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Query: UMLS:C0023467 (
acute myeloid leukemia
)
35,200
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Partial deletion of the long arm of chromosome 5, del(5q), is the cytogenetic hallmark of the 5q-syndrome, a distinct subtype of myelodysplastic syndrome-refractory anemia (MDS-RA). Deletions of 5q also occur in the full spectrum of other de novo and therapy-related MDS and
acute myeloid leukemia
(
AML
) types, most often in association with other chromosome abnormalities. However, the loss of genetic material from 5q is believed to be of primary importance in the pathogenesis of all del(5q) disorders. In the present study, we performed fluorescence in situ hybridization (FISH) studies using a chromosome 5-specific whole chromosome painting probe and a 5q subtelomeric probe to determine the incidence of cryptic translocations. We studied archival fixed chromosome suspensions from 36 patients with myeloid disorders (predominantly MDS and
AML
) and del(5q) as the sole abnormality. In 3
AML
patients studied, this identified a translocation of 5q subtelomeric sequences from the del(5q) to the short arm of an apparently normal chromosome 11. FISH with chromosome 11-specific subtelomeric probes confirmed the presence of 11p on the shortened 5q. Further FISH mapping confirmed that the 5q and 11p translocation breakpoints were the same in all 3 cases, between the nucleophosmin (
NPM1
) and fms-related tyrosine kinase 4 (FLT4) genes on 5q35 and the Harvey ras-1-related gene complex (HRC) and the radixin pseudogene (RDPX1) on 11p15.5. Importantly, all 3 patients with the cryptic t(5;11) were children: a total of 3 of 4
AML
children studied. Two were classified as
AML
-M2 and the third was classified as M4. All 3 responded poorly to treatment and had short survival times, ranging from 10 to 18 months. Although del(5q) is rare in childhood AML, this study indicates that, within this subgroup, the incidence of cryptic t(5;11) may be high. It is significant that none of the 24 MDS patients studied, including 11 confirmed as having 5q-syndrome, had the translocation. Therefore, this appears to be a new nonrandom chromosomal translocation, specifically associated with childhood AML with a differentiated blast cell phenotype and the presence of a del(5q).
...
PMID:A new recurrent translocation, t(5;11)(q35;p15.5), associated with del(5q) in childhood acute myeloid leukemia. The UK Cancer Cytogenetics Group (UKCCG) 1039 45
Nucleophosmin (NPM) is a nucleocytoplasmic shuttling protein involved in leukemia-associated chromosomal translocations, and it regulates the alternate reading frame (ARF)-p53 tumor-suppressor pathway. Recently, it has been demonstrated that mutations of the
NPM1
gene alter the protein at its C-terminal, causing its cytoplasmic localization. Cytoplasmic NPM was detected in 35% of adult patients with primary non-French-American-British (FAB) classification M3
acute myeloid leukemia
(
AML
), associated mainly with normal karyotype. We evaluated the prevalence of the
NPM1
gene mutation in non-M3 childhood AML patients enrolled in the ongoing Associazione Italiana di Ematologia e Oncologia Pediatrica (AIEOP-AML02) protocol in Italy.
NPM1
mutations were found in 7 (6.5%) of 107 successfully analyzed patients.
NPM1
-mutated patients carried a normal karyotype (7/26, 27.1%) and were older in age. Thus, the
NPM1
mutation is a frequent abnormality in
AML
patients without known genetic marker; the mutation may represent a new target to monitor minimal residual disease in
AML
and a potential candidate for alternative and targeted treatments.
...
PMID:Nucleophosmin mutations in childhood acute myelogenous leukemia with normal karyotype. 1587 Jan 72
Recently, somatic mutations of the nucleophosmin gene (
NPM1
), which alter the subcellular localization of the product, have been reported in
acute myeloid leukemia
(
AML
). We analyzed the clinical significance of
NPM1
mutations in comparison with cytogenetics, FLT3, NRAS, and TP53 mutations, and a partial tandem duplication of the MLL gene (MLL-TD) in 257 patients with
AML
. We found
NPM1
mutations, including 4 novel sequence variants, in 64 of 257 (24.9%) patients.
NPM1
mutations were associated with normal karyotype and with internal tandem duplication (ITD) and D835 mutations in FLT3, but not with other mutations. In 190 patients without the M3 French-American-British (FAB) subtype who were treated with the protocol of the Japan Adult Leukemia Study Group, multivariate analyses showed that the
NPM1
mutation was a favorable factor for achieving complete remission but was associated with a high relapse rate. Sequential analysis using 39 paired samples obtained at diagnosis and relapse showed that
NPM1
mutations were lost at relapse in 2 of the 17 patients who had
NPM1
mutations at diagnosis. These results suggest that the
NPM1
mutation is not necessarily an early event during leukemogenesis or that leukemia clones with
NPM1
mutations are sensitive to chemotherapy.
...
