concern stems from certain epidemiology studies reporting an association, although particulars of endpoints and dosimetry are inconsistent across studies and several other studies show no such effects. Animal studies generally report neither hematotoxicity nor leukemia associated with formaldehyde inhalation, and hematotoxicity studies in humans are inconsistent. Formaldehyde''s reactivity has been thought to preclude systemic exposure following inhalation, and its apparent inability to reach and affect the target tissues attacked by known leukemogens has, heretofore, led to skepticism regarding its potential to cause human lymphohematopoietic cancers. Recently, however, potential modes of action for formaldehyde leukemogenesis have been hypothesized, and it has been suggested that formaldehyde be identified as a known human leukemogen. In this article, we apply our hypothesis-based weight-of-evidence (HBWoE) approach to evaluate the large body of evidence regarding formaldehyde and leukemogenesis, attending to how human, animal, and mode-of-action results inform one another. We trace the logic of inference within and across all studies, and articulate how one could account for the suite of available observations under the various proposed hypotheses. Upon comparison of alternative proposals regarding what causal processes may have led to the array of observations as we see them, we conclude that the case for a causal association is weak and strains biological plausibility. Instead, apparent association between formaldehyde inhalation and leukemia in some human studies is better interpreted as due to chance or confounding. [ABSTRACT FROM AUTHOR]

Published

2011

20. Activation of Paired-homeobox gene PITX1 by del(5)(q31) in T-cell acute lymphoblastic leukemia.

Author

Nagel, Stefan, Venturini, Letizia, Przybylski, Grzegorz K., Grabarczyk, Piotr, Schneider, Björn, Meyer, Corinna, Kaufmann, Maren, Schmidt, Christian A., Scherr, Michaela, Drexler, Hans G., and Macleod, Roderick A. F.

Subjects

*HOMEOBOX genes, *LYMPHOBLASTIC leukemia, *T cells, *INTERLEUKIN-2, *LEUKEMIA etiology, *DISEASES

Abstract

In T-cell acute lymphoblasic leukemia (T-ALL), neoplastic chromosomal rearrangements are known to deregulate members of the homeobox gene families NKL and HOXA. Here, analysis of T-ALL cell lines and primary cells identified aberrant expression of a third homeobox gene group, the Paired (PRD) class. LOUCY cells revealed chromosomal deletion at 5q31, which targets the downstream regulatory region of the PRD homeobox gene PITX1, removing a STAT1 binding site. STAT1 mediates repressive interleukin 2 (IL2)--STAT1 signaling, implicating IL2 pathway avoidance as a possible activation mechanism. Among primary T-ALL samples, 2/22 (9%%) aberrantly expressed PITX1, highlighting the importance of this gene. Forced expression of PITX1 in JURKAT cells and subsequent target gene analysis prompted deregulation of genes involved in T-cell development including HES1, JUN, NKX3-1, RUNX1, RUNX2, and TRIB2. Taken together, our data show leukemic activation of PITX1, a novice PRD-class homeobox gene in a subset of early-staged T-ALL, which may promote leukemogenesis by inhibiting T-cell development. [ABSTRACT FROM AUTHOR]

Published

2011

21. Role of hERG1 K+ channels in leukemia cells as a positive regulator in SDF-1a-induced proliferation.

Author

Zheng, Fang, Li, Huiyu, Du, Wen, and Huang, Shiang

Subjects

*LEUKEMIA etiology, *POTASSIUM channels, *CELL proliferation, *BONE marrow, *POLYMERASE chain reaction, *APOPTOSIS, *GENE expression

Abstract

Previous work from our laboratory has confirmed that human ether-à-go-go-related gene 1 (hERG1) K+ channels are constitutively expressed in leukemia cells and enhanced cell proliferation. More importantly, it has shown that stromal cell-derived factor-1a (SDF-1a) significantly increases hERG1 K+ tail current and a specific hERG1 K+ channels inhibitor significantly blocks SDF-1a-induced migration of leukemic cells. In this study, we investigated a possible regulatory effect of hERG1 K+ channels upon SDF-1a-mediated cell proliferation as a mean to uncover new molecular events involved in bone marrow microenvironment and leukemogenesis. RT-PCR showed that SDF-1a enhanced hERG1 expression in a dose-dependent manner. Cell proliferation assay illustrated that SDF-1a promoted cell proliferation in a dose-dependent manner, whereas this effect was impaired by E-4031. In addition, E-4031 inhibited SDF-1a-stimulated leukemic cell proliferation by inducing G0/G1 arrest. Interestingly, E-4031 promoted SDF-1a-induced apoptosis in HL-60 and leukemic blasts, which markedly impaired the protection effect of SDF-1a in AML. Moreover, SDF-1a increased the expression of Wnt/beta-catenin target genes, including beta-catenin, cyclin-D1, and c-myc; however, this manner was abolished by blockage with the hERG1 K+ channels. Taken together, our results provide evidence of a novel mechanism involved in the proliferative effects of SDF-1a and highlight hERG1 K+ channels as a therapeutic target for leukemia treatment and prevention. [ABSTRACT FROM AUTHOR]

Published

2011

22. Inhibition of autophagy: a new strategy to enhance sensitivity of chronic myeloid leukemia stem cells to tyrosine kinase inhibitors.

