ABSTRACT
Los inhibidores adquiridos son defectos raros. Se asocian a diferentes manifestaciones clínicas con morbimortalidad significativa. Su detección es importante para implementar el tratamiento sin demora. Hay inhibidores específicos (bloquean función), contra todos los factores de la coagulación y además VWF, o de interferencia (afectan una o varias vías de la coagulación). Los inhibidores específicos son alo-anticuerpos desarrollados en pacientes deficitarios (complicación terapéutica) o auto-anticuerpos presentes en individuos sin alteraciones previas. Hay anticuerpos específicos que pueden afectar la depuración pero no inhiben función. Inhibidores de interferencia: inmunoglobulinas u otras sustancias (heparina/heparinoides, PDF/pdf, PIVKAS, moléculas anómalas, etc.) asociadas a diferentes situaciones clínicas (asintomáticos, sangrados, trombosis y/o complicaciones obstétricas). El laboratorio es fundamental para el diagnóstico. Las pruebas globales detectan el defecto, que no corrigen por el agregado de plasma normal; se caracteriza luego el tipo de inhibidor y eventualmente se titula. Esto es complejo; hay variabilidad en los resultados y posibilidad de falsos positivos o negativos, además las pruebas no son estrictamente específicas. Los algoritmos diagnósticos son útiles, pero no contemplan la posibilidad de defectos combinados. Es crítico caracterizar al inhibidor y descartar posibles interferencias o defectos concomitantes; ello requiere aplicar las pruebas adecuadas e interpretarlas correctamente.
Acquired inhibitors are rare disorders. They are associated with different clinical behaviours and significant morbi-mortality. Detection is important in order to start treatment urgently. There are either specific inhibitors, which block function, against all coagulation factors, and VWF, or with interference effects, on one or more coagulation pathways. Specific inhibitors are either allo-antibodies developed in deficient patients, which give rise to therapeutic complication; or auto-antibodies, which are present in individuals without previous defects. There are specific antibodies that can affect clearance but which cannot block the function. Inhibitors with interference effects are immunoglobulins or other substances (heparin/heparinoids, FDP/fdp, PIVKAS, abnormal molecules, etc.) associated with different clinical settings (asymptomatic, bleeding, thrombosis and/or obstetric complications). Laboratory results are fundamental for the diagnosis. Global tests are able to detect the defect, which is not corrected by the addition of normal plasma; the type of inhibitor is then characterized and titration of the inhibitor is eventually performed. This is complex; there is variability in the results and there is likelihood of false positive or negative results; moreover, the tests are not strictly specific. Diagnostic algorithms are useful tools but they do not consider combined defects. It is a critical point to characterize the inhibitor and exclude possible interferences or concomitant defects; this demands application of the correct tests without misinterpretations.
Os inibidores adquiridos são defeitos raros. Associam-se a diferentes manifestações clínicas com morbimortalidade significativa. Sua detecção é importante para implementar o tratamento sem demora. Há inibidores específicos (bloqueiam função), contra todos os fatores da coagulação e também VWF, ou de interferência (afetam uma ou várias vias da coagulação). Inibidores específicos: - aloanticorpos desenvolvidos em pacientes deficitários (complicação terapêutica); - autoanticorpos, em indivíduos sem alterações prévias. Existem anticorpos específicos que podem afetar a depuração, mas não inibem função. Inibidores de interferência: imunoglobulinas ou outras substâncias (heparina/heparinoides, PDF/pdf, PIVKAS, moléculas anômalas, etc.) associadas a diferentes situações clínicas (assintomáticos, sangramentos, tromboses e/ou complicações obstétricas). O laboratório é fundamental para o diagnóstico. Os testes globais detectam o defeito, que não corrige pelo acréscimo de plasma normal; caracteriza-se depois o tipo de inibidor e eventualmente é titulado. Isto é complexo; há variabilidade nos resultados e possibilidade de falsos positivos ou negativos, além disso os testes não são rigorosamente específicos. Os algoritmos diagnósticos são úteis, mas não consideram a possibilidade de defeitos combinados. É crítico caracterizar o inibidor e descartar possíveis interferências ou defeitos concomitantes; isso requer aplicar os testes adequados e interpretá-los corretamente.
