Kidney and Body Fluids (eBook)
688 Seiten
Elsevier Science (Verlag)
978-1-4831-5380-3 (ISBN)
Advances in Physiological Sciences, Volume 11: Kidney and Body Fluids offers a thorough discussion of the experiments, research, and investigations done on the function, composition, and chemical reactions the kidney and body fluids undergo. Divided into 10 parts and having 88 chapters, the book features lengthy literature of authors who have actively pursued research on kidney and body fluids. Areas covered include renal cell cultures and blood flow; glomerulotubular balance; cell ionic activity and element analysis; electrophysiology and epithelial transport; and tubular handling of phosphate and calcium. Tubular acidification, regulation of water balance, and extracellular volume control are also discussed. The text presents as well how the study of the kidney and body fluids have captured the interest of physiologists and other individuals interested in this discipline. The book is a dependable source of information for those interested in the composition, function, and chemical reactions of the kidney and body fluids. The text is highly recommended to scholars and students who find this field of study interesting.
NEURAL CONTROL OF RENAL FUNCTION*
Carl W. Gottschalk**, Romulo E. Colindres, Nicholas G. Moss, Paula R. Rogenes and Laszlo Szalay***, Departments of Medicine and Physiology University of North Carolina School of Medicine, Chapel Hill, North Carolina, USA
Publisher Summary
This chapter discusses that efferent renal nerve stimulation affect both proximal tubular transport of salt and water and the resistance of the renal vessels. It highlights the possibility of a neural mechanism, a renorenal reflex, being responsible for the coordination of the excretory activity of the two kidneys that occurs when the function of one of the kidneys is altered. The condition under which the mechanism becomes operative requires further identification, but it is not restricted to the anesthetized state. Renal chemoreceptors and the mechanoreceptors provide an afferent mechanism for ipsilateral and contralateral renorenal reflexes integrated at the spinal cord level. This appears to be the operative mechanism in at least one instance of coordination of renal excretory activity. The full extent of the neural mechanism, involving different neurotransmitters with opposing effects, almost certainly exceeds in complexity of the simple system.
This morning I wish to consider the role of the renal nerves in maintaining the homeostasis of the body fluids. I will discuss the efferent control of excretory activity and the nature of the renal receptors that send afferent impulses to the neural axis when stimulated. I will also consider the possibility of a neural mechanism, a renorenal reflex, being responsible for the coordination of the excretory activity of the two kidneys that occurs when the function of one of the kidneys is altered.
Claude Bernard (1859) was the first to report that acute section of the splanchnic nerves in an anesthetized dog results in an increase in urine production by the ipsilateral kidney. This observation has been repeatedly confirmed over the subsequent years. The two problems addressed by most investigators have been, (first) whether the effect is exclusively hemodynamic in origin due to an increase in glomerular filtration rate and renal blood flow, or whether there is also an effect on the tubular mechanisms for reabsorption, and secondly, whether the effect, whatever its mechanism, is evident only under the abnormal circumstances of anesthesia and surgery, and thus should not be considered a response to “physiological” alterations. Until recently the answer to the first question was that the effect was exclusively hemodynamic, but I will review the compelling evidence that the sympathetic efferent inflow to the kidney has a direct effect on tubular reabsorptive mechanisms which may under certain circumstances be magnified by hemodynamic factors, although the latter need not occur. I do not believe that the answer to the second question has yet been completely resolved. Almost all of the published evidence favors the view that it is apparent only when the animal is severely stressed. More recent studies, however, indicate that the effects of denervation may be seen in conscious animals.
The neural efferent mechanism for control of salt and water excretion has been intensively investigated in recent years in 3 laboratories, by Dr. Takacs and his colleagues at Semmelweis University here in Budapest, by Dr. DiBona and colleagues at the University of Iowa, and by my associates in the Chapel Hill Micropuncture Laboratory. The results obtained in these laboratories have been complementary.
The recent description of a tubular innervation provides an anatomical basis for the tubular functional effects reported by these 3 laboratories. It has been known since the studies of Bradford (1889) that there is a rich sympathetic innervation of the blood vessels of the kidney; although there have been periodic reports of a direct tubular innervation there have been at least as many reports denying this. In the early 1970s Barajas and Mueller presented for the first time convincing evidence for a direct innervation of the tubular cells in the cortex of monkey and rat kidneys (Barajas and Mueller 1973 and Mueller and Barajas 1972). Using electron microscopic and histochemical methods these investigators demonstrated adrenergic nerve terminals separated from proximal and distal tubular cells only by basement membrane material. This relationship is identical to that observed between similar vesiculated varicosities and vascular smooth muscle, a site where synaptic transmission is thought to occur.
MICROPUNCTURE AND CLEARANCE EXPERIMENTS
Although a proximal tubular effect was first reported by Bencsath et al. (1972), the Chapel Hill group was the first to provide extensive micropuncture documentation for such a result. Bello-Reuss et al. (1975) characterized the renal response to acute unilateral denervation in an extensive study of sham denervated and denervated kidneys. Denervation of a kidney was accomplished by stripping the renal artery of its adventitia and coating it with a solution of 10% phenol in alcohol. For a variety of reasons the functional changes observed cannot be attributed to a direct effect of phenol on kidney function: no norepinephrine could be detected in the kidneys several days after denervation; incomplete denervation from splanchnic nerve crushing produced similar, but quantitatively smaller results than the apparently complete chemical denervation, and these effects were reversed by electrical stimulation of the distal end of the cut splanchnic nerve. Coating the artery with lidocaine instead of phenol produced similar but transitory effects.
