Corpora amylacea in the neocortex in patients with temporal lobe epilepsy and focal cortical dysplasia.

INTRODUCTION: Corpora amylacea (CoA) are present in about 60% of atrophic hippocampi resected from patients with drug resistant temporal lobe epilepsy (DRTLE). They have also been described in the lateral temporal neocortex, although less frequently. OBJECTIVE: The objective is to measure the presence, distribution and density of CoA in the lateral temporal lobes of patients with DRTLE and focal cortical dysplasia (FCD), also examining how CoA density may be linked to demographic and clinical traits. METHODS: Resected tissue from 35 patients was analysed. CoA density was assessed with a semi-quantitative scale according to the criteria established by Cherian et al. RESULTS: Presence of CoA in the neocortex of 9 patients was associated with hippocampal sclerosis (FCD type iiia, 7 cases), disembryoplastic neuroepithelial tumour (FCD type iiib, 1 case), and cavernous angioma (FCD type iiic, 1 case). The meningeal surface (MS) was involved in all cases, and 8 cases displayed CoA in the cerebral parenchyma (white matter) and around blood vessels. CoA density on the MS showed a negative correlation with age at seizure onset (r = -0.828, P<.05) and a positive correlation with disease duration (r = 0.678, P<.05) but not with postoperative clinical outcome. CONCLUSIONS: Patients with DRTLE and a primary lesion (hippocampal sclerosis, tumour, vascular malformation) associated with mild FCD were shown to have CoA deposits in the neocortex. No association was found between presence of CoA and clinical outcome one year after surgery.

[Immune events in central nervous system of early and late onset Alzheimer's disease patients]. / Eventos inmunológicos en el sistema nervioso central de pacientes con enfermedad de Alzheimer temprana y tardía.

INTRODUCTION: Alzheimer s disease (AD) is a progressive degenerative disease affecting a significant proportion of the elderly population. The disease is characterized clinically by a progressive loss of memory function and mental impairment associated with the presence of degenerative well known pathological lesions. Although, the pathogenesis of AD is unclear; several reports indicate the involvement of immune factors. PATIENTS AND METHODS: This paper evaluates some cerebrospinal fluid immune markers from 21 patients with early and late AD and 20 age matched non-demented subjects. The analytical method included the evaluation of T cell subpopulations (using AcMc CD2, CD4, CD8) and activated T cells (AcMc HLA-DR and CD25) from CSF and peripheral blood by immunocytochemical techniques on a fixed cell slide as described by Bernd. The lymphocyte phenotype expressed as a percentage of positively stained cells for each cell surface marker evaluated. RESULTS: Some significant differences were observed for T cell subpopulations from different compartments, between the different AD groups and the controls (p< 0.05). Nevertheless, the most significant differences were found in the activated T cells from cerebrospinal fluid between AD groups and controls (p< 0.01). CONCLUSIONS: These results support the theory of neuroimmune dysregulation, probably involved in the progressive neurodegeneration and dementia in some AD.

[Nerve growth factor in neurodegeneration and neurorestorative therapy]. / El factor de crecimiento nervioso en la neurodegeneración y el tratamiento neurorrestaurador.

AIMS: The purpose of this work was to gather the information currently available about the content of nerve growth factor (NGF) in experimental models of neurodegeneration and in neurodegenerative diseases, including Alzheimer's, Parkinson's and Huntington's diseases, as well as to analyse how NGF content is affected by the application of different neurorestorative therapies (transplant and trophic therapy) in these neurological entities. DEVELOPMENT: Neurotrophins are proteins that promote the differentiation, growth and survival of many populations of peripheral neurons and the central nervous system during development and adulthood. NGF is the best known and most widely researched member of this family, which is also made up of the growth factor derived from the brain and neurotrophins 3, 4/5, 6 and 7. In the last few decades, significant progress has been made in the knowledge available about the biological role played by these factors, their molecular characterisation and regulation, as well as their signalling mechanisms. Yet, little is known about the role played by the neurotrophic factors in neurodegenerative diseases or whether the levels of these factors are modified following the use of neurorestorative treatment. CONCLUSIONS: Neurodegenerative disorders, especially Parkinson and Alzheimer, are accompanied by modifications in the levels of NGF that depend on the extent to which the disease has progressed. A model of the changes in NGF content during neurodegenerative processes is also proposed.

