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1.
Consensus in acute myeloid leukemia in Mexico.
Arana-Luna, Luara L; Alvarado-Ibarra, Martha; Silva-Michel, Luis G; Morales-Maravilla, Adrián; González-Rubio, María Del C; Chávez-Aguilar, Lénica A; Tena-Iturralde, Ma Fernanda; Mojica-Balceras, Liliana; Zapata-Canto, Nidia; Galindo-Delgado, Patricia; Miranda-Madrazo, Ma Raquel; Morales-Hernández, Alba E; Silva-Vera, Karina; Grimaldo-Gómez, Flavio A; Hernández-Caballero, Álvaro; Bates-Martin, Ramón A; Álvarez-Vera, José L; Tepepa-Flores, Fredy; Teomitzi-Sánchez, Óscar; Fermín-Caminero, Denisse J; Peña-Celaya, José A de la; Salazar-Ramírez, Óscar; Flores-Villegas, Luz V; Guerra-Alarcón, Lidia V; Leyto-Cruz, Faustino; Inclán-Alarcón, Sergio I; Milán-Salvatierra, Andrea I; Ventura-Enríquez, Yanet; Pérez-Lozano, Uendy; Báez-Islas, Pamela E; Tapia-Enríquez, Ana L; Palma-Moreno, Orlando G; Aguilar-Luévano, Jocelyn; Espinosa-Partida, Arturo; Pérez-Jacobo, Luis F; Rojas-Castillejos, Flavio; Ruiz-Contreras, Josué I; Loera-Fragoso, Sergio J; Medina-Coral, Jesús E; Acosta-Maldonado, Brenda L; Soriano-Mercedes, Emely J; Saucedo-Montes, Erick E; Valero-Saldana, Luis M; González-Prieto, Susana G; Nava-Villegas, Lorena; Hernández-Colin, Ana K; Hernández-Alcántara, Areli E; Zárate-Rodríguez, Pedro A; Ignacio-Ibarra, Gregorio; Meillón-García, Luis A.
Gac Med Mex ; 158(M3): M1-M48, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-35350063

RESUMO

Acute myeloid leukemia (AML) comprises a heterogeneous group of hematopoietic cell neoplasms of myeloid lineage that arise from the clonal expansion of their precursors in the bone marrow, interfering with cell differentiation, leading to a syndrome of bone marrow failure. AML is a consequence of genetic and epigenetic changes (point mutations, gene rearrangements, deletions, amplifications, and arrangements in epigenetic changes that influence gene expression) in hematopoietic precursor cells, which create a clone of abnormal cells that are capable of proliferating but cannot differentiate into mature hematopoietic cells or undergo programmed cell death. The diagnosis requires more than 20% myeloid blasts in the bone marrow and certain cytogenic abnormalities. Treatment will depend on age, comorbidities, and cytogenetic risk among the most frequent.

La leucemia mieloide aguda (LMA) comprende un grupo heterogéneo de neoplasias de células hematopoyéticas de linaje mieloide que surgen de la expansión clonal de sus precursores en la médula ósea, interfiriendo con la diferenciación celular, lo que conlleva a un síndrome de falla medular. La LMA es una consecuencia de cambios genéticos y epigenéticos (mutaciones puntuales, rearreglos de genes, deleciones, amplificaciones y arreglos en cambios epigenéticos que influyen en la expression del gen) en las células hematopoyéticas precursoras, la cual crea una clona de células anormales que son capaces de proliferar, pero no se pueden diferenciar en células hematopoyéticas maduras ni sufrir una muerte celular programada. El diagnostic requiere más del 20% de blastos mieloides en médula ósea y ciertas anormalidades citogénicas. El tratamiento dependerá de la edad, comorbilidades, riesgo citogenético entre las más frecuentes.


