ABSTRACT
RESUMEN Saprochaete capitata es una causa rara de infección fúngica invasiva en pacientes inmunocomprometidos con alta mortalidad y resistencia antifúngica. Presentamos el caso de un niño de cinco años con diagnóstico de aplasia medular, sometido a trasplante de progenitores hematopoyéticos (TPH), que cursó con neutropenia febril persistente, dolor abdominal intenso, aparición de lesiones maculopapulares en piel y deterioro de la función renal. Se identificó la presencia de S. capitata, en hemocultivos transcatéter venoso central. Esta infección fúngica invasiva resulta ser rara, pero emergente y potencialmente mortal, en pacientes con neutropenia febril persistente y uso prolongado de dispositivos invasivos intravasculares como catéter venoso central.
ABSTRACT Saprochaete capitata is a rare cause of invasive fungal infection in immunocompromised patients with high mortality and antifungal resistance. We present the case of a 5-year-old boy with bone marrow aplasia, who underwent hematopoietic stem cell transplantation (HSCT) and presented persistent febrile neutropenia, abdominal pain, appearance of maculopapular lesions on the skin, and impaired renal function. The presence of S. capitata was identified by blood culture from a central venous catheter. This invasive fungal infection is rare but emergent and life-threatening, especially in immunocompromised patients with persistent febrile neutropenia and prolonged use of invasive devices such as central venous catheters.
Subject(s)
Humans , Male , Child, Preschool , Immunocompromised Host , Invasive Fungal Infections/microbiology , Geotrichosis/microbiology , Geotrichum/isolation & purification , Anemia, Aplastic/complications , Fatal Outcome , Invasive Fungal Infections/drug therapy , Geotrichosis/drug therapy , Antifungal Agents/therapeutic useABSTRACT
Introducción: La anemia de Fanconi es una enfermedad genética rara, de herencia autosómica o ligada al X, caracterizada por inestabilidad genómica e hipersensibilidad a los agentes de entrecruzamiento del ADN, como el diepoxibutano y la mitomicina C (MMC). La respuesta anormal a estas sustancias, que constituye un marcador celular único y se manifiesta como un incremento de la frecuencia de roturas cromosómicas, es la base de su diagnóstico. Objetivo: Realizar el análisis de roturas cromosómicas inducidas por la mitomicina C en linfocitos de sangre periférica de pacientes cubanos con sospecha de anemia de Fanconi. Métodos: Se realizó estudio de roturas cromosómicas inducidas por la mitomicina C a diferentes concentraciones en cultivos de linfocitos T provenientes de sangre venosa periférica en 32 pacientes con sospecha clínica de anemia de Fanconi e igual cantidad de sujetos controles. Resultados: Al finalizar el análisis seis pacientes (20 por ciento) fueron diagnosticados con anemia de Fanconi. De ellos, cuatro presentaron alto porcentaje de rupturas y dos un mosaicismo somático. Desde el punto de vista clínico, cuatro mostraban anemia aplásica y dos exhibían únicamente rasgos dismórficos típicos de la enfermedad. Conclusiones: El ensayo de roturas cromosómicas inducidas por la mitomicina C permitió el diagnóstico definitivo de anemia de Fanconi en pacientes con antecedentes de anemia aplásica, aún sin anomalías congénitas. Este constituye el primer estudio de este tipo en un grupo de pacientes cubanos(AU)
Introduction: Fanconi anemia is a rare genetic disease of autosomal inheritance or X-linked, characterized by genomic instability and hypersensitivity to DNA cross-linking agents like diepoxybutane and mitomycin C (MMC). The basis for its diagnosis is an abnormal response to these substances, which constitutes a unique cell marker and manifests as an increased chromosomal breakage rate. Objective: To perform the analysis of the chromosomal breakages induced by mitomycin C in peripheral blood lymphocytes of Cuban patients with suspicion of Fanconi anemia. Methods: A study was conducted of chromosomal breakages induced by mitomycin C at various concentrations in cultures of T lymphocytes from venous peripheral blood of 32 patients with clinical suspicion of Fanconi anemia and an equal number of control subjects. Results: At the end of the analysis, six patients (20 percent) were diagnosed with Fanconi anemia. Of these, four showed a high percentage of breakages and two had somatic mosaicism. From a clinical point of view, four had aplastic anemia and two only presented dysmorphic features typical of the disease. Conclusions: Evaluation of the chromosomal breakages induced by mitomycin C led to the definitive diagnosis of Fanconi anemia in patients with a history of aplastic anemia, even in the absence of congenital anomalies. This is the first study of its type in a group of Cuban patients(AU)
Subject(s)
Humans , Congenital Abnormalities , Lymphocytes , Genomic Instability , Fanconi Anemia , Genetic Diseases, Inborn , Hypersensitivity , Cuba/epidemiologyABSTRACT
Resumen La infección por parvovirus humano B19 es una de las complicaciones comunes en pacientes diagnosticados de enfermedad de células falciformes (ECF). Se caracteriza por una anemia grave con reticulocitopenia, pudiendo estar acompañada de otras manifestaciones clínicas. En ocasiones, la infección puede ocurrir de modo simultáneo en contactos intrafamiliares de un paciente también con ECF. Es fundamental el reconocimiento temprano de esta complicación y el diagnóstico diferencial con otras patologías para su correcto manejo y tratamiento. Presentamos el caso de dos hermanos con ECF e infección por parvovirus humano B19.