Author

Calabretta, Bruno and Salomoni, Paolo

Subjects

*TREATMENT of chronic myeloid leukemia, *PROTEIN-tyrosine kinase inhibitors, *CHLOROQUINE, *CANCER cell growth, *LEUKEMIA etiology, *SERVICES for cancer patients, *THERAPEUTICS

Abstract

Imatinib mesylate (IM) has become standard therapy for patients with chronic myeloid leukemia (CML), but CML stem cells are intrinsically resistant to IM and to second/third-generation tyrosine kinase inhibitors (TKIs), allowing the persistence of a ''reservoir'' of BCR--ABL-expressing CML-initiating cells potentially responsible for disease progression. Although it is still controversial whether the ''insensitivity'' of CML stem cells to treatment with TKIs is due to BCR--ABL-dependent or independent mechanisms, recent evidence indicates that treatment with IM suppresses BCR--ABL-dependent signaling in CML stem cells with no adverse effects on their survival. Treatment of CML cells with IM/TKIs induces autophagy, a genetically regulated process of adaptation to metabolic stress which may allow tumor cells to become metabolically inert, enabling their survival under conditions that may mimic growth factor/nutrient deprivation. Based on this hypothesis, TKI-induced autophagy may ''antagonize'' TKI-induced cell death and inhibition of autophagy may eliminate this survival mechanism by restoring ''sensitivity'' of CML stem cells to treatment with IM/TKIs. Consistent with this, recent evidence indicates that phenotypically and functionally defined CML-enriched stem cells that are insensitive to treatment with TKIs are efficiently eliminated by the combination of TKI and chloroquine, an inhibitor of late stage autophagy. Thus, inhibition of autophagy may ''sensitize'' CML stem cells to treatment with TKIs, thus preserving the high specificity of TKI-based therapies. [ABSTRACT FROM AUTHOR]

Published

2011

23. New developments in the treatment of chronic myeloid leukemia and Philadelphia-positive acute lymphoblastic leukemia.

Author

Fullmer, Amber, Kantarjian, Hagop, Cortes, Jorge, and Jabbour, Elias

Subjects

*LYMPHOBLASTIC leukemia treatment, *CHRONIC myeloid leukemia, *STEM cell transplantation, *IMATINIB, *PROTEIN-tyrosine kinase inhibitors, *LEUKEMIA etiology, *SERVICES for cancer patients, *PROGNOSIS, *THERAPEUTICS

Abstract

Although imatinib revolutionized the management of chronic myeloid leukemia (CML), recent data indicate a transformation in the treatment approach likely in the near future. The superiority of second-generation tyrosine kinase inhibitors (TKIs) over imatinib in newly diagnosed disease has been recognized. Several investigational agents specific for those patients with the T315I mutation remain under evaluation. In Philadelphia-positive (Ph-positive) acute lymphoblastic leukemia (ALL), the addition of imatinib improved response rates. However, short remission durations with single agent therapy limit the benefit on survival. Early molecular remissions achieved with dasatinib will enable more patients to proceed to stem cell transplant (SCT), with increased likelihood of positive outcomes post-SCT. [ABSTRACT FROM AUTHOR]

Published

2011

24. Repression of Transcriptional Activity of C/EBPα by E2F-Dimerization Partner Complexes.

Author

Zaragoza, Katrin, Bégay, Valérie, Schuetz, Anja, Heinemann, Udo, and Leutz, Achim

Subjects

*GENETIC transcription, *FAT cells, *KERATINOCYTES, *LIVER cells, *LEUKEMIA etiology, *CARCINOGENESIS, *CARRIER proteins

Abstract

The transcription factor CCAAT/enhancer-binding protein α (C/EBPα) coordinates proliferation arrest and the differentiation of myeloid progenitors, adipocytes, hepatocytes, keratinocytes, and cells of the lung and placenta. C/EBPα transactivates lineage-specific differentiation genes and inhibits proliferation by repressing E2F-regulated genes. The myeloproliferative C/EBPα BRM2 mutant serves as a paradigm for recurrent human C-terminal bZIP C/EBPα mutations that are involved in acute myeloid leukemogenesis. BRM2 fails to repress E2F and to induce adipogenesis and granulopoiesis. The data presented here show that, independently of pocket proteins, C/EBPα interacts with the dimerization partner (DP) of E2F and that C/EBPα-E2F/DP interaction prevents both binding of C/EBPα to its cognate sites on DNA and transactivation of C/EBP target genes. The BRM2 mutant, in addition, exhibits enhanced interaction with E2F-DP and reduced affinity toward DNA and yet retains transactivation potential and differentiation competence that becomes exposed when E2F/DP levels are low. Our data suggest a tripartite balance between C/EBPα, E2F/DP, and pocket proteins in the control of proliferation, differentiation, and tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2010

25. DIFFERENTIAL microRNA EXPRESSION IN CHILDHOOD B-CELL PRECURSOR ACUTE LYMPHOBLASTIC LEUKEMIA.

Author

Ju, Xiuli, Li, Dong, Shi, Qing, Hou, Huaishui, Sun, Nianzheng, and Shen, Baijun

Subjects

*LYMPHOBLASTIC leukemia in children, *LYMPHOCYTIC leukemia, *HEMATOPOIESIS, *LEUKEMIA etiology, *HEMATOPOIETIC agents

Abstract

MiRNAs play important roles in the development of both hematopoiesis and leukemogenesis. The analysis of differential microRNA expression profiles may be a powerful tool to allow us insight on the mechanisms of childhood B-cell precursor acute lymphoblastic leukemia (pre-B-ALL). The present study provides an informative profile of the expression of miRNAs in pre-B-ALL using two independent and quantitative methods: miRNA chip and qRT-PCR of mature miRNA from 40 newly diagnosed pre-B-ALL children. Additionally, putative hematopoiesis-specific target genes were analyzed with informatics technique. Both approaches showed that miR-222, miR-339, and miR-142-3p were dramatically overexpressed in pre-B-ALL patients, and downregulation of hsa-miR-451 and hsa-miR-373* was confirmed. The results of this study offer a comprehensive and quantitative profile of miRNA expression in pre-B-ALL and their healthy counterpart, suggesting that miRNAs could play a primary role in the disease itself. [ABSTRACT FROM AUTHOR]

Published

2009

26. Mutated IgHV1-69 gene usage represents a distinct subgroup associated with indolent disease in chronic lymphocytic leukemia.

