Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Mutation frequencies of SF3B1 (9·7%), NOTCH1 (8·6%), BIRC3 (1·1%), ATM (16·9%) or TP53 (8·1%), and frequencies of cytogenetic abnormalities including trisomy 12 (18·6%), del(17p) (10·4%), del(13q) (43·7%) and IGH translocation (10·1%) were comparable to those reported from Western countries, except del(11q) (6·9%) which was lower in our patients.
|
31230372 |
2019 |
Congenital chromosomal disease
|
0.100 |
Biomarker
|
group |
BEFREE |
Cases with mutated and unmutated IGHV status showed increased CA and MN frequencies compared to controls (P ≤ 0.0007), but no differences between both groups were found.
|
31037299 |
2019 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
The data on cytogenetic aberrations (11q22, 13q14, trisomy 12) and IGHV mutation status were also considered in PFS analyses.
|
31054420 |
2019 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Of 6 AL patients with MM, 5 (83%) patients had cytogenetic abnormalities: 1q gain (4/6, 67%), gains of chromosome 9 (3/6, 50%), IGH rearrangement and RB1 (13q) deletions (2/6 each, 33%).
|
27015231 |
2016 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Prognostic factors such as chromosome abnormalities (trisomy 12, 11q deletions and 17p deletions), β2 microglobulin, thymidine kinase, CD38 and ZAP-70 expression, IGHV mutation status, and mutations in genes such as NOTCH1, MYD88, SF3B1, and ATM are also predictors of prognosis.
|
27742074 |
2016 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
In the overall patient population, prognostic parameters such as IGHV gene mutational status (P < .0001), CD38 expression (P < .0001), 70-kDa zeta-associated protein (ZAP-70) expression (P < .0001), and cytogenetic abnormalities (P = .01) predicted for TTFT on univariate analysis.
|
25445470 |
2015 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Multiprobe FISH detected the chromosomal aberrations identified by G-banding, as well as additional aberrations in 6 of 30 (20.0%) cases, which included ETV6/RUNX1 translocation, p16 deletion, TP53 deletion, and IGH break-apart.
|
24790906 |
2014 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Differences related to the expression of 25 miRNAs were found to be independent from IGHV mutation status or cytogenetic aberrations.
|
24916701 |
2014 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Ten patients (45%) showed cytogenetic aberrations using FISH: 6q deletion in eight (37%) and IGH rearrangement in four (18%).
|
24895570 |
2014 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
IGHV-mutated cases were significantly more frequent among cMBLs (P = 0.005), whereas the distribution of CD38 and ZAP-70 positive cases, of patients with NOTCH1 and SF3B1 mutations or exhibiting the major CLL cytogenetic abnormalities, was similar in the two groups.
|
24036852 |
2013 |
Congenital chromosomal disease
|
0.100 |
Biomarker
|
group |
BEFREE |
In our cohort of 104 untreated patients carrying +12, NOTCH1 mutations occurred in 24% of cases and were associated to unmutated IGHV genes (P=0.003) and +12 as a sole cytogenetic abnormality (P=0.008).
|
22207691 |
2012 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
CCND1-IGH@ translocation is considered pathognomonic of mantle cell lymphoma (MCL), as this distinct chromosomal abnormality has not been reported in any other subtypes of mature B-cell lymphoma.
|
21677543 |
2011 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
On pooled multivariable analysis of patients in both cohorts adjusting for age, sex, Rai stage, CD38 status, ZAP-70 status, immunoglobulin heavy chain variable (IGHV) gene mutation status, CD49d status, and cytogenetic abnormalities assessed by interphase fluorescent in situ hybridization testing, 25(OH)D insufficiency remained an independent predictor of TTT (HR = 1.47; P = .008), although the association with OS was not significant (HR = 1.47; P = .07).
|
21048153 |
2011 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
The t(14;19)(q32;q13) involving the IGH@ and BCL3 loci is an infrequent cytogenetic abnormality detected in B-cell malignancies.
|
21502423 |
2011 |
Congenital chromosomal disease
|
0.100 |
Biomarker
|
group |
BEFREE |
In recent years, major attention was drawn to the significance of chromosomal aberrations involving chromosome arm 13q and the IGH region on chromosome band 14q32 as a prognostic indicator in MM.
|
19787791 |
2010 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Clinical features and molecular/biologic factors such as ZAP-70, immunoglobulin heavy chain (IGHV) gene mutation status, and cytogenetic abnormalities on fluorescent in situ hybridization (FISH) have been found to be robust predictors of treatment-free survival and overall survival among newly diagnosed patients.
|
20008228 |
2009 |
Congenital chromosomal disease
|
0.100 |
GeneticVariation
|
group |
BEFREE |
We evaluated its relevance as independent prognosticator for overall survival and time to treatment (TTT) in a series of 303 (232 for TTT) CLLs, in comparison with other biologic or clinical prognosticators (CD38, ZAP-70, immunoglobulin variable heavy chain (IGHV) gene status, cytogenetic abnormalities, soluble CD23, beta2-microglobulin, Rai staging).
|
17959854 |
2008 |
Congenital chromosomal disease
|
0.100 |
Biomarker
|
group |
BEFREE |
Probes for 13q14 (D13S319), 17p13 (p53), the centromere of chromosome 12 (CEP12), and 14q32 (IGHC/IGHV) were applied to detect chromosomal aberrations in peripheral blood samples from 83 B-CLL patients (60 men, 23 women).
|
17562621 |
2007 |
Congenital chromosomal disease
|
0.100 |
Biomarker
|
group |
BEFREE |
The cytogenetic abnormalities that are found in chronic lymphoid malignancies (and in acute leukemias deriving from relatively mature cells) fall mainly into two groups according to whether the malignant cells are of B-lineage or T-lineage.In most of the B-lineage cases. there is some abnormality of the IgH gene which is located at 14q32 or, less frequently, the other immunoglobulin genes located at 2p12 and 22q11.
|
12744209 |
2003 |