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Literature DB >> 7957445

In vivo distribution of ferric-ATP complex.

Abstract

At physiological pH, ferric-ATP complex presents ionic characteristics unlike those of ferric lactate. Its rapid diffusion into the tissues, and its reactivity which is not impaired by polymerization seem responsible for its toxicity. In comparison with ferric lactate, after parenteral administration there is a much higher spleen, lung, kidney and bone accumulation. After oral administration, on the other hand, the values are lower. ATP hydrolysis by the stomach's pH, and the subsequent iron insolubilization as phosphate could be the reason for this behaviour.

Entities: Chemical Disease

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Year: 1994 PMID： 7957445 DOI： 10.1007/BF03188815

Source DB: PubMed Journal: Eur J Drug Metab Pharmacokinet ISSN： 0378-7966 Impact factor: 2.441

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References

8 in total

In vivo distribution of ferric-ATP complex.

1. Soft tissue calcification induced by iron complexes.

2. Changes in calcium uptake by liver induced by ferric lactate.

3. Iron bound to low MW ligands: interactions with mitochondria and cytosolic proteins.

4. Low-Mr iron isolated from guinea pig reticulocytes as AMP-Fe and ATP-Fe complexes.

5. Effects of Fe(3+)-tumor cell interaction on Ca(2+)-uptake by Ehrlich ascites tumor cells.

6. Effects of complexed iron and aluminium on brain calcium.

7. In vivo behaviour of low molecular weight iron complexes.

8. Early events in guinea pig reticulocyte iron uptake.