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Mutational Landscape of CEBPA in Mexican Pediatric Acute Myeloid Leukemia Patients: Prognostic Implications.
Molina Garay, Carolina; Carrillo Sánchez, Karol; Flores Lagunes, Luis Leonardo; Jiménez Olivares, Marco; Muñoz Rivas, Anallely; Villegas Torres, Beatríz Eugenia; Flores Aguilar, Hilario; Núñez Enríquez, Juan Carlos; Jiménez Hernández, Elva; Bekker Méndez, Vilma Carolina; Torres Nava, José Refugio; Flores Lujano, Janet; Martín Trejo, Jorge Alfonso; Mata Rocha, Minerva; Medina Sansón, Aurora; Espinoza Hernández, Laura Eugenia; Peñaloza Gonzalez, José Gabriel; Espinosa Elizondo, Rosa Martha; Flores Villegas, Luz Victoria; Amador Sanchez, Raquel; Pérez Saldívar, María Luisa; Sepúlveda Robles, Omar Alejandro; Rosas Vargas, Haydeé; Jiménez Morales, Silvia; Galindo Delgado, Patricia; Mejía Aranguré, Juan Manuel; Alaez Verson, Carmen.
Affiliation
  • Molina Garay C; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Carrillo Sánchez K; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Flores Lagunes LL; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Jiménez Olivares M; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Muñoz Rivas A; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Villegas Torres BE; Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
  • Flores Aguilar H; Instituto de Diagnóstico y Referencia Epidemiológicos (InDRE), Mexico City, Mexico.
  • Núñez Enríquez JC; Unidad de Investigación Médica en Epidemiología Clínica, UMAE Hospital de Pediatría, Centro Médico Nacional "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Jiménez Hernández E; Servicio de Hematología Pediátrica, Hospital General "Gaudencio González Garza", Centro Médico Nacional (CMN) "La Raza", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Bekker Méndez VC; Unidad de Investigación Médica en Inmunología e Infectología, Hospital de Infectología "Dr. Daniel Méndez Hernández", "La Raza", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Torres Nava JR; Servicio de Oncología, Hospital Pediátrico de Moctezuma, Secretaria de Salud del D.F., Mexico City, Mexico.
  • Flores Lujano J; Unidad de Investigación Médica en Epidemiología Clínica, UMAE Hospital de Pediatría, Centro Médico Nacional "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Martín Trejo JA; Servicio de Hematología Pediátrica, UMAE Hospital de Pediatría, Centro Médico Nacional (CMN) "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Mata Rocha M; Unidad de Investigación Médica en Epidemiología Clínica, UMAE Hospital de Pediatría, Centro Médico Nacional "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Medina Sansón A; Servicio de Hemato-Oncología, Hospital Infantil de México Federico Gómez, Secretaria de Salud (SSa), Mexico City, Mexico.
  • Espinoza Hernández LE; Unidad de Investigación Médica en Epidemiología Clínica, UMAE Hospital de Pediatría, Centro Médico Nacional "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Peñaloza Gonzalez JG; Servicio de Onco-Pediatría, Hospital Juárez de México, Secretaria de Salud (SSa), Mexico City, Mexico.
  • Espinosa Elizondo RM; Servicio de Hematología Pediátrica, Hospital General de México, Secretaria de Salud (SSa), Mexico City, Mexico.
  • Flores Villegas LV; Servicio de Hematología Pediátrica, Centro Médico Nacional (CMN) "20 de Noviembre", Instituto de Seguridad Social al Servicio de los Trabajadores del Estado (ISSSTE), Mexico City, Mexico.
  • Amador Sanchez R; Hospital General Regional No. 1 "Carlos McGregor Sánchez Navarro", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Pérez Saldívar ML; Unidad de Investigación Médica en Epidemiología Clínica, UMAE Hospital de Pediatría, Centro Médico Nacional "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Sepúlveda Robles OA; Unidad de Investigación Médica en Genética Humana, UMAE Hospital de Pediatría, Centro Médico Nacional (CMN) "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Rosas Vargas H; Unidad de Investigación Médica en Genética Humana, UMAE Hospital de Pediatría, Centro Médico Nacional (CMN) "Siglo XXI", Instituto Mexicano del Seguro Social (IMSS), Mexico City, Mexico.
  • Jiménez Morales S; Laboratorio de Genómica del Cáncer, Instituto Nacional de Medicina Genómica (Inmegen), Mexico City, Mexico.
  • Galindo Delgado P; Hospital Central Sur de Alta Especialidad de Pemex, Mexico City, Mexico.
  • Mejía Aranguré JM; Laboratorio de Genómica del Cáncer, Instituto Nacional de Medicina Genómica (Inmegen), Mexico City, Mexico.
  • Alaez Verson C; Facultad de Medicina, Universidad Nacional Autónoma de México, Mexico City, Mexico.
Front Pediatr ; 10: 899742, 2022.
Article in En | MEDLINE | ID: mdl-35967564
ABSTRACT

Background:

In Mexico, the incidence of acute myeloid leukemia (AML) has increased in the last few years. Mortality is higher than in developed countries, even though the same chemotherapy protocols are used. CCAAT Enhancer Binding Protein Alpha (CEBPA) mutations are recurrent in AML, influence prognosis, and help to define treatment strategies. CEBPA mutational profiles and their clinical implications have not been evaluated in Mexican pediatric AML patients. Aim of the Study To identify the mutational landscape of the CEBPA gene in pediatric patients with de novo AML and assess its influence on clinical features and overall survival (OS). Materials and

Methods:

DNA was extracted from bone marrow aspirates at diagnosis. Targeted massive parallel sequencing of CEBPA was performed in 80 patients.

Results:

CEBPA was mutated in 12.5% (10/80) of patients. Frameshifts at the N-terminal region were the most common mutations 57.14% (8/14). CEBPA biallelic (CEBPA BI) mutations were identified in five patients. M2 subtype was the most common in CEBPA positive patients (CEBPA POS) (p = 0.009); 50% of the CEBPA POS patients had a WBC count > 100,000 at diagnosis (p = 0.004). OS > 1 year was significantly better in CEBPA negative (CEBPA NEG) patients (p = 0.0001). CEBPA POS patients (either bi- or monoallelic) had a significantly lower OS (p = 0.002). Concurrent mutations in FLT3, CSF3R, and WT1 genes were found in CEBPA POS individuals. Their contribution to poor OS cannot be ruled out.

Conclusion:

CEBPA mutational profiles in Mexican pediatric AML patients and their clinical implications were evaluated for the first time. The frequency of CEBPA POS was in the range reported for pediatric AML (4.5-15%). CEBPA mutations showed a negative impact on OS as opposed to the results of other studies.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Type of study: Guideline / Prognostic_studies Country/Region as subject: Mexico Language: En Journal: Front Pediatr Year: 2022 Document type: Article Affiliation country: México
Fulltext
Add to My VHL
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Full text: 1 Collection: 01-internacional Database: MEDLINE Type of study: Guideline / Prognostic_studies Country/Region as subject: Mexico Language: En Journal: Front Pediatr Year: 2022 Document type: Article Affiliation country: México