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1.
Indian J Dermatol Venereol Leprol ; 2007 Sep-Oct; 73(5): 336-9
Article de Anglais | IMSEAR | ID: sea-52460

RÉSUMÉ

Keloids are the result of excessive fibroblast proliferation and then over-abundant collagen deposition. There is no method able to guarantee absolute success in the therapeutic approach to keloids. Our case report involves a female patient with six lesions treated with a 32P-patch brachyradiotherapy. Pre-treatment and adjuvant treatment of the lesions were performed with thiomucase, 5-fluoruracil, procaine and triamcinolone. Taking into account the activity contained in each of the patches and the total radiation dose to be administered according to clinical practice, dosimetric calculations were done for each lesion. Separate silicone patches with chromic [32P]phosphate were designed for each lesion based on these calculations. Total remission was achieved in three treated lesions. The other lesions did not achieve total remission yet, but their sizes are diminishing. The differences observed in treatment outcome may be related with lesion features, adjuvant treatments and/or treatment schedule.


Sujet(s)
Sujet âgé de 80 ans ou plus , Curiethérapie/méthodes , Cicatrice hypertrophique/anatomopathologie , Femelle , Humains , Chéloïde/anatomopathologie , Radio-isotopes du phosphore/usage thérapeutique , Dose de rayonnement , Peau/anatomopathologie
3.
Arch. latinoam. nutr ; Arch. latinoam. nutr;53(2): 119-132, jun. 2003.
Article de Espagnol | LILACS | ID: lil-356578

RÉSUMÉ

Iron is an essential micronutrient involved in multiple biochemical and physiological process. In this review we discuss the most relevant aspect of its metabolism in order to reach a better comprehension of the relevant roll that this micronutrient plays in human health.


Sujet(s)
Humains , Fer/métabolisme , Micronutriments/métabolisme , Absorption , Fer/pharmacocinétique , Micronutriments/pharmacocinétique
4.
Article de Anglais | LILACS | ID: lil-339351

RÉSUMÉ

El surfactante natural exógeno (ENS) marcado con 99mTc (99mTc-ENS) es un nuevo agente ventilatorio para la centellografía aérea pulmonar. Con el fin de elegir una formulación estable de ENS para ser marcado rutinariamente con 99mTc en Centros de Medicina Nuclear, las propiedades de dos formulaciones (ENS + cloruro estannoso + ácido gentísico y ENS + cloruro estannoso + ácido ascórbico) y una formulación control liofiolizada del ENS fueron analizadas mensualmente por un período de 12 meses. Sus propiedades fisicoquímicas, sus porcentajes de marcación y sus distribuciones biológicas fueron adecuadas durante este período. La formulación ENS + cloruro estannoso + ácido gentísico presenta la menor dispersión en los resultados de biodistribución, por lo cual esta formulación fue elegida para la futura producción de 99mTc-ENS. El estudio de toxicidad aguda de esta última formulación demostró que la dosis tóxica es al menos 1000 veces mayor que la dosis diagnóstica


Sujet(s)
Humains , Tensioactifs , Scintigraphie , Technétium , Radiopharmaceutiques/pharmacologie
5.
Acta physiol. pharmacol. ther. latinoam ; 49(2): 101-7, 1999. tab, graf
Article de Anglais | LILACS | ID: lil-245925

