Utilização de conjugados anticorpo-lectina no imunodiagnostico da neurocisticercose

Rossi, Claudio Lucio, 1950-

16 July 2018

Orientador: Luis Sebastião Prigenzi / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-07-16T05:31:47Z (GMT). No. of bitstreams: 1 Rossi_ClaudioLucio_D.pdf: 1343251 bytes, checksum: a21ab924a2b8724ea15753db2edb1df9 (MD5) Previous issue date: 1986 / Resumo: Não informado / Abstract: Not informed. / Doutorado / Doutor em Imunologia

Imunoglobulinas

Cisticercose cerebrospinal

Saúde pública

Effects of Blood Contamination on Cerebrospinal Fluid Cell Counts, Protein, and D-dimer Concentrations

Rossmeisl, John H. Jr.

29 January 2003

Cerebrospinal fluid analysis (CSF) is commonly performed in clinical neurology, and is a sensitive, but non-specific indicator of central nervous system (CNS) pathology. Blood contaminated CSF samples have the potential to adversely affect results of cytologic, serologic, microbiologic, and molecular biologic diagnostics. A clear consensus of the effects of blood contamination on CSF analysis could not be drawn following a review of the existing veterinary literature. Based on data from earlier reports, it was hypothesized that iatrogenic blood contamination of CSF would result in significant increases in both the CSF total protein (TP) concentration and nucleated cell count (WBC). As hypothesized, in vitro CSF blood contamination resulted in statistically significant (p < 0.01) linear increases in both the CSF TP and WBC with increasing RBC concentration in CSF from sixteen normal dogs. Although increases in TP and WBC are statistically significant, their clinical impact is negligible. Results of this study demonstrate that in normal dogs, the mean CSF TP concentration collected from the cerebellomedullary cistern, is lower than previously reported. D-dimers are plasminolytic cleavage products formed by the cross-linkage of fibrin by Factor XIIIa. In humans, D-dimer analysis can be used to differentiate iatrogenic from pathologic CNS hemorrhage. An additional objective of this study was to determine if canine D-dimers could be assayed using commercially available latex agglutination (LA) and enzymatic immunoassay (EIA) kits in normal and diseased subjects. It was hypothesized that qualitative and quantitative determinations of blood and CSF D-dimer activities could be aid in the diagnosis of dogs with altered CNS and/or systemic coagulation. D-dimers were able to be assayed in all subjects studied. D-dimer concentrations in CSF samples, when analyzed using a qualitative LA assay system, from healthy dogs with iatrogenically blood contaminated CSF were consistently negative. Quantitation of CSF D-dimer concentrations in normal dogs using an EIA assay resulted in lower values (mean 16.2 + 4.3 ng/ml; range, 0 to 54 ng/ml) than detected in the peripheral blood of dogs and humans (normal cutoff value < 250 ng/ml). These findings suggest that D-dimer formation does not occur in canine CSF freshly contaminated with blood. Significantly (p < 0.001) higher mean blood D-dimer concentrations were present in dogs with systemic coagulation disorders (1,093.4 + 172.3 ng/ml; range, 0 to > 2,000 ng/ml) when compared to normal dogs (54.6 + 19.8 ng/ml; range, 0 to 190 ng/ml), when assayed with the EIA. When used as an adjunct in the diagnosis of systemic coagulation abnormalities, the EIA assay had an overall sensitivity of 92%, specificity of 100%, positive predictive value (PPV) of 100%, and negative predictive value (NPV) of 94%. When applied to the same dogs, the LA D-dimer was less sensitive and specific (sensitivity of 73%, specificity of 100%, PPV of 100%, and NPV of 80%) than the EIA. Evidence of intrathecal fibrinolysis in the absence of systemic abnormalities was also demonstrated using CSF LA and EIA D-dimer assays in some dogs with a variety of infectious (Rocky mountain spotted fever), non-infectious inflammatory (granulomatous meningoencephalitis, steroid-responsive meningitis), traumatic (intervertebral disc disease, spinal fracture), and neoplastic (meningioma) diseases. When all dogs with CNS diseases were examined together, the mean EIA D-dimer concentration was significantly (p = 0.03) higher (511.6 + 279.8 ng/ml) than normal dogs (mean 16.2 + 4.3 ng/ml). Future studies will be required before the definitive role of D-dimer analysis can be defined in veterinary medicine. / Master of Science