Abstract Human parvovirus B19 infection is one of the common complications of patients diagnosed with Sickle cell disease (SCD). Parvovirus infections are characterized by a severe anemia with reticulocytopenia, sometimes presenting with other clinical manifestations. The infection can occur simultaneously in patient's cohabitants also diagnosed with SCD. Early recognition and differential diagnosis are essential for a proper disease management and treatment. We present two siblings with SCD and human parvovirus B19 infection.
Subject(s)
Humans , Male , Child , Parvovirus B19, Human , Erythema Infectiosum , Parvoviridae Infections , Anemia, Sickle Cell , Parvovirus B19, Human/genetics , Erythema Infectiosum/diagnosis , Parvoviridae Infections/complications , Parvoviridae Infections/diagnosis , Siblings , Anemia, Sickle Cell/complicationsABSTRACT
Resumen La pandemia de enfermedad por coronavirus 2019 (COVID-19) ha cambiado la perspectiva médica para el tratamiento de no solo de enfermedades hematológicas, sino en general de la medicina. Respecto a la anemia aplásica (AA), principalmente la muy severa, en la que el paciente se presenta con menos de 200 neutrófilos absolutos, el riesgo de infección potencialmente mortal es alta y el inicio de terapia inmunosupresora también representa un riesgo, al menos temporal, para COVID-19. Se ha recomendado incluso aplazar el trasplante de células progenitoras hematopoyéticas en muchos pacientes para evitar un contagio. Una inmunosupresión moderada preferentemente ambulatoria que incluya agentes trombomiméticos es la opción terapéutica en tiempos de la pandemia actual. En esta revisión se enlistan las recomendaciones internacionales y nacionales respecto al tratamiento y seguimiento de pacientes con AA con base en experiencias de países que ya han pasado por esta emergencia sanitaria.
Abstract Medical practice in general has changed due to coronavirus disease 2019 (COVID-19) pandemic. Some hematologic diseases require immunosuppresive therapy placing patients at high risk of infection, including severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Aplastic anemia (AA) especially the very severe type in which the count of absolute neutrophils is less than 200/ml is a life-threatening condition. Although bone marrow transplant is a potential curative treatment, it should be delayed temporally in order to prevent a contagion. Hospitalization may expose patients to infection, thus an ambulatory immunosuppression with oral cyclosporine and thrombopoietin agonist should be an adequate option. This work reviews international and national treatment recommendations and follow-up of patients with AA based on experiences from countries that have already faced this health emergency.
ABSTRACT
Resumen Objetivo: La anemia aplásica es una enfermedad rara, potencialmente mortal sin diagnóstico y tratamiento temprano. El objetivo del estudio fue describir la epidemiología de la anemia aplásica en la población de 0 a 13 años a nivel nacional, atendida en el Hospital Nacional de Niños "Dr. Carlos Sáenz Herrera", de la Caja Costarricense de Seguro Social, único centro del país disponible para la atención en hematología pediátrica. Métodos: Se realizó un estudio observacional retrospectivo de los pacientes atendidos en el Servicio de Hematología Pediátrica, con diagnóstico de anemia aplásica adquirida y las diversas formas de aplasias congénitas, en el periodo de enero 2006 a junio de 2016. Se registró el tipo de tratamiento recibido, su respuesta y la mortalidad asociada con la enfermedad, así como algunos datos epidemiológicos. Resultados: Se analizó un total de 27 casos, 23 con anemia aplásica adquirida y 4 con diversos tipos de anemias congénitas. La edad media al momento del diagnóstico fue de 81,7 meses, con una relación hombre: mujer de 1.1:1. De los 23 pacientes con anemia aplásica adquirida, 10 recibieron tratamiento con globulina antitimocito y presentaron respuesta a la globulina equina 2/5 pacientes como primera línea de tratamiento y 1 como segunda línea; con la globulina de conejo se obtuvo respuesta en 1/5 pacientes como primera línea y en 2 como segunda línea. Tres pacientes recibieron tratamiento con trasplante de médula ósea y presentaron una respuesta completa, sin evidenciar datos de enfermedad de injerto versus huésped u otras complicaciones al finalizar el estudio. No se logró demostrar diferencia significativa respecto al sexo, edad de diagnóstico, valores del hemograma, frecuencia de requerimiento de plaquetas o glóbulos rojos, grado de severidad ni mortalidad. Conclusión: Se confirmó la baja prevalencia de la anemia aplásica; la muestra obtenida durante el periodo analizado es pequeña y limita la observación de características relevantes ante referentes internacionales.