PMID:Clinical characteristics and prognostic implications of NPM1 mutations in acute myeloid leukemia. 1599 85
Nucleophosmin (
NPM1
) exon-12 gene mutations are the hallmark of a large
acute myelogenous leukemia
(
AML
) subgroup with normal karyotype, but their prognostic value in this
AML
subset has not yet been determined. We screened 401
AML
patients with normal karyotype treated within the German
AML
Cooperative Group Protocol 99 (AMLCG99) study for
NPM1
mutations. Results were related with partial tandem duplications within the MLL gene (MLL-PTD), Fms-like tyrosine kinase 3-length mutations (FLT3-LM), the tyrosine kinase domain of FLT3 (FLT3-TKD), NRAS, KIT, and CEBPA mutations and with clinical characteristics and outcome.
NPM1
mutations were detected in 212 (52.9%) of 401 patients. Fourteen mutations, including 8 new variants, were identified.
NPM1
-mutated cases associated frequently with FLT3 mutations but rarely with other mutations. The
NPM1
-mutated group had a higher complete remission (CR) rate (70.5% vs 54.7%, P = .003), a trend to a longer overall survival (OS; median 1012 vs 549 days, P = .076), and significantly longer event-free survival (EFS; median 428 vs 336 days; P = .012). The favorable impact of
NPM1
mutations on OS and EFS clearly emerged in the large group (264 [66.8%] of 395 cases) of normal-karyotype
AML
without FLT3-LM. This positive effect was lost in the presence of a concomitant FLT3-LM, since survival of the NPM1+/FLT3-LM+ double positive was similar to
NPM1
-/FLT3-LM+ cases. In conclusion, this study demonstrates that NPM1+/FLT3-LM- mutations are an independent predictor for a favorable outcome in
AML
with normal karyotype.
...
PMID:Nucleophosmin gene mutations are predictors of favorable prognosis in acute myelogenous leukemia with a normal karyotype. 1607 67
Mutations in nucleophosmin
NPM1
are the most frequent acquired molecular abnormalities in
acute myeloid leukemia
(
AML
). We determined the
NPM1
mutation status in a clinically and molecularly well-characterized patient cohort of 275 patients with newly diagnosed
AML
by denaturing high-performance liquid chromatography (dHPLC). We show that
NPM1
mutations are significantly underrepresented in patients younger than 35 years.
NPM1
mutations positively correlate with
AML
with high white blood cell counts, normal karyotypes, and fms-like tyrosine kinase-3 gene (FLT3) internal tandem duplication (ITD) mutations.
NPM1
mutations associate inversely with the occurrence of CCAAT/enhancer-binding protein-alpha (CEBPA) and NRAS mutations. With respect to gene expression profiling, we show that
AML
cases with an
NPM1
mutation cluster in specific subtypes of
AML
with previously established gene expression signatures, are highly associated with a homeobox gene-specific expression signature, and can be predicted with high accuracy. We demonstrate that patients with intermediate cytogenetic risk
AML
without FLT3 ITD mutations but with
NPM1
mutations have a significantly better overall survival (OS) and event-free survival (EFS) than those without
NPM1
mutations. Finally, in multivariable analysis
NPM1
mutations express independent favorable prognostic value with regard to OS, EFS, and disease-free survival (DFS).
...
PMID:Mutations in nucleophosmin (NPM1) in acute myeloid leukemia (AML): association with other gene abnormalities and previously established gene expression signatures and their favorable prognostic significance. 1610 76
Mutations of the nucleophosmin (
NPM1
) gene have recently been described in patients with
acute myeloid leukemia
(
AML
). To clarify the prevalence as well as the clinical impact of this mutation, we investigated 1485 patients with
AML
for
NPM1
exon 12 mutations using fragment analysis. A 4 bp insert was detected in 408 of 1485 patients (27.5%). Sequence analysis revealed known mutations (type A, B, and D) as well as 13 novel alterations in 229 analyzed cases.
NPM1
mutations were most prevalent in patients with normal karyotype (NK) (324 of 709; 45.7%) compared with 58 of 686 with karyotype abnormalities (8.5%; P < .001) and were significantly associated with several clinical parameters (high bone marrow [BM] blasts, high white blood cell [WBC] and platelet counts, female sex).
NPM1
alterations were associated with FLT3-ITD mutations, even if restricted to patients with NK (
NPM1
-mut/FLT3-ITD: 43.8%; versus
NPM1
-wt/FLT3-ITD: 19.9%; P < .001). The analysis of the clinical impact in 4 groups (
NPM1
and FLT3-ITD single mutants, double mutants, and wild-type [wt] for both) revealed that patients having only an
NPM1
mutation had a significantly better overall and disease-free survival and a lower cumulative incidence of relapse. In conclusion,
NPM1
mutations represent a common genetic abnormality in adult AML. If not associated with FLT3-ITD mutations, mutant
NPM1
appears to identify patients with improved response toward treatment.
...
