8 resultados para neonatal survival

em Archivo Digital para la Docencia y la Investigación - Repositorio Institucional de la Universidad del País Vasco


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La neonatología es una modalidad de cuidados relativamente nueva, que ha ido evolucionando paralelamente al desarrollo tecnológico. A pesar de disminuir la mortalidad neonatal, el pronóstico en su desarrollo no se puede predecir. Muchos de los niños prematuros sufren alteraciones en el desarrollo infantil. En la mayoría de los casos, las complicaciones no sólo se deben a la prematuridad, si no que surgen a consecuencia de la traumática estancia hospitalaria. La Dra. Als pionera en los Cuidados Centrados en el Desarrollo en niños prematuros, impulsó la importancia de los factores externos que rodean al neonato, determinantes para el correcto desarrollo sensomotor, cognitivo y conductual. Por ello, Als crea el Programa de Evaluación y Atención Individualizada y Orientada al Desarrollo Neonatal (NIDCAP) que se establece como una metodología de cuidado para mejorar la calidad asistencial del neonato, con el fin de mejorar su desarrollo y disminuir las posibles complicaciones que se dan en la infancia. El objetivo de este trabajo es valorar la eficacia del NIDCAP en la disminución de secuelas en el desarrollo de niños prematuros a largo plazo mediante la evidencia científica, utilizando metodología PBE. Se realiza una búsqueda bibliográfica a través de la base de datos pubmed y The Cochrane library, para contrastar los resultados y hallar la evidencia. Los resultados recogidos no confirman de manera contundente que el NIDCAP sea determinante para la disminución de secuelas sensomotoras en la infancia, aunque si sugiere que el programa no es perjudicial y si en todo caso beneficioso para los cuidados de estos recién nacidos.

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Durante muchos años se consideró que los neonatos no experimentaban el dolor por su incapacidad para verbalizarlo. Así, concepciones erróneas hicieron que el dolor neonatal no fuese tratado. En la actualidad, existe evidencia científica que corrobora la capacidad para percibir el dolor, siendo necesario su tratamiento. Aun así, el miedo a los posibles efectos secundarios de los fármacos ha obstaculizado el estudio de nuevos fármacos para el tratamiento del dolor. Es por eso que las estrategias no farmacológicas han tomado gran relevancia en el tratamiento de procedimientos dolorosos menores, y como coadyuvantes de los fármacos en procedimientos de mayor intensidad. El método canguro que se define como un contacto piel a piel entre madre e hijo, surgió como una alternativa ante la escasez de incubadoras. Sin embargo, numerosas investigaciones han demostrado los grandes beneficios que aporta, considerándolo también como una medida no farmacológica eficaz en el alivio del dolor neonatal. El objetivo de este estudio es evaluar la efectividad del método canguro junto a la administración de sacarosa oral en la disminución del dolor, en comparación con el procedimiento estándar al realizar la prueba de talón. Para ello, se realizará un ensayo clínico aleatorizado dirigido a los neonatos prematuros y de bajo peso gestacional ingresados en la unidad de neonatal del Hospital universitario de Cruces. La variable principal a estudio es la valoración del dolor medido mediante la escala PIPP. Se compararán los datos recogidos en el grupo control e intervención y el análisis de datos se realizará usando el programa informático SPSS.

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Background: Recently, with the access of low toxicity biological and targeted therapies, evidence of the existence of a long-term survival subpopulation of cancer patients is appearing. We have studied an unselected population with advanced lung cancer to look for evidence of multimodality in survival distribution, and estimate the proportion of long-term survivors. Methods: We used survival data of 4944 patients with non-small-cell lung cancer (NSCLC) stages IIIb-IV at diagnostic, registered in the National Cancer Registry of Cuba (NCRC) between January 1998 and December 2006. We fitted one-component survival model and two-component mixture models to identify short-and long-term survivors. Bayesian information criterion was used for model selection. Results: For all of the selected parametric distributions the two components model presented the best fit. The population with short-term survival (almost 4 months median survival) represented 64% of patients. The population of long-term survival included 35% of patients, and showed a median survival around 12 months. None of the patients of short-term survival was still alive at month 24, while 10% of the patients of long-term survival died afterwards. Conclusions: There is a subgroup showing long-term evolution among patients with advanced lung cancer. As survival rates continue to improve with the new generation of therapies, prognostic models considering short-and long-term survival subpopulations should be considered in clinical research.

