Sex differences in the beneficial cardiac effects of chronic treatment with atrial natriuretic Peptide in spontaneously hypertensive rats.

INTRODUCTION: The aim of this study was to investigate both the effects of chronic treatment with atrial natriuretic peptide (ANP) on systolic blood pressure (SBP), cardiac nitric oxide (NO) system, oxidative stress, hypertrophy, fibrosis and apoptosis in spontaneously hypertensive rats (SHR), and sex-related differences in the response to the treatment. METHODS: 10 week-old male and female SHR were infused with ANP (100 ng/hr/rat) or saline (NaCl 0.9%) for 14 days (subcutaneous osmotic pumps). SBP was recorded and nitrites and nitrates excretion (NOx) were determined. After treatment, NO synthase (NOS) activity, eNOS expression, thiobarbituric acid-reactive substances (TBARS) and glutathione concentration were determined in left ventricle, as well as the activity of glutathione peroxidase (GPx), catalase (CAT) and superoxide dismutase (SOD). Morphological studies in left ventricle were performed in slices stained with hematoxylin-eosin or Sirius red to identify collagen as a fibrosis indicator; immunohistochemistry was employed for identification of transforming growth factor beta; and apoptosis was evaluated by Tunel assay. RESULTS: Female SHR showed lower SBP, higher NO-system activity and less oxidative stress, fibrosis and hypertrophy in left ventricle, as well as higher cardiac NOS activity, eNOS protein content and NOx excretion than male SHR. Although ANP treatment lowered blood pressure and increased NOS activity and eNOS expression in both sexes, cardiac NOS response to ANP was more marked in females. In left ventricle, ANP reduced TBARS and increased glutathione concentration and activity of CAT and SOD enzymes in both sexes, as well as GPx activity in males. ANP decreased fibrosis and apoptosis in hearts from male and female SHR but females showed less end-organ damage in heart. Chronic ANP treatment would ameliorate hypertension and end-organ damage in heart by reducing oxidative stress, increasing NO-system activity, and diminishing fibrosis and hypertrophy.

Blood pressure-lowering effect of dietary (-)-epicatechin administration in L-NAME-treated rats is associated with restored nitric oxide levels.

Epidemiological and intervention studies have shown that the intake of certain chocolates or cocoa products decreases blood pressure (BP) in humans. (-)-Epicatechin is the most abundant flavanol present in cocoa seeds and its derived foods. This work investigates the effects of dietary (-)-epicatechin on BP in rats that received N(ω)-nitro-l-arginine methyl ester (L-NAME) for 4 days. (-)-Epicatechin administration prevented the 42mm Hg increase in BP associated with the inhibition of NO production in a dose-dependent manner (0.2-4.0g/kg diet). This BP effect was associated with a reduction in L-NAME-mediated increase in the indexes of oxidative stress (plasma TBARS and GSSG/GSH(2) ratio) and with a restoration of the NO concentration. At the vascular level, none of the treatments modified NOS expression, but (-)-epicatechin administration avoided the L-NAME-mediated decrease in eNOS activity and increase in both superoxide anion production and NOX subunit p47(phox) expression. In summary, (-)-epicatechin was able to prevent the increase in BP and in oxidative stress and restored NO bioavailability. The fact that (-)-epicatechin is present in several plants usually consumed by humans gives the possibility of developing diets rich in those plants or pharmacological strategies using that flavonoid to diminish BP in hypertensive subjects.

Programación de hipertensión arterial por restricción moderada de cinc durante la vida fetal y la lactancia: Alteraciones morfológicas y funcionales tempranas del sistema cardiovascular en ratas de ambos sexos / Fetal Programming of Hypertension Induced by Moderate Zinc Restriction during Prenatal Life and Lactation: Early Morphological and Functional Alterations in Cardiovascular System in Both Sexes / Fetal Programming of Hypertension induced by Moderate Zinc Restriction during Prenatal Life and Lactation: early Morphological and Functional alterations in cardiovascular system in both sexes