Author

Galligan, Leeona, Catherwood, Mark A., Matthews, Christine, 'Curly' Morris, T. C. M, and Dennis Alexander, H

Subjects

*IMMUNOGLOBULINS, *CHRONIC lymphocytic leukemia, *LEUKEMIA etiology, *HEALTH outcome assessment, *CELL membranes, *DRUG therapy

Abstract

Biased IgHV gene usage in chronic lymphocytic leukemia (CLL) is well documented and suggests antigen involvement in leukemogenesis. IgHV1-69 is one of the most frequently rearranged IgHV genes in CLL and the majority of IgHV1-69 cases lack somatic hypermutation and display poor prognosis. However, its independent prognostic impact remains uncertain given reports showing a low proportion of mutated IgHV1-69 cases and stereotyped IgHV1-69 subsets with divergent clinical outcome. We assessed the frequency and clinical significance of IgHV1-69 gene usage in a cohort of 330 CLL patients. Functional IgHV1-69 gene rearrangements were detected in 32 cases (9.7%), 31 of which were characterised further. Seven (22.6%) were found to have undergone somatic hypermutation. This subgroup had shorter and more diverse complementarity determining region 3 (CDR3) sequences compared with unmutated IgHV1-69 cases. In addition, mutated IgHV1-69 gene status was associated with lower cell surface CD38 expression and less progressive disease as monitored by Binet staging, lymphocyte doubling time and requirement of chemotherapeutic intervention. To conclude, we present data confirming that IgHV1-69 gene rearrangements in CLL are not exclusively associated with unmutated IgHV status. In addition, we show that a somatically hypermutated subgroup may demonstrate more indolent characteristics despite the general association of IgHV1-69 gene usage with aggressive disease. [ABSTRACT FROM AUTHOR]

Published

2008

27. Association of the NQO1, MPO, and XRCC1 Polymorphisms and Chromosome Damage Among Workers at a Petroleum Refinery.

Author

Yang Jee Kim, Jun Yeol Choi, Domyung Paek, and Hai Won Chung

Subjects

*CHROMOSOME polymorphism, *GENETIC polymorphisms, *PETROLEUM refineries, *BENZENE, *LEUKEMIA etiology, *CHROMOSOME analysis, *CHROMOSOME abnormalities

Abstract

Benzene is a leukemogen, and exposure to benzene is an occupational hazard in the petroleum refining industries. The effects of genetic polymorphisms in the NQO1 (rs1800566), MPO (rs2333227), and XRCC1 (rs25487) genes on benzene-induced chromosome abnormalities were assessed in 108 benzene-exposed workers and 33 office workers. The mean benzene exposure for exposed workers was 0.51 ppm for full-shift workers, and the time-weighted average ranged from 0.004 to 4.25 ppm. The frequencies of micronuclei (MN) and chromosome aberrations (CA) were significantly higher in workers exposed to benzene than unexposed controls. Exposed workers with the T/T genotype for NQO1 showed significant 1.9-fold (95% CI = 1.5-2.3) and 2.6-fold (95% CI = 1.7-3.9) increases in MN and CA frequencies, respectively, compared to controls with C/C and C/T genotypes, after adjusting for age, smoking status, and alcohol intake. Among exposed workers, subjects with the combination of MPO G/G and XRCC1 Arg/Gln or Gln/Gln showed a significantly higher CA frequency compared to those with the combination of MPO G/A or A/A and XRCC1 Arg/Arg genotypes. These results indicated that the genotoxicity induced by a chronic benzene exposure is modulated by genes involved in both DNA repair and benzene metabolic pathways. [ABSTRACT FROM AUTHOR]

Published

2008

28. The State of the Art in the Pathogenesis of ATL and New Potential Targets Associated with HTLV-1 and ATL.

Author

Murata, Ken and Yamada, Yasuaki

Subjects

*HTLV-I, *LEUKEMIA etiology, *CELL proliferation, *MONOCLONAL antibodies

Abstract

Almost 30 years have passed since adult T-cell leukemia (ATL) was identified as a new disease entity in Japan. During this period, its causative agent, human T-cell leukemia virus (HTLV-1), was discovered, and a crucial role of the viral product Tax in ATL leukemogenesis was demonstrated. Recently, another HTLV-1 product, HBZ, which is encoded on the negative strand, was found, and it has now become a subject of intensive research because of its possible activity in cell proliferation. It is, however, impossible to elucidate the whole process of ATL leukemogenesis by studying only HTLV-1, and aberrations of cellular genes such as tumor suppressor genes are also profoundly involved in the later stages of ATL development. In contrast with the progress in the understanding of ATL pathogenesis, more progress in developing therapy for ATL is needed, and there has been only slight improvement in the prognosis. Recently, unique therapeutic approaches targeting molecules and/or mechanisms involved in the pathogenesis have been explored, and some of them produced encouraging results that might lead to breakthrough therapies. One of these approaches, the use of monoclonal antibody against chemokine receptor CCR4, is now ongoing as a multicenter clinical trial in Japan. Here we review the state of the art regarding our understanding of ATL leukemogenesis and new potential molecular targets in ATL therapy. [ABSTRACT FROM AUTHOR]

Published

2007

29. Follicular lymphoma: a historical overview.

Author

van Besien, Koen and Schouten, Harry

Subjects

*LYMPHOMAS, *LEUKEMIA etiology, *AUTOTRANSPLANTATION, *RITUXIMAB, *ANTINEOPLASTIC agents, *DRUG therapy