Abstract Objective: Aplastic anemia is a rare and life-threatening disease without diagnosis and early treatment. The objective of this study was to describe the epidemiological characters of patients with aplastic anemia and 0-13 years old in Costa Rica, to treat in the Hospital Nacional de Niños Dr.Carlos Sáenz Herrera, CajaCostarricense de Seguro Social; only there offers Pediatric Hematology service. Methods: We performed an observational retrospective study, there including the patients diagnosed with both acquired aplastic anemia and inherited bone marrow failure syndromes from January 2006 to June 2016, regardless of sex or ethnicity. We evaluated the treatment received, the response to each treatment, and mortality associated with the disease. Results: An overall of 27 patients were included, 23 diagnosed with acquired aplastic anemia and, 4 with bone marrow failure syndrome. The mean age of diagnosis was 81.7 months, with a male to female ratio of 1.1:1. Of the 23 patients diagnosed with acquired aplastic anemia, 10 received immunosuppressive therapy with antithymocite globulin, with a response to horse globulin as a first line treatment in 2/5 patients, and 1 as a second line treatment. Patients with rabbit globulin showed to response in 1/5 cases when used as a first line treatment, and a response as a second line treatment after a no response treatment with horse globulin in 2/3 patients. Three patients treated with a matched related donor bone marrow transplant and showed complete response, without complications including graft versus host disease by the end of the study period. There was no statistical difference regarding sex, age of diagnosis, blood cell counts, frequency of blood product transfusions, degree of severity associated or, mortality. Conclusions: Our results confirm the low incidence of aplastic anemia, it's a little study population and has limited results of relevant characteristics and can´t compare with international studies.
Subject(s)
Humans , Infant, Newborn , Infant , Child, Preschool , Child , Adolescent , Bone Marrow Transplantation/statistics & numerical data , Anemia, Aplastic/epidemiology , Costa Rica , Hospitals, PediatricABSTRACT
We present the case of a pregnant woman with aplastic anemia. The 22-year-old patient presented with 27 weeks of gestation and lymphoproliferative syndrome at the Instituto Nacional de Perinatología in Mexico City. The bone marrow biopsy confirmed the diagnosis and the immunophenotype was negative for malignancy. The treatment consisted of transfusions and planned birth at 35 weeks. Afterwards, the patient was referred to a bone marrow transplant unit.
Se presenta los resultados perinatales de una paciente con anemia aplásica. Se revisa el caso atendido en el Instituto Nacional de Perinatología, Ciudad de México. La paciente tenía 22 años de edad y embarazo de 27,0 semanas con síndrome linfoproliferativo. La biopsia de médula ósea determinó anemia aplásica; el inmunofenotipo fue negativo a malignidad. El manejo consistió en soporte transfusional, con resolución del embarazo a las 35 semanas. Luego, se refirió la paciente a la unidad de trasplante de médula ósea.
ABSTRACT
La aplasia medular es una enfermedad poco frecuente en pediatría, siendo el tratamiento de elección en las formas severas el trasplante de células progenitoras hematopoyéticas (TCPH). Gracias a los avances en TCPH, los nuevos tratamientos inmunosupresores y al adecuado tratamiento de sostén, se ha logrado en las últimas décadas una franca disminución de la mortalidad asociada a esta patología. Es por ello que uno de los principales desafíos consiste en prevenir la aparición de infecciones asociadas a la neutropenia severa y prolongada que padecen estos pacientes, siendo actualmente las infecciones bacterianas y fúngicas una de las principales causas de morbimortalidad. Por otra parte, la mayoría de las guías de manejo y tratamiento de sostén se basan en recomendaciones de expertos, siendo la evidencia escasa, más aún en pediatría. Gran parte de las recomendaciones de tratamiento empírico se basan en guías de neutropenia febril de pacientes hemato-oncológicos. A su vez, existe gran variabilidad, de acuerdo al centro de atención, en cuanto al uso de antimicrobianos para profilaxis primaria, debiéndose tener en cuenta la mayor propensión a presentar infecciones invasivas por hongos filamentosos y, en el caso de pacientes con linfopenia marcada, de enfermedad por P jirovecii a la hora de valorar la indicación de profilaxis de estos pacientes.Se detallarán a continuación las principales recomendaciones sobre manejo de prevención de infecciones y tratamiento precoz de pacientes pediátricos con aplasia medular severa.
