Claude Feo
University of Paris-Sud
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Featured researches published by Claude Feo.
Journal of Clinical Investigation | 1981
Margaret R. Clark; Narla Mohandas; Claude Feo; Mark S. Jacobs; Stephen B. Shohet
Membrane rigidity has been widely accepted as the dominant cause of reduced deformability both of ATP-depleted erythrocytes and erythrocytes containing excess calcium (Ca). However, recent studies have shown normal membrane deformability in ATP-depleted erythrocytes. In addition, Ca accumulation causes massive ion and water loss, and it has been shown that extensive dehydration causes an increase in intracellular viscosity with attendant loss of whole cell deformability. To obtain a detailed understanding of the processes accompanying ATP depletion and/or Ca accumulation that limit cell deformability, we have used a viscodiffractometric method to identify the cellular factors contributing to reduced whole cell deformability. Analysis of the influence of the suspending medium osmolality on deformability showed the presence of two independent processes. One was a Ca-independent reduction in cell surface area/volume ratio, resulting from the spheroechinocyte formation that follows total ATP consumption. The other was a Ca-dependent increase in intracellular viscosity resulting from a Ca-induced loss of intracellular potassium and water. This deformability loss due to increased intracellular viscosity was found for cells depleted of ATP in the presence of Ca and in cells treated with Ca and A23187 without prior depletion. Ionophore-treated cells at high Ca concentration (>500 muM) formed spheroechinocytes with reduced surface area and a further loss of whole cell deformability. The rate of deformability loss associated with Ca-induced spheroechinocytosis was much more rapid than that associated with ATP-depletion-induced spheroechinocytosis, suggesting different mechanisms for the morphologic changes. No major effects of altered membrane elasticity on the reduced deformability of either ATP-depleted or Ca-loaded cells were observed.
Journal of Clinical Investigation | 1990
William T. Tse; Marie Christine Lecomte; Fernando Costa; Michel Garbarz; Claude Feo; Pierre Boivin; Didier Dhermy; Bernard G. Forget
Blood | 1990
Michel Garbarz; Marie-Christine Lecomte; Claude Feo; Isabelle Devaux; Christiane Picat; C Lefebvre; F Galibert; Huguette Gautero; Odile Bournier; Colette Galand
Journal of Clinical Investigation | 1982
Didier Dhermy; Marie Christine Lecomte; Michel Garbarz; O Bournier; C Galand; H Gautero; Claude Feo; Nicole Alloisio; Jean Delaunay; Pierre Boivin
Blood | 1985
Marie-Christine Lecomte; Didier Dhermy; C Solis; A Ester; Claude Feo; Huguette Gautero; Odile Bournier; Pierre Boivin
Blood | 1989
Marie-Christine Lecomte; Michel Garbarz; Bernard Grandchamp; Claude Feo; Huguette Gautero; Isabelle Devaux; Odile Bournier; Colette Galand; L d'Auriol; F Galibert
Blood | 1987
Brigitte Pothier; L Morle; Nicole Alloisio; M. T. Ducluzeau; Caldani C; Claude Feo; Michel Garbarz; Isabelle Chaveroche; Didier Dhermy; Marie Christine Lecomte
Blood | 1986
Michel Garbarz; Marie Christine Lecomte; Didier Dhermy; Claude Feo; Isabelle Chaveroche; Huguette Gautero; Odile Bournier; Christiane Picat; Anne Goepp; Pierre Boivin
Blood | 1984
Michel Garbarz; Didier Dhermy; Marie-Christine Lecomte; Claude Feo; Isabelle Chaveroche; Colette Galand; Odile Bournier; Olivier Bertrand; Pierre Boivin
Archive | 1990
William T. Tse; Mane-Christine Lecomte; Fernando Ferreira Costa; Michel Garbarz; Claude Feo; Pierre Boivin; Didier Dhermy; Bernard G. Forget