Abstract

Lymphoma was first described in 1862 and follicular lymphoma in 1925. Initially considered a benign disorder, and named Brill – Symmers disease after the authors of the original papers, it was rapidly recognized as a malignancy with a variable but often indolent course. Most of its clinical features were described by the early 1940s. Despite discussion about its cell of origin, and in contrast to many other lymphoma subtypes, follicular lymphoma could always be accurately recognized and diagnosed using light microscopy morphological features. B-cell origin was demonstrated in the 1970s and the important role of t(14;18) and bcl-2 gene rearrangement in the pathogenesis of follicular lymphoma was established shortly thereafter. The etiology of follicular lymphoma, the reason for marked geographic variation in its incidence, the role of alternative molecular pathways in its pathogenesis, and the cause for its variable clinical behavior all remain unknown. Several observations suggest an important role for the normal immune response in regulating the clinical behavior of follicular lymphoma. From the earliest descriptions, radiation therapy was shown to be very effective in follicular lymphoma, but not curative. Combination chemotherapy was tested in the 1970s, but despite high rates of response, there was only minimal impact on survival. Interferon combined with anthracycline based chemotherapy was the first treatment to improve survival, but was not widely adopted in the USA. Randomized studies have shown an impact of autologous transplantation on progression free survival. Allogeneic transplantation is a curative therapy, but is too toxic for widespread application. Targeted therapies, particularly rituximab have revolutionized the treatment of follicular lymphoma. A convergence of technological and biological advances will likely lead to further dramatic progress in the next decade. For the first time consistent improvements in survival of follicular lymphoma are reported. [ABSTRACT FROM AUTHOR]

Published

2007

30. Donor cell leukemia: A critical review.

Author

Ruiz-Argüelles, Guillermo J., Ruiz-Argüelles, Alejandro, and Garcés-Eisele, Javier

Subjects

*BONE marrow, *LEUKEMIA etiology, *HOMOGRAFTS, *CORD blood, *GENETICS

Abstract

Approximately 40 cases of DCL have been reported in the literature; cases have been reported after allografts from bone marrow, peripheral blood and cord blood. The study of these cases may provide new insights into the mechanisms of leukemogenesis. Some data suggest that the prevalence of this complication has been under-estimated. Most cases of DCL have occurred following transplantation for leukemia, but there have also been cases reported after transplantation for non-malignant conditions. Various mechanisms have been proposed to explain how DCL arise and are briefly discussed. Additional studies are needed to define with more detail both the true prevalence of this complication and its precise pathogenetic mechanism. [ABSTRACT FROM AUTHOR]

Published

2007

31. NSD1 in erythroid differentiation and leukemogenesis.

Author

Tauchmann, Samantha, Almosailleakh, Marwa, and Schwaller, Juerg

Subjects

*LEUKEMIA etiology, *HISTONE methyltransferases, *CHROMATIN, *PROTEIN-protein interactions, *GENETIC transcription

Abstract

We have uncovered a novel role for the nuclear receptor-binding SET domain protein 1 (NSD1) in human and murine erythroid differentiation. Mechanistically, we found that the histone methyltransferase activity of NSD1 is essential for chromatin binding, protein interactions and target gene activation of the erythroid transcriptional master regulator GATA1. [ABSTRACT FROM AUTHOR]

Published

2020

32. Transcription factor GATA-1 and Down syndrome leukemogenesis.

Author

Muntean, Andrew G., Ge, Yubin, Taub, Jeffrey W., and Crispino, John D.

Subjects

*TRANSCRIPTION factors, *DOWN syndrome, *LEUKEMIA etiology, *GENETIC mutation, *STEM cells, *HUMAN chromosome abnormalities

Abstract

Mutations in transcription factors constitute one means by which normal hematopoietic progenitors are converted to leukemic stem cells. Recently, acquired mutations in the megakaryocytic regulator GATA1 have been found in essentially all cases of acute megakaryoblastic leukemia (AMkL) in children with Down syndrome and in the closely related malignancy transient myeloproliferative disorder. In all cases, mutations in GATA1 lead to the expression of a shorter isoform of GATA-1, named GATA-1s. Because GATA-1s retains both DNA binding zinc fingers, but is missing the N-terminal transactivation domain, it has been predicted that the inability of GATA-1s to regulate its normal class of megakaryocytic target genes is the mechanism by which mutations in GATA1 contribute to the disease. Indeed, several recent reports have confirmed that GATA-1s fails to properly regulate the growth of megakaryocytic precursors, likely through aberrant transcriptional regulation. Although the specific target genes of GATA-1 mis-regulated by GATA-1s that drive this abnormal growth remain undefined, multiple candidate genes have been identified via gene array studies. Finally, the inability of GATA-1s to promote expression of important metabolic genes, such as cytadine deaminase, likely contributes to the remarkable hypersensitivity of AMkL blasts to cytosine arabinoside. Future studies to define the entire class of genes dysregulated by mutations in GATA1 will provide important insights into the etiology of these malignancies. [ABSTRACT FROM AUTHOR]

Published

2006

33. Disruption of Sept6, a Fusion Partner Gene of MLL, Does Not Meet Ontogeny, Leukemogenesis Induced by MLL-SEPT6, or Phenotype Induced by the Loss of Sept4.