Blood

Cerebrospinal fluid

D-dimers

Quantitative determination of cerebrospinal fluid bilirubin on a high throughput chemistry analyzer

Said Ahmed, Degmo

January 2009

<p><strong>Background</strong> Subarachnoid hemorrhage is a condition with high rates of mortality and morbidity. The diagnosis requires an urgent cerebral computed tomography scan and also a lumbar puncture if the scan fails to demonstrate intracranial blood. In Sweden the cerebrospinal fluid (CSF) is analyzed by spectrophotometric scanning for the presence of hemoglobin and bilirubin. The aim of the study was to develop a quantitative diazo reagent based analysis of cerebrospinal fluid bilirubin as a replacement for spectrophotometric scanning.</p><p><strong>Methods</strong> The CSF bilirubin assay on an Architect C8000 chemistry analyzer was compared with spectrophotometry using patient samples.</p><p><strong>Results</strong> The method correlates with spectrophotometry, has a good linearity and precision.</p><p><strong>Conclusions</strong> Quantitative bilirubin measurement offers shorter turnaround times, simplifies the interpretation of the results and reduces work load in comparison with spectrophotometry.</p>

Bilirubin

Cerebrospinal Fluid

Diagnosis

Humans

Subarachnoid Hemorrhage

Quantitative determination of cerebrospinal fluid bilirubin on a high throughput chemistry analyzer

Said Ahmed, Degmo

January 2009

Background Subarachnoid hemorrhage is a condition with high rates of mortality and morbidity. The diagnosis requires an urgent cerebral computed tomography scan and also a lumbar puncture if the scan fails to demonstrate intracranial blood. In Sweden the cerebrospinal fluid (CSF) is analyzed by spectrophotometric scanning for the presence of hemoglobin and bilirubin. The aim of the study was to develop a quantitative diazo reagent based analysis of cerebrospinal fluid bilirubin as a replacement for spectrophotometric scanning. Methods The CSF bilirubin assay on an Architect C8000 chemistry analyzer was compared with spectrophotometry using patient samples. Results The method correlates with spectrophotometry, has a good linearity and precision. Conclusions Quantitative bilirubin measurement offers shorter turnaround times, simplifies the interpretation of the results and reduces work load in comparison with spectrophotometry.

Bilirubin

Cerebrospinal Fluid

Diagnosis

Humans

Subarachnoid Hemorrhage

Quantification of alpha-synuclein in cerebrospinal fluid

Kronander, Björn

January 2012

To date there is no accepted clinical diagnostic test for Parkinson's disease (PD) based on biochemical analyses of blood or cerebrospinal uid. Currently, diagnosis, measurement of disease progression and response to therapeutic intervention are based on clinical observation, but the rst neuronal dysfunction precede the earliest recognition of symptom by at least 5 - 10 years. A potential diagnostic biomarker is oligomeric alpha-synuclein which in recent papers have reported a signicant quantitative dierence between PD and controls. In this master thesis, a method for measuring oligomeric levels of alpha-synuclein is presented together with a monomeric measuring commercial kit used to measure alpha-synuclein in a preclinical model of PD. A signicant dierence of monomeric levels could be detected between two weeks and four weeks post injection of a vector containing the gene for human alpha-synuclein, no signicant dierence between four and eight weeks was found.

Methods development and application of two-dimensional chromatography and tandem mass spectrometry in proteomics

Wenner, Brett Romain.

January 2003

Thesis (Ph. D.)--University of Kentucky, 2003. / Title from document title page (viewed onJune 21, 2004). Document formatted into pages; contains xii, 151 p. : ill. Includes abstract and vita. Includes bibliographical references (p. 137-149).

Oxygen metabolism of Neisseria meningitidis.

Yu, Ernest Kar-cheung.

