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dc.contributor.authorRojas, Glenda
dc.contributor.authorParkhouse, Michael
dc.contributor.authorCarpio Rodas, Luis Arturo
dc.contributor.authorCampoverde Cisneros, Manuel Alfredo
dc.contributor.authorSastre, Patricia
dc.contributor.authorCortez, María Milagros
dc.date.accessioned2023-07-12T17:17:14Z-
dc.date.available2023-07-12T17:17:14Z-
dc.date.issued2018
dc.identifier.issn0001706X
dc.identifier.urihttp://dspace.ucuenca.edu.ec/handle/123456789/42382-
dc.identifier.urihttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85034668629&origin=inward
dc.descriptionAbstract To evaluate diagnosis of active neurocysticercosis, paired cerebral spinal fluid (CSF) and serum samples from 24 neurocysticercosis (NCC) patients and 17 control neurological patients were assayed in the HP10 Taenia antigen (Ag) ELISA. The CSF samples were also tested with an HP10 Lateral Flow Assay (LFA). The HP10 Ag was detected by ELISA in the CSF of 5/5 patients with Definitive extraparenchymal NCC, and in 4/5 of the corresponding sera. In the Definitive parenchymal group, on the other hand, the HP10 Ag was absent in 2/3 CSF (with a very low value in the one positive sample) and all the corresponding serum samples. Samples of CSF from 4/7 patients in the Probable parenchymal group, were also significantly HP10 Ag positive, suggesting the presence of extraparenchymal cysts not identified by the imaging studies. With the possible exception of one patient, the corresponding serum samples of the Probable parenchymal NCC group, were all HP10 Ag negative. Samples of CSF from 9 NCC patients diagnosed with Mixed parenchymal and extraparenchymal NCC were all significantly HP10 Ag positive, confirming the presence of extraparenchymal cysts, with only 7/9 of the corresponding serum samples being HP10 positive. Thus detection of the HP10 Ag indicates extraparenchymal and not parenchymal cyst localization and is more sensitive with CSF than serum. Three neurological patients clinically diagnosed as subarachnoid cyst, hydrocephalus and tuberculoma, respectively, were clearly positive for HP10 Ag. Of these, two were confirmed as NCC by subsequent imaging; the third died prior to further examination. Thus, a total of 8 patients had their clinical diagnosis questioned. Finally, there was good agreement between the HP10 Ag ELISA and LFA with CSF samples giving an optical density ≥0.4 in the ELISA assay. In conclusion, the HP10 Ag assay should provide a valuable and reciprocal tool in the clinical diagnosis and follow up of extraparenchymal NCC.
dc.description.abstractAbstract To evaluate diagnosis of active neurocysticercosis, paired cerebral spinal fluid (CSF) and serum samples from 24 neurocysticercosis (NCC) patients and 17 control neurological patients were assayed in the HP10 Taenia antigen (Ag) ELISA. The CSF samples were also tested with an HP10 Lateral Flow Assay (LFA). The HP10 Ag was detected by ELISA in the CSF of 5/5 patients with Definitive extraparenchymal NCC, and in 4/5 of the corresponding sera. In the Definitive parenchymal group, on the other hand, the HP10 Ag was absent in 2/3 CSF (with a very low value in the one positive sample) and all the corresponding serum samples. Samples of CSF from 4/7 patients in the Probable parenchymal group, were also significantly HP10 Ag positive, suggesting the presence of extraparenchymal cysts not identified by the imaging studies. With the possible exception of one patient, the corresponding serum samples of the Probable parenchymal NCC group, were all HP10 Ag negative. Samples of CSF from 9 NCC patients diagnosed with Mixed parenchymal and extraparenchymal NCC were all significantly HP10 Ag positive, confirming the presence of extraparenchymal cysts, with only 7/9 of the corresponding serum samples being HP10 positive. Thus detection of the HP10 Ag indicates extraparenchymal and not parenchymal cyst localization and is more sensitive with CSF than serum. Three neurological patients clinically diagnosed as subarachnoid cyst, hydrocephalus and tuberculoma, respectively, were clearly positive for HP10 Ag. Of these, two were confirmed as NCC by subsequent imaging; the third died prior to further examination. Thus, a total of 8 patients had their clinical diagnosis questioned. Finally, there was good agreement between the HP10 Ag ELISA and LFA with CSF samples giving an optical density ≥0.4 in the ELISA assay. In conclusion, the HP10 Ag assay should provide a valuable and reciprocal tool in the clinical diagnosis and follow up of extraparenchymal NCC.
dc.language.isoes_ES
dc.sourceActa Tropica
dc.subjectParenchymal
dc.subjectDiagnosis
dc.subjectExtraparenchymal
dc.subjectHP10 antigen ELISA
dc.subjectHP10 antigen LFA
dc.subjectNeurocysticercosis
dc.titleReciprocal contribution of clinical studies and the HP10 antigen ELISA for the diagnosis of extraparenchymal neurocysticercosis.
dc.typeARTÍCULO
dc.ucuenca.idautorSgrp-1074-6
dc.ucuenca.idautor0102517265
dc.ucuenca.idautor0100737956
dc.ucuenca.idautorSgrp-1074-1
dc.ucuenca.idautorSgrp-1074-4
dc.ucuenca.idautorSgrp-1074-5
dc.identifier.doi10.1016/j.actatropica.2017.11.005,
dc.ucuenca.embargoend2050-12-31
dc.ucuenca.versionVersión publicada
dc.ucuenca.embargointerno2050-12-31
dc.ucuenca.areaconocimientounescoamplio09 - Salud y Bienestar
dc.ucuenca.afiliacionSastre, P., INGENASA (Madrid), Madrid, España
dc.ucuenca.afiliacionCarpio, L., Universidad de Cuenca, Facultad de Ciencias Médicas, Cuenca, Ecuador
dc.ucuenca.afiliacionCortez, M., Universidad de Carabobo, Valencia, Venezuela
dc.ucuenca.afiliacionParkhouse, M., Instituto de Ciencias Gulbenkian, Oeiras, Portugal
dc.ucuenca.afiliacionRojas, G., Universidad de Carabobo, Valencia, Venezuela
dc.ucuenca.afiliacionCampoverde, M., Universidad de Cuenca, Facultad de Ciencias Médicas, Cuenca, Ecuador
dc.ucuenca.correspondenciaParkhouse, Michael, parkhous@igc.gulbenkian.pt
dc.ucuenca.volumenvolumen 178
dc.ucuenca.indicebibliograficoSCOPUS
dc.ucuenca.factorimpacto1.052
dc.ucuenca.cuartilQ1
dc.ucuenca.numerocitaciones0
dc.ucuenca.areaconocimientofrascatiamplio3. Ciencias Médicas y de la Salud
dc.ucuenca.areaconocimientofrascatiespecifico3.2 Medicina Clínica
dc.ucuenca.areaconocimientofrascatidetallado3.2.27 Neurología Clínica
dc.ucuenca.areaconocimientounescoespecifico091 - Salud
dc.ucuenca.areaconocimientounescodetallado0912 - Medicina
dc.ucuenca.urifuentehttp://www.sciencedirect.com/science/journal/0001706X
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