[Immunological disorders in epileptic patients are associated to the epileptogenic focus localization]. / Alteraciones inmunológicas en pacientes epilépticos asociadas a la localización del foco epileptogénico.

OBJECTIVE: Clinical and experimental data support the role of immune mechanisms in the pathogeny of epilepsy. The purpose of this work was to study the immunological aspects in 30 epileptic patients with complex partial crisis resistant to antiepileptic drugs. PATIENTS AND METHODS: The patients were evaluated by EEG-Video and they were grouped attending to epileptogenic focus localization in: temporals (n = 16), lateralized (n = 6) and extratemporals (n = 4). We also studied a group with psychogenic epilepsy (n = 4), this group was diagnosed after EEG-video evaluation. The following immunological evaluations has been carried out: levels of serum immunoglobulins (IgG, IgM e IgA) by radial immunodiffusion test and lymphocytic subpopulations using immunocytochemical methods. We measured the percent of T and B lymphocytes (CD3 and CD20), helper/inductor lymphocyte T (CD4), suppressor/cytotoxic (CD8), interleukine-2 receptor (CD25) and human leukocyte antigen (HLA-DR). RESULTS: The results show a significant increase of CD8+ lymphocytes (p < 0.05) and in the activation markers (CD25+ and HLA-DR+ cells). The evaluation of immunological parameters applied to different group of epileptogenic focus localization shown that the increase of CD8+ lymphocytes is limited to temporal and lateralized patients (p < 0.01). The patients with extratemporal localization of focus and the psychogenic cases shown normal values for the evaluated immunological lymphocyte markers. We did not find a deficit in the humoral immunological aspects. CONCLUSIONS: Taking into account that patients diagnosed as psychogenic received an antiepileptic drug treatment identical to that of the other group, the observed immunological changes might be related with the patogeny of certain epilepsy variants associated with the focus localization and not with the medication.

[Endogenous nerve growth factor in patients with Alzheimer s disease]. / Factor de crecimiento nervioso endógeno en pacientes con enfermedad de Alzheimer.

INTRODUCTION: Nerve growth factor (NGF) is the best characterized neurotrophic polypeptide. Initially it was postulated that alterations in the expression of NGF within its production sites may be responsible for the consistent atrophy and loss of cholinergic basal forebrain neurons in dementing illness such as Alzheimer s Disease (AD). OBJECTIVE: We analyze the NGF concentration in serum from control and patients with AD in order to elucidate something alteration in this fluid related with AD neuropathology. PATIENTS AND METHODS: We applied a twosite enzyme immunoassay to determine NGF levels in sera of patients with AD. RESULTS: Sera from Alzheimer s patients (36+/-7 pg/ml) showed slight but non significant reduction in NGF levels when compared with age related controls (66+/-18 pg/ml). On the another hand, the NGF concentrations in AD patients and control subjects to the sex were following: female AD patients showed a mean of 33.27+/-10.43 pg/ml vs 57.83+/-22 pg/ml founded in female controls, while the mean value for male AD patients was 40.87+/-12.29 pg/ml vs 37.47+/-12.28 pg/ml for the male controls. In all the cases studied, no significant differences were observed according to Student t-Test. CONCLUSIONS: Even when no significant differences were observed between controls and AD patients, the results show a tendency NGF concentration decrease in this illness. Certainly, NGF is produced not only in the forebrain but throughout the body, for this reason, more studies, including the analysis of cerebrospinal fluid would be useful to define the real relationship between NGF concentration changes in serum and AD-related changes in endogenous NGF concentrations, taking into account increasing levels by exogenous NGF administration could still be useful in maintaining the cholinergic neurons.

[Stromal cell transplant in the 6-OHDA lesion model]. / Trasplante de células estromales en el modelo de lesión por 6-OHDA.