PMID:Prevalence and prognostic impact of NPM1 mutations in 1485 adult patients with acute myeloid leukemia (AML). 1645 56
Mutations in exon 12 of the nucleophosmin (
NPM1
) gene occur in about 60% of adult AML with normal karyotype. By exploiting a specific feature of
NPM1
mutants, that is insertion at residue 956 or deletion/insertion at residue 960, we developed highly sensitive, real-time quantitative (RQ) polymerase chain reaction (PCR) assays, either in DNA or RNA, that are specific for various
NPM1
mutations. In all 13
AML
patients carrying
NPM1
mutations at diagnosis, cDNA RQ-PCR showed >30 000 copies of
NPM1
-mutated transcript. A small or no decrease in copies was observed in three patients showing partial or no response to induction therapy. The number of
NPM1
-mutated copies was markedly reduced in 10 patients achieving complete hematological remission (five cases: <100 copies; five cases: 580-5046 copies). In four patients studied at different time intervals, the number of
NPM1
copies closely correlated with clinical status and predicted impending hematological relapse in two. Thus, reliable, sensitive RQ-PCR assays for
NPM1
mutations can now monitor and quantify MRD in
AML
patients with normal karyotype and
NPM1
gene mutations.
...
PMID:Quantitative assessment of minimal residual disease in acute myeloid leukemia carrying nucleophosmin (NPM1) gene mutations. 1654 Nov 44
To determine whether gene expression profiling could improve risk classification and outcome prediction in older
acute myeloid leukemia
(
AML
) patients, expression profiles were obtained in pretreatment leukemic samples from 170 patients whose median age was 65 years. Unsupervised clustering methods were used to classify patients into 6 cluster groups (designated A to F) that varied significantly in rates of resistant disease (RD; P < .001), complete response (CR; P = .023), and disease-free survival (DFS; P = .023). Cluster A (n = 24), dominated by
NPM1
mutations (78%), normal karyotypes (75%), and genes associated with signaling and apoptosis, had the best DFS (27%) and overall survival (OS; 25% at 5 years). Patients in clusters B (n = 22) and C (n = 31) had the worst OS (5% and 6%, respectively); cluster B was distinguished by the highest rate of RD (77%) and multidrug resistant gene expression (ABCG2, MDR1). Cluster D was characterized by a "proliferative" gene signature with the highest proportion of detectable cytogenetic abnormalities (76%; including 83% of all favorable and 34% of unfavorable karyotypes). Cluster F (n = 33) was dominated by monocytic leukemias (97% of cases), also showing increased
NPM1
mutations (61%). These gene expression signatures provide insights into novel groups of
AML
not predicted by traditional studies that impact prognosis and potential therapy.
...
PMID:Gene expression profiling of adult acute myeloid leukemia identifies novel biologic clusters for risk classification and outcome prediction. 1659 96
NPM1
gene mutations are the most frequent genetic lesion in the 60% of adult acute myeloid leukemias (AMLs) with normal karyotype and no evidence of typical fusion genes (BCR/ABL1, PML/RARA, AML1/ETO, CBFB/MYH11, DEK/CAN). Using direct sequencing we previously identified six different heterozygous mutants within exon 12 encoding the nucleophosmin C-terminus. Because of these mutations the shuttling protein nucleophosmin is aberrantly delocalized in the cytoplasm of leukemic cells (NPMc+). Here, we designed and tested a denaturing high-performance liquid chromatography (DHPLC) assay to detect
NPM1
mutated variants. To assess specificity, sensitivity, reliability, and reproducibility, we analyzed DNA from 120 primary adult AMLs and compared DHPLC results with immunohistochemistry and sequencing. All electropherogram profiles in the 26 NPMc+ leukemias were different from the wild type, indicating 100% sensitivity. Sequencing categorized mutations A, B, and D, and all mutation A cases gave identical elution profiles. The other mutations showed typical chromatograms, with mutations B and D differing for one nucleotide. Elution profiles and sequencing also identified four new variants. Our results suggest that DHPLC detects NPM1mutations as well as direct sequencing and immunohistochemistry, providing a helpful approach in the diagnosis of NPMc+
AML
.
...
PMID:Denaturing high-performance liquid chromatography: a valid approach for identifying NPM1 mutations in acute myeloid leukemia. 1664 13
Mutations at exon 12 of the nucleophosmin (
NPM1
) gene are the most frequent acquired molecular abnormalities in adult and pediatric
acute myeloid leukaemia
(
AML
) with normal karyotype. We screened 28 patients with new diagnosed primary
AML
with normal karyotype, 38 patients with myelodysplastic symdromes (MDS) and 19 healthy volunteer for mutations at exon 12 of
NPM1
gene.
NPM1
mutations were identified in four
AML
patients and two MDS patients, including one novel sequence variant. As far as we know, this is the first report of
NPM1
mutation in patients with MDS in the English literature until now, and our primary data support that
NPM1
mutations may be also involved in the pathogenesis of MDS.
...
PMID:NPM1 mutations in myelodysplastic syndromes and acute myeloid leukemia with normal karyotype. 1667 98
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