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A microperfusion investigation of bicarbonate secretion by the rat submaxillary gland (1970)

Young, J. A. ; Martin, C. J. ; Asz, M. ; [et al.]

Springer

Pflügers Archiv 319 (1970), S. 185-199

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ISSN: 1432-2013

Keywords: Submaxillary Gland ; Bicarbonate Secretion ; Microperfusion ; Acetazolamide ; Carbachol ; Submaxillardrüse ; Bicarbonatsekretion ; Mikroperfusion ; Acetazolamid ; Carbachol

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Bicarbonate transport in the rat submaxillary main duct has been studied by microperfusion. Bicarbonate was concentrated in the duct lumen against an electrochemical gradient and the equilibrium concentration was estimated to be 56.5 mEq/l±3.1 (S.E.M.,n=11). The secretory mechanism could not be inhibited by 6 mMolar cyanide although such concentrations caused marked inhibition of both net sodium efflux and net potassium influx. Bicarbonate secretion in the main duct was not inhibited by acetazolamide whether applied from the duct lumen or given intravenously. Similarly, the drug was without effect on bicarbonate excretion by the intact gland even when maximum excretory rates had been induced with carbachol. It was concluded that catalytic hydration of carbon dioxide to carbonic acid was not a rate-limiting step in the bicarbonate secretory process. The data did not permit a distinction to be made between a bicarbonate secretory processper se and a process of either H+ reabsorption or OH− secretion. The parasympathomimetic agent, carbachol, when given parenterally was found to increase sharply the net influx of bicarbonate into the microperfused main duct as well as to reduce net sodium efflux and net potassium influx. Previously it had been postulated that final saliva was formed in two stages. First a plasma-like primary secretion was formed at a rate depending on the degree of stimulation, and second, the primary secretion was modified in the gland duct system by reabsorptive and secretory processes whose transport rates were presumed to be independent of the degree of stimulus. It now becomes necessary to postulate that stimulation can act on electrolyte transport at both primary and secondary levels; at present, however, no data are available to show whether appreciable net water influx can ever occur at the secondary level.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00586449

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Electrolyte concentrations in primary and final saliva of the rat sublingual gland studied by micropuncture and catheterization techniques (1971)

Martin, C. J. ; Young, J. A.

Springer

Pflügers Archiv 324 (1971), S. 344-360

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ISSN: 1432-2013

Keywords: Rat Sublingual Gland ; Micropuncture ; Electrolyte Transport ; Parasympathomimetic Stimulation ; Sublingualdrüse ; Mikropunktion ; Elektrolyttransport ; Parasympathicomimetische Stimulation

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The salivary electrolyte concentrations at various secretory rates have been studied in the rat sublingual gland and compared with the concentrations found in acinar-intercalated duct (primary) fluid obtained by micropuncture. The primary fluid had the following composition: [Na]=126±1.6 (S.E.M.,n=39) mEq/l; [K]=11.9±1.2 mEq/l (n=39); [Cl]=99.3±2.3 mEq/l (n=33). The Na and K concentrations differed significantly from those of plasma and from those observed previously in the primary fluid of rat parotid and submaxillary glands. The composition of primary fluid was not altered by carbachol stimulation. After carbachol stimulation, the final saliva, like that of the human but unlike that of the cat and dog sublingual gland, was hypotonic and the electrolyte concentrations showed flow-rate dependence. At the lowest flow rate the Na concentrations averaged 24.6±3.9 mEq/l (n=25) which fell first to a minimum and then rose to a plateau of about 60 mEq/l as flow rate increased to a maximum. The excretory curve showed no tendency to approach the concentrations seen in primary saliva. The K excretory curve was typical of that seen in most other salivary glands, having high concentrations at low flow rates which fell towards a plateau above primary fluid levels as flow rate increased. The salivary bicarbonate concentration was always above that in plasma; it tended to rise to a plateau of about 48 mEq/l at the highest flow rates. This concentration is probably greater than that present in primary fluid although the primary levels have not been measured directly. The results are best interpreted in terms of a modified two-stage hypothesis. First a primary, Na-rich, K-poor secretion is formed in the acinar-intercalated duct region whose composition, although decidedly not plasma-like, is constant irrespective of the degree of gland stimulation. Then, secondarily, this fluid is modified during passage along the striated and excretory ducts by processes of Na reabsorption and K and HCO3 secretion. These secondary transport processes are not transport-maximum-limited but appear to increase with increasing degree of stimulation resulting in a phenomenon which could be termed acinar-tubular balance. Although it has not proven possible to micropuncture striated ducts in the rat submaxillary or parotid glands, in the sublingual gland we were able to do so in a few cases. For the first time we are able to offer direct proof that these ducts do contain hypotonic fluid.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00592462

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The effect of a sympatho- and a parasympathomimetic drug on the electrolyte concentrations of primary and final saliva of the rat submaxillary gland (1971)

Young, J. A. ; Martin, C. J. ; Weber, F. D.

