m7FLIPI and targeted sequencing in high-risk follicular lymphoma

Marc Sorigue; Anna Oliveira; Santiago Mercadal; Gustavo Tapia; Fina Climent; Laia Perez-Roca; Irian Lorences; Eva Domingo-Domenech; Marta Cabezon; Jose Tomas Navarro; Eva Gonzalez-Barca; Lurdes Zamora; Josep María Ribera; Anna Sureda; Maria Pilar Armengol; Juan Manuel Sancho

doi:10.1002/hon.2674

m7FLIPI and targeted sequencing in high-risk follicular lymphoma

Marc Sorigue, Anna Oliveira, Santiago Mercadal, Gustavo Tapia, Fina Climent, Laia Perez-Roca, Irian Lorences, Eva Domingo-Domenech, Marta Cabezon, Jose Tomas Navarro, Eva Gonzalez-Barca, Lurdes Zamora, Josep María Ribera, Anna Sureda, Maria Pilar Armengol, Juan Manuel Sancho^*

^*Autor corresponent d’aquest treball

Producció científica: Contribució a revista › Article › Recerca › Avaluat per experts

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Resum

Patients with follicular lymphoma (FL) refractory to front-line immunochemotherapy (ICT) have a poor overall survival (OS). Gene mutation analysis may be more accurate than classical risk factors to pick out these patients before treatment. This study aimed to describe the prevalence of selected genetic mutations in a cohort of patients with high-risk FL. Twenty-five patients with FL refractory to front-line ICT and 10 non-refractory patients matched for age, sex, and FLIPI score were included. We sequenced 18 genes (custom targeted sequencing panel) previously reported to potentially have prognostic impact, including the seven genes necessary to determine m7FLIPI risk. The 35 patients had a median age of 62. The FLIPI and FLIPI2 were high in 27 (84%) and 14 (48%), respectively. Three-year progression-free survival (PFS) and OS probabilities were 25% (95% CI, 13%-41%) and 53% (34%-69%), respectively. There were 73 variants in the 18 genes among the 35 patients. The median number of mutations per patient was 1 (interquartile range, 0-3). The most commonly mutated genes were CREBBP (11 of 35, 31%) and EP300 (10 of 35, 29%). EP300 mutations were associated with refractoriness to treatment (10 of 25 among refractory and 0 of 10 among non-refractory). In conclusion, in this study, patients with high-risk follicular lymphoma were genetically heterogeneous.

Idioma original	Anglès nord-americà
Pàgines (de-a)	564-568
Nombre de pàgines	5
Revista	Hematological Oncology
Volum	37
Número	5
DOIs	https://doi.org/10.1002/hon.2674
Estat de la publicació	Publicada - 1 de des. 2019

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10.1002/hon.2674

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Sorigue, M., Oliveira, A., Mercadal, S., Tapia, G., Climent, F., Perez-Roca, L., Lorences, I., Domingo-Domenech, E., Cabezon, M., Navarro, J. T., Gonzalez-Barca, E., Zamora, L., Ribera, J. M., Sureda, A., Armengol, M. P., & Sancho, J. M. (2019). m7FLIPI and targeted sequencing in high-risk follicular lymphoma. Hematological Oncology, 37(5), 564-568. https://doi.org/10.1002/hon.2674

@article{1efd52c890a84ee79b03409dd7e8a359,

title = "m7FLIPI and targeted sequencing in high-risk follicular lymphoma",

abstract = "Patients with follicular lymphoma (FL) refractory to front-line immunochemotherapy (ICT) have a poor overall survival (OS). Gene mutation analysis may be more accurate than classical risk factors to pick out these patients before treatment. This study aimed to describe the prevalence of selected genetic mutations in a cohort of patients with high-risk FL. Twenty-five patients with FL refractory to front-line ICT and 10 non-refractory patients matched for age, sex, and FLIPI score were included. We sequenced 18 genes (custom targeted sequencing panel) previously reported to potentially have prognostic impact, including the seven genes necessary to determine m7FLIPI risk. The 35 patients had a median age of 62. The FLIPI and FLIPI2 were high in 27 (84%) and 14 (48%), respectively. Three-year progression-free survival (PFS) and OS probabilities were 25% (95% CI, 13%-41%) and 53% (34%-69%), respectively. There were 73 variants in the 18 genes among the 35 patients. The median number of mutations per patient was 1 (interquartile range, 0-3). The most commonly mutated genes were CREBBP (11 of 35, 31%) and EP300 (10 of 35, 29%). EP300 mutations were associated with refractoriness to treatment (10 of 25 among refractory and 0 of 10 among non-refractory). In conclusion, in this study, patients with high-risk follicular lymphoma were genetically heterogeneous.",