INTRODUCTION: A good deal of evidence currently exists to show that transplanting foetal mesencephalic tissue can produce symptomatic benefits both in patients and in disease models. Nevertheless, the technical and ethical difficulties involved in obtaining enough suitable foetal cerebral tissue have been a serious obstacle to its application. Stromal cells derived from bone marrow, due to their potential capacity to generate different types of cells, could be an ideal source of material for cell restoration in neurodegenerative diseases. AIMS: Our aim was to evaluate the effect of transplanting stromal cells derived from bone marrow on the behaviour of 6-OHDA rats, when they are inserted into the striatum. MATERIAL AND METHODS: In this study we used rats with a lesion in the substantia nigra induced by 6-hydroxydopamine, divided into several experimental groups. Rotary activity induced by D-amphetamine (5 mg/kg, intraperitoneally) was evaluated before and throughout the three months following the transplant in all the experimental groups, except in the group of healthy controls. Hemiparkinsonian rats received a total of 350 000 foetal ventral mesencephalic cells and 8 x 10(4) stromal cells/microL, which were implanted in the striatum. RESULTS AND CONCLUSIONS: Animals with stromal cells transplanted in the body of the striatum significantly reduced the number of turns induced by amphetamine (p < 0.05); yet this reduction was not greater than that induced by foetal mesencephalic cell transplants. We were also unable to demonstrate any significant improvement in the motor skills of the forelimbs.

[Effects of simultaneous transplant of foetal mesencephalic cells in the striatum and the subthalamic nucleus of hemiparkinsonian rats]. / Efectos del trasplante simultáneo de células mesencefálicas fetales en el estriado y el núcleo subtalámico de ratas hemiparkinsonianas.

INTRODUCTION: The main strategy followed in neural transplants as a method of treatment for Parkinson s disease, both experimental and clinical, has been to introduce foetal mesencephalic cells into the target area: the striatum. However, when the dopaminergic cells in the substantia nigra degenerate, not only is the dopaminergic innervation of the striatum affected but also other nuclei: globus pallidus, substantia nigra, substantia nigra pars reticulata and subthalamic nucleus. A series of data from pharmacological and physiological studies offer strong evidence that the dopamine released in these nuclei may play an important role in regulating the output nuclei of the basal ganglia. AIM: To evaluate the effect of transplanting foetal mesencephalic cells on the behaviour of 6 OH DA rats when introduced into the striatum and the subthalamic nucleus. MATERIALS AND METHODS: 6 OH DA was used to induce lesions in the substantia nigra of rats, which were divided into several experimental groups. The rotating activity induced by D amphetamine (5 mg/kg, intraperitoneally) and apomorphine (0.05 mg/kg, subcutaneously) was evaluated before and three months after the transplant in all the experimental groups, except in the control group of healthy rats. The hemiparkinsonian rats received a total of 350,000 foetal ventral mesencephalic cells, which were implanted within small deposits in the striatum (8) and in the subthalamic nucleus (4). RESULTS AND CONCLUSIONS: Rotation induced by both drugs was significantly lower (p= 0.05) in animals that had had dopaminergic cells transplanted into the striatum body. No significant improvement in this behaviour was to be found when transplants were limited to just the subthalamus or, simultaneously, also to the striatum. A significant increase in rotating behaviour induced by apomorphine was observed in the group which received a transplant in just the subthalamus.

BDNF in quinolinic acid lesioned rats after bone marrow cells transplant.

Brain-derived neurotrophic factor (BDNF) concentration was measured in the striatum and cortex after quinolinic acid intrastriatal lesion and transplantation of bone marrow cells (BMSC). The results showed a significant increase of the BDNF levels in the striatum and cortex of the lesioned animals and the ability of the transplanted cells to increase the levels of BDNF in both sites. This recovery of BDNF production and distribution might have beneficial effects and ameliorate the negative consequences of the striatal lesion, a mechanism of potential interest for the treatment of Huntington's disease (HD).

Tumores cerebrales en el programa de cirugía de la epilepsia del Centro Internacional de Restauración Neurológica (La Habana) / Brain tumors in the epilepsy surgery program of International Center for Neurological Restoration (La Habana)