Springer

Pflügers Archiv 327 (1971), S. 285-302

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ISSN: 1432-2013

Keywords: Parasympathicomimetic ; Sympathicomimetics ; Submaxillary Gland ; Potassium Secretion ; Bicarbonate Secretion ; Isoproterenol ; Carbachol ; Parasympathomimetica ; Sympathomimetica ; Glandula submaxillaris ; Kalium-Sekretion ; bicarbonat-Sekretion ; Isoproterenol ; Carbachol

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Salivary glands are generally supposed to produce their secretions in 2 stages: 1. A plasma-like secretion is formed in the acinar-intercalated duct region of the gland, the rate of production but not the electrolyte composition of this fluid being increased by gland stimulation. 2. This primary saliva is then modified during its passage along the gland duct system by processes of Na reabsorption and K and HCO3 secretion. In general terms this hypothesis accounts for the behaviour of salivary glands undergoing parasympathetic or parasympathomimetic stimulation. However, when sympathetic or sympathomimetic stimulation occurs the electrolyte excretory patterns are anomalous and the 2-stage hypothesis cannot easily account for them. Thus, after sympathomimetic stimulation the rat submaxillary saliva was found to be nearly isotonic with [K]=150 mEq/l and [HCO3]=135 mEq/l, the concentrations being independent of flow rate. To elucidate this problem the Na, K and HCO3 excretory curves in rat submaxillary saliva have been studied in animals undergoing parasympathomimetic, sympathomimetic and combined sympatho- and parasympathomimetic stimulation and these have been compared with the electrolyte concentrations of primary saliva obtained at rest and after stimulation. The results suggest: 1. That both types of drug stimulate formation of an approximately plasma-like primary secretion whose composition changes only slightly with stimulation. Parasympathomimetics, however, cause production of 6–8 times more primary fluid per unit time than sympathomimetics. 2. That contrary to all previous opinion, the drugs have a direct action at the ductal level where they stimulate secretion of K and HCO3. At this site the effects of the two types of drug are approximately equal which explains why sympathetic saliva is so rich in K and HCO3. The ductal action of parasympathomimetics may also explain why ductal secretion of both K and HCO3 do not undergo saturation as gland stimulation is progressively increased.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00588449

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Amicroperfusion investigation of the effects of a sympathomimetic and a parasympathomimetic drug on water and electrolyte fluxes in the main duct of the rat submaxillary gland (1971)

Martin, C. J. ; Young, J. A.

Springer

Pflügers Archiv 327 (1971), S. 303-323

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ISSN: 1432-2013

Keywords: Parasympathomimetics ; Sympathomimetics ; Electrolyte Transport ; Submaxillary Gland ; Microperfusion ; Parasympathicomimetica ; Sympathicomimetica ; Elektrolyttransport ; Glandula submaxillaris ; Mikroperfusion

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Previous studies on the intact rat submaxillary gland led to the hypothesis that sympathomimetic and parasympathomimetic drugs, in addition to stimulating glandular production of primary saliva, also stimulated secondary secretion of K and HCO3 by the striated and excretory ducts. It was postulated that parasympathomimetics were more effective stimulants than sympathomimetics atthe primary level but atthe secondary level the two types of drug had actions that were of approximately the same magnitude and that, when administered together, the effects of the drugs were additive. To test this hypothesis the effects of a parasympathomimetic drug (carbachol) and a sympathomimetic drug (isoproterenol) on nett electrolyte transport and transepithelial electrical potential differences were studied in the perfused main duct of the rat submaxillary gland. It was found: 1. That both carbachol and isoproterenol stimulated ductal secretion of bicarbonate irrespective of the electrolyte composition of the perfusion fluid. 2. Both drugs stimulated a parallel nett secretion of potassium when the perfusion fluid contained a low concentration of NaCl. 3. When the lumen contained a high concentration of NaCl, ductal Na reabsorption and K secretion were reduced and HCO3 secretion was accomplished partly in exchange for chloride and partly in parallel with K secretion. 4. In supra-maximal doses the effects of both drugs were of the same order of magnitude and when administered together the effect was always greater than that which could be produced by the same doses of either drug alone. It is concluded that, during pharmacological stimulation of the submaxillary gland, stimulation of ductal secretion of K and HCO3 did indeed occur and that such an occurrence could account for anomalies previously observed in the electrolyte excretory patterns of the intact gland undergoing parasympathomimetic and sympathomimetic stimulation. Since the electrolyte excretory patterns found in saliva collected after nerve and pharmacological stimulation are quite similar it was felt that stimulation of ductal K and HCO3 secretion probably also occurred in this and other salivary glands during nerve stimulation.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00588450

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The effects of carbachol on water and electrolyte fluxes and transepithelial electrical potential differences of the rabbit submaxillary main duct perfusedin vitro (1973)

Martin, C. J. ; Frömter, E. ; Gebler, B. ; [et al.]

Springer

Pflügers Archiv 341 (1973), S. 131-142

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ISSN: 1432-2013

Keywords: Carbachol ; Parasympathomimetic Drug ; Sodium Conductance ; Submaxillary Gland ; Microperfusion ; Electrolyte Transport

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The effect of carbachol on transepithelial potential difference and transepithelial nett electrolyte transport has been studied in the rabbit submaxillary main duct perfusedin vivo andin vitro with bicarbonate saline. The two preparations function similarly, reabsorbing Na, Cl and water and secreting K. In control ducts nett Na reabsorption was 683±55 nmol · cm−2 · min−1 and K secretion was 31.2±2.4 nmol · cm−2 · min−1. Nett water reabsorption was 970±71 nl · cm−2 · min−1 and the hydraulic conductivity was (14.0±1.6)×10−6 ml · cm−2 · s−1 · atm−1. The mean transepithelial potential difference was 13.1±0.8 mV (lumen negative) and, assuming no active transport of Cl, the partial conductance of the duct to Cl was (12.7±2.6)×10−2 mho · cm−2. Carbachol,in vivo andin vitro, caused partial depolarization of the transepithelial potential difference and reduction of nett Na and Cl reabsorption. It was without effect on duct K and HCO3 transport.In vitro, the drug was effective in concentrations as low as 10−7 M and perhaps lower. Atropine was able completely to block the effects of carbachol present at twice the atropine concentration. The results are consistent with the hypothesis that carbachol acts in some way to reduce the sodium conductance of the luminal face of the duct epithelial cell, this response being secondary to an undefined primary action of carbachol on the interstitial face of the cell.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00587320

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