January 1980

The physiology of oxygen metabolism in Group B N. meningitidis was investigated. The respiratory components of the electron transport chain included dehydrogenases, ubiquinone, multiple b- and c-type cytochromes, and cytochromes o and a as terminal oxidases. Independent variations in the respiratory components were determined for cells grown under different conditions of iron concentrations and aeration (including anaerobiosis). Studies on oxidase activities in envelope preparations suggested branching of the respiratory chain at the levels of dehydrogenases, cytochrome b and terminal oxidases. Work on L-cysteine oxidase activity associated with the envelope preparations indicated the presence of an additional "alternate" oxidase insensitive to terminal oxidase inhibitors. A soluble CO- and NO-binding c-type cytochrome was shown to be present in the supernatant fluids and might be involved in an ascorbate-TMPD oxidase activity. A model of a branched electron transport system is proposed. The levels of catalase, peroxidase and superoxide dismutase in the organism were shown to vary with the growth conditions.

Meningitis, Cerebrospinal

Energy metabolism

Microorganisms -- Physiology

Assay of glutamine synthetase in cerebrospinal fluid as a specific marker in Alzheimer's disease

Oettle, Nicola

January 1997

Thesis (Master's Degree (Medical Technology)-- Cape Technikon, Cape Town, 1997 / There is, at present, no recognised diagnostic biochemical marker of Alzheimer's Disease (AD). Recently, Gunnerson and Haley, (1992), reported that the presence of glutamine synthetase (GS) in cerebrospinal fluid (CSF) samples showed a 97% correlation with patients diagnosed as having AD. GS was detected by photolabelling with [y32P]2-azido-ATP or [y32P]8azido- ATP and visualisation following sodium dodecyl sulphate polyacrylamide gel electrophoresis (SOS-PAGE) and autoradiography. This study set out to reproduce Gunnerson and Haley's methodology for labelling sheep GS in CSF using [y32P]8-azidoATP, to develop this assay or possibly another, using a fluorescent probe of ATP binding sites, into a robust procedure suitable for a routine diagnostic laboratory, and finally to assess whether the presence of GS in CSF is indeed a marker of AD.

Alzheimer's disease

Cerebrospinal fluid -- Examination

Glutamine synthetase

TRPV4 in the Choroid Plexus Epithelium: Pathway Analysis and Implications for Cerebrospinal Fluid Production

Preston, Daniel

12 1900

Indiana University-Purdue University Indianapolis (IUPUI) / Hydrocephalus is a disease characterized by an increase in cerebrospinal fluid (CSF) in the ventricles of the brain. This manifests as a result of either overproduction or underabsorption of CSF leading to increases in pressure, swelling and loss of brain matter. Current treatments for this disease include surgical interventions via the introduction of shunts or endoscopic third ventriculostomy, both of which aim to redirect flow of CSF in to another cavity for absorption. Limited pharmacotherapies are available in the treatment of hydrocephalus, and there exists a clinical need for drug therapies, which can ameliorate the pathophysiology associated with hydrocephalus and ventriculomegaly. CSF is produced primarily by the choroid plexus (CP), found in the ventricles of the brain. Composed of a high resistance epithelium surrounding a capillary network, the CP epithelium acts as a barrier, regulating ion transport between the CSF and blood. Transient Receptor Potential Vanilloid-4 (TRPV4) is a nonselective Ca2+-permeable cation channel expressed in the CP which is being investigated for its role in CSF production. To study hydrocephalus, we utilize two model systems; the TMEM67-/- Wpk rat, and the PCP-R cell line. The Wpk rat model is used to study the effects of drug intervention on the development and progression of hydrocephalus. The PCP-R cell line is utilized for studies which aim to understand the mechanisms by which CSF is produced. Using Ussing chamber electrophysiology, we are able to study the role of specific channels, transporters and modulators in driving epithelial ion flux across the CP. This research aims to establish a role for TRPV4 in production and regulation of CSF, and to interrogate a mechanism by which this ion transport occurs. The chapters that follow describe components of the pathway by which TRPV4 is activated and ion flux is stimulated.

Hydrocephalus

Choroid Plexus

CSF

Cerebrospinal Fluid

TRPV4

Cerebrospinal fluid concentrations of p-tau/Aβ42 associate with cognitive decline in Alzheimer’s disease, mild cognitive impairment, and cognitively unimpaired older adults

McKenna, Michael Robert

January 2021

No description available.

Psychology

cerebrospinal fluid biomarkers

Alzheimer’s disease

cognition