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Biochimica et Biophysica Acta | 1981

Rat enterocyte Na+ transport in vitro. Action of parathyroid hormone and calcitonin.

Bernard Lacour; Tilman B. Drüeke; Evelyne Pierandreï; Bernadette Nabarra; Funck-Brentano Jl

Parathyroid hormone (PTH) and calcitonin exert well known effects on the renal tubule which are thought to involve specific hormone receptors and adenyl cyclase. In the intestine, it is not clear whether the action of PTH and calcitonin is only indirect or also direct, and their mechanisms of action are much less well established. In the present study, possible direct effects of PTH and calcitonin on Na+ transport in isolated intestinal epithelial cells of rats were investigated. In the presence of bovine PTH (1.2 I.U/ml) in the incubation medium, the Na+ efflux rate constant (oKNa) of isolated enterocytes was significantly reduced when compared to that in control experiments with the hormone vehicle only. The mean depression of oKNa induced by bovine PTH was 26% as compared to the control (100%) and to that induced by ouabain (4.0 mM) which was 44%. No depressant effect of bovine PTH on oKNa was observed when the isolated enterocytes were incubated with ouabain (4.0 mM). Thus, bovine PTH appeared to inhibit the ouabain-sensitive Na+ pump. When incubating the isolated epithelial cells in an EGTA-containing CA2+-free medium, bovine PTH lost its capacity to inhibit oKNa. Thus, the presence of extracellular Ca2+ appeared necessary for the inhibitory effect of bovine PTH. In contrast to its effect on oKNa, bovine PTH induced no change in net Na+ uptake by isolated enterocytes. Moreover, no significant effect on enterocyte Na+ transport could be demonstrated for salmon or porcine calcitonin at two different concentrations in the incubation medium, Neither bovine PTH nor salmon calcitonin induced significant changes in enterocyte cyclic AMP or cycle GMP concentrations. It was concluded that bovine PTH, but not calcitonin, exerted a directed inhibitory effect on the ouabain-sensitive oKNa of isolated rat enterocytes. The effect of bovine PTH occurred without measurable activation of the cyclic nucleotide system but needed the presence of Ca2+ in the incubation medium to be operative.


Asaio Journal | 1973

An approach to "middle molecules" identification in artificial kidney dialysate, with reference to neuropathy prevention.

Man Nk; Bernard Terlain; Jean Paris; Georges Werner; Sausse A; Funck-Brentano Jl


Kidney International | 1978

Experimental chronic renal failure in the rat by electrocoagulation of the renal cortex

Jane Boudet; Man Nk; Peter Pils; Sausse A; Funck-Brentano Jl


Asaio Journal | 1976

Characterization of a 1100-1300 MW uremic neurotoxin.

Funck-Brentano Jl; Man Nk; Sausse A; Zingraff J; Boudet J; Becker A; Cueille Gf


Artificial Organs | 1980

Uremic Neurotoxin in the Middle Molecular Weight Range

Man Nk; Cueille G; J. Zingraff; Boudet J; Sausse A; Funck-Brentano Jl


Kidney International | 1975

Effect of more porous dialysis membranes on neuropathic toxins.

Funck-Brentano Jl; Man Nk; Sausse A


Kidney International | 1975

Neuropathy and "middle" molecule toxins.

Funck-Brentano Jl; Man Nk; Sausse A; Cueille Gf; Zinfraff J; Drueke T; Jungers P; Billon Jp


Kidney International | 1978

A defense of the middle molecule hypothesis.

Funck-Brentano Jl; Cueille Gf; Man Nk


Artificial Organs | 1981

Characterization of sub-peak b4.2, middle molecule.

Cueille G; Man Nk; Sausse A; Farges Jp; Funck-Brentano Jl


Artificial Organs | 1981

Technical aspects on middle molecules: separation, isolation, and identification.

Cueille G; Man Nk; Sausse A; Farges Jp; Funck-Brentano Jl

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Sausse A

French Institute of Health and Medical Research

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