No changes were observed in any function of either kidney of sham-denervated rats. Following unilateral denervation in hydropenic animals urine volume from the denervated kidney increased to about twice its control value, and urinary sodium excretion increased sixfold. There was no change in urine volume or sodium excretion from the innervated kidney. Glomerular filtration rate (GFR) and renal plasma flow (RPF) remained unchanged in both kidneys after the procedure. SNGFR remained unchanged after denervation. The fluid-to-plasma ratio of inulin decreased in samples of fluid collected from late proximal tubules of denervated kidneys indicating a 60% decrease in water and sodium reabsorption by the proximal tubule. Absolute water and sodium reabsorption increased in the loop of Henle, distal convolution, and collecting ducts, but not enough to compensate for the 60% decrease in the proximal tubule.
Denervation caused no change in estimated glomerular capillary or efferent arteriolar pressure. There were very small increases in hydrostatic pressure in proximal and distal convolutions and in small peritubular capillaries. Since there was no change in whole kidney or single nephron GFR and renal plasma flow was unchanged, it is unlikely that there was a change in overall or superficial nephron colloid osmotic pressure or significant redistribution of renal blood flow. It thus appears that the physical factors did not play an important role in the observed changes in tubular reabsorption.
Similar results were observed in animals expanded 10% above their body weight by an infusion of isotonic saline solution (Bello-Reuss et al. 1977). There was no change in GFR or RPF in either kidney after unilateral denervation or sham denervation. Urine flow and sodium excretion by denervated kidneys was doubled. Simultaneously urine flow and sodium excretion by the contralateral innervated kidneys fell by half so that there was little change in total salt and water excretion. I will return to this striking finding shortly. After denervation SNGFR remained unchanged. The F/P inulin ratio in fluid from late proximal tubules decreased, indicating a fall in water and sodium reabsorption in the proximal tubule of more than 50%. Absolute water and sodium reabsorption increased after denervation in the loop of Henle, distal convolution and collecting ducts but not enough to prevent the natriuresis and diuresis.
In another series of experiments in anesthetized rats the natriuresis and diuresis resulting from unilateral crushing of the greater splanchnic nerve was reversed by electrical stimulation of the distal portion of the cut nerve with square wave pulses of 0.5 msec duration, voltage twice threshold, and 1 or 2 Hz frequency (Bello-Reuss et al. 1976). Kidney GFR and RPF and SNGFR remained unchanged during stimulation. Nerve stimulation produced a reduction of approximately 25% in urine flow and sodium excretion due to increased water reabsorption in the proximal tubule. In 5 of 6 animals, stimulation at 1 Hz was followed by an increase in proximal F/P inulin ratio. In the one animal in which there was no change in F/P inulin there was no change in sodium excretion by the kidney. For unknown reasons, the appropriate fibers apparently were not stimulated in that animal. On cessation of stimulation the F/P inulin ratio returned to control values. Subsequent stimulation at 2 Hz caused an increase in F/P inulin ratio in all animals. Recordings of the compound action potential of the stimulated nerves indicated that the effect on tubular reabsorption resulted from stimulation of slowly conducting C fibers.
Recent studies both in Budapest (Bencsath et al. 1979) and in Chapel Hill (Colindres et al. 1980) demonstrate that the denervation effect is not a transient one that is observed only...
| Erscheint lt. Verlag | 22.10.2013 |
|---|---|
| Sprache | englisch |
| Themenwelt | Studium ► 1. Studienabschnitt (Vorklinik) ► Biochemie / Molekularbiologie |
| Studium ► 1. Studienabschnitt (Vorklinik) ► Physiologie | |
| Naturwissenschaften ► Biologie ► Humanbiologie | |
| ISBN-10 | 1-4831-5380-0 / 1483153800 |
| ISBN-13 | 978-1-4831-5380-3 / 9781483153803 |
| Haben Sie eine Frage zum Produkt? |
EPUB (Adobe DRM)Größe: 13,3 MB
Kopierschutz: Adobe-DRM
Adobe-DRM ist ein Kopierschutz, der das eBook vor Mißbrauch schützen soll. Dabei wird das eBook bereits beim Download auf Ihre persönliche Adobe-ID autorisiert. Lesen können Sie das eBook dann nur auf den Geräten, welche ebenfalls auf Ihre Adobe-ID registriert sind.
Details zum Adobe-DRM
Dateiformat: EPUB (Electronic Publication)
EPUB ist ein offener Standard für eBooks und eignet sich besonders zur Darstellung von Belletristik und Sachbüchern. Der Fließtext wird dynamisch an die Display- und Schriftgröße angepasst. Auch für mobile Lesegeräte ist EPUB daher gut geeignet.
Systemvoraussetzungen:
PC/Mac: Mit einem PC oder Mac können Sie dieses eBook lesen. Sie benötigen eine
eReader: Dieses eBook kann mit (fast) allen eBook-Readern gelesen werden. Mit dem amazon-Kindle ist es aber nicht kompatibel.
Smartphone/Tablet: Egal ob Apple oder Android, dieses eBook können Sie lesen. Sie benötigen eine
Geräteliste und zusätzliche Hinweise
Zusätzliches Feature: Online Lesen
Dieses eBook können Sie zusätzlich zum Download auch online im Webbrowser lesen.
Buying eBooks from abroad
For tax law reasons we can sell eBooks just within Germany and Switzerland. Regrettably we cannot fulfill eBook-orders from other countries.
aus dem Bereich