keywords = "EP300, follicular lymphoma, m7FLIPI, prognosis, refractoriness, sequencing, TP53",

author = "Marc Sorigue and Anna Oliveira and Santiago Mercadal and Gustavo Tapia and Fina Climent and Laia Perez-Roca and Irian Lorences and Eva Domingo-Domenech and Marta Cabezon and Navarro, {Jose Tomas} and Eva Gonzalez-Barca and Lurdes Zamora and Ribera, {Josep Mar{\'i}a} and Anna Sureda and Armengol, {Maria Pilar} and Sancho, {Juan Manuel}",

note = "Funding Information: This study was funded by the clinical research unit ICO‐Badalona. Funding Information: Anna Sureda reports consultancy, advisory board, travel grants, and educational activities/symposia for Takeda; consultancy, advisory board, travel grants, and educational activities/symposia for BMS; advisory board and educational activities/symposia for MDS; travel grants from Roche; advisory boards and travel grants from Celgene; travel grants and advisory board for Janssen; travel grants and advisory boards for Sanofi; advisory board and consultancy for Gilead; and advisory board and consultancy for Novartis. Juan‐Manuel Sancho reports advisory boards for Roche, Gilead, Janssen, Celgene, BMS, Kern Pharma, and Celltrion; speaker's honoraria from Roche, Gilead, Janssen, Kern, Mundipharma, Novartis, Celgene, Kern Pharma, Celltrion, Sanofi, and Servier; consultancy for Sandoz and Celgene; and financial support for clinical research from TEVA and Gilead. Eva Domingo reports advisory board for Takeda and BMS; consultancy for Takeda; and travel expenses from Takeda, BMS, and Roche. All other authors report no potential conflicts of interest. Publisher Copyright: {\textcopyright}2019 John Wiley & Sons, Ltd. Copyright: Copyright 2020 Elsevier B.V., All rights reserved.",

year = "2019",

month = dec,

day = "1",

doi = "10.1002/hon.2674",

language = "Ingl{\'e}s estadounidense",

volume = "37",

pages = "564--568",

journal = "Hematological Oncology",

issn = "0278-0232",

publisher = "John Wiley and Sons Ltd",

number = "5",

}

Sorigue, M, Oliveira, A, Mercadal, S, Tapia, G, Climent, F, Perez-Roca, L, Lorences, I, Domingo-Domenech, E, Cabezon, M, Navarro, JT, Gonzalez-Barca, E, Zamora, L, Ribera, JM, Sureda, A, Armengol, MP & Sancho, JM 2019, 'm7FLIPI and targeted sequencing in high-risk follicular lymphoma', Hematological Oncology, vol. 37, núm. 5, pàg. 564-568. https://doi.org/10.1002/hon.2674