Aplastic anemia (AA) is a rare condition in children. Hematopoietic stem cell transplantation (HSCT) is the treatment of choice for severe idiopatic AA. Survival in severe AA has markedly improved in the past decades due to advances in HSCT, immunosuppressive and biologic drugs, as well as supportive care. Since bacterial and fungal infections are one of the principal causes of morbidity and mortality in AA, one of the main challenges is to prevent the appearance of infections associated with severe and prolonged neutropenia. Most guidelines of treatment and prophylaxis are based on expert recommendations. Given the lack of controlled studies in children with AA, most recommendations of empiric treatment rely on guidelines for febrile-neutropenia management in hemato-oncologycal patients. A great variability exists in the use of antimicrobials for primary prophylaxis among different institutions. Due to the fact that patients with severe and prolonged AA present high incidence of filamentous fungal infections, an adecuate antifungal prophylaxis is recommended. In the case of severe lymphopenia, prophylaxis against P jirovecii should also be considered. Recommendations in prophylaxis and early treatment of infections in severe pediatric AA are detailed
Subject(s)
Humans , Infant, Newborn , Infant , Child, Preschool , Child , Infection Control , Hematopoietic Stem Cell Transplantation , Early Diagnosis , Disease Prevention , Invasive Fungal Infections/therapy , Anemia, Aplastic/pathology , Anemia, Aplastic/prevention & controlABSTRACT
La aplasia medular asociada a hepatitis (HAAA) es una reconocida entidad clínica donde la falla medular es precedida de una hepatitis; se observa hasta en el 5% de las aplasias en Europa occidental y América del Norte y hasta en el 10% de ellas en el Este asiático. Se ha sospechado de los virus hepatotropos y otros virus como responsables de HAAA, pero esta asociación raramente se ha confirmado. La hepatitis por virus E es la causa más frecuente de hepatitis viral en el mundo. Su genotipo 3, de mayor circulación en la Argentina y otros países de Latinoamérica, puede presentar complicaciones extrahepáticas (renales, neurológicas, pancreáticas y hematológicas). Hasta aquí, en nuestro conocimiento solo se ha publicado un caso de HAAA por virus de la hepatitis E en Pakistán; el que ahora presentamos sería el primero comunicado en la Argentina. La paciente fue tratada con timoglobulina, ciclosporina, corticosteroides, filgastrim y soporte transfusional. Desarrolló fungemia por Candida tropicalis que respondió a equinocandinas, y luego infiltrados pulmonares e imagen nodular cerebral con galactomananos en suero (índice DO > 1.0 ng/ml) que resolvieron con voriconazol. Fue dada de alta independiente de transfusiones, tres meses después de su admisión, con hepatograma normal. Teniendo en cuenta este caso, sería conveniente investigar la hepatitis E como causa de HAAA en la Argentina.
Hepatitis-associated aplastic anemia (HAAA) is a well-recognized clinical syndrome in which marrow failure follows the development of hepatitis; it can be observed in up to 5% in the aplastic anemia in West Europe and North American countries and 10% in the East Asia. Although hepatotropic and other viruses were suspected of causing HAAA, this hypothesis was rarely confirmed. Currently, the infection with hepatitis E virus represents the first cause of acute hepatitis in the world. Its genotype 3, the most frequent in Argentina and other Latin American countries, was associated with extrahepatic complications (renal, pancreatic, neurologic and hematologic). To our knowledge, only one case of hepatitis E virus-associated aplastic anemia has been previously reported, in Pakistan; the case presented here would be the first in Argentina. The patient was treated with thymoglobulin, cyclosporine, corticosteroids, filgastrim and transfusional support. She developed fungemia due to Candida tropicalis that remitted with equinocandins and therefore fever, pulmonary infiltrates and a solitary nodular cerebral image with serum galactomannan (DO index > 1.0 ng/ml) that resolved with voriconazol. She was discharged three months after her admission without transfusion requirements and normal hepatic values.With this in mind, it would be advisable to investigate hepatitis E (HEV) as a cause of HAAA in Argentina.
