Mutations in TLR/MYD88 pathway identify a subset of young chronic lymphocytic leukemia patients with favorable outcome

被引：94

作者：

Martinez-Trillos, Alejandra ^{[1
]}

Pinyol, Magda ^{[2
]}

Navarro, Alba ^{[2
]}

Aymerich, Marta ^{[1
]}

Jares, Pedro ^{[2
]}

Juan, Manel ^{[3
]}

Rozman, Maria ^{[1
]}

Colomer, Dolors ^{[1
]}

Delgado, Julio ^{[4
]}

Gine, Eva ^{[4
]}

Gonzalez-Diaz, Marcos ^{[5
]}

Hernandez-Rivas, Jesus M. ^{[5
]}

Colado, Enrique ^{[6
]}

Rayon, Consolacion ^{[6
]}

Payer, Angel R. ^{[6
]}

Jose Terol, Maria ^{[7
]}

Navarro, Blanca ^{[7
]}

Quesada, Victor ^{[8
]}

Puente, Xose S. ^{[8
]}

Rozman, Ciril ^{[9
]}

Lopez-Otin, Carlos ^{[8
]}

Campo, Elias ^{[1
,10
]}

Lopez-Guillermo, Armando ^{[4
]}

Villamor, Neus ^{[1
]}

机构：

[1] Hosp Clin Barcelona, Serv Anat Patol, Unitat Hematopatol, IDIBAPS, E-08036 Barcelona, Spain

[2] IDIBAPS, Unitat Genom, Barcelona, Spain

[3] Hosp Clin Barcelona, IDIBAPS, Serv Inmunol, E-08036 Barcelona, Spain

[4] Hosp Clin Barcelona, IDIBAPS, Serv Hematol, E-08036 Barcelona, Spain

[5] Univ Salamanca, Inst Biol Mol & Celular Canc Salamanca, Inst Invest Biomed Salamanca, Serv Hematol,Hosp Clin Univ,Ctr Invest Canc, E-37008 Salamanca, Spain

[6] Hosp Univ Cent Asturias, Serv Hematol, Asturias, Spain

[7] Hosp Clin Valencia, Serv Hematol, Valencia, Spain

[8] Univ Oviedo, Inst Univ Oncol, Dept Bioquim & Biol Mol, Asturias, Spain

[9] Josep Carreras Leukemia Res Inst, Barcelona, Spain

[10] Univ Barcelona, Barcelona, Spain

来源：

BLOOD | 2014年 / 123卷 / 24期

关键词：

TOLL-LIKE RECEPTORS; SF3B1; MUTATIONS; RECURRENT MUTATIONS; REGRESSION-MODELS; SPLICING FACTOR; NOTCH1; EXPRESSION; SURVIVAL; GENE; TRANSFORMATION;

D O I：

10.1182/blood-2013-12-543306

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Mutations in Toll-like receptor (TLR) and myeloid differentiation primary response 88 (MYD88) genes have been found in chronic lymphocytic leukemia (CLL) at low frequency. We analyzed the incidence, clinicobiological characteristics, and outcome of patients with TLR/MYD88 mutations in 587 CLL patients. Twenty-three patients (3.9%) had mutations, 19 in MYD88 (one with concurrent IRAK1 mutation), 2 TLR2 (one with concomitant TLR6 mutation), 1 IRAK1, and 1 TLR5. No mutations were found in IRAK2 and IRAK4. TLR/MYD88-mutated CLL overexpressed genes of the nuclear factor kappa B pathway. Patients with TLR/MYD88 mutations were significantly younger (83% age <= 50 years) than those with no mutations. TLR/MYD88 mutations were the most frequent in young patients. Patients with mutated TLR/MYD88 CLL had a higher frequency of mutated IGHV and low expression of CD38 and ZAP-70. Overall survival (OS) was better in TLR/MYD88-mutated than unmutated patients in the whole series (10-year OS, 100% vs 62%; P = .002), and in the subset of patients age <= 50 years (100% vs 70%; P = .02). In addition, relative OS of TLR/MYD88-mutated patients was similar to that in the age-and gender-matched population. In summary, TLR/MYD88 mutations identify a population of young CLL patients with favorable outcome.

引用

页码：3790 / 3796

页数：7

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