In vitro studies of the dual properties of Allopurinol anti- and photo-oxidants Mechanisms / Estudio in vitro de dos propiedades del Alopurinol.

The objective of this study was to investigate the ability of allopurinol (1) to inhibit free radical or reactive oxygen species (.OH, ¹O2, H2O2) as well as the study of its photochemical activity. We investigated the ability of 1 to scavenge oxygen metabolites generated by cell-free systems using luminol enhanced-chemiluminescence and electronic absorption spectra as monitors. Both absorbance and fluorescence scans reveal that 1 is able to react with equimolar quantities of H2O2. In the presence of 1 a dose-dependent inhibition period was observed in this system as assayed by isoluminol-enhanced chemiluminescence (ILCL) in the presence of horseradish peroxidase (HRP), as well as by luminol-enhanced chemiluminescence (LCL) in the presence of H2O2 or ferrous ion. On the other hand, 1 did not show an efficient scavenging activity of galvanoxyl radical in ethanolic solutions. Furthermore, in a separate experiment, it was not observed trapping of singlet oxygen (¹O2) generated by Rose Bengal, in the presence of 1. The activity of 1 was compared with that of vitamins E and C. In vitro experiments of photohemolysis in presence of 1 and cinoxacin, a phototoxic antibacterial quinolone, the photohemolytic effect of cinoxacin was diminished. Allopurinol alone did not show any phototoxic effect under irradiation with UV-A or visible light but was photo-unstable and phototoxic in vitro with UV-B light.

Se estudió la habilidad del alopurinol (1) para inhibir radicales libres o especies reactivas de oxigeno (.OH, ¹O2, H2O2), igualmente se determinó su actividad fotoquímica. De otro lado se midió la habilidad de 1 para eliminar los metabolitos de oxígeno generados por un sistema libre de células basado en quimioluminicencia aumentada de luminol y se monitoreo el espectro de absorción electrónica. Las dos determinaciones, absorbancia y fluorescencia, revelan que 1 es capaz de reaccionar con cantidades equimoleculares de H2O2. En presencia de alopurinol se observan periodos de inhibición dosis dependiente al usar isoluminol como intensificador de luminiscencia (ILCL) en presencia de peroxidasa de rábano o ión ferroso. Por otro lado, 1 no mostró una eficiente actividad frente a radicales galvanoxil en solución etanólica. En otros experimentos en presencia de 1 no se observó bloqueo de especies de oxígeno singlete (¹O2) generado por rosa bengala. La habilidad de 1 fue comparada con la de vitaminas E y C. En experimentos de fotohemólisis in vitro en presencia de 1 y cinoxacin, quinolona fototóxico antibanterial, el efecto fotohemolítico del cinoxacin fue disminuido. El alopurinol no mostró efecto fototóxico por irradiación con luz UV-A o luz visible, sin embargo se mostró foto - inestable y fototóxico in vitro bajo irradiación con luz UV-B.

Photodegradation and in vitro phototoxicity of aceclofenac.

Aceclofenac (Airtal) (1) is a photoallergic and phototoxic anti-inflammatory and analgesic agent. This drug is photolabile under aerobic and anaerobic conditions. Irradiation of an ethanol-solution of aceclofenac under oxygen or argon at 290-320 nm affords via decarboxlation compound 2 as the main isolated and spectroscopically identified photoproduct, besides hydroxylamine derivates 3 and 4. A radical intermediate was evidenced spectrophotometrically with GSH and DTNB, as well as by the dimerization of cysteine. Red blood cell lysis photosensitized by 1-4 was investigated. Furthermore, in a lipid-photoperoxidation test with linoleic acid the in vitro phototoxicity of aceclofenac was also verified. The photoinduced generation of peroxide by compound 1 was determined during the irradiation in presence of NADPH by chemiluminescence. In relation to the photoallergic activity of this drug, the interaction of aceclofenac with human serum albumin (HSA) has been studied through fluorescence spectroscopy. No photoinduced binding was observed after irradiation of compounds 1 in the presence of human serum albumin.

A novel paraptosis pathway involving LEI/L-DNaseII for EGF-induced cell death in somato-lactotrope pituitary cells.