Subject(s)
Female , Humans , Middle Aged , Anemia, Aplastic/complications , Hepatitis E/complications , Anemia, Aplastic/diagnosisABSTRACT
Introduction: The laboratory diagnosis of paroxysmal nocturnal hemoglobinuria (PNH), disease that is categorized by reduced synthesis of glycosylphosphatidylinositol (GPI) anchor, is based on the detection of blood cells deficient in GPI-anchored proteins by flow cytometry. PNH clones have been detected in patients with aplastic anaemia (AA) and myelodysplastic syndrome (MDS), with therapeutic implications. Objectives: To validate a sensitive assay for detection of GPI-anchored protein-deficient cells, by flow cytometry, and to analyze the clone frequency in AA and MDS patients. Methods: Samples from 20 AA patients, 30 MDS patients and 20 adult volunteers (control group) were analyzed using monoclonal antibodies to CD16, CD24, CD55 and CD59 (neutrophils); CD14 and CD55 (monocytes); CD55 and CD59 (erythrocytes); besides fluorescent aerolysin reagent (FLAER) (neutrophils and monocytes) and lineage markers. The proportions of PNH cells detected in neutrophils and monocytes, using different reagent combinations, were compared by analysis of variance (ANOVA) and Pearson's correlation. Results: PNH cells were detected in five (25%) AA patients, and the proportions of PNH cells varied from 0.14% to 94.84% of the analyzed events. PNH cells were not detected in the MDS patients. However, by the analysis of these samples, it was possible to identify the technical challenges caused by the presence of immature and dysplastic circulating cells. FLAER showed clear distinction of GPI-deficient cells. Conclusion: Multiparameter flow cytometry analysis offers high sensitivity and accuracy in the detection of subclinical PNH clones. FLAER shows excellent performance in detection of PNH neutrophils and monocytes...
Introdução: O diagnóstico laboratorial da hemoglobinúria paroxística noturna (HPN), doença caracterizada por deficiência de síntese da molécula de ancoragem glicosilfosfatidilinositol (GPI), baseia-se na detecção de células sanguíneas deficientes em proteínas ancoradas ao GPI, por citometria de fluxo. Clones de células com fenótipo HPN podem ser detectados em pacientes com anemia aplásica (AA) e síndrome mielodisplásica (SMD), com implicações terapêuticas. Objetivos: Validar técnica sensível para detecção de células HPN, por citometria de fluxo, e avaliar a frequência dos clones em pacientes com AA e SMD. Métodos: Amostras de 20 pacientes com AA, 30 pacientes com SMD e 20 voluntários (controles) foram analisadas, utilizando anticorpos monoclonais anti-CD16, CD24, CD55 e CD59 (neutrófilos); CD14 e CD55 (monócitos); e CD55 e CD59 (hemácias); além do reagente de aerolisina fluorescente (FLAER) (neutrófilos e monócitos) e marcadores de linhagem celular. A comparação do tamanho dos clones HPN detectados em neutrófilos e monócitos, pelas diferentes combinações de reagentes, foi realizada por análise de variância (ANOVA) e correlação de Pearson. Resultados: Em cinco (25%) pacientes com AA foram identificadas células HPN, em proporções entre 0,14% e 94,84% dos eventos analisados. O clone não foi detectado nos pacientes com SMD. Contudo, a análise dessas amostras permitiu evidenciar as dificuldades técnicas secundárias à presença de células imaturas e displásicas circulantes. O reagente FLAER propiciou separação precisa das células alteradas. Conclusão: A análise multiparamétrica por citometria de fluxo apresenta sensibilidade...
Subject(s)
Humans , Male , Female , Adult , Middle Aged , Diagnostic Techniques and Procedures , Flow Cytometry , Hemoglobinuria, Paroxysmal/diagnosis , Analysis of Variance , Anemia, Aplastic , Myelodysplastic SyndromesABSTRACT
Dipirona es un analgésico, antipirético, espasmolítico y antiinflamatorio de amplio uso en Colombia y Latinoamérica, proscrito por agencias regulatorias de referencia, por el riesgo de agranulocitosis y otras discrasias sanguíneas. Estos antecedentes han generado controversia e incluso aprensión dentro de los prescriptores, lo cual justifica esta revisión. Una vez revisada la literatura se encuentra que dipirona es eficaz como antipirético y para manejo del dolor agudo, crónico, postoperatorio, cólico renal y migraña. La prevalencia de agranulocitosis es de 0,03 al 0,5% en pacientes europeos y la incidencia de pacientes hispanos está alrededor de 0,38 casos por un millón de habitantes/año y aun menor en anemia aplásica. El riesgo de lesión gástrica es menor que el de otros AINEs de uso habitual y es un medicamento relativamente seguro en el embarazo. Otros efectos adversos incluyen hipersensibilidad, anafilaxia, pénfigo e hipotensión arterial relacionada con la administración intravenosa rápida del medicamento. Conclusiones: Dipirona conlleva un riesgo muy bajo de generar discrasias sanguíneas en población latinoamericana posiblemente por factores farmacogenéticos aún no identificados. Los principales factores de riesgo incluyen la duración del tratamiento, la dosis empleada y el uso concomitante de otros medicamentos que generen mielotoxicidad.
