In Vivo Fates of Degradable Poly(β-Malic Acid) and of its Precursor, Malic Acid

Author:

Domurado Dominique1,Fournié Philippe1,Braud Christian1,Vert Michel1,Guérin Philippe2,Simonnet Françoise3

Affiliation:

1. Centre de Recherche sur les Biopolymères Artificiels UMR 5473 CNRS, INSERM Faculty of Pharmacy 15 avenue Charles Flahault, BP 14491, 34093 Montpellier cedex 5, France

2. LRP UMR C7581 CNRS 2-8 rue Henry Dunant 94320 Thiais, France

3. Laboratoire de Radiobiologie Institut National des Sciences et Techniques Nucléaires BP 6, 91190 Gif-sur-Yvette, France

Abstract

To determine whether degradation could influence the in vivo elimination pattern of poly(β-malic acid) in mice, radioactive urinary excretion and 14CO2 expiration were studied after intravenous injection of 14C-radiolabeled poly(β-malic acid) and of its precursor, 14C-malate. The precursor administration led to rapid 14CO2 exhalation, and only negligible urinary elimination. The reverse was observed for the polymer. It was concluded that: (i) the in vivo degradation of poly(β-malic acid) chains, if any during the 24-h period of the study, did not release detectable malate molecules, (ii) the large urinary excretion of poly(β-malic acid) was due to the molar masses being less than the renal filtration threshold, (iii) the degradation of the poly(β-malic acid) chains in blood was slow enough to allow the fraction with higher molar masses to enter the interstitial space of the tissues, and possibly cells.

Publisher

SAGE Publications

Subject

Materials Chemistry,Polymers and Plastics,Biomaterials,Bioengineering

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