Author

Ono, Ryoichi, Ihara, Masafumi, Nakajima, Hideaki, Ozaki, Katsutoshi, Kataoka-fujiwara, Yuki, Taki, Tomohiko, Nagata, Koh-ichi, Inagaki, Masaki, Yoshida, Nobuaki, Kitamura, Toshio, Hayashi, Yasuhide, Kinoshita, Makoto, and Nosaka, And Tetsuya

Subjects

*CYTOLOGY, *CARCINOGENESIS, *ACUTE leukemia, *CANCER, *CYTOKINESIS, *ONTOGENY, *LEUKEMIA etiology, *LABORATORY mice

Abstract

Septins are evolutionarily conserved GTP-binding proteins that can heteropolymerize into filaments. Recent studies have revealed that septins are involved in not only diverse normal cellular processes but also the pathogenesis of various diseases, including cancer. SEPT6 is ubiquitously expressed in tissues and one of the fusion partner genes of MLL in the 11q23 translocations implicated in acute leukemia. However, the roles of this septin in vivo remain elusive. We have developed Sept6-deficient mice that exhibited neither gross abnormalities, changes in cytokinesis, nor spontaneous malignancy. Sept6 deficiency did not cause any quantitative changes in any of the septins evaluated in this study, nor did it cause any additional changes in the Sept4-deficient mice. Even the depletion of Sept 11, a close homolog of Sept6, did not affect the Sept6-null cells in vitro, thus implying a high degree of redundancy in the septin system. Furthermore, a loss of Sept6 did not alter the phenotype of myeloproliferative disease induced by MLL-SEPT6, thus suggesting that Sept6 does not function as a tumor suppressor. To our knowledge, this is the first report demonstrating that a disruption of the translocation partner gene of MLL in 11q23 translocation does not contribute to leukemogenesis by the MLL fusion gene. [ABSTRACT FROM AUTHOR]

Published

2005

34. Acute promyelocytic leukemia: A model of molecular target based therapy.

Author

Guang-Biao Zhou, Sai-Juan Chen, and Zhu Chen

Subjects

*LEUKEMIA, *BLOOD diseases, *CELL proliferation, *APOPTOSIS, *MYELOID leukemia, *LEUKEMIA etiology, *ACUTE leukemia

Abstract

Leukemia, a group of hematological malignancies characterized by clonal expansion of hematopoietic cells with uncontrolled proliferation, decreased apoptosis and blocked differentiation, is one of the most notorious enemies of mankind which accounts for some 300,000 new cases and 222,000 deaths each year worldwide 1234. Leukemia can be divided into acute or chronic, lymphoid or myeloid types, based on the disease progression and hematopoietic lineages involved 5. The responses of leukemia to therapies differ from one type or subtype to another. Hence, to improve the clinical outcome, the therapeutic strategies should be disease pathogenesis-based and individualized. The close collaboration between bench and bedside may not only shed new lights on leukemogenesis, gain insights into therapeutic mechanisms, but also provide opportunities for designing more rational therapies. The development of curative approaches for acute promyelocytic leukemia (APL) may serve as a paradigm 6. [ABSTRACT FROM AUTHOR]

Published

2005

35. Wilms' tumor 1 (WT1) gene in hematopoiesis: a surrogate marker of cell proliferation as a possible mechanism of action?

Author

Olszewski, M., Huang, W., Chou, P. M., Duerst, R., and Kletzel, M.

Subjects

*GENE expression, *HEMATOPOIETIC growth factors, *HEMATOPOIETIC system cancer, *LEUKEMIA, *LEUKEMIA etiology, *CELL proliferation

Abstract

Background Wilms' tumor 1 (WT1) gene expression is seen in a significant number of cases of human neoplasia; however, the mechanism of action remains to be clarified. We hypothesized that WT1 gene is a surrogate marker of proliferation in normal hematopoietic cells and leukemias. While we and others have recognized its value as a tool for the detection of minimal residual disease (MRD), the objective of this study was to confirm our hypothesis regarding normal. Methods Samples from healthy donors ( n =16) and UC blood ( n =9) were cultured in Methocult™ for 21 days. Colonies were analyzed on days 7, 14 and 21 by RT-PCR for WT1 gene expression. Our positive controls were samples from patients with leukemia ( n =91). Negative controls were from normal volunteers without stimulation ( n =26). Results Results showed a statistically significant difference ( P <0.0001) between cultured groups, with the highest level of WT1 gene expression in the positive controls and on day 14, when cells are at their maximal proliferation. Discussion In conclusion, WT1 gene expression in the proliferating colonies was highest on day 14, although less than in leukemia samples, confirming our hypothesis that WT1 gene is a surrogate marker of proliferation, not only in leukemogenesis but also, to a lesser degree, in normal cell proliferation. [ABSTRACT FROM AUTHOR]

Published

2005

36. Leukemogenesis Caused by Incapacitated GATA-1 Function.

Author

Shimizu, Ritsuko, Kuroha, Takashi, Ohneda, Osamu, Xiaoqing Pan, Ohneda, Kinuko, Takahashi, Satoru, Philipsen, Sjaak, and Yamamoto, Masayuki

Subjects

*LEUKEMIA etiology, *DIAGNOSIS of blood diseases, *BLOOD testing, *LYMPHOCYTIC leukemia, *LYMPHOPROLIFERATIVE disorders, *CELL proliferation, *LYMPHATIC diseases

Abstract

GATA-1 is essential for the development of erythroid and megakaryocytic lineages. We found that GATA-1 gene knockdown female (GATA-1.05/X) mice frequently develop a hematopoietic disorder resembling myelodysplastic syndrome that is characterized by the accumulation of progenitors expressing low levels of GATA-1. In this study, we demonstrate that GATA-1.05/X mice suffer from two distinct types of acute leukemia, an early-onset c-Kit-positive nonlymphoid leukemia and a late-onset B-lymphocytic leukemia. Since GATA-1 is an X chromosome gene, two types of hematopoietic cells reside within heterozygous GATA-1 knockdown mice. bearing either an active wild-type GATA.I allele or an active mutant GATA-1.05 allele. In the hematopoietic progenitors with the latter allele, low-level GATA-1 expression is sufficient to support survival and proliferation but not differentiation, leading to the accumulation of progenitors that are easily targeted by oncogenic stimuli. Since such leukemia has not been observed in GATA-1-null/X mutant mice, we conclude that the residual GATA-1 activity in the knockdown mice contributes to the development of the malignancy. This de novo model recapitulates the acute crisis found in preleukemic conditions in humans. [ABSTRACT FROM AUTHOR]

Published

2004

37. Hematopoietic Cell Fate and the Initiation of Leukemic Properties in Primitive Primary Human Cells Are Influenced by Ras Activity and Farnesyltransferase Inhibition.