Dipyrone is an analgesic, antipyretic, antispasmodic and anti-inflammatory widely used in Colombia and Latin America, outlawed by reference regulatory agencies due to the risk of agranulocytosis and other blood dyscrasias. These facts have generated controversy and even apprehension within prescribers, which justifies this review. After reviewing the literature is that dipyrone is effective as antipyretic and management of acute pain, chronic, postoperative, renal colic and migraine. The prevalence of agranulocytosis is 0.03 to 0.5% in European patients and the incidence in Hispanic patients is about 0.38 cases per million inhabitants / year and even lower for aplastic anemia. Gastric injury risk is lower than that of other commonly used NSAIDs and is a relatively safe drug during pregnancy. Other adverse effects include hypersensitivity, anaphylaxis, pemphigus and hypotension related to rapid intravenous administration of the drug. Conclusions: Dipyrone carries a very low risk of blood dyscrasias in Latin American population, possibly due to pharmacogenetic factors not yet identified. The main risk factors include duration of treatment, the dose used and the concomitant use of other drugs that produce myelotoxicity.
ABSTRACT
La artritis reumatoide es una enfermedad crónica, sistémica e inflamatoria, de etiología desconocida, que afecta, principalmente la membrana sinovial de las articulaciones. Se caracteriza por dolor crónico, y destrucción articular que conlleva un aumento de la mortalidad y un elevado riesgo de invalidez con altos costos para el enfermo y la sociedad. Describimos el caso de un paciente joven con anemia aplásica desde los 8 años, que inicia en 2009 cuadro de dolor y aumento de volumen articular en manos, muñecas y tobillos bilaterales, cumpliendo los criterios para artritis reumatoide.
Rheumatoid arthritis (RA) is a chronic, systemic, and inflammatory disease of unknown etiology that mainly affects the synovial membrane of the joints. It is characterized by chronic pain and joint destruction, which leads to premature mortality and risk of disability, with high costs to the patient and society. The case is presented of a young male patient with aplastic anemia since 8 years old who, in 2009, began with swelling and joint pain in the hands, wrists and ankles, fulfilling criteria for rheumatoid arthritis.
Subject(s)
Humans , Male , Adult , Arthritis, Rheumatoid , Anemia, Aplastic , Pain , Synovial MembraneABSTRACT
Aunque rara vez se encuentra durante el embarazo, la anemia aplásica (AA) es una complicación grave que aumenta el riesgo de infección y hemorragia, aumentando la morbi-mortalidad materna; por tal motivo, se propone reportar un caso clínico de AA y embarazo. Caso Clínico: Se reporta el caso de una adolescente de 16 años, primigesta, con gestación intrauterina de 15 semanas por biometría fetal y diagnóstico de AA desde hace tres meses, tratada con ciclosporina A y prednisona; la cual ingresa por pancitopenia y cifras tensionales elevadas; conllevando a la decisión de interrumpir el embarazo debido al progresivo deterioro de la salud materna. Conclusión: Si bien la anemia en una de las principales complicaciones durante la gestación, la asociación de AA y embarazo es infrecuente(AU)
Although rarely the aplastic anemia (AA) is present during pregnancy, this is a serious complication that increases the risk of infection and hemorrhage, increased maternal morbidity and mortality; for this reason, we proposed to report a clinical case of AA and pregnancy. Case Report: To report a case of a 16-year-old adolescent, primigravida, with intrauterine gestation of 15 weeks by fetal biometry and diagnosis of AA for three months ago, treated with cyclosporine A and prednisone which is admits by pancytopenia and elevated blood pressure, leading to the decision to interrupt the pregnancy because of the progressive deterioration of maternal health. Conclusion: Although anemia in one of the major complications during pregnancy, the association of AA and pregnancy is uncommon(AU)
Subject(s)
Humans , Female , Adolescent , Pancytopenia , Pregnancy , Cyclosporine/therapeutic use , Anemia, Aplastic/pathology , Gastroenterology , Hemorrhage , InfectionsABSTRACT
Rash is a common side effect associated with antiepileptic drugs. The rate of a phenytoin rash is 5.9 percent and increases to 25 percent in those with another antiepileptic drug rash. Aplastic anemia is an adquired hematopoietic stem-cell disorder characterized by pancytopenia of the peripheral blood and hypocellular bone marrow. The use of phenytoin is associated with a 3.5 fold increased risk of aplastic anemia. We report a case of a 70-year-old woman who developed two severe adverse reactions simultaneously with phenytoin: a maculopapular pruritic rash with involvement of mucous and an aplastic anemia. Both conditions normalized after phenytoin withdrawal.
