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Time to first treatment and P53 dysfunction in chronic lymphocytic leukaemia: results of the O-CLL1 study in early stage patients
by
Lionetti, Marta
, Colombo, Monica
, Fais, Franco
, Ibatici, Adalberto
, Menichini, Paola
, Fronza, Gilberto
, Morabito, Fortunato
, Matis, Serena
, Fabris, Sonia
, Cutrona, Giovanna
, Speciale, Andrea
, De Luca, Giuseppa
, Neri, Antonino
, Ferrarini, Manlio
, Zupo, Simonetta
, Recchia, Anna Grazia
, Monti, Paola
, Dono, Mariella
, Barbieri, Marzia
, Gentile, Massimo
in
692/308
/ 692/308/2778
/ 692/4017
/ CD38 antigen
/ Chemotherapy
/ Chromosome 17
/ Chronic lymphocytic leukemia
/ Female
/ Gene frequency
/ Genes, p53
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Inactivation
/ Leukemia
/ Leukemia, Lymphocytic, Chronic, B-Cell - genetics
/ Leukemia, Lymphocytic, Chronic, B-Cell - therapy
/ Male
/ Middle Aged
/ multidisciplinary
/ Mutation
/ Notch1 protein
/ Observational studies
/ p53 Protein
/ Patients
/ Prospective Studies
/ Science
/ Science (multidisciplinary)
/ Time-to-Treatment
2020
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Time to first treatment and P53 dysfunction in chronic lymphocytic leukaemia: results of the O-CLL1 study in early stage patients
by
Lionetti, Marta
, Colombo, Monica
, Fais, Franco
, Ibatici, Adalberto
, Menichini, Paola
, Fronza, Gilberto
, Morabito, Fortunato
, Matis, Serena
, Fabris, Sonia
, Cutrona, Giovanna
, Speciale, Andrea
, De Luca, Giuseppa
, Neri, Antonino
, Ferrarini, Manlio
, Zupo, Simonetta
, Recchia, Anna Grazia
, Monti, Paola
, Dono, Mariella
, Barbieri, Marzia
, Gentile, Massimo
in
692/308
/ 692/308/2778
/ 692/4017
/ CD38 antigen
/ Chemotherapy
/ Chromosome 17
/ Chronic lymphocytic leukemia
/ Female
/ Gene frequency
/ Genes, p53
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Inactivation
/ Leukemia
/ Leukemia, Lymphocytic, Chronic, B-Cell - genetics
/ Leukemia, Lymphocytic, Chronic, B-Cell - therapy
/ Male
/ Middle Aged
/ multidisciplinary
/ Mutation
/ Notch1 protein
/ Observational studies
/ p53 Protein
/ Patients
/ Prospective Studies
/ Science
/ Science (multidisciplinary)
/ Time-to-Treatment
2020
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Time to first treatment and P53 dysfunction in chronic lymphocytic leukaemia: results of the O-CLL1 study in early stage patients
by
Lionetti, Marta
, Colombo, Monica
, Fais, Franco
, Ibatici, Adalberto
, Menichini, Paola
, Fronza, Gilberto
, Morabito, Fortunato
, Matis, Serena
, Fabris, Sonia
, Cutrona, Giovanna
, Speciale, Andrea
, De Luca, Giuseppa
, Neri, Antonino
, Ferrarini, Manlio
, Zupo, Simonetta
, Recchia, Anna Grazia
, Monti, Paola
, Dono, Mariella
, Barbieri, Marzia
, Gentile, Massimo
in
692/308
/ 692/308/2778
/ 692/4017
/ CD38 antigen
/ Chemotherapy
/ Chromosome 17
/ Chronic lymphocytic leukemia
/ Female
/ Gene frequency
/ Genes, p53
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Inactivation
/ Leukemia
/ Leukemia, Lymphocytic, Chronic, B-Cell - genetics
/ Leukemia, Lymphocytic, Chronic, B-Cell - therapy
/ Male
/ Middle Aged
/ multidisciplinary
/ Mutation
/ Notch1 protein
/ Observational studies
/ p53 Protein
/ Patients
/ Prospective Studies
/ Science
/ Science (multidisciplinary)
/ Time-to-Treatment
2020
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Time to first treatment and P53 dysfunction in chronic lymphocytic leukaemia: results of the O-CLL1 study in early stage patients
Journal Article
Time to first treatment and P53 dysfunction in chronic lymphocytic leukaemia: results of the O-CLL1 study in early stage patients
2020
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Overview
Chronic lymphocytic leukaemia (CLL) is characterised by a heterogeneous clinical course. Such heterogeneity is associated with a number of markers, including
TP53
gene inactivation. While
TP53
gene alterations determine resistance to chemotherapy, it is not clear whether they can influence early disease progression. To clarify this issue,
TP53
mutations and deletions of the corresponding locus [del(17p)] were evaluated in 469 cases from the O-CLL1 observational study that recruited a cohort of clinically and molecularly characterised Binet stage A patients. Twenty-four cases harboured somatic
TP53
mutations [accompanied by del(17p) in 9 cases], 2 patients had del(17p) only, and 5 patients had
TP53
germ-line variants. While del(17p) with or without
TP53
mutations was capable of significantly predicting the time to first treatment, a reliable measure of disease progression,
TP53
mutations were not. This was true for cases with high or low variant allele frequency. The lack of predictive ability was independent of the functional features of the mutant P53 protein in terms of transactivation and dominant negative potential.
TP53
mutations alone were more frequent in patients with mutated IGHV genes, whereas del(17p) was associated with the presence of adverse prognostic factors, including CD38 positivity, unmutated-IGHV gene status, and NOTCH1 mutations.
Publisher
Nature Publishing Group UK,Nature Publishing Group
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