Author

Dorrell, Craig, Takenaka, Katsuto, Minden, Mark D., Hawley, Robert G., and Dick, John E.

Subjects

*LEUKEMIA, *MONOCYTES, *MACROPHAGES, *CELL proliferation, *LEUKEMIA etiology

Abstract

The Ras pathway transduces divergent signals determining normal cell fate and is frequently activated in hematopoietic malignancies, but the manner in which activation contributes to human leukemia is poorly understood. We report that a high level of activated H-Ras signaling in transduced primary human hematopoietic progenitors reduced their proliferation and enhanced monocyte/macrophage differentiation. However, the exposure of these cells to a farnesyltransferase inhibitor and establishment of a moderate level of Ras activity showed increased proliferation, an elevated frequency of primitive blast-like cells, and progenitors with enhanced self-renewal capacity. These results suggest that the amplitude of Ras pathway signaling is a determinant of myeloid cell fate and that moderate Ras activation in primitive hematopoietic cells can be an early event in leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2004

38. Xenobiotic Metabolism and the Mechanism(s) of Benzene Toxicity.

Author

Snyder, Robert

Subjects

*METABOLISM, *BENZENE, *LEUKEMIA etiology, *TOXICITY testing, *XENOBIOTICS, *BIOCHEMISTRY

Abstract

The investigation of the mechanism(s) of benzene toxicity/leukemogenesis over the past 50 years has been contemporaneous with developments in the study of xenobiotic metabolism. Research on the cytochrome P450(CYP) enzyme system, and related systems in vivo and in vitro, which culminated in the isolation and reconstitution of the many CYPs, established pathways for the study of xenobiotic metabolism and its relationship to the biological activity of many chemicals. The essential role for metabolism of benzene as a precursor to the demonstration of benzene toxicity led to extensive studies of benzene metabolism, many of which will be reviewed here. Benzene toxicity/leukemogenesis, however, is a function of the bone marrow, a site remote from the liver where most benzene metabolism occurs. Studies of benzene metabolism have delineated the array of metabolites which appear to play a role in bone marrow damage, but further studies, both in vivo and in vitro, using appropriate animal models, will be needed to fully understand the impact of benzene and its metabolites on bone marrow function. [ABSTRACT FROM AUTHOR]

Published

2004

39. The Prenatal Origin of Childhood Acute Lymphoblastic Leukemia.

Author

Taurb, Jeffrey W. and Ge, Yubin

Subjects

*LYMPHOBLASTIC leukemia, *MYELOID leukemia, *LEUKEMIA etiology, *NEWBORN infants

Abstract

Until recently, the etiology of childhood acute lymphoblastic leukemia (ALL) has remained relatively elusive. Several studies have established a time frame for the development of ALL which could lead to the identification of specific exposures linked to leukemogenesis from the generation of the initial leukemic clone until clinical diagnosis. Utilizing newborn screening ('Guthrie') cards, leukemic clones have been detected retrospectively in dried blood spots using two different PCR-based approaches: (i) the amplification of patient/leukemia-specific breakpoint fusion sequences of rearranged oncogenes; and (ii) the amplification of clonal immunoglobulin heavy chain gene (IgH) or T cell receptor (TcR) gene rearrangements. These studies support the hypothesis that a large proportion of childhood ALL cases arise in utero . In several studies, a long latency period from the generation in utero of the initial ALL clone to clinical diagnosis, indicates that additional genetic events are required for the full development of the leukemia phenotype, potentially from postnatal exposures (e.g. infections). The identification of leukemia-associated translocations in umbilical cord blood samples of healthy newborns, suggest that in the future children may be identified prospectively who have an increased risk of developing leukemia. [ABSTRACT FROM AUTHOR]

Published

2004

40. Aberrant Eukaryotic Translation Initiation Factor 4E-Dependent mRNA Transport Impedes Hematopoietic Differentiation and Contributes to Leukemogenesis.

Author

Topisirovic, Ivan, Guzman, Monica L., McConnell, Melanie J., Licht, Jonathan D., Culjkovic, Biljana, Neering, Sarah J., Jordan, Craig T., and Borden, Katherine L.B.

Subjects

*EUKARYOTIC cells, *NUCLEOTIDE sequence, *GENETIC transcription, *LEUKEMIA etiology, *HEMATOPOIETIC growth factors, *MESSENGER RNA

Abstract

The eukaryotic translation initiation factor 4E (eIF4E) acts as both a key translation factor and as a promoter of nucleocytoplasmic transport of specific transcripts. Traditionally, its transformation capacity in vivo is attributed to its role in translation initiation in the cytoplasm. Here, we demonstrate that elevated eIF4E impedes granulocytic and monocytic differentiation. Our subsequent mutagenesis studies indicate that this block is a result of dysregulated eIF4E-dependent mRNA transport. These studies indicate that the RNA transport function of eIF4E could contribute to leukemogenesis. We extended our studies to provide the first evidence that the nuclear transport function of eIF4E contributes to human malignancy, specifically in a subset of acute and chronic myelogenous leukemia patients. We observe an increase in eIF4E-dependent cyclin D1 mRNA transport and a concomitant increase in cyclin D1 protein levels. The aberrant nuclear function of eIF4E is due to abnormally large eIF4E bodies and the loss of regulation by the proline-rich homeodomain PRH. We developed a novel tool to modulate this transport activity. The introduction of IκB, the repressor of NF-κB, leads to suppression of eIF4E, elevation of PRH, reorganization of eIF4E nuclear bodies, and subsequent downregulation of eIF4E-dependent mRNA transport. Thus, our findings indicate that this nuclear function of eIF4E can contribute to leukemogenesis by promoting growth and by impeding differentiation. [ABSTRACT FROM AUTHOR]