El rash es un efecto secundario común asociado al uso de fármacos antiepilépticos. La frecuencia de rash con fenitoína se ha estimado en un 5,9 por ciento y asciende a un 25 por ciento en pacientes que han presentado rash con otro fármaco antiepiléptico. La anemia aplásica es una anomalía adquirida de las células madre hematopoyéticas caracterizada por pancitopenia de la sangre periférica y médula ósea hipocelular. Los pacientes tratados con fenitoína presentan un riesgo 3,5 veces mayor de desarrollar anemia aplásica. Presentamos el caso de una mujer de 70 años que desarrolló dos reacciones adversas severas y simultáneas a la fenitoína: un exantema maculopapular pruriginoso con compromiso de mucosas y una anemia aplásica. Ambas condiciones se resolvieron completamente con la suspensión del fármaco.
Subject(s)
Humans , Female , Aged , Anemia, Aplastic/complications , Anemia, Aplastic/chemically induced , Anticonvulsants/adverse effects , Exanthema/complications , Exanthema/chemically induced , Phenytoin/adverse effectsABSTRACT
As diretrizes apresentadas neste trabalho foram elaboradas e aprovadas na I Reunião de Diretrizes Brasileiras em Transplante de Células-Tronco Hematopoéticas (TCTH) realizada no Rio de Janeiro, entre os dias 19 e 21 de julho de 2009. O evento foi promovido pela SBTMO (Sociedade Brasileira de Transplante de Medula Óssea). Neste artigo, tratamos da anemia aplásica severa (AAS), considerada uma urgência hematológica, que, identificada e manejada de forma precoce, apresenta grande possibilidade de recuperação da hematopoese seja através de transplante de medula óssea ou terapia imunossupressora. Objetiva-se nortear o manejo terapêutico no contexto do transplante e indicar formas de condicionamento, de acordo com as características clínicas dos pacientes, como o número de transfusões, com intuito de minimizar a rejeição primária e secundária, garantindo a melhora da sobrevida global e livre de doença (observadas pela literatura e já validadas por resultados na população brasileira). No que concerne à anemia de Fanconi, o transplante é a única modalidade curativa para o componente aplásico de medula óssea; embora não modificando as outras características da síndrome também demanda perícia e agilidade na busca de um doador com resultados expressivos de sobrevida.
The guidelines presented in this article have been prepared and approved in the I Meeting of Brazilian Guidelines in Hematopoietic Stem Cell Transplantation (HSCT) - Rio de Janeiro, July 19-21, 2009. The event was sponsored by SBTMO (Brazilian Society of Bone Marrow Transplantation). In this paper, we treat the severe aplastic anemia (SAA), considered a hematological emergency, that when identified and medically treated early, shows a great chance of recovery of the hematopoiesis, either through bone marrow transplantation or immunosuppressive therapy. Its objective is to guide the management of the transplantation, and indicate methods of conditioning, according to clinical characteristics of each patient, including the number of transfusions, in order to minimize the primary and secondary rejection, ensuring better overall and disease-free survival observed in literature and already validated by the results in our population. In the Fanconi Anemia, transplantation is the only curative option for the aplastic bone marrow component, although insignificant for the other components of the syndrome, it also requires skill and agility in finding a donor with important results.