RÉSUMÉ

The (13)C-UBT has been demonstrated to be a reliable method for the evaluation of Helicobacter pylori infection. The aim of our work is to determine the cut-off point of the (13)C-UBT for samples collected as gas or collected in a solution of triethanolamine. For this purpose, patients fasted for at least 6 hours were able to collect basal samples before the administration of 65 mg of (13)C-urea solution. Breath samples were taken 10,30 and 60 minutes after the administration of the labeled solution. All the samples were collected in gas collectors and in glass vials containing 1 ml of a 7 per cent triethanolamine solution. The cut-off points for gas collected samples were established in 4.0 per cent and for 10, 30 and 60 minutes samples, respectively, while for the samples, collected in triethanolamine solution, cut-off points were established in 5.0 per cent, for the 10 minutes samples, in 3.5 per cent for the 30 minutes samples and 4.7 per cent for the 60 minutes samples. We found that this test has a sensitivity of 100 per cent and a specificity of 100 per cent for H. pylori detection in both experimental conditions, when multiple breath samples are taken. If we considered only the 30 minutes time, sensitivity and specificity diminish for the gas collected samples. We conclude that the collection of breath samples in triethanolamine solution allows a better differentiation between H. pylori infected and non infected patients than gas collected samples.


Sujet(s)
Humains , Mâle , Femelle , Tests d'analyse de l'haleine , Infections à Helicobacter/diagnostic , Helicobacter pylori , Urée , Analyse de variance , Isotopes du carbone , Infections à Helicobacter/microbiologie , Helicobacter pylori/isolement et purification , Sensibilité et spécificité , Facteurs temps
6.
Article de Espagnol | LILACS | ID: lil-245927

RÉSUMÉ

Se ha postulado que el aporte de hierro a las células usuarias se halla bajo un control dependiente del tamaño de la fracción intracelular libre del metal, cuyos cambios se reflejarían en mensajes a la expresión de los receptores séricos o de membrana para ajustar la oferta a la demanda. La posibilidad de que los receptores de membrana pudieran estar afectados por la malnutrición calórico-proteica se exploró en estudios a través de los cambios de la capacidad de los reticulocitos circulantes de ratón normal para incorporar hierro in vitor, observando el diferente comportamiento ocasionado por la incubación de las células con suero humano de dadores normales y de pacientes de anemia nutricional. Los resultados muestran una significativa caída de dicha capacidad cuando se utilizó suero de pacientes afectados de anemia nutricional. Se discute el probable mecanismo responsable de dicha diferencia.


Sujet(s)
Enfant , Animaux , Humains , Rats , Souris , Adulte , Zinc , Absorption intestinale/physiologie , Besoins nutritifs , Valeur nutritive , Zinc/déficit , Zinc/métabolisme , Zinc/pharmacocinétique , Zinc/physiologie
7.
Acta physiol. pharmacol. ther. latinoam ; 48(4): 175-90, 1998. ilus, tab
Article de Espagnol | LILACS | ID: lil-226085

RÉSUMÉ

El surfactante pulmonar es una mezcla lipoproteica sintetizada y secretada por las células alveolares pulmonares tipo II. Su principal función es la disminución de la tensión superficial formando una monocapa en la superficie alveolar. Su deficiencia es el principal factor asociado al síndrome de dificultad respiratoria del recién nacido (RDS) y al síndrome de dificultad respiratoria del adulto (ARDS). Desde 1980 se está estudiando la administración exógena del surfactante pulmonar para el tratamiento de estos dos síndromes. En este trabajo se describen los surfactantes exógenos disponibles para uso clínico, las técnicas de administración y el esquema de dosificación. La utilización del surfactante natural exógeno (ENS) marcado con (99m)Tc((99m)Tc-ENS) para su utilización como radiofármaco en centellografía aérea pulmonar también es descripta en este trabajo.


Sujet(s)
Humains , Nouveau-né , Adulte , Surfactants pulmonaires , Syndrome de détresse respiratoire du nouveau-né/traitement médicamenteux , 12549/traitement médicamenteux , Surfactants pulmonaires , Surfactants pulmonaires/composition chimique , Surfactants pulmonaires/déficit , Surfactants pulmonaires/physiologie , Surfactants pulmonaires/usage thérapeutique
8.
Acta physiol. pharmacol. ther. latinoam ; 46(2): 83-9, 1996. tab, graf
Article de Anglais | LILACS | ID: lil-172312