Objetivo: Determinar la asociación de los tumores cerebrales con otras lesiones en los pacientes sometidos a cirugía de epilepsia en el Centro Internacional de Restauración Neurológica (CIREN La Habana,Cuba), así como el impacto en la evolución clínica posterior a la resección guiada por electrocorticografía (ECoG).Métodos: De los 47 pacientes con epilepsia farmacorresistente operados en el CIREN, se realizó un estudio descriptivo de aquellos con diagnóstico confirmado de tumor cerebral. Se efectuaron resecciones guiadas por ECoG y el diagnóstico histopatológico se realizó según la clasificación de la Organización Mundial de la Salud. Para el diagnóstico microscópico de displasia cortical focal se utilizó el sistemapropuesto por la Liga Internacional contra la Epilepsia. La escala de Engel modificada fue aplicada para el seguimiento postquirúrgico.Resultados: El promedio de edad previo a la cirugía fue de 32,8 años (5-19 años) y la duración promedio de la epilepsia fue de 21,5 años (2-42 años). El análisis histológico confirmó la presencia de tumor en 6 pacientes (3 gangliogliomas, 2 astrocitomas pilocíticos y 1 tumor neuroepitelial disembrioplásico); 4 correspondieron al lóbulo temporal y 2 extratemporales y de ellos, 3 estuvieron asociados a displasia cortical focal. La evolución postquirúrgica fue satisfactoria, estando libres de crisis en su última evaluación, 5 pacientes (rango de 7 y 9 años, estadios Ia, Ib y Ic). La paciente restante logró una reducción considerable de las crisis (5 años y medio de operada con un estadio IIIa).Conclusiones: La resección del tumor guiada por ECoG permite diagnosticar otras lesiones no identificadas en las resonancias magnéticas en el 50 Por ciento de los casos y cuya epileptogenicidad ha sido demostrada. La evolución clínica favorable en la mayoría de los pacientes sugiere la utilidad de la ECoG intraoperatoria para la adecuada resección de la zona epileptogénica(AU)

OBJECTIVE: To determine the association of brain tumors with other lesions in patients undergoing epilepsy surgery at the International Center for Neurological Restoration (CIREN –Havana, Cuba), as well as the impact on clinical evolution following the resection guided by electrocorticography (ECoG).METHODS: Of the 47 patients with epilepsy operated in the CIREN, a descriptive study was conducted of those with confirmed diagnosisof brain tumor. Resections guided by ECoG were carried out and the histopathological diagnosis was carried out according to the classification of the World Health Organization. The system proposed by the International League against Epilepsy was used for themicroscopic diagnosis of focal cortical dysplasia. The modified Engel scale was applied for post-surgical follow-up.RESULTS: The average age prior to surgery was 32.8 years (5-19 years) and the mean duration of epilepsy was 21.5 years (2-42 years).Histological analysis confirmed the presence of tumor in 6 patients (3 Gangliogliomas, 2 pilocytic astrocytomas and 1 dysembryoplasticneuroepithelial tumor); 4 corresponded to the temporal lobe and 2 extratemporals and of them, 3 were associated with focal cortical dysplasia. The postsurgical evolution was satisfactory, being free of seizures in its last evaluation, 5 patients (range of 7 and 9 years, grades Ia, Ib and Ic). The remaining patient achieved a considerable reduction in seizures (5 and half years of surgery with a grade IIIa).CONCLUSIONS: The resection of the tumor guided by ECoG allows diagnosing other unidentified lesions in the magnetic resonances in 50 Per cent of the cases and whose epileptogenicity has been demonstrated. Favorable clinical evolution in most patients suggests the usefulness of intraoperative ECoG for the adequate resection of the epileptogenic zone(AU)

Cuerpos amiláceos en la neocorteza de pacientes con epilepsia del lóbulo temporal y displasia cortical focal / Corpora amylacea in the neocortex in patients with temporal lobe epilepsy and focal cortical dysplasia

Introducción: Los cuerpos amiláceos (CoA) se presentan en aproximadamente el 60% de los hipocampos atróficos resecados de pacientes con epilepsia del lóbulo temporal farmacorresistente (ELTFR). Su presencia en la neocorteza temporal lateral ha sido observada con menor frecuencia. Objetivo: El objetivo es evaluar la presencia, la distribución y la densidad de CoA en el lóbulo temporal lateral de pacientes con ELTFR y displasia cortical focal (DCF) y la relación de su densidad con variables demográficas y clínicas. Métodos: Analizamos histológicamente el tejido resecado de 35 pacientes con ELTFR. La densidad de los CoA fue evaluada con una escala semicuantitativa según los criterios de Cherian et al. Resultados: La presencia de CoA en la neocorteza de 9 pacientes estuvo asociada a esclerosis hipocampal (DCF tipo IIIa, 7 casos), tumor neuroepitelial disembrioplásico (DCF tipo IIIb, un caso) y angioma cavernoso (DCF tipo IIIc, un caso). Todos los pacientes tuvieron afectación de la superficie meníngea (SM) y en 8 casos se localizaron en el parénquima cerebral (sustancia blanca) y alrededor de los vasos sanguíneos. La densidad de los CoA en SM tuvo una correlación negativa con la edad de inicio de las crisis (r = -0,828, p < 0,05) y positiva con la duración de la enfermedad (r = 0,678, p < 0,05) pero no con la evolución clínica postquirúrgica. Conclusiones: En pacientes con ELTFR con lesión principal (EH, tumor, malformación vascular) asociada a DCF ligeras se constata la acumulación de CoA en la neocorteza. No se encontró una asociación entre la presencia de CoA y la evolución clínica al año de la cirugía