Subject(s)
Humans , Anemia, Aplastic , Fanconi Anemia , Hematopoietic Stem Cell TransplantationABSTRACT
A aplasia de medula é uma das mais raras (<1 por cento) e sérias complicações após o transplante hepático por insuficiência hepática aguda grave viral não A, não B e não C. Esta condição clínica, que acomete simultaneamente o tecido hepático e o hematopoético, foi descrita pela primeira vez em 1987, por Stock, e a fisiopatologia relacionada é uma condição imunomediada, provavelmente secundária à infecção viral desconhecida, e associada a grave prognóstico. A recuperação espontânea da aplasia medular adquirida habitualmente é muito rara e 50 por cento-70 por cento dos pacientes respondem ao tratamento imunossupressor com ciclosporina A (CsA) e glubulina antitimocítica (ATG), mesmo após o transplante hepático. Além do tratamento imunossupressor, outra opção é o transplante de medula óssea (TMO). Apresentamos o caso de uma criança com aplasia medular grave após transplante hepático, por insuficiência hepática aguda grave, que recebeu tratamento imunossupressor com CsA e ATG e evoluiu com recuperação completa das três séries do hemograma.
Aplastic anemia (AA) is one of the rarest (<1 percent) and most serious complications of liver transplantation for fulminant non-A, non-B and non-C hepatitis. It was first described in 1987 by Stock; the mechanism involved is an immunologically mediated condition secondary to an unknown viral infection. The disease is associated with a dismal prognosis. Spontaneous recovery from acquired AA is very rare however some patients (50-70 percent) recover after immunosuppressive therapy, such as Cyclosporin A (CsA) and Antithymocyte globulin (ATG), even after liver transplantation. Another treatment option is bone marrow transplantation. We report on a child who developed AA following liver transplantation for fulminant viral hepatitis that was treated with intensive immunosuppression including CsA and ATG and achieved complete recovery.
Subject(s)
Humans , Male , Child , Anemia, Aplastic , Bone Marrow Diseases , Bone Marrow Transplantation , Liver Transplantation/adverse effectsABSTRACT
Hematopoietic progenitor cell transplantation from HLA-identical sibling donors cures 70-90 percent of Severe Aplastic Anemia (sAA) patients. Older age, heavy exposure to transfusions, immunosuppression treatment (IST) with a long interval from diagnosis to transplant and infection at procedure are associated with poor outcomes. We transplanted 18 patients with sAA and at least one risk factor (RF) for poor prognosis (age >35 years, >50 transfusions prior to transplant, unresponsiveness to previous IST and bacterial or fungal infection at transplant) from 2001 to 2005, using cyclophosphamide (CY - 5 patients) or busulfan plus CY (13 patients). Sixteen patients engrafted, two died with no engraftment, three patients had evidence of graft failure at days +67, +524 and +638 (two died and one was rescued with IST). Grade III/IV mucositis occurred in 39 percent but neither aGVHD nor cGVHD were observed. The Kaplan-Meier probability of survival was 75 percent at 2.14 years, with a trend favoring survival by number of RF (1 versus =2 RF) (P = 0.06). These results are comparable to recent data reported with fludarabine-based conditioning in patients with poor prognosis sAA. Due to the small sample size, prospective clinical trials with larger cohorts of patients are needed to confirm the real benefits of fludarabine-based conditioning, and also to define the best agent(s) to be associated with Fludarabine as preparative regimen for sAA patients with poor prognosis.
Transplante de medula óssea de doador irmão HLA-idêntico pode curar 70 por cento-90 por cento dos portadores de anemia aplásica severa (AAs). Pacientes mais idosos, muito transfundidos, longamente tratados com imunossupressão (IS) e com infecções ao tempo do transplante têm pior evolução. Nós transplantamos 18 pacientes com AAs e pelo menos um dos fatores associados a pior prognóstico (idade >35 anos, >50 transfusões antes do transplante, falta de resposta à imunossupressão prévia e infecção bacteriana ou fúngica ao transplante) de 2001 a 2005, com ciclofosfamida (Cy - 5 pacientes) ou bussulfan mais Cy (13 pacientes). Dezesseis pacientes apresentaram pega do enxerto, dois morreram sem pega, três tiveram rejeição aos dias +67, +524 e +638 (dois morreram e um foi resgatado com IS). Mucosite grau III/IV ocorreu em 39 por cento e não observamos DECH aguda ou crônica. A probabilidade de sobrevida pelo método de Kaplan-Meier foi de 75 por cento aos 2,14 anos, e uma tendência a melhor sobrevida foi encontrada entre os portadores de apenas um fator de risco ao transplante (P: .06). Estes resultados são comparáveis a recentes relatos de literatura envolvendo condicionamentos baseados em fludarabina para tratar pacientes com alto risco. Devido à pequena amostra analisada, estudos clínicos prospectivos com maior número de pacientes são necessários, visando comprovar o real benefício dos condicionamentos baseados em fludarabina, definir o melhor agente a ser a ela associado e assim obter o melhor condicionamento para portadores de AAs com fatores de mau prognóstico para o transplante.