Introducción Numerosos estudios sugieren que trastornos metabólicos y desequilibrios nutricionales durante la vida intrauterina pueden inducir adaptaciones que programen enfermedades cardiovasculares e hipertensión arterial. En trabajos previos mostramos que la restricción moderada de cinc durante la vida fetal, la lactancia y/o el crecimiento conduce al desarrollo de hipertensión arterial y disfunción renal en la adultez. Objetivos Evaluar la presencia de alteraciones cardiovasculares tempranas en ratas sometidas a una deficiencia moderada de cinc durante la vida fetal y la lactancia y si existen diferencias respecto del sexo. Material y métodos Ratas Wistar hembras recibieron durante la preñez hasta el destete una dieta control o baja en cinc. En el momento del nacimiento se conformaron cuatro grupos experimentales: machos y hembras nacidos de madres bajas y machos y hembras nacidos de madres controles. A los 6 y a los 21 días de vida se sacrificaron y se determinaron el peso corporal, el peso del corazón, parámetros morfométricos cardiovasculares, la actividad de la óxido nítrico sintasa en el sistema cardiovascular y el estado oxidativo cardíaco. Resultados El aporte insuficiente de cinc durante la vida fetal y la lactancia indujo un proceso de re­modelación del cardiomiocito, diferente en machos que en hembras, un aumento del estrés oxidativo cardíaco, una remodelación hipotrófica de la aorta torácica y una disminución de la actividad de la óxido nítrico sintasa en el sistema cardiovascular. Conclusiones Este trabajo demuestra que la deficiencia de cinc induce alteraciones cardiovasculares, dis­tintas en machos que en hembras, tempranas en el desarrollo, que podrían contribuir a la programación de enfermedades en la vida adulta.

Background Several studies suggest that metabolic disorders and nutrition imbalance during prenatal life may induce adaptations that program cardiovascular diseases and hypertension. We have previously shown that moderate zinc restriction during prenatal life, lactation and/or growth leads to the development of hypertension and renal dysfunction in adulthood. Objectives To evaluate the presence of early cardiovascular alterations in rats exposed to a moderate zinc deficient diet during pre­natal life and lactation, and to determine whether there are differences between males and females. Material and Methods Female Wistar rats received low zinc diet or control diet from the beginning of pregnancy up to weaning. Four experimental groups were established at birth: males and females born from low-diet mothers, and males and females born from control-diet mothers. Male and female offspring were sacrificed at 6 and 21 days of life to evaluate body weight, heart weight, cardiovascular morphometric parameters and nitric oxide synthase activity in the cardiovascular system and cardiac oxidative status. Results The insufficient zinc intake during prenatal life and lacta-tion induced a remodeling process of the cardiomyocyte which was different in males and females, increased cardiac oxidative stress, produced a hypotrophic remodeling of the thoracic aorta and reduced nitric oxide synthase activity in the cardiovascular system. Conclusions This study shows that zinc deficiency induces cardiovascular abnormalities in early stages of development, which are different in males and females that may contribute to programming of diseases in adulthood.

Osteoblastic behavior of human bone marrow cells cultured over adsorbed collagen layer, over surface of collagen gels, and inside collagen gels.

While collagen type I is often used as a substrate for cell culturing and as a coating in biomedical implants, as far as we know a simple systematic study comparing the effects of the different presentations of collagen type I on the osteoblastic behavior of cells is missing. In this work, human bone marrow cells (hBMCs) were cultured under osteoblastic-inducing conditions, for 21 days, over a layer of adsorbed collagen (monomeric) and on the surface and inside collagen gels (fibrillar). Comparison was made based on three classical parameters; cell proliferation/viability, alkaline phosphatase (ALP) activity, and production of mineral deposits. The three types of collagen type I substrates allowed the adhesion, proliferation, and the osteoblastic differentiation of cells. However, hBMCs behavior was influenced by the monomeric/fibrillar and 2-/3-dimensional nature of the collagen substrates, namely: monomeric collagen favored cell attachment; cells on 2D substrates presented higher proliferation rates during the exponential phase of growth with formation of spiral-like multilayered structures; cells seeded inside 3D collagen gels formed a regular dense cellular mesh and had a low proliferating rate; cells cultured over or inside fibrillar collagen differentiated faster, with the 3D cultures presenting higher levels of ALP activity; and the extension of mineralization was greater for the cultures done over or inside fibrillar collagen. Thus, cells cultured over collagen gels showed both the ability for cell proliferation and for earlier differentiation, a fact that can be exploited in the biomaterials field.

Programación temprana de alteraciones en el sistema del óxido nítrico renal y vascular inducidas por la deficiencia de cinc / Early Programming of Alterations in Renal and Vascular Nitric Oxide System Induced by Zinc-Related Deficiencies