Introduction: Corpora amylacea (CoA) are present in about 60% of atrophic hippocampi resected from patients with drug resistant temporal lobe epilepsy (DRTLE). They have also been described in the lateral temporal neocortex, although less frequently. Objective: The objective is to measure the presence, distribution and density of CoA in the lateral temporal lobes of patients with DRTLE and focal cortical dysplasia (FCD), also examining how CoA density may be linked to demographic and clinical traits. Methods: Resected tissue from 35 patients was analysed. CoA density was assessed with a semi-quantitative scale according to the criteria established by Cherian et al. Results: Presence of CoA in the neocortex of 9 patients was associated with hippocampal sclerosis (FCD type IIIa, 7 cases), disembryoplastic neuroepithelial tumour (FCD type IIIb, 1 case), and cavernous angioma (FCD type IIIc, 1 case). The meningeal surface (MS) was involved in all cases, and 8 cases displayed CoA in the cerebral parenchyma (white matter) and around blood vessels. CoA density on the MS showed a negative correlation with age at seizure onset (r = -0.828, P < .05) and a positive correlation with disease duration (r = 0.678, P < .05) but not with postoperative clinical outcome. Conclusions: Patients with DRTLE and a primary lesion (hippocampal sclerosis, tumour, vascular malformation) associated with mild FCD were shown to have CoA deposits in the neocortex. No association was found between presence of CoA and clinical outcome one year after surgery

Microscopic mild focal cortical dysplasia in temporal lobe dual pathology: an electrocorticography study.

BACKGROUND: Associations between electrophysiological and histological findings might provide an insight into the epileptogenicity of mild focal cortical dysplasia (FCD) in patients with temporal lobe epilepsy (TLE) and a dual pathology. SUBJECTS AND METHODS: A total of 22 patients with pharmacoresistant TLE were included in the study, 16 of them with histologically confirmed hippocampal sclerosis (HS) associated with neocortical temporal mild Palmini Type-I FCD subtypes and 6 with HS. Intraoperative electrocorticography (ECoG) recordings were analysed for epileptiform discharge frequency and morphology. Associations between histological, and electrocorticography pattern findings in these patients were analysed. Electroclinical outcomes in these patients were also evaluated. RESULTS: Neocortical areas with mild Palmini Type-I FCD showed a significantly higher spike frequency (SF) recorded in the inferior temporal gyrus than those neocortical areas in patients with HS. There was a tendency to higher spike frequency and lower amplitude in neocortical areas with histopathologic subtype IB FCD in relation with IA during intraoperative ECoG. Post-SF excision and amplitude were significantly lower during neocortical post-excision intraoperative ECoG than during neocortical pre-excision recording. There was no difference found in the clinical outcome between patients with and without FCD. CONCLUSIONS: Intraoperative electrocorticographic interictal spike frequency recorded in the neocortical inferior temporal gyrus may help to characterize the histopathologic subtypes of mild Palmini Type-I FCD in patients with temporal lobe epilepsy (TLE) and a dual pathology. Our data support the epileptogenicity of neocortical mild FCD in TLE and assessments of ECoG patterns are relevant to determine the extent of the resection in these patients which can influence the electroclinical outcome.

[Neuronal death in the neocortex of drug resistant temporal lobe epilepsy patients]. / Muerte neuronal en la neocorteza de pacientes con epilepsia del lóbulo temporal resistente a fármacos.