Assuntos
Leucemia Mieloide Aguda , Diferenciação Celular , Consenso , Humanos , Leucemia Mieloide Aguda/diagnóstico , Leucemia Mieloide Aguda/genética , Leucemia Mieloide Aguda/terapia , México
2.
Chronic Lymphocytic Leukemia in the SARS-CoV-2 Pandemic.
Arellano-Llamas, Abril Adriana; Vela-Ojeda, Jorge; Hernandez-Caballero, Alvaro.
Curr Oncol Rep ; 24(2): 209-213, 2022 02.
Artigo em Inglês | MEDLINE | ID: mdl-35061199

RESUMO

PURPOSE OF REVIEW: Chronic lymphocytic leukemia (CLL) is the most frequent lymphoproliferative disease in the elderly of the western world. Immune defective responses and treatment can worsen the immune system's competence of CLL patients. Consequently, they may present a higher incidence of recurrent severe infections, second malignancies, and reduced efficacy of vaccines. The outbreak of COVID-19 is an ongoing pandemic, and patients with comorbidities experience more severe forms of the disease. Hematological malignancies are associated with higher case fatality rates (CFRs) than other cancers. Knowledge about COVID-19 incidence, clinical course, and immune response to the infection and vaccination in CLL may contribute to design strategies that improve the outcomes of patients in the future. RECENT FINDINGS: The prevalence of SARS-CoV-2 positivity in CLL is not significantly higher than seen in the general population. CFRs for CLL patients are 16.5-fold more elevated than the median reported worldwide and even higher in older patients, those who require hospitalization have significant comorbidities or need oxygen therapy. CLL status decreases the anti-SARS-CoV-2 positivity after infection or vaccination by around 40%, and the spike-specific antibody titers are 74-fold lower than healthy age-matched controls. The response rate to COVID-19 vaccines is even worse in patients with active CLL-directed therapies like BTKi, BCL-2 antagonists, or anti-CD20 monoclonal antibodies. CLL patients are at a greater risk of death from COVID-19. Inherent immunosuppression of CLL and immune deficiencies caused by treatment significantly decrease the ability to produce natural or vaccine-induced anti-SARS-CoV-2 immune responses.


Assuntos
COVID-19/epidemiologia , Leucemia Linfocítica Crônica de Células B/imunologia , SARS-CoV-2 , Adulto , Idoso , Idoso de 80 Anos ou mais , Anticorpos Antivirais/sangue , Vacinas contra COVID-19/imunologia , Humanos , Leucemia Linfocítica Crônica de Células B/tratamento farmacológico , Pessoa de Meia-Idade , SARS-CoV-2/imunologia , Vacinação
3.
Transplantation of hematopoietic progenitors in myelofibrosis.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 38-44, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734044

RESUMO

The objective of this work is to generate recommendations on the management of allogeneic stem cell transplantation (allo-SCT) in primary myelofibrosis (PMF). A comprehensive systematic review of articles published between 1999 and 2015 (January) was used as a source of scientific evidence. The recommendations were produced through a Delphi process involving a panel of 23 experts appointed by the European LeukemiaNet and the European Blood and Marrow Transplantation Group. Key questions included patient selection, donor selection, pre-transplant management, conditioning regimen, post-transplant management, prevention, and management of post-transplant relapse. Patients with intermediate-2 or high-risk disease and age < 70 years should be considered candidates for allo-SCT. Patients with intermediate-risk 1 disease and age < 65 years should be considered candidates if they have refractory transfusion-dependent anemia, or a peripheral blood (PB) blast percentage > 2%, or adverse cytogenetics. Splenectomy before transplantation must be decided on a case-by-case basis. Patients with intermediate-2 or high-risk disease who lack a human leukocyte antigen (HLA)-matched sibling or unrelated donor should be enrolled in a protocol that uses HLA non-identical donors. PB was considered the most appropriate source of hematopoietic stem cells for transplants from HLA-matched unrelated donors and siblings. The optimal intensity of the conditioning regimen has yet to be defined. Strategies such as discontinuation of immunosuppressive drugs, infusion of donor lymphocytes, or both were considered adequate to prevent clinical relapse. In conclusion, we provide consensus-based recommendations aimed at optimizing allo-SCT in PMF. Unmet clinical needs were highlighted.

