Incidence, clinical and biological characteristics and outcome of secondary acute lymphoblastic leukemia after solid organ or hematologic malignancy

Acute lymphoblastic leukemia (ALL) following solid organ or hematologic malignancy (secondary ALL, s-ALL) is not well characterized. We analyzed the characteristics and outcome of patients with s-ALL and compared them with those of patients with de novo- ALL. Of 448 patients, 24 (5%) had previous ne...

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Published inLeukemia & lymphoma Vol. 57; no. 1; pp. 86 - 91
Main Authors Kelleher, Nicholas, Gallardo, David, González-Campos, José, Hernández-Rivas, Jesús M., Montesinos, Pau, Sarrá, Josep, Gil, Cristina, Barba, Pere, Guàrdia, Ramon, Brunet, Salut, Bernal, Teresa, Martínez, Maria-Pilar, Abella, Eugènia, Bermúdez, Arantxa, Sánchez-Delgado, Magdalena, Antònia, Cladera, Gayoso, Jorge, Calbacho, María, Ribera, Josep-Maria
Format Journal Article
LanguageEnglish
Published United States 02.01.2016
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ISSN1042-8194
1029-2403
1026-8022
1029-2403
DOI10.3109/10428194.2015.1040013

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Summary:Acute lymphoblastic leukemia (ALL) following solid organ or hematologic malignancy (secondary ALL, s-ALL) is not well characterized. We analyzed the characteristics and outcome of patients with s-ALL and compared them with those of patients with de novo- ALL. Of 448 patients, 24 (5%) had previous neoplasia. Sixteen patients had received previous cytotoxic therapy (therapy-associated ALL, t-ALL), and eight had not (antecedent-malignancy ALL, am-ALL). Except for more advanced age in patients with s-ALL, no statistically significant differences were observed in WBC count, CNS involvement, immunophenotype or cytogenetics between the groups, nor in complete remission (t-ALL: 94%; am-ALL: 75%; de novo-ALL: 85%), 3-year remission duration (58%; 50%; 72%), overall survival (71%; 38%; 60%) or event-free survival (53%, 38%; 53%). Our study did not show poor clinical or cytogenetic features or inferior outcome in ALL patients with antecedent neoplastic disease, irrespective of the type of treatment received for the neoplasia.
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ISSN:1042-8194
1029-2403
1026-8022
1029-2403
DOI:10.3109/10428194.2015.1040013