Introduction. Participation of apoptotic death mechanisms in drug resistant temporal lobe epilepsy (DRTLE) is currently under great debate. We have investigated if there is neuronal loss and the immunodetection to different markers in neocortical tissue death in eigth patients with DRTLE. The neocortexes of five patients deceased due to non-neurological causes, paired in age and gender were evaluated as control tissue. Methods. The evaluation of neuronal loss was made by means of a stereological study and with immunohistochemical techniques with the synaptophysin marker. Immunopositivity to different apoptotic markers (annexin V, caspase 3 and 8, bcl-2 and p53) and detection of deoxyribonucleic acid (DNA) fragmentation (TUNEL) were analyzed and double labeling with synaptophysin was performed in every case. The results were evaluated with confocal microscope and analyzed with the Zeiss LSM 5 Image Browser Program, 2.80.1113 (Germany). Results. A statistically significant decrease in the total number of cells (p < 0.05) and the synaptophysin cells+ (p<0.01) in the neocortex (layer IV) of the patients with DRTLE when compared with the control tissue was found. No significant differences were found in the apoptotic markers bcl-2, p53, caspase 3 and 8 for any of the neocortex layers while there was a statistically significant increase in the number of TUNEL cells+ (p<0.05) and annexin V+ (p<0.05) in the neocortical layer IV of the patients. Conclusions. This group of evidence speaks in favor of the existence of an effect on the neuronal number in the neocortex layer IV that may be associated with noncaspase dependent apoptotic death process, without being able to rule out death by necrosis. Key words: Drug resistant temporal lobe epilepsy. Apoptosis. Necrosis. Neuronal loss. Neurología 2008;23(9):555-565.

[Pathological neocortical findings in patients with medication-resistant medial temporal lobe epilepsy submitted to surgery]. / Hallazgos patológicos neocorticales en pacientes con epilepsia del lóbulo temporal medial farmacorresistente sometidos a cirugía.

INTRODUCTION: The dual pathology consisting of hippocampal sclerosis plus focal cortical dysplasia (FCD) is often reported in patients with medication-resistant medial temporal lobe epilepsy (MTLE). AIMS: To determine the histopathological changes that take place in the neocortex of patients with medication-resistant MTLE submitted to surgery and to evaluate the relation between the histopathological changes, pathological background and the clinical course of patients who had received surgical treatment. MATERIALS AND METHODS: Tissue obtained by en bloc resection from the neocortex of 18 patients with MTLE refractory to medical treatment was processed histologically and a tailored temporal lobectomy was performed with electrocorticography. RESULTS: Dual pathology was diagnosed in 13 patients (72.2%). Imaging studies confirmed the existence of mesial sclerosis of the temporal in 100% of cases and there was no evidence of neocortical lesions. Histologically, 46.15% and 38.46% of the patients were diagnosed as belonging to FCD type 1a and FCD type 1b, respectively. Only one patient presented FCD type 2a. A statistically significant relation was found between the presence of dual pathology and the existence of an early precipitating injury (p = 0.04). One year after surgery, 72.7% (8/11) patients with dual pathology were classified as belonging to Engel class I. CONCLUSIONS: In patients with MTLE there are microscopic FCD-type alterations in the neocortex. There is an association between these alterations and the existence of an initial precipitating injury. Complete resection of the epileptogenic area, which is guaranteed by the lobectomy tailored by electrocorticography, allows patients to enjoy a favourable post-surgical progression one year after surgery.

Purification and characterization of murine beta-nerve growth factor.

Beta-nerve growth factor (beta-NGF) is a trophic factor in the nervous system. We aimed to isolate and characterize this protein in view of its potential therapeutic use in neurodegenerative diseases. For purification a two-step ion-exchange procedure was followed. The characterization was performed using separation and immunological techniques, as well as a biological assay. These studies showed that the obtained protein consisted of a mixture of beta-NGF molecules, intact at their NH2-terminal extreme, and molecules which have lost the NH2-terminal octapeptide and exhibit modifications increasing its hydrophobicity. All these molecular species were recognized immunologically and showed biological activity.

Hallazgos patológicos neocorticales en pacientes con epilepsia del lóbulo temporal medial farmacorresistente sometidos a cirugía / Pathological neocortical findings in patients with medication-resistant medial temporal lobe epilepsy submitted to surgery