El objetivo de este trabajo es generar recomendaciones sobre el manejo del trasplante alogénico de células madre (alo-SCT) en la mielofibrosis primaria (MFP). Se utilizó una revisión sistemática integral de artículos publicados entre 1999 y 2015 (enero) como fuente de evidencia científica. Las recomendaciones se produjeron mediante un proceso Delphi en el que participó un panel de 23 expertos designados por la European LeukemiaNet y el European Blood and Marrow Transplantation Group. Las preguntas clave incluyeron la selección de pacientes, la selección de donantes, el manejo previo al trasplante, el régimen de acondicionamiento, el manejo posterior al trasplante, la prevención y el manejo de la recaída después del trasplante. Los pacientes con enfermedad de riesgo intermedio 2 o alto y edad < 70 años deben ser considerados candidatos para alo-SCT. Los pacientes con enfermedad de riesgo intermedio 1 y edad < 65 años deben ser considerados candidatos si presentan anemia refractaria dependiente de transfusiones, o un porcentaje de blastos en sangre periférica > 2%, o citogenética adversa. La esplenectomía previa al trasplante debe decidirse caso por caso. Los pacientes con enfermedad de riesgo intermedio 2 o alto que carecen de un hermano compatible con el antígeno leucocitario humano (HLA) o de un donante no emparentado deben inscribirse en un protocolo que utilice donantes no idénticos de HLA. PB se consideró la fuente más apropiada de células madre hematopoyéticas para trasplantes de hermanos y donantes no emparentados compatibles con HLA. La intensidad óptima del régimen de acondicionamiento aún debe definirse. Se consideraron adecuadas estrategias como la suspensión de los fármacos inmunosupresores, la infusión de linfocitos del donante o ambas para evitar la recaída clínica. En conclusión, proporcionamos recomendaciones basadas en consenso destinadas a optimizar el alo-SCT en MFP. Se destacaron las necesidades clínicas insatisfechas.

4.
Essential thrombocythaemia.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Ángeles Rosales-López, Ma de Los; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 17-25, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734042

RESUMO

Essential thrombocythemia (ET) is a chronic Philadelphia-negative myeloproliferative neoplasm that has its main involvement in the megakaryopoietic lineage, generating sustained thrombocytosis in peripheral blood and an increase in the number of mature megakaryocytes in the bone marrow. In addition to marked thrombocytosis, it is characterized by increased thrombotic or hemorrhagic risk and the presence of constitutional symptoms. Patients with ET have a low but known risk of disease progression to myelofibrosis and/or acute leukemia. The diagnosis is made based on the 2016 WHO criteria. At present, available treatments for patients with ET are mainly aimed at minimizing the risk of thrombosis and/or bleeding.

La trombocitemia esencial (TE) es una neoplasia mieloproliferativa crónica Filadelfia negativa que tiene su principal involucro en la línea megacariopoyética, generando trombocitosis sostenida en la sangre periférica y un incremento en el número de megacariocitos maduros en médula ósea. Además de una marcada trombocitosis, se caracteriza por un mayor riesgo trombótico o hemorrágico y la presencia de síntomas constitucionales. Los pacientes con TE tienen un riesgo bajo, pero conocido, de evolución de la enfermedad a mielofibrosis y/o leucemia aguda. El diagnóstico se realiza con base en los criterios de la Organización Mundial de la Salud del 2016. Los tratamientos actualmente disponibles para los pacientes con TE están dirigidos principalmente a minimizar el riesgo de trombosis y/o hemorragia.

5.
Pregnancy in myeloproliferative neoplasms.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 59-62, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734045

RESUMO

Myeloproliferative neoplasms (MPN) are associated with a significant risk of thrombosis and the hypercoagulable environment of pregnancy increases this risk. The most frequent gestational complications consist of spontaneous abortion, thrombosis, bleeding, and hypertensive disease of pregnancy. Treatment depends on thrombotic risk, gestational trimester, and myeloproliferative neoplasm.

Las neoplasias mieloproliferativas (NMP) están asociadas a un riesgo notable de trombosis y el entorno de hipercoagulabilidad propio del embarazo aumenta este riesgo. Las complicaciones gestacionales más frecuentes consisten en: aborto espontáneo, trombosis, sangrado y enfermedad hipertensiva del embarazo. El tratamiento depende del riesgo trombótico, trimestre gestacional y neoplasia mieloproliferativa.