Introducción Numerosos estudios mostraron que la deficiencia nutricional durante la vida fetal y posnatal predisponen al desarrollo de patologías en la vida adulta, como la hipertensión arterial y las enfermedades renales. La distribución ubicua del cinc y sus propiedades químicas determinan su esencialidad en los sistemas biológicos. Objetivos Evaluar si las alteraciones renales y cardiovasculares en la vida adulta inducidas por la restricción moderada de cinc durante la vida fetal, la lactancia y/o el crecimiento se asocian con cambios en el sistema del óxido nítrico. Material y métodos Ratas Wistar hembra recibieron durante la preñez hasta el destete de las crías una dieta control o una baja en cinc. Luego del destete, las crías macho se asignaron al azar a dos grupos que recibieron una dieta control o una baja en cinc durante 60 días. Resultados Los resultados mostraron que el aporte insuficiente de cinc durante el crecimiento previo y/o posterior al destete indujo un aumento de la presión arterial y una disminución del volumen de filtrado glomerular en la vida adulta, asociados con una disminución del sistema del óxido nítrico renal y vascular. Además, el bajo aporte de este mineral durante la vida fetal indujo un peso menor al nacer, que se correlacionó en forma negativa con la presión arterial en la vida adulta. Conclusiones Este trabajo brinda evidencias importantes que sugieren que el aporte inadecuado de cinc durante el crecimiento prenatal y posnatal constituye un factor de riesgo cardiovascular y renal, dado que induce alteraciones en la regulación de la presión arterial y en la función renal en el individuo adulto.

Background Several studies have reported that nutritional deficiencies during fetal and postnatal life predispose to the development of diseases such as hypertension and renal disorders during adulthood. The ubiquitous distribution of zinc and its chemical properties determine their essentiality in the biological systems. Objectives To assess whether renal and cardiovascular alterations induced by moderate zinc restriction during fetal life, lactation period and/or growth are associated with changes in the nitric oxide system. Material and Methods Female Wistar rats received low zinc diet or control diet from the beginning of pregnancy up to weaning. After weaning, male offspring were randomly fed with low zinc diet or control diet for 60 days. Results Zinc deficiency through pre-weaning and post-weaning growth induced increase in blood pressure and reduced glomerular filtration volume in adult life; these findings were associated with reductions in renal and vascular nitric oxide system. In addition, low zinc intake during intrauterine life induced low birth weight offspring which had a negative correlation with blood pressure in adulthood. Conclusions Zinc deficiency during prenatal and postnatal growth constitutes a risk factor for cardiovascular and kidney diseases as it induces alterations in blood pressure and renal function regulation in adult life.

Respuesta hipotensora al tratamiento agudo con péptido natriurético auricular: su relación con la expresión y la actividad de la óxido nítrico sintetasa cardíaca en ratas espontáneamente hipertensas / Hypotensive Response to Acute Treatment with Atrial Natriuretic Peptide: Its Relationship with Cardiac Nitric Oxide Synthase Expression and Activity in Spontaneously Hypertensive Rats

Introducción El péptido natriurético auricular (ANP) y el óxido nítrico (NO) aumentan la diuresis y la natriuresis y disminuyen el tono vascular. Previamente demostramos que el NO está involucrado en el efecto hipotensor del ANP en ratas normotensas. Objetivo Estudiar el efecto del ANP sobre la presión arterial media (PAM) y el sistema del NO en ratas espontáneamente hipertensas (SHR) y Wistar Kyoto (WKY) y la participación de la isoforma inducible de la NO-sintasa (iNOS). Material y métodos Protocolo 1: los animales fueron infundidos con solución salina (0,05 ml/min) o con ANP (0,2 µg/kg/min) durante 1 hora. Se determinaron: PAM y nitritos y nitratos urinarios (NOx). Se extrajo el corazón y se determinaron la actividad, con L-[U14C]-arginina, y la expresión (Western blot) de iNOS y NOS endotelial (eNOS). Protocolo 2: luego del agregado de ANP (1 µM), cANP(4-23) (agonista NPR-C,1µM) o aminoguanidina (inhibidor de iNOS, 1 µM) se determinó la actividad de la NOS en la aurícula derecha y en el ventrículo izquierdo de SHR y WKY. Resultados La infusión con ANP disminuyó la PAM y aumentó los NOx en ambos grupos. La actividad NOS fue mayor en SHR y se incrementó con la infusión de ANP. Se observaron niveles proteicos mayores para eNOS e iNOS en SHR, que no se modificaron con ANP. La actividad basal de iNOS fue mayor en SHR. En la aurícula, el ANP sólo interactuaría con el NPR-C para activar la NOS y en el ventrículo también participarían los receptores NPR-A/B. El desarrollo y/o el mantenimiento de la hipertensión en este modelo experimental involucraría alteraciones en la interacción entre ambos sistemas, ANP y NO.