Introducción. La patología dual compuesta por esclerosis hipocampal y displasia cortical focal (DCF) se describecon frecuencia en pacientes con epilepsia del lóbulo temporal medial (ELTM) farmacorresistente. Objetivos. Determinar los cambios histopatológicos en la neocorteza de pacientes con ELTM farmacorresistente sometidos a cirugía y evaluar la relación entre los cambios histopatológicos, los antecedentes patológicos y la evolución clínica en los pacientes operados. Materialesy métodos. Se procesó histológicamente el tejido resecado en bloque (neocorteza) de 18 pacientes con ELTM refractaria a tratamiento médico, y se les realizó lobectomía temporal ajustada por electrocorticografía. Resultados. Se diagnóstico patología dual en 13 pacientes (72,2por ciento). Los estudios imagenológicos confirmaron en el 100por ciento de los casos la esclerosis mesial del temporal y no existieron evidencias de lesión neocortical. Histológicamente, el 46,15 por ciento y el 38,46 por ciento de los pacientesfueron diagnosticados como DCF tipo 1a y DCF tipo 1b, respectivamente. Sólo un paciente presentó DCF tipo 2a. Se demostró una relación estadísticamente significativa entre la presencia de patología dual y la existencia de una daño precipitante inicial (p = 0,04). El 72,7por ciento (8/11) de los pacientes con patología dual un año después de la cirugía se clasificó en la clase Ide Engel. Conclusiones. En los pacientes con ELTM existen alteraciones microscópicas en la neocorteza del tipo DCF. Estas alteraciones se asocian a la existencia de un daño precipitante inicial. La resección completa de la zona epileptogénica, garantizada por la lobectomía ajustada por electrocorticografía, permite una buena evolución posquirúrgica un año después de la cirugía(AU)

INTRODUCTION: The dual pathology consisting of hippocampal sclerosis plus focal cortical dysplasia (FCD) is often reported in patients with medication-resistant medial temporal lobe epilepsy (MTLE). AIMS: To determine the histopathological changes that take place in the neocortex of patients with medication-resistant MTLE submitted to surgery and to evaluate the relation between the histopathological changes, pathological background and the clinical course of patients who had received surgical treatment. MATERIALS AND METHODS: Tissue obtained by en bloc resection from the neocortex of 18 patients with MTLE refractory to medical treatment was processed histologically and a tailored temporal lobectomy was performed with electrocorticography. RESULTS: Dual pathology was diagnosed in 13 patients (72.2percent). Imaging studies confirmed the existence of mesial sclerosis of the temporal in 100 percent of cases and there was no evidence of neocortical lesions. Histologically, 46.15 percent and 38.46 percent of the patients were diagnosed as belonging to FCD type 1a and FCD type 1b, respectively. Only one patient presented FCD type 2a. A statistically significant relation was found between the presence of dual pathology and the existence of an early precipitating injury (p = 0.04). One year after surgery, 72.7percent (8/11) patients with dual pathology were classified as belonging to Engel class I. CONCLUSIONS: In patients with MTLE there are microscopic FCD-type alterations in the neocortex. There is an association between these alterations and the existence of an initial precipitating injury. Complete resection of the epileptogenic area, which is guaranteed by the lobectomy tailored by electrocorticography, allows patients to enjoy a favourable post-surgical progression one year after surgery(AU)

El factor de crecimiento nervioso en la neurodegeneración y el tratamiento neurorrestaurador / Nerve growth factor in neurodegeneration and neurorestorative therapy

AIMS: The purpose of this work was to gather the information currently available about the content of nerve growth factor (NGF) in experimental models of neurodegeneration and in neurodegenerative diseases, including Alzheimer's, Parkinson's and Huntington's diseases, as well as to analyse how NGF content is affected by the application of different neurorestorative therapies (transplant and trophic therapy) in these neurological entities. DEVELOPMENT: Neurotrophins are proteins that promote the differentiation, growth and survival of many populations of peripheral neurons and the central nervous system during development and adulthood. NGF is the best known and most widely researched member of this family, which is also made up of the growth factor derived from the brain and neurotrophins 3, 4/5, 6 and 7. In the last few decades, significant progress has been made in the knowledge available about the biological role played by these factors, their molecular characterisation and regulation, as well as their signalling mechanisms. Yet, little is known about the role played by the neurotrophic factors in neurodegenerative diseases or whether the levels of these factors are modified following the use of neurorestorative treatment. Neurodegenerative disorders, especially Parkinson and Alzheimer, are accompanied by modifications in the levels of NGF that depend on the extent to which the disease has progressed. A model of the changes in NGF content during neurodegenerative processes is also proposed(AU)

Eventos inmunológicos en el sistema nervioso central de pacientes con enfermedad de Alzheimer temprana y tardía / Immune events in central nervous system of early and late onset Alzheimerïs disease patients