6.
Polycythemia vera.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Gissell Aguirre-Reyes, Oyuky; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Alberto Bates-Martín, Ramón; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Ángeles Rosales-López, Ma de Los; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 11-16, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734046

RESUMO

Polycythemia vera (PV) is mainly characterized by erythrocytosis, thrombotic and hemorrhagic predisposition, a variety of symptoms, and cumulative risks of fibrotic progression and/or leukemic evolution over time. The diagnosis is made based on the 2016 WHO criteria. The treatment of PV focuses on rapidly reducing the erythrocyte mass, either by means of phlebotomies or with cytoreductive treatment, and the reduction of thrombotic risk by correcting cardiovascular risk factors and the use of platelet antiaggregants.

La policitemia vera (PV) se caracteriza principalmente por eritrocitosis, predisposición trombótica y hemorrágica, una variedad de síntomas y riesgos acumulativos de progresión fibrótica y/o evolución leucémica a lo largo del tiempo. El diagnóstico se realiza con base en los criterios de la Organización Mundial de la Salud del 2016. El tratamiento de la PV se centra en reducir rápidamente la masa eritrocitaria, ya sea por medio de flebotomías o con tratamiento citorreductor, y la disminución del riesgo trombótico mediante la corrección de factores de riesgo cardiovascular y el uso de antiagregantes plaquetarios.

7.
Risks in invasive procedures.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Luis Álvarez-Vera, José; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Alejandro Carballo-Zarate, Adrián; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 63-65, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734049

RESUMO

Patients with myeloproliferative neoplasms have an increased risk of thrombosis and bleeding. This risk must be identified, as well as individualizing the therapeutic strategy before invasive procedures; adequate cytoreduction reduces the risk of complications.

Los pacientes con neoplasias mieloproliferativas tienen un riesgo incrementado de trombosis y sangrado. Se debe identificar dicho riesgo, así como individualizar la estrategia terapéutica previo a los procedimientos invasivos; una adecuada citorreducción disminuye el riesgo de complicaciones.

8.
Symptom control.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 55-58, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734050

RESUMO

In addition to symptoms secondary to splenomegaly, microvascular abnormalities, and thrombohemorrhagic complications, patients with MPN may experience a significant symptom burden attributed to an increase in circulating inflammatory cytokines. These symptoms can be severe and limit quality of life. Therefore, in addition to the prevention of complications, one of the objectives of the treatment of MPN is the control of symptoms.

Además de la sintomatología secundaria a la esplenomegalia, a las alteraciones microvasculares y a las complicaciones trombohemorrágicas, los pacientes con neoplasias mieloproliferativas (NMP) pueden experimentar una importante carga sintomática atribuida a un aumento de citocinas inflamatorias circulantes. Estos síntomas pueden ser severos y limitar la calidad de vida. Por ello, además de la prevención de las complicaciones, uno de los objetivos del tratamiento de las NMP es el control de los síntomas.

9.
Thrombotic events.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 45-54, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734051

RESUMO

Major thrombotic complications in myeloproliferative neoplasms (MPNs) represent an important clinical problem due to their high morbidity, the complexity of their management, and their associated mortality. The appearance of a thrombosis implies a high thrombotic risk stratification of the MPN and determines the initiation or optimization of cytoreductive treatment and the use of antiplatelet or anticoagulant therapy as secondary prophylaxis. The incidence of thrombosis at the time of diagnosis is higher than during the course of the disease, being located in the arterial territory in 60-70% of cases. Once thrombosis has occurred, up to 20-33% of patients experience thrombotic recurrence in the same initial vascular territory.

Las complicaciones trombóticas mayores en las neoplasias mieloproliferativas (NMP) representan un importante problema clínico debido a su elevada morbilidad, la complejidad de su manejo y su mortalidad asociada. La aparición de una trombosis comporta una estratificación de alto riesgo trombótico de la NMP y determina el inicio o la optimización del tratamiento citorreductor y el uso de terapia antiplaquetaria o anticoagulante como profilaxis secundaria. La incidencia de trombosis en el momento del diagnóstico es mayor que durante la evolución de la enfermedad, localizándose en territorio arterial en el 60-70% casos. Una vez se ha producido una trombosis, hasta el 20-33% de los pacientes sufre una recurrencia trombótica en el mismo territorio vascular inicial.