Published

2003

41. STAT5 and Oct-1 Form a Stable Complex That Modulates Cyclin D1 Expression.

Author

Magné, Sophie, Caron, Sandrine, Charon, Martine, Rouyez, Marie-Christine, and Dusanter-Fourt, Isabelle

Subjects

*CELLULAR signal transduction, *CYTOKINES, *BLOOD cells, *LEUKEMIA etiology, *CELLS, *GENES

Abstract

Signal transducer and activator of transcription 5 (STAT5) is activated by numerous cytokines that control blood cell development. STAT5 was also shown to actively participate in leukemogenesis. Among the target genes involved in cell growth, STAT5 had been shown to activate cyclin D1 gene expression. We now show that thrombopoietin-dependent activation of the cyclin D1 promoter depends on the integrity of a new bipartite proximal element that specifically binds STAT5A and -B transcription factors. We demonstrate that the stable recruitment of STAT5 to this element in vitro requires the integrity of an adjacent octamer element that constitutively binds the ubiquitous POU homeodomain protein Oct-1. We observe that cytokine-activated STAT5 and Oct-1 form a unique complex with the cyclin D1 promoter sequence. We find that STAT5 interacts with Oct-1 in vivo, following activation by different cytokines in various cellular contexts. This interaction involves a small motif in the carboxy-terminal region of STAT5 which, remarkably, is similar to an Oct-1 POU-interacting motif present in two well-known partners of Oct-1, namely, OBF-1/Bob and SNAP190. Our data offer new insights into the transcriptional regulation of the key cell cycle regulator cyclin D1 and emphasize the active roles of both STAT5 and Oct-1 in this process. [ABSTRACT FROM AUTHOR]

Published

2003

42. Megakaryoblastic Leukemia 1, a Potent Transcriptional Coactivator for Serum Response Factor (SRF), Is Required for Serum Induction of SRF Target Genes.

Author

Bo Cen, Selvaraj, Ahalya, Burgess, Rebecca C., Hitzler, Johann K., Zhigui Ma, Morris, Stephan W., and Prywes, Ron

Subjects

*LEUKEMIA etiology, *TRANSCRIPTION factors, *SERUM

Abstract

Megakaryoblastic leukemia 1 (MKL1) is a myocardin-related transcription factor that we found strongly activated serum response element (SRE)-dependent reporter genes through its direct binding to serum response factor (SRF). The c-fos SRE is regulated by mitogen-activated protein kinase phosphorylation of ternary complex factor (TCF) but is also regulated by a RhoA-dependent pathway. The mechanism of this pathway is unclear. Since MKL1 (also known as MAL, BSAC, and MRTF-A) is broadly expressed, we assessed its role in serum induction of c-fos and other SRE-regulated genes with a dominant negative MKL1 mutant (DN-MKL1) and RNA interference (RNAi). We found that DN-MKL1 and RNAi specifically blocked SREdependent reporter gene activation by serum and RhoA. Complete inhibition by RNAi required the additional inhibition of the related factor MKL2 (MRTF-B), showing the redundancy of these factors. DN-MKL1 reduced the late stage of serum induction of endogenous c-fos expression, suggesting that the TCF- and RhoA-dependent pathways contribute to temporally distinct phases of c-fos expression. Furthermore, serum induction of two TCF-independent SRE target genes, SRF and vinculin, was nearly completely blocked by DN-MKL1. Finally, the RBM15-MKL1 fusion protein formed by the t(1;22) translocation of acute megakaryoblastic leukemia had a markedly increased ability to activate SRE reporter genes, suggesting that its activation of SRF target genes may contribute to leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2003

43. Vascularity, Angiogenesis and Angiogenic Factors in Leukemias and Myelodysplastic Syndromes.

Author

Aguayo, Alavro, Giles, Francis, and Albitar, Maher

Subjects

*BONE marrow, *LEUKEMIA etiology

Abstract

Bone marrow microenvironment plays a crucial role in the leukemogenic process. New studies suggest that the bone marrow vascularity changes significantly in the leukemic process and that angiogenic factors play a major role in leukemia and myelodysplasia. However, hematologic malignancies appear to be particularly vulnerable to the effects of angiogenic factors because most of these factors appear to be secreted by hematopoietic cells, and they may have autocrine and paracrine regulatory effects on the hematopoietic system. The use of angiogenesis inhibitors for the treatment of hematologic malignancies is particularly attractive because it may target not only the environment but also the malignant cells. [ABSTRACT FROM AUTHOR]

Published

2003

44. A HEMATOLOGICAL STUDY IN MICE FOR EVALUATION OF LEUKEMOGENESIS BY EXTREMELY LOW FREQUENCY MAGNETIC FIELDS.

Author

Vallejo, D., Sanz, P., and Picazo, M.