RÉSUMÉ

The difficulty of a reliable diagnosis of pancreatic diseases by scintiscanning, is mainly derived from the lack of adequate radiopharmaceuticals. With this purpose (125) I-L(-3) Iodo-a-Methyl Tyrosine ((125) I-IMT) has been studied, which has also been used for the diagnosis of different kind of brain tumors. The purpose of this work is the development of a quick and easy method for the synthesis and purification of the (125) I-IMT in order to be used in a Nuclear Medicine Service. The L-(-Methly Tyrosine was labeled with (125) I using I-/I03 and afterwards purified by an aniomic exchange resin. The labeling yield obtained was (96.0+0.5) per cent when the incubation time was 15 minutes. No significant statistical differences were observed when the incubation time was extended to 1 hour. Biodistribution studies in mice show that the percentage of activity concentration in pancreas is (34.24+14.03) per cent at 15 minutes post injection, remaining constant for 30 minutes. The pancreas/liver ratio 15 minutes after the injection of the labeled product was (12.22+3.59) and it remained constant for 45 minutes more. These results show that (125) I-IMT cab be used as a diagnostic agent for pancreatic diseases. Since (123) I was not avilable at the moment, this new methodology was developed with (125) I.


Sujet(s)
Souris , Animaux , Imagerie diagnostique , Méthyltyrosines , Tumeurs du pancréas , Analyse de variance , Électrophorèse sur papier , Radio-isotopes de l'iode
9.
Acta physiol. pharmacol. ther. latinoam ; 46(2): 103-10, 1996. tab, graf
Article de Anglais | LILACS | ID: lil-172315

RÉSUMÉ

With the purpose studying the effectivity of an intratumoral single dose of chromic [(32)P] phosphate with great particles for the treatment of solid tumors, studies of biolimination, biodistribution and therapeutic action were carried out. Only for comparative purpose, similar studies were undertaken using a solution of sodium [(32)P] orthophosphategelatine. The results show that when sodium [(32)P] orthophosphategelatine is used, the percentage of total elimination is (85.90+8,70) per cent with a higler percentage in urine (64.50+13.70) per cent than in faeces (21.40+4.50) per cent. In biodistribution studies, the greater percentage is found in bone (15.54+2.21) per cent while only a (2.51+0.39) per cent remains in the tumor. When great particles chromic [(32)P] phosphate was intratumorally injected, we determined that the total elimination is equal (36.28+6.27) per cent, finding a higler amount in faeces (29.44+5.26) per cent than in urine (6.84+2.21) per cent. Biodistribution studies demonstrated that (49.82+5.41) per cent remains in the tumor and (9.63+4.89) per cent of the injected activity is found in the liver. On the other hand, when therapeutic action was evoluted, we observed that the percentage of tumor regression (P.T.R) is 52.0 per cent for the tumors injected with chromic [(32)P] phosphate and 0.0 per cent for those injected with sodium [(32)P] orthophosphate-gelatine. These results show that the great particles colloid of chromic [(32)P] phosphate is not safe enough for the tratment of solid tumors, since it is mobilezed from the injection point, delivering a high dose to the whole organism.


Sujet(s)
Animaux , Rats , Femelle , Adénocarcinome/radiothérapie , Composés du chrome/usage thérapeutique , Tumeurs expérimentales de la mamelle/radiothérapie , Phosphates/usage thérapeutique , Radio-isotopes du phosphore/usage thérapeutique , Sodium/usage thérapeutique , Composés du chrome/administration et posologie , Composés du chrome/pharmacocinétique , Colloïdes , Fèces/composition chimique , Injections , Phosphates/administration et posologie , Phosphates/pharmacocinétique , Radio-isotopes du phosphore/administration et posologie , Radio-isotopes du phosphore/pharmacocinétique , Rat Sprague-Dawley , Induction de rémission , Sodium/administration et posologie , Sodium/pharmacocinétique , Résultat thérapeutique , Urine/composition chimique
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