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Orally administered [14C]DPA and [14C]DHA are metabolised differently to [14C]EPA in rats

journal contribution
posted on 2024-11-01, 11:47 authored by Gunveen Kaur, Juan Carlos Molero - Navajas, Harrison S. Weisinger, Andrew Sinclair
Previous studies have revealed that C20 PUFA are significantly less oxidised to CO2 in whole-body studies compared with SFA, MUFA and C18 PUFA. The present study determined the extent to which three long-chain PUFA, namely 20 : 5n-3 EPA, 22 : 5n-3 docosapentaenoic acid (DPA) and 22 : 6n-3 DHA, were catabolised to CO2 or, conversely, incorporated into tissue lipids. Rats were administered a single oral dose of 2·5 µCi [1-14C]DPA, [1-14C]EPA, [1-14C]DHA or [1-14C]oleic acid (18 : 1n-9; OA), and were placed in a metabolism chamber for 6 h where exhaled 14CO2 was trapped and counted for radioactivity. Rats were euthanised after 24 h and tissues were removed for analysis of radioactivity in tissue lipids. The results showed that DPA and DHA were catabolised to CO2 significantly less compared with EPA and OA (P < 0·05). The phospholipid (PL) fraction was the most labelled for all three n-3 PUFA compared with OA in all tissues, and there was no difference between C20 and C22 n-3 PUFA in the proportion of label in the PL fraction. The DHA and DPA groups showed significantly more label than the EPA group in both skeletal muscle and heart. In the brain and heart tissue, there was significantly less label in the cholesterol fraction from the C22 n-3 PUFA group compared with the C20 n-3 PUFA group. The higher incorporation of DHA and DPA into the heart and skeletal muscle, compared with EPA, suggests that these C22 n-3 PUFA might play an important role in these tissues.

History

Related Materials

  1. 1.
    DOI - Is published in 10.1017/S0007114512001419
  2. 2.
    ISSN - Is published in 00071145

Journal

British Journal of Nutrition

Start page

1

End page

8

Total pages

8

Publisher

Cambridge University Press

Place published

United Kingdom

Language

English

Copyright

© The Authors 2012, Cambridge University Press

Former Identifier

2006032532

Esploro creation date

2020-06-22

Fedora creation date

2013-02-11

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