Subjects

*LEUKEMIA etiology, *MAGNETIC fields, *HEMATOLOGY

Abstract

OF1 mice were chronically exposed to a 50-Hz sinusoidal East-West magnetic field of 15 μT (rms), in order to make a peripheral blood study for a leukemogenic evaluation of this non-ionizing radiation. Mating and pregnancy of ancestors (first generation), and birth, lactation, and development of secondgeneration female mice until adulthood occurred in the experimental field. A hematological study of both control and exposed 14- to 15-week-old and 50to 52-week-old, second-generation females was realized. Individual diagnosis of specimens and statistical analysis of results revealed a high incidence of blood leukoproliferative disorders in 14- to 15-week-old exposed females (relative risk [RR] = 3.00, p = 0.0033), despite the resistance of this strain of mice to developing malignancies under normal environmental conditions before they are 26 weeks old. Especially elevated incidences of lymphocytic (RR = 6.50, p = 0.0021) and chronic (RR = 4.00, p = 0.0153) leukemias were associated with medium-term (14-15 weeks) exposure. After 50-52 weeks of exposure, the mortality of exposed mice was 30% versus 0% of control mice. From dead exposed females, 67% revealed some type of malignancy. Corresponding RR for blood leukoproliferative disorders of those exposed which survived was 2.57 (p = 0.0351). Especially important was the proportion of chronic leukemias after long-term (50-52 weeks) exposure (RR = 8.57, p = 0.0118). Moreover, a statistically nonsignificant increase of lymphoblastic-myeloblastic leukemias pointed to a relation between age of specimen and type of alteration. We suggest that the increase in blood leukemias in OF1 mice agrees with the results of numerous epidemiological studies. [ABSTRACT FROM AUTHOR]

Published

2001

45. RECENT DEVELOPMENTS IN BENZENE RISK ASSESSMENT.

Author

Kacew, Sam and Lemaire, Irma

Subjects

*BENZENE, *LEUKEMIA etiology

Abstract

Examines the leukemogenic mechanisms of benzene. Importance of benzene metabolism on bone-marrow toxicity; Factors contributing to benzene toxicity; Use of benzene in inducing chromosome deletions and large-scale chromosomal alterations.

Published

2000

46. RECENT DEVELOPMENTS IN THE UNDERSTANDING OF BENZENE TOXICITY AND LEUKEMOGENESIS.

Author

Snyder, Robert

Subjects

*BENZENE, *LEUKEMIA etiology, *AROMATIC compounds

Abstract

Discusses developments in the understanding of benzene toxicity and leukemogenesis as of February 2002. Adverse effects of benzene and suggested dose relationships; Benzene metabolism; Factors which contribute to the mechanism of benzene toxicity.

Published

2000

47. Microsatellite instability in hematological malignancies.

Author

Maletzki, Claudia, Stier, Saskia, and Linnebacher, Michael

Subjects

*COLON cancer treatment, *MICROSATELLITE repeats, *IMMUNOREGULATION, *LEUKEMIA etiology, *HEMATOLOGY

Abstract

The genome of colorectal carcinomas displaying pronounced microsatellite instability codes for an extraordinarily high number of mutated proteins that elicit tumor-specific cellular immune responses. We have recently demonstrated that leukemic cells are also vulnerable to T cells specific for tumor-associated antigens produced in the context of microsatellite instability. This finding extends our understanding of secondary and therapy-related leukemogenesis, linking it to the mutual interaction between immune control and escape. [ABSTRACT FROM AUTHOR]

Published

2013

48. Urine Phenol and Myeloperoxidase Index: An Observation in Benzene Exposed Subjects.

Author

Wiwanitkit, Viroj, Soogarun, Suphan, and Suwansaksri, Jamsai

Subjects

*PHENOLS, *BENZENE, *LEUKEMIA, *AROMATIC compounds, *LEUKEMIA etiology, *MEDICAL sciences

Abstract

Benzene is a colorless poisonous liquid with a sweet odor. At present, it is documented as a known inducer of leukemia. Potential metabolic mechanisms underlying the hemopoietic toxicity of benzene include bioactivation of phenolic metabolites of benzene by myeloperoxidases in bone marrow, which results in hydroquinolone, a major leukemogen. There is no previous correlative study between the level of phenol, urine benzene metabolite, and the myeloperoxidase index (MPXI). Here, the correlation between the urine phenol and MPXI were studied in 24 Thai subjects occupationally exposed to benzene. Of interest, the regression analysis show no significant correlation between urine phenol level and MPXI ( r  = - 0.05, P  = 0.81). [ABSTRACT FROM AUTHOR]

Published

2004

49. SET-NUP214 rearrangement in isolation is insufficient to induce leukemia: a single center experience.

Author

Prokopiou, Chrystalla, Koumas, Sotiris, Neokleous, Nikolaos, Seimeni, Ourania, and Barmpouti, Aikaterini

Subjects

*LEUKEMIA, *REVERSE transcriptase polymerase chain reaction, *CHIMERIC proteins, *CHROMOSOME abnormalities, *LEUKEMIA etiology, *PATIENTS, BONE marrow examination

Abstract

The article reports that rearrangement of SET-NUP214 in isolation is scarce to build leukemia. It states that patients with lymphadenopathy and bone pain were screened with bone marrow biopsy and finds that single SET-NUP214 transcript was increased by reverse transcription polymerase chain reaction (RT-PCR). It mentions that SET-NUP rearrangement build a fusion protein that slows cell apoptosis caused by cytotoxic T-cells and needs chromosomal aberrations to move leukemogenesis.

Published

2016

50. T-cell leukemogenesis is an inappropriate lineage decision-making process: implications for precision oncology.

Author

Rodríguez-Hernández, Guillermo, Bhatia, Sanil, Vicente-Dueñas, Carolina, Borkhardt, Arndt, Hauer, Julia, and Sánchez-García, Isidro

Subjects

*LEUKEMIA etiology, *T cells, *LYMPHOCYTES, *DECISION making, *THYMUS

Abstract

Genetic lineage tracing in cell type-specific mouse models of T-cell acute lymphoblastic leukemia (T-ALL) have revealed that tumor cell identity is imposed by expression of the oncogene Lim Domain Only 2 (LMO2), rather than by the target cell phenotype. This approach allowed to identify that secondary genomic alterations, like Notch1 mutations, appeared late and only took place within the thymus during T-ALL development. These concepts are therefore critical for the development of modern therapies aimed at curing T-ALL. [ABSTRACT FROM AUTHOR]

Published

2018