La enfermedad de Alzheimer es un trastorno neurodegenerativo de carácter progresivo que afecta a una proporción significativa de la población de edad avanzada. La enfermedad se caracteriza clínicamente por una pérdida progresiva de la memoria y deterioro intelectual asociado a la presencia de lesiones patológicas degenerativas bien conocidas. Sin embargo, la patogénesis de la enfermedad de Alzheimer no está clara; numerosos estudios indican la implicación de factores inmunológicos. Pacientes y métodos. Este artículo evalúa algunos marcadores inmunológicos del líquido cefalorraquídeo de 21 pacientes con Alzheimer temprano o tardío y 20 sujetos sin demencia de la misma edad que los afectados. El método analítico incluye la evaluación de la subpoblación de células T (utilizando AcMc CD2, CD4, CD8) y de las células T activadas (AcMc HLA-DR y CD25), del líquido cefalorraquídeo y de la sangre periférica mediante técnicas inmunohistoquímicas sobre preparaciones celulares fijadas en láminas según lo descrito por Bernd. El fenotipo del linfocito se expresó como porcentaje de células teñidas positivamente para cada uno de los marcadores de la superficie celular evaluados. Resultados. Se han observado algunas diferencias significativas entre las subpoblaciones de células T en los diferentes fluidos, para los diferentes grupos de Alzheimer y los controles (p<0,05). No obstante, las diferencias más significativas se encontraron entre las células T activadas del líquido cefalorraquídeo en los grupos de Alzheimer comparados con los controles (p<0,01). Conclusiones. Estos resultados apoyan la teoría de la disregulación neuroinmunológica, que probablemente está implicada en la progresiva degeneración y demencia en algunos casos de Alzheimer(AU)

Alteraciones inmunológicas en pacientes epilépticos asociadas a la localización del foco epileptogénico

Datos clínicos y experimentales evidencian el papel del sistema inmune en la patogenia de la epilepsia. El propósito de este trabajo es mostrar los resultados de los estudios inmunológicos realizados a 30 pacientes epilépticos con crisis parciales complejas refractarias a tratamiento médico, evaluados por vídeo-EEG. Pacientes y métodos. Los pacientes se agruparon de acuerdo con la localización del foco epileptogénico en: temporales (n = 16), lateralizados (n = 6) y extratemporales (n = 4). Se estudiaron, además, pacientes (n = 4) diagnosticados según la evaluación por vídeo-EEG como epilepsia psicógena. Se determinaron los niveles de inmunoglobulinas (IgG, IgM e IgA) por inmunodifusión radial y se cuantificaron por inmunocitoquímica los linfocitos T y B (CD3 y CD20), así como los marcadores linfocitarios: CD4, CD8, CD25 y HLA-DR. Resultados. Se evidenció un aumento significativo en el porcentaje de linfocitos T CD8+ (supresores/citotóxicos, p < 0,05) y de los marcadores de activación CD25 (células receptor IL-2) y HLA-DR (antígeno leucocitario humano DR). La evaluación de los parámetros inmunológicos en los diferentes grupos de localización del foco epileptogénico mostró que el aumento significativo de los linfocitos CD8+ se limita a los casos temporales y lateralizados (p < 0,01). Los pacientes con localización extratemporal y los casos psicógenos mostraron valores normales para todos los marcadores evaluados; este último grupo recibía el mismo tratamiento médico que el resto de los pacientes. Conclusiones. Estos resultados evidencian que existen alteraciones del sistema inmune en los pacientes epilépticos con crisis parciales complejas no asociadas al tratamiento antiepiléptico; las mismas pueden ser factores relevantes en la patogenia de la epilepsia y guardan relación con la localización del foco epileptogénico(AU)

Trasplante de células estromales en el modelo de lesión por 6-OHDA / Stromal cell transplant in the 6-OHDA lesion model

A good deal of evidence currently exists to show that transplanting foetal mesencephalic tissue can produce symptomatic benefits both in patients and in disease models. Nevertheless, the technical and ethical difficulties involved in obtaining enough suitable foetal cerebral tissue have been a serious obstacle to its application. Stromal cells derived from bone marrow, due to their potential capacity to generate different types of cells, could be an ideal source of material for cell restoration in neurodegenerative diseases. AIMS: Our aim was to evaluate the effect of transplanting stromal cells derived from bone marrow on the behaviour of 6-OHDA rats, when they are inserted into the striatum(AU)