10.
First inter-institutional consensus on Chronic Myeloproliferative Neoplasms.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Luis Álvarez-Vera, José; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Alejandro Carballo-Zarate, Adrián; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Edna Moralws-Hernández, Alba; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Alejandro Jiménez-Ochoa, Marco; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 1-10, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734052

RESUMO

The objective of the consensus is to make available to the professionals of the different public health institutions in our country, who are in charge of these diseases, the most relevant and up-to-date information about their diagnosis and treatment in clinical practice. With this inter-institutional consensus we hope to contribute to improving the quality of care for patients with chronic myeloproliferative neoplasms throughout the Mexican Republic, to unify criteria in both diagnosis and treatment of the different myeloproliferative diseases.

OBJETIVO: El objetivo del consenso es poner a disposición de los profesionales de las diferentes instituciones de salud pública en nuestro país, quienes se encuentran a cargo de estas enfermedades, la información más relevante y actualizada acerca de su diagnóstico y tratamiento en la práctica clínica. Con este consenso interinstitucional esperamos contribuir a mejorar la calidad de la atención de los pacientes con neoplasias mieloproliferativas crónicas a todo lo ancho y largo de la República Mexicana, con el fin de unificar criterios tanto en diagnóstico como en tratamiento de las diferentes enfermedades mieloproliferativas.

11.
Myelofibrosis: diagnosis and treatment.
Barranco-Lampón, Gilberto; Martínez-Castro, Raúl; Arana-Luna, Luara; Álvarez-Vera, José Luis; Rojas-Castillejos, Flavio; Peñaloza-Ramírez, Rosalinda; Carballo-Zarate, Adrián Alejandro; Olarte-Carrillo, Irma; Minamy, Jaime Israel-García; López-Salazar, Javier; Navarrete, Juan José; Espinosa-Partida, Arturo; Ventura-Enríquez, Yanet; Ruiz-Contreras, Josué Isel; Aguirre-Reyes, Oyuky Gissell; Anaya-Cuéllar, Irene; Aguilar-Luévano, Jocelyn; Díaz-Ramírez, Hugo Francisco; Herrera-Olivares, Wilfrido; Aguilar-Hidalgo, José Antonio; Alcívar-Cedeño, Luisa Ma; Hernández-Caballero, Álvaro; Galaz-Cordero, Lourdes Elena; Peña-Celaya, José Antonio de la; Báez-Islas, Pamela Elena; Bates-Martín, Ramón Alberto; Cano-León, Ana Ma de la Luz; Espitia-Ríos, Ma Eugenia; Barbosa, Diego; Morales-Adrián, Javier; Pacheco, Martín Jacobo; Delgado-López, Nancy; Neme-Yunes, Yvette; Moralws-Hernández, Alba Edna; Mújica-Martínez, Aldo; Pérez-Lizardi, Alejandra Betsabé; Pérez-Gómez, Karen Daniela; Barragán-Ibáñez, Gabriel; Martínez, Adolfo; Flores-Ordúñez, Karen; Ramírez-Hoyos, Paulina; Rosales-López, Ma de Los Ángeles; Acosta-Maldonado, Brenda Lizeth; Jiménez-Ochoa, Marco Alejandro; Garzón-Velásquez, Katheryn Betsabé; Hernández-Ruiz, Eleazar; McNally-Guillén, Bosco Martín; Saucedo-Montes, Erick Eduardo; Aguilar-Andrade, Carolina; Vivas-Arteaga, Cindy Lissette.
Gac Med Mex ; 158(Supl 1): 26-37, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-37734057

RESUMO

Myelofibrosis (MF) is a BCR-ABL1-negative myeloproliferative neoplasm characterized by clonal myeloproliferation, dysregulated kinase signaling, and release of abnormal cytokines. In recent years, important progress has been made in the knowledge of the molecular biology and the prognostic assessment of MF. Conventional treatment has limited impact on the patients' survival; it includes a wait-and-see approach for asymptomatic patients, erythropoiesis-stimulating agents, androgens, or immunomodulatory agents for anemia, cytoreductive drugs such as hydroxyurea for the splenomegaly and constitutional symptoms, and splenectomy or radiotherapy in selected patients. The discovery of the Janus kinase (JAK) 2 mutation triggered the development of molecular targeted therapy of MF. The JAK inhibitors are effective in both JAK2-positive and JAK2-negative MF; one of them, ruxolitinib, is the current best available therapy for MF splenomegaly and constitutional symptoms. Although ruxolitinib has changed the therapeutic scenario of MF, there is no clear indication of a disease-modifying effect. Allogeneic stem cell transplantation remains the only curative therapy of MF, but due to its associated morbidity and mortality, it is usually restricted to eligible high- and intermediate-2-risk MF patients. To improve current therapeutic results, the combination of JAK inhibitors with other agents is currently being tested, and newer drugs are being investigated.