We have recently reported that EGF triggers an original form of cell death in pituitary cell line (GH4C1) with a phenotype sharing some characteristics of both apoptosis (internucleosomal DNA fragmentation) and paraptosis (caspase-independence and cytoplasmic vacuolization). However, the endonuclease involved in EGF-induced DNA fragmentation has not been assessed so far. In the present work we therefore further explored the putative paraptosis involvement in EGF-induced cell death and asked whether L-DNaseII might be involved. Indeed, this endonuclease is known to mediate internucleosomal DNA fragmentation in caspase independent manner. Our Western blot, immunocytochemistry and enzymatic measurement assays show that EGF triggers a cleavage of Leukocyte Elastase Inhibitor (LEI) precursor into L-DNaseII, its subsequent enzymatic activation and nuclear translocation thus pointing to the involvement of this endonuclease pathway in caspase-independent DNA fragmentation. In addition, EGF-induced cell death can be blocked by paraptosis inhibitor AIP-1/Alix, but not with its anti-apoptotic C-terminal fragment (Alix-CT). Altogether these data suggest that EGF-induced cell death defines a novel, L-DNaseII-mediated form of paraptosis.

The steroid antagonist RU486 given at pro-oestrus induces hypersecretion of follicle-stimulating hormone from oestrus afternoon to early metoestrus in the rat.

Administration of the steroid antagonist RU486 to cyclic rats at pro-oestrus blunts the preovulatory surge of LH and suppresses the first and second surges of FSH. In addition, administration of oestradiol to RU486-treated rats reactivates the LH surge the following day. The present study explored the effects of RU486 (4 mg/0.2 ml oil), administered at 0800 h on the day of pro-oestrus, on serum FSH and LH concentrations through oestrus and early metoestrus. RU486 induced a hypersecretion of FSH, which started at 1400 h on the day of oestrus and was maintained until 0800 h on the day of metoestrus. Because the timing and magnitude of this secretion of FSH were similar to those of the periovulatory secretion of FSH during pro-oestrus and early oestrus in intact cyclic rats, we investigated the effects of: 1) LHRH antagonist (LHRHa) injected at either 0900 h or 2000 h on the day of oestrus, 2) oestradiol benzoate injected at 1600 h on the day of pro-oestrus and at 0900 h on the day of oestrus, 3) bovine follicular fluid (bFF) given either at 1100 h or at 2000 h on the day of oestrus, or 4) adrenalectomy (ADX) at 1100 h on the day of oestrus, on serum FSH and LH concentrations at 1800 h on the day of oestrus and at 0200 h on the day of metoestrus in rats injected with RU486 at pro-oestrus. The results showed that 1) both components (late oestrus and early metoestrus) of FSH hypersecretion in RU486-injected rats in pro-oestrus were inhibited by oestradiol benzoate and bFF, 2) the metoestrous component was not affected by LHRHa, whereas the oestrous component was partially reduced, and 3) ADX partially reduced serum FSH concentrations only on the day of metoestrus, possibly because, as the serum concentrations of corticosterone reflected, the antiglucocorticoid activity of 4 mg RU486 lasted only 24 h. The results support the hypothesis that blockade of progesterone actions at pro-oestrus results in the maintenance of the daily neural signal that activates the release of gonadotrophins. Whereas the expression of LH secretion requires high levels of oestradiol, FSH secretion is expressed against a background of low oestradiol levels. The results of this study also indicate that the release of FSH during oestrus and metoestrus in rats injected with RU486 at pro-oestrus is a consequence of the lack of ovarian negative feedback inhibition on the pituitary.

Alteraciones ventilatorias encontradas en pacientes con artritis reumatoidea / Alterations opposing ventilators in patient with arthritis reumatoidea

Se hace un estudio de 56 pacientes escogidos al azar simple de un universo de 112 pacientes que asisten a la consulta de reumatología del Hospital Provincial Clínico Quirúrgico Docente Dr. Gustavo Aldereguía Lima, afectados de artritis rematoidea, a los que se les realizó pruebas funcionales respiratorias, se consideró la edad, sexo y tiempo de evolución de la enfermedad. Predominó el sexo femenino y el grupo etareo de 45 a 59 años. Todos los parámetros ventilatorios investigados mostraron diferentes alteraciones, pero el mas afectado fue la capacidad vital, también se mostraron mas alterados, mientras mas años de evolución presentó la enfermedad y las pruebas funcionales respiratorias normales predominaron en los pacientes con menos de 2 años de evolución de la artritis reumatoidea