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Literature DB >> 7925850

Inhibition of glucose transport in human erythrocytes by 2,3-dioxoindole (isatin).

M L Gargari¹, R C Bansal, K Singh, A Mahmood.

Abstract

10 mM isatin (2,3-dioxoindole) inhibited glucose influx into human erythrocytes by over 30%. The inhibition is of the competitive type, where the affinity constant (Kt) was increased from 5.71 (control) to 11.11 mM in the presence of isatin with no change in Vmax (130 nmol/min/ml packed cells). The observed inhibition of sugar transport by isatin was not mediated through membrane -SH groups accessible to iodoacetate, iodoacetamide, DTNB, DNP or sodium arsenite. Isatin inhibited sugar transport in the presence of 2 mM harmaline, an alkaloid inhibitor of Na+, K(+)-ATPase activity. The inhibition was non additive which suggests that these two compounds interact with the same or a similar site on the erythrocyte membrane.

Entities: Chemical Species

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Year: 1994 PMID： 7925850 DOI： 10.1007/bf01956465

Source DB: PubMed Journal: Experientia ISSN： 0014-4754

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References

11 in total

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Authors: R Bloch
Journal: J Biol Chem Date: 1974-03-25 Impact factor: 5.157

Inhibition of glucose transport in human erythrocytes by 2,3-dioxoindole (isatin).

Review 1. Isatin--a new biological factor.

2. Symbiotic marine bacteria chemically defend crustacean embryos from a pathogenic fungus.

3. Harmaline: a competitive inhibitor of Na ion in the (Na+ + K+)-ATPase system.

4. Human erythrocyte sugar transport. Identification of the essential residues of the sugar carrier by specific modification.

5. Isatin: an inhibitor of sodium-dependent D-glucose uptake in rat intestine.

6. Harmaline interaction with sodium-binding sites in intestinal brush border sucrase.

7. Inhibition of D-glucose uptake by isatin in rat intestine: effect of harmaline and various sulfhydryl reagents.

8. The kinetics of glucose transport in human red blood cells.

9. Asymmetric binding of steroids to internal and external sites in the glucose carrier of erythrocytes.

10. Isatin: identity with the purified endogenous monoamine oxidase inhibitor tribulin.