La mielofibrosis (MF) es una neoplasia mieloproliferativa negativa para BCR-ABL1 caracterizada por mieloproliferación clonal, señalización de cinasa desregulada y liberación de citocinas anormales. En los últimos años se han realizado importantes avances en el conocimiento de la biología molecular y la valoración pronóstica de la MF. El tratamiento convencional tiene un impacto limitado en la supervivencia de los pacientes; incluye un enfoque de espera para pacientes asintomáticos, agentes estimulantes de la eritropoyesis, andrógenos o agentes inmunomoduladores para la anemia, fármacos citorreductores como la hidroxiurea para la esplenomegalia y los síntomas constitucionales, y esplenectomía o radioterapia en pacientes seleccionados. El descubrimiento de la mutación Janus cinasa (JAK) 2 desencadenó el desarrollo de la terapia dirigida molecular de la MF. Los inhibidores de JAK son efectivos tanto en MF con JAK2 positivo como con JAK2 negativo; uno de ellos, el ruxolitinib, es la mejor terapia disponible actualmente para la esplenomegalia y los síntomas constitucionales de la MF. Sin embargo, aunque el ruxolitinib ha cambiado el escenario terapéutico de la MF, no hay indicios claros de un efecto modificador de la enfermedad. El alotrasplante de células madre sigue siendo la única terapia curativa de la MF, pero debido a su morbilidad y mortalidad asociadas, generalmente se restringe a pacientes elegibles con MF de riesgo alto e intermedio 2. Para mejorar los resultados terapéuticos actuales, actualmente se está probando la combinación de inhibidores de JAK con otros agentes y se están investigando fármacos más nuevos.

12.
Consenso de leucemia mieloide aguda en México / Mexican consensus in acute myeloid leukemia in Mexico
Arana-Luna, Luara L.; Alvarado-Ibarra, Martha; Silva-Michel, Luis G.; Morales-Maravilla, Adrián; González-Rubio, María del C.; Chávez-Aguilar, Lénica A.; Tena-Iturralde, María Fernanda; Mojica-Balceras, Liliana; Zapata-Canto, Nidia; Galindo-Delgado, Patricia; Miranda-Madrazo, María Raquel; Morales-Hernández, Alba E.; Silva-Vera, Karina; Grimaldo-Gómez, Flavio A.; Hernández-Caballero, Álvaro; Bates-Martin, Ramón A.; Álvarez-Vera, José L.; Tepepa-Flores, Fredy; Teomitzi-Sánchez, Óscar; Fermín-Caminero, Denisse J.; Peña-Celaya, José A. de la; Salazar-Ramírez, Óscar; Flores-Villegas, Luz V.; Guerra-Alarcón, Lidia V.; Leyto-Cruz, Faustino; Inclán-Alarcón, Sergio I.; Milán-Salvatierra, Andrea I.; Ventura-Enríquez, Yanet; Pérez-Lozano, Uendy; Báez-Islas, Pamela E.; Tapia-Enríquez, Ana L.; Palma-Moreno, Orlando G.; Aguilar-Luévano, Jocelyn; Espinosa-Partida, Arturo; Pérez-Jacobo, Luis F.; Rojas-Castillejos, Flavio; Ruiz-Contreras, Josué I.; Loera-Fragoso, Sergio J.; Medina-Coral, Jesús E.; Acosta-Maldonado, Brenda L.; Soriano-Mercedes, Emely J.; Saucedo-Montes, Erick E.; Valero-Saldana, Luis M.; González-Prieto, Susana G.; Nava-Villegas, Lorena; Hernández-Colin, Ana K.; Hernández-Alcántara, Areli E.; Zárate-Rodríguez, Pedro A.; Ignacio-Ibarra, Gregorio; Meillón-García, Luis A.; Espinosa-Bautista, Karla A.; Ledesma de la Cruz, Cindy; Barbosa-Loría, Diego M.; García-Castillo, Carolina; Balderas-Delgado, Carolina; Cabrera-García, Álvaro; Pérez-Zúñiga, Juan M.; Hernández-Ruiz, Eleazar; Villela-Peña, Atenas; Gómez Cortés, Sue Cynthia; Romero-Rodelo, Hilda; Garzón-Velásquez, Katheryn B.; Serrano-Hernández, Cristina; Martínez-Ríos, Annel; Pedraza-Solís, María Luisa; Martínez-Coronel, Jorge A.; Narváez-Davalos, Iris M.; García-Camacho, Alinka S.; Merino-Pasaye, Laura E.; Aguilar-Andrade, Carolina; Aguirre-Domínguez, Juan A.; Guzmán-Mera, Pedro G.; Delgado-de la Rosa, Elizabeth; Flores López, Perla E.; González-Aguirre, Lilia L.; Ramírez-Alfaro, Edgar M.; Vera-Calderón, Heidi; Meza-Dávalos, María Lizeth; Murillo-Cruz, Juan; Pichardo-Cepín, Yayra M.; Ramírez-Romero, Eva F..
Gac. méd. Méx ; 158(spe): M1-M51, ene. 2022. tab, graf
Artigo em Espanhol | LILACS-Express | LILACS | ID: biblio-1375542