TY - JOUR

T1 - m7FLIPI and targeted sequencing in high-risk follicular lymphoma

AU - Sorigue, Marc

AU - Oliveira, Anna

AU - Mercadal, Santiago

AU - Tapia, Gustavo

AU - Climent, Fina

AU - Perez-Roca, Laia

AU - Lorences, Irian

AU - Domingo-Domenech, Eva

AU - Cabezon, Marta

AU - Navarro, Jose Tomas

AU - Gonzalez-Barca, Eva

AU - Zamora, Lurdes

AU - Ribera, Josep María

AU - Sureda, Anna

AU - Armengol, Maria Pilar

AU - Sancho, Juan Manuel

N1 - Funding Information: This study was funded by the clinical research unit ICO‐Badalona. Funding Information: Anna Sureda reports consultancy, advisory board, travel grants, and educational activities/symposia for Takeda; consultancy, advisory board, travel grants, and educational activities/symposia for BMS; advisory board and educational activities/symposia for MDS; travel grants from Roche; advisory boards and travel grants from Celgene; travel grants and advisory board for Janssen; travel grants and advisory boards for Sanofi; advisory board and consultancy for Gilead; and advisory board and consultancy for Novartis. Juan‐Manuel Sancho reports advisory boards for Roche, Gilead, Janssen, Celgene, BMS, Kern Pharma, and Celltrion; speaker's honoraria from Roche, Gilead, Janssen, Kern, Mundipharma, Novartis, Celgene, Kern Pharma, Celltrion, Sanofi, and Servier; consultancy for Sandoz and Celgene; and financial support for clinical research from TEVA and Gilead. Eva Domingo reports advisory board for Takeda and BMS; consultancy for Takeda; and travel expenses from Takeda, BMS, and Roche. All other authors report no potential conflicts of interest. Publisher Copyright: ©2019 John Wiley & Sons, Ltd. Copyright: Copyright 2020 Elsevier B.V., All rights reserved.

PY - 2019/12/1

Y1 - 2019/12/1

N2 - Patients with follicular lymphoma (FL) refractory to front-line immunochemotherapy (ICT) have a poor overall survival (OS). Gene mutation analysis may be more accurate than classical risk factors to pick out these patients before treatment. This study aimed to describe the prevalence of selected genetic mutations in a cohort of patients with high-risk FL. Twenty-five patients with FL refractory to front-line ICT and 10 non-refractory patients matched for age, sex, and FLIPI score were included. We sequenced 18 genes (custom targeted sequencing panel) previously reported to potentially have prognostic impact, including the seven genes necessary to determine m7FLIPI risk. The 35 patients had a median age of 62. The FLIPI and FLIPI2 were high in 27 (84%) and 14 (48%), respectively. Three-year progression-free survival (PFS) and OS probabilities were 25% (95% CI, 13%-41%) and 53% (34%-69%), respectively. There were 73 variants in the 18 genes among the 35 patients. The median number of mutations per patient was 1 (interquartile range, 0-3). The most commonly mutated genes were CREBBP (11 of 35, 31%) and EP300 (10 of 35, 29%). EP300 mutations were associated with refractoriness to treatment (10 of 25 among refractory and 0 of 10 among non-refractory). In conclusion, in this study, patients with high-risk follicular lymphoma were genetically heterogeneous.

AB - Patients with follicular lymphoma (FL) refractory to front-line immunochemotherapy (ICT) have a poor overall survival (OS). Gene mutation analysis may be more accurate than classical risk factors to pick out these patients before treatment. This study aimed to describe the prevalence of selected genetic mutations in a cohort of patients with high-risk FL. Twenty-five patients with FL refractory to front-line ICT and 10 non-refractory patients matched for age, sex, and FLIPI score were included. We sequenced 18 genes (custom targeted sequencing panel) previously reported to potentially have prognostic impact, including the seven genes necessary to determine m7FLIPI risk. The 35 patients had a median age of 62. The FLIPI and FLIPI2 were high in 27 (84%) and 14 (48%), respectively. Three-year progression-free survival (PFS) and OS probabilities were 25% (95% CI, 13%-41%) and 53% (34%-69%), respectively. There were 73 variants in the 18 genes among the 35 patients. The median number of mutations per patient was 1 (interquartile range, 0-3). The most commonly mutated genes were CREBBP (11 of 35, 31%) and EP300 (10 of 35, 29%). EP300 mutations were associated with refractoriness to treatment (10 of 25 among refractory and 0 of 10 among non-refractory). In conclusion, in this study, patients with high-risk follicular lymphoma were genetically heterogeneous.

KW - EP300

KW - follicular lymphoma

KW - m7FLIPI

KW - prognosis

KW - refractoriness

KW - sequencing

KW - TP53

UR - http://www.scopus.com/inward/record.url?scp=85074565933&partnerID=8YFLogxK

U2 - 10.1002/hon.2674

DO - 10.1002/hon.2674

M3 - Artículo

C2 - 31475375

AN - SCOPUS:85074565933

SN - 0278-0232

VL - 37

SP - 564

EP - 568

JO - Hematological Oncology

JF - Hematological Oncology

IS - 5

ER -

m7FLIPI and targeted sequencing in high-risk follicular lymphoma

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