Subject(s)
Humans , Male , Female , Blood Coagulation , Lupus Coagulation Inhibitor , Antibodies , Clinical Laboratory Techniques , Enzyme InhibitorsABSTRACT
El inhibidor lúpico (IL) es uno de los criterios de laboratorio para Síndrome Antifosfolipídico (SAF); sin embargo, puede detectarse en individuos asintomáticos o estar asociado a otras situaciones clínicas. Presentamos un análisis retrospectivo de 1000 exámenes consecutivos para IL (TTPA, DRVVT) de los cuales 249 casos no presentaban criterios clínicos de SAF. Aplicando los criterios SSC-ISTH, hallamos IL+ en 27,30% (205/751) y 43,37% (108/249) de los casos con y sin criterios clínicos de SAF respectivamente; analizándose en estos últimos casos las características clínicas y de laboratorio. Contexto clínico de casos IL+ sin SAF: 18,52% asintomáticos, 34,26% síntomas de sangrado y 47,22% otras manifestaciones. Otras alteraciones de laboratorio en casos IL+ sin SAF, con síntomas de sangrado: detectamos alteraciones plaquetarias, descenso de VWF:RCo y/o VWF:Ag, disminución de FVIII, FV, FVII, FXI o fibrinógeno e hiperfibrinolisis en el 54,05% de los casos. El análisis mostró detección de IL+ en un número importante de estudios (108/1000) sin criterios SAF. Los casos con IL+ y sangrado representan un desafío particular, al requerir evaluar otros posibles defectos subyacentes, que pudiesen justificar el comportamiento clínico. La detección e identificación de defectos combinados requiriere de un análisis minucioso, a fin de alcanzar un diagnóstico correcto, esencial para tomar decisiones terapéuticas adecuadas. (AU)
Despite lupus anticoagulant (LA) is one of the laboratory criteria for antiphospholipid syndrome (APS), it can be present in asymptomatic subjects or it can be associated with other clinical settings. We present a retrospective analysis of 1000 consecutive LA assays (APTT, DRVVT), 249 of them were performed in patients without clinical criteria for APS. According to ISTH criteria, positive LA was found in 27.30% (205/751) and 43.37% (108/249) of cases with or without APS criteria respectively; in the last group, the analysis of clinical background and laboratory characteristics was done. Clinical background of LA+ cases without APS: 18.52% asymptomatic, 34.26% bleeding symptoms and 47.22% other clinical settings. Other abnormal laboratory tests in LA+ cases without APS and bleeding symptoms: platelet dysfunction; low VWF:RCo and/or VWF:Ag; decrease of FVIII, FV, FVII, FXI or fibrinogen and hyperfibrinolysis were found in the 54.05% of the cases. The analysis showed positive LA in an important number of cases (108/1000) without criteria of APS. Those LA+ cases with bleeding symptoms represent a particular challenge because other possible underlying defects have to be analysed in order to explain the clinical behaviour. The detection and identifications of combined defects required a careful analysis in order to achieve accurate diagnosis, essential for therapeutic decisions. (AU)
Subject(s)
Humans , Lupus Coagulation Inhibitor/analysis , Lupus Coagulation Inhibitor/blood , Antiphospholipid Syndrome , Blood Platelet Disorders , Diagnosis, DifferentialABSTRACT
Introducción: Los antagonistas de la vitamina K, tienen como blanco el complejo vitamina K epóxido reductasa. Hay polimorfismos (SNPs) en el gen de la subunidad 1 (VKORC1), como 1173 C>T (rs9934438) (intrón 1) y -1639 G>A (rs9923231) (región 3'UTR), asociados con diferente sensibilidad a los dicumarínicos. Objetivo: confirmar la relación entre estos SNPs y la dosis media requerida para una correcta anticoagulación. Material y Método: Estudiamos 102 pacientes (15-87 años) bajo tratamiento anticoagulante oral crónico, principalmente acenocumarol. La genotipificación fue realizada usando RFLPs (amplificación del ADN por PCR, seguida por digestión con Msp I para -1639 G>A y Sty I para 1173 C>T); analizándose luego la dosis media en los portadores de los diferentes SNPs. La frecuencia alélica obtenida para 1173 C>T fue similar a la calculada para -1639 G>A, observándose que 1179 C>T y -1639 G>A se hallan en desequilibrio de unión. La dosis media fue más alta en los pacientes portadores hemocigotos del alelo 1173 CC o -1639 GG que en los no portadores. La dosis media fue menor en individuos mayores de 70 años, independientemente de su genotipo. Reultados: Estos confirman la relación entre los SNPs analizados y la dosis de dicumarínicos.
Vitamin K epoxide reductase complex is the target of Vitamin K antagonists. Polymorphism (SNPs) in the gene of subunit 1 (VKORC1), 1173 C>T (rs9934438) (intrón 1) y -1639 G>A (rs9923231) (3'UTR), are associated with different sensitivity to oral anticoagulants. Objectives: our aim was to comfirm the relationship between these SNPs and the mean dose required for anticoagulation. Material and methods: One hundred and two patients (15-87 years) on chronic oral anticoagulant therapy, mainly acenocoumarol, were tested. Genotyping was performed using RFLPs (DNA's PCR amplification, followed by digestion with Msp I to Sty I to 1173 C>T). The mean dose of anticoagulantin carriers of different SNPs was calculated. A similar allelic frequency was obtained for 1173 C>T and -1639 G>A with linkage desequilibrium between them. The mean dose was higher in patients homozygous for 1173 CC or -1639 GG alleles than in non carriers. In those individuals over the age of 70, regardless of genotype, a lower mean dose was observed. Results: The results confirm the relationship between SNPs and oral anticoagulants.