RESUMO

resumen está disponible en el texto completo

Abstract Acute myeloid leukemia (AML) comprises a heterogeneous group of hematopoietic cell neoplasms of myeloid lineage that arise from the clonal expansion of their precursors in the bone marrow, interfering with cell differentiation, leading to a syndrome of bone marrow failure. AML is a consequence of genetic and epigenetic changes (point mutations, gene rearrangements, deletions, amplifications, and arrangements in epigenetic changes that influence gene expression) in hematopoietic precursor cells, which create a clone of abnormal cells that are capable of proliferating but cannot differentiate into mature hematopoietic cells or undergo programmed cell death. The diagnosis requires more than 20% myeloid blasts in the bone marrow and certain cytogenic abnormalities. Treatment will depend on age, comorbidities, and cytogenetic risk among the most frequent.

13.
Post-treatment improvement of NK cell numbers predicts better survival in myeloma patients treated with thalidomide-based regimens.
Vela-Ojeda, Jorge; Esparza, Miriam America García-Ruiz; Majluf-Cruz, Abraham; García-Chavez, Jaime; Montiel-Cervantes, Laura Arcelia; Reyes-Maldonado, Elba; Hernandez-Caballero, Alvaro; Rodríguez-González, Maria Guadalupe.
Int J Hematol ; 110(3): 306-312, 2019 Sep.
Artigo em Inglês | MEDLINE | ID: mdl-31168767

RESUMO

Multiple myeloma (MM) is a disease characterized by antitumoral immune dysfunction. The objective of the present study was to determine lymphocyte subsets (B, T, NK, NKT, iNKT, dendritic cells, and regulatory T cells) in 68 newly diagnosed patients and 113 healthy donors. Lymphocyte subsets were studied in the same patients 6 months after treatment. Pre-treatment values of CD4+ T cells, NK cells, type 2 dendritic cells, and B cells in MM patients were lower than in healthy donors. Forty patients (59%) received MPT treatment and 28 (41%) thal-dex. Patients with no response to treatment, exhibited a decrease in CD4+ T cells and NK cells, as well as an increase in Treg cell numbers. Median DFS and OS was lower in patients not achieving response, in patients having low numbers of NK cells, and higher values of LDH. The number of CD4 T cells, NK, DC2, and B cells at diagnosis is lower in patients with MM. Non-responder patients had lower CD4 and NK, but higher Treg cell values. Patients in which response is not achieved, and those holding lower values of NK cells and higher levels of LDH, have poor DFS and OS.