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Objective: Aerosol delivery holds potential to release surfactant or perfluorocarbon (PFC) to the lungs of neonates with respiratory distress syndrome with minimal airway manipulation. Nevertheless, lung deposition in neonates tends to be very low due to extremely low lung volumes, narrow airways and high respiratory rates. In the present study, the feasibility of enhancing lung deposition by intracorporeal delivery of aerosols was investigated using a physical model of neonatal conducting airways. Methods: The main characteristics of the surfactant and PFC aerosols produced by a nebulization system, including the distal air pressure and air flow rate, liquid flow rate and mass median aerodynamic diameter (MMAD), were measured at different driving pressures (4-7 bar). Then, a three-dimensional model of the upper conducting airways of a neonate was manufactured by rapid prototyping and a deposition study was conducted. Results: The nebulization system produced relatively large amounts of aerosol ranging between 0.3 +/- 0.0 ml/min for surfactant at a driving pressure of 4 bar, and 2.0 +/- 0.1 ml/min for distilled water (H(2)Od) at 6 bar, with MMADs between 2.61 +/- 0.1 mu m for PFD at 7 bar and 10.18 +/- 0.4 mu m for FC-75 at 6 bar. The deposition study showed that for surfactant and H(2)Od aerosols, the highest percentage of the aerosolized mass (similar to 65%) was collected beyond the third generation of branching in the airway model. The use of this delivery system in combination with continuous positive airway pressure set at 5 cmH(2)O only increased total airway pressure by 1.59 cmH(2)O at the highest driving pressure (7 bar). Conclusion: This aerosol generating system has the potential to deliver relatively large amounts of surfactant and PFC beyond the third generation of branching in a neonatal airway model with minimal alteration of pre-set respiratory support.

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Introduction Hypoxia-ischemia (HI) is a major perinatal problem that results in severe damage to the brain impairing the normal development of the auditory system. The purpose of the present study is to study the effect of perinatal asphyxia on the auditory pathway by recording auditory brain responses in a novel animal experimentation model in newborn piglets. Method Hypoxia-ischemia was induced to 1.3 day-old piglets by clamping 30 minutes both carotid arteries by vascular occluders and lowering the fraction of inspired oxygen. We compared the Auditory Brain Responses (ABRs) of newborn piglets exposed to acute hypoxia/ischemia (n = 6) and a control group with no such exposure (n = 10). ABRs were recorded for both ears before the start of the experiment (baseline), after 30 minutes of HI injury, and every 30 minutes during 6 h after the HI injury. Results Auditory brain responses were altered during the hypoxic-ischemic insult but recovered 30-60 minutes later. Hypoxia/ischemia seemed to induce auditory functional damage by increasing I-V latencies and decreasing wave I, III and V amplitudes, although differences were not significant. Conclusion The described experimental model of hypoxia-ischemia in newborn piglets may be useful for studying the effect of perinatal asphyxia on the impairment of the auditory pathway.

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Sphingolipids are major constituents of biological membranes of eukaryotic cells. Many studies have shown that sphingomyelin (SM) is a major phospholipid in cell bilayers and is mainly localized to the plasma membrane of cells, where it serves both as a building block for cell architecture and as a precursor of bioactive sphingolipids. In particular, upregulation of (C-type) sphingomyelinases will produce ceramide, which regulates many physiological functions including apoptosis, senescence, or cell differentiation. Interestingly, the venom of some arthropodes including spiders of the genus Loxosceles, or the toxins of some bacteria such as Corynebacterium tuberculosis, or Vibrio damsela possess high levels of D-type sphingomyelinase (SMase D). This enzyme catalyzes the hydrolysis of SM to yield ceramide 1-phosphate (C1P), which promotes cell growth and survival and is a potent pro-inflammatory agent in different cell types. In particular, C1P stimulates cytosolic phospholipase A2 leading to arachidonic acid release and the subsequent formation of eicosanoids, actions that are all associated to the promotion of inflammation. In addition, C1P potently stimulates macrophage migration, which has also been associated to inflammatory responses. Interestingly, this action required the interaction of C1P with a specific plasma membrane receptor, whereas accumulation of intracellular C1P failed to stimulate chemotaxis. The C1P receptor is coupled to Gi proteins and activates of the PI3K/Akt and MEK/ERK1-2 pathways upon ligation with C1P. The proposed review will address novel aspects on the control of inflammatory responses by C1P and will highlight the molecular mechanisms whereby C1P exerts these actions.