Background Atrial natriuretic peptide (ANP) and nitric oxide (NO) increase diuresis and natriuresis and reduce vascular tone. We have previously demonstrated that NO is involved in ANP hypotensive effect in normotensive rats. Objective To assess the effect of ANP on mean blood pressure (MBP) and on NO system in spontaneously hypertensive rats (SHR) and Wistar Kyoto (WKY), and the role of the inducible isoform of nitric oxide synthase (iNOS). Material and Methods Protocol 1: animals were instilled with saline solution (0.05 ml/min) or with ANP (0.2 µg/kg/min) for an hour. MBP and urinary nitrites and nitrates (NOx) were assessed. The heart was extracted and iNOS and endothelial iNOS (eNOS) activity (with L-[U14C]-arginine) and expression (Western blot) were determined. Protocol 2: after adding ANP (1 µM), cANP(4-23) (NPR-C agonist, 1µM) or aminoguanidine (iNOS inhibitor, 1 µM) NOS activity in the right atrium and left ventricle of SHR and WKY was determined. Results Instillation with ANP reduced MBP and increased NOx in both groups. NOS activity was greater in SHR, and increased with the instillation of ANP. In SHR, greater eNOS and iNOS protein levels were observed, which were not modified by ANP. iNOS basal activity was greater in SHR. In the atrium, ANP interacts only with NPR-C in order to activate NOS, and NPR-A/B receptors would also take part in the ventricle. In this experimental model, the development and maintenance of hypertension could involve alterations in the interaction between both systems, ANP and NO.

Participación del receptor NPR-C en la activación de la sintetasa de óxido nítrico inducida por el péptido natriurético auricular en el corazón, la arteria aorta y el riñón / The role of NPR-C receptor on the activation of nitric oxide synthase induced by atrial natriuretic peptide in the heart, aorta artery and kidney

En trabajos previos demostramos que la activación de la sintetasa de óxido nítrico (NOS) mediaría, al menos en parte, las acciones hipotensoras, diuréticas y natriuréticas del péptido natriurético auricular (ANP). El objetivo fue investigar el tipo de receptor natriurético y los mecanismos de señalización involucrados en la activación de la NOS en presencia de ANP. Se trabajó con aurícula, aorta y riñon de ratas Wistar macho, previamente sacrificadas por decapitación. En dichos tejidos se midió la actividad de las NOS (pmol L-[U14C] citrulina/g tejido) utilizando L-[U14C] arginina como sustrato. Tanto el ANP como el cANP (4-23) (agonista específico de receptores NPR-C) aumentaron la actividad de la NOS en todos los tejidos y este aumento fue mayor para el ANP en el riñón y la aorta y similar para ambos péptidos en la aurícula. Estos efectos fueron bloqueados por la nifedipina (bloqueante de canales de Ca²+ tipo L). La inhibición de la proteína Gi1-2 con toxina pertussis bloqueó el efecto del cANP sobre la enzima tanto en la aurícula y la arteria como en el riñón. En la aurícula, la activación de la NOS mediada por el ANP se debería a la interacción del péptido con el receptor natriurético NPR-C, mientras que en el riñón y en la aorta participarían además los receptores natriuréticos NPR-A y/o B. El ANP interactuaría con el receptor NPR-C acoplado a la vía de la proteína Gi, activando la NOS Ca²+ dependiente.

Assignment of disulphide bridges in Par j 2.0101, a major allergen of Parietaria judaica pollen.

Par j 2.0101, a major allergen of the Parietaria judaica pollen, was expressed in E. coli, purified to homogeneity and fully characterised both at the structural and the functional level. The recombinant rPar j 2.0101 protein showed an allergenic activity in histamine release, skin prick tests and capacity to bind IgE, almost identical to that of the native allergens purified from aqueous pollen extract. The complete pattern of S-S bridges of rPar j 2.0101 was determined by enzymatic digestion with endoproteinase Lys-C followed by mass spectrometric analysis of the resulting peptide mixtures. The eight cysteines occurring in the allergenic protein were found to be paired into the following four disulphides: Cys35-Cys83, Cys45-Cys60, Cys61-Cys106 and Cys81-Cys121. This structural information probes Par j 2.0101 to attain a 3-D fold consistent with that of the non-specific lipid transfer protein (ns-LTP) family and it represents an effective molecular basis to develop modified antigens by selective site-directed mutagenesis for immunotherapy.

Heat shock protein-27 protects human bronchial epithelial cells against oxidative stress-mediated apoptosis: possible implication in asthma.

Inflammation of the human bronchial epithelium, as observed in asthmatics, is characterized by the selective death of the columnar epithelial cells, which desquamate from the basal cells. Tissue repair initiates from basal cells that resist inflammation. Here, we have evaluated the extent of apoptosis as well as the Hsp27 level of expression in epithelial cells from bronchial biopsy samples taken from normal and asthmatic subjects. Hsp27 is a chaperone whose expression protects against oxidative stress. We report that in asthmatic subjects the basal epithelium cells express a high level of Hsp27 but no apoptotic morphology. In contrast, apoptotic columnar cells are devoid of Hsp27 expression. Moreover, we observed a decreased resistance to hydrogen peroxide-induced apoptosis in human bronchial epithelial 16-HBE cells when they were genetically modified to express reduced levels of Hsp27.