Assuntos
Protocolos de Quimioterapia Combinada Antineoplásica/administração & dosagem , Células Matadoras Naturais , Mieloma Múltiplo , Idoso , Dexametasona/administração & dosagem , Intervalo Livre de Doença , Feminino , Humanos , Contagem de Linfócitos , Masculino , Melfalan/administração & dosagem , Pessoa de Meia-Idade , Mieloma Múltiplo/sangue , Mieloma Múltiplo/tratamento farmacológico , Mieloma Múltiplo/mortalidade , Prednisolona/administração & dosagem , Taxa de Sobrevida , Talidomida/administração & dosagem
14.
Prognostic Value of CD95, Active Caspase-3, and Bcl-2 Expression in Adult Patients with De Novo Acute Lymphoblastic Leukemia.
Montiel-Cervantes, Laura Arcelia; Reyes-Maldonado, Elba; Garcia-Chavez, Jaime; Hernandez-Caballero, Alvaro; Molina-Aguilar, Rubiraida; Garcia-Ruiz Esparza, Miriam America; Vela-Ojeda, Jorge.
Arch Med Res ; 49(1): 44-50, 2018 01.
Artigo em Inglês | MEDLINE | ID: mdl-29680307

RESUMO

BACKGROUND: Acute lymphoblastic leukemia is an aggressive malignant disease with high mortality rates in adults. AIM OF THE STUDY: The expression levels of CD95, active caspase-3, and Bcl-2 were determined in 111 patients with de novo acute lymphoblastic leukemia (ALL) and correlated with overall survival (OS) and disease-free survival (DFS). METHODS: The immunophenotyped ok leukemia and the expression of CD95, active caspase-3, and Bcl-2, were determined by flow cytometry. Apoptotic variables were correlated by Spearman test, and survival by Kaplan-Meier method. Log-rank test was used to compare survival curves. RESULTS: From a total of 111 patients, 56 cases were B-ALL, 16 T-ALL, 16 B-ALL/CD33+, and 23 ambiguous lineage-AL (AmbLin-AL). The median expression of CD95 (61.5%) and active-caspase-3 (19.4%) was higher in T-ALL (p <0.05), whereas Bcl-2 was lower in T-ALL (p <0.038). There was a highly significant correlation in B-ALL, B-ALL/CD33+ and AmbLin-AL between CD95 and Bcl-2, CD95-Active caspase-3, and Bcl-2-Active caspase-3; while in T-ALL, there was only a correlation between CD95-Active caspase-3, and Bcl-2-Active caspase-3. OS and DFS were better for T-ALL than the other groups, especially in patients having higher values of CD95 and active caspase 3, and lower values of Bcl-2. The worse survival rates were observed in patients with B-ALL/CD33+, and AmbLin-AL. CONCLUSIONS: The prognosis of ALL in adults is influenced by the expression levels of Bcl-2, active-caspase-3, and CD95.


Assuntos
Caspase 3/biossíntese , Leucemia-Linfoma Linfoblástico de Células Precursoras/patologia , Proteínas Proto-Oncogênicas c-bcl-2/biossíntese , Receptor fas/biossíntese , Adulto , Apoptose/imunologia , Caspase 2/biossíntese , Cisteína Endopeptidases/biossíntese , Intervalo Livre de Doença , Feminino , Citometria de Fluxo , Humanos , Imunofenotipagem , Masculino , Pessoa de Meia-Idade , Prognóstico , Adulto Jovem
15.
Genetic susceptibility variants for chronic lymphocytic leukaemia in Mexican mestizos.
Hernandez-Caballero, Alvaro; Arellano-Llamas, Abril Adriana; Cruz-Rico, Jorge; Ojeda, Jorge Vela; Tuna-Aguilar, Elena; Aguayo-Gonzalez, Alvaro; Oropeza-Martinez, Martha Patricia; Montiel-Cervantes, Larua Arcelia; Anaya, Luis Solis; Canizales-Quinteros, Samuel; Majluf-Cruz, Abraham Salvador.
Br J Haematol ; 169(6): 909-11, 2015 Jun.
Artigo em Inglês | MEDLINE | ID: mdl-25522770

Assuntos
Predisposição Genética para Doença , Variação Genética , Leucemia Linfocítica Crônica de Células B/genética , Alelos , Frequência do Gene , Humanos , México , Razão de Chances , Polimorfismo de Nucleotídeo Único
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