Docosahexaenoate is usually considered to be the principal endpoint of α-linolenate metabolism in mammals. Nevertheless, several studies over the past 30 y have shown that more carbon from α-linolenate is recycled into newly synthesized lipids than is used to make docosahexaenoate. Our objective in this study was to assess carbon recycling from α-linolenate in suckling rats made deficient in n-3 polyunsaturated fatty acids (PUFA). Female Long-Evans rats were given a diet deficient in n-3 PUFA at weaning and then bred 8 wk later. Pups from the second generation were nursed by their respective dams and gavaged with 1 mg [U-13C]-α-linolenate at 10 d old. Brain and liver were obtained 24 h later, and the fatty acid profiles and 13C enrichment analyzed. Docosahexaenoate was markedly depleted in brain (-82%) and liver (-97%) of the n-3 PUFA-deficient rats. In the controls, 13C enrichment in products of carbon recycling (cholesterol and fatty acids other than n-3 PUFA) exceeded that in docosahexaenoate by 2.4-fold (river) and 7.5-fold (brain). n-3 PUFA deficiency reduced the ratio of 13C enrichment in products of carbon recycling compared with 13C incorporated into docosahexaenoate by 63% in the brain but not in the liver. Despite severe n-3 PUFA deficiency, carbon recycling still consumed 50% more 13C from α-linolenate than went into docosahexaenoate in the liver and 2.8-fold more in the brain. We conclude that carbon recycling is an integral part of neonatal metabolism of α-linolenate and is not simply an overflow pathway arising from excess availability of preformed docosahexaenoate. Copyright © 2005 International Pediatric Research Foundation, Inc.
CITATION STYLE
Cunnane, S. C., Ryan, M. A., Yu, H. L., Lim, S. Y., & Salem, N. (2006). Suckling rats actively recycle carbon from α-linolenate into newly synthesized lipids even during extreme dietary deficiency of n-3 polyunsaturates. Pediatric Research, 59(1), 107–110. https://doi.org/10.1203/01.pdr.0000190569.07991.ed
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