Tesis
Ajustes cardiorrespiratórios em ratos submetidos a diferentes tipos de desidratações
Fecha
2016-09-06Registro en:
Autor
Fávero, Michele Thaís
Institución
Resumen
Arthropods and vertebrates have a great ability to concentrate urine by the kidney and behaviors
directed the conservation and acquisition of water and salt due to activities controlled by
mechanisms involving hormones and neural circuits. The loss of water or body volume can occur
in the intracellular compartment (intracellular dehydration), the extracellular compartment
(extracellular dehydration) or both (absolute or duble dehydration). Studies from our laboratory
had shown that in unanesthetized animals extracellular dehydration produced by furosemide
injection followed by keeping animals with a sodium deficient diet does not alter the basal
cardiovascular parameters, but change the basal ventilation.Therefore, the objectives of our study
in unanesthetized rats submitted to intracellular dehydration or duble dehydration were: 1) to
characterize the baseline cardiorespiratory responses; 2) evaluate the arterial blood gas
parameters; 3) to evaluate plasma concentrations of sodium, potassium and plasma osmolality; 4)
evaluate the cardiorespiratory responses to the activation of glutamate NMDA receptors in the
NTS before and after pretreatment with glutamate NMDA receptor antagonist (AP5) of rats
submitted to mixed dehydration. Holtzman rats were implanted with cannula in the NTS and
catheter inserted in the abdominal aorta via the femoral artery and femoral vein. The ventilation
(VE) measurement were obtained by whole body plethysmography method. The protocols was
performed in rats euhydrated (before dehydration), dehydrated (following the methodology to
induce dehydration) and/or rehydrated rats (2 h after free access to water and 0.3 M NaCl). The
intracellular dehydration induced by intragastric overload 2 M NaCl (2 mL) produced an increase
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in mean arterial pressure (MAP), without change the heart rate (HR), tidal volume (VT),
respiratory rate (fR) and VE. The duble dehydration (intracellular and extracellular combined)
induced by 24 h of water deprivation, produced an increase in MAP and VT without modifying
the HR, fR and VE. In rehydrated rats PAM and VT returned to baseline. Unilateral injections of
L-glutamate and NMDA glutamatergic receptor agonist into NTS of euhydrated rats produced
pressor responses and bradycardia. After 24 hours of water deprivation these pressor and
bradycardic responses produced by NMDA injection in the NTS were reduced, without changing
the bradycardia produced by L-glutamate injection in the NTS. After rehydration, the pressor
responses to L-glutamate and NMDA receptors in the NTS remained low and bradycardia
produced by NMDA injection in the NTS. Furthermore, the objectives of our study in
anesthetized animals subjected to extracellular dehydration were: 1) to characterize the baseline
cardiorespiratory responses and renal sympathetic nerve activity (RSNA); 2) to evaluate the effect
of peripheral blockade of AT1 receptors angiotensinergic on basal cardiorespiratory responses and
on RSNA; 3) to evaluate the arterial blood gas parameters; 4) to evaluate plasma concentrations of
sodium and potassium. Extracellular dehydration induced by subcutaneous injection of the
diuretic furosemide did not affect the basal MAP and HR, phrenic nerve activity (PNA) and
RSNA. Extracellular dehydration did not affect the pressor response produced by intravenous (iv)
injection of ANG II, decreased ASNR and did not change the HR and PNA. The iv injection of
losartan (AT1 receptor antagonist, 1 mg/kg body weight) induced a decrease in MAP without
changing HR, and RSNA and PNA. The hypotensive response after iv injection of losartan was
greater in dehydrated animals. Extracellular dehydration did not affect the response of RSNA and
PNA after losartan administration. The results suggest that changes in the volume and
composition of body fluids affect the cardiovascular control in animals with intracellular
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dehydration. Furthermore, it affects the cardiorespiratory control in animals with mixed
dehydration and glutamatergic neurotransmission in the NTS. Moreover, in anesthetized animals
with extracellular dehydration showed no changes in baseline cardiorespiratory responses and
RSNA.