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Department of Animal Sciences and Nutrition Program, Washington State University, Pullman, WA 99164-6320
The flux of energy-yielding compounds through the pathways of lipogenesis, esterification into triglycerides and lipolysis in adipose tissue plays a pivotal role in supplying the demands of lactation and maternal health. The critical importance of these pathways is demonstrated by the number of highly coordinated and redundant metabolic control elements that regulate the enzyme activity in these pathways, including protein and several steroid hormones, catecholamines, and blood concentrations of several nutrients. Control on these pathways is exerted by all of these elements during lactation. Insights have been gained recently into the adaptations of these pathway reactions due to genetic propensity for milk production, stage of lactation, and intake of energy-yielding components such as starch, cellulose and triglycerides. The rates of these pathways vary exponentially with the intakes of key substrates and demands for milk precursors. The parameters of equations describing these pathways are not constant, but vary with genotype and with prolonged changes in nutritional and environmental conditions. Two major regulatory systems are critical to alterations of carbon flux during the entire lactational period. One is the interaction of growth hormone and insulin to control lipogenesis; the other is the counter-regulation by norepinephrine and insulin on cyclic AMP-initiated enzyme phosphorylation to regulate lipolysis. Examples of specific control points having a critical impact on lactational success and that are associated with genetic selection for milk production are the activities of acetyl-CoA carboxylase and hormone sensitive lipase. Further insights into the mechanisms of these adaptations will help us to improve the efficiency of metabolic flux during lactation. However, the complexity of the chemical interconversions of nutrients and of their regulation during lactation requires a coordinated effort to study both physiological control mechanisms and to improve our quantitative understanding of key parameters of lipid metabolism as influenced by a variety of genetic and environmental situations.
KEY WORDS: • lactation • metabolic control systems • lipid metabolism • adipose • lipolysis
1 Paper no. 8074, College of Agriculture and Home Economics Research Center, Washington State University, Pullman, Project Number 0663, CSRS Regional Project no. NC185 and W181. Supported in part by a grant (HD24529) from the National Institutes of Health.
2 Presented as part of the 34th Annual Ruminant Nutrition Conference: Regulating Lipid Metabolism to Increase Productive Efficiency, given at the 78th Annual Meeting of the Federation of American Societies for Experimental Biology, New Orleans, LA, March 28, 1993. This conference was sponsored by the American Institute of Nutrition and was supported by grants from Agway Inc.; Cargill, Nutrena Feed Division; Carolina By-Products, Inc., Church & Dwight Co. Inc.; Farmland Industries, Inc.; Hoffman La Roche, Inc.; Eli Lilly and Company, Inc.; Merck, Inc.; Purina Mills Inc.; Rhone-Poulenc Animal Nutrition; SmithKline Beecham Animal Health; Syntex Research; and The Upjohn Company. Guest editor for this symposium was Carl L. Davis, professor emeritus, Department of Animal and Dairy Sciences, University of Illinois, Urbana, IL 61801.
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  J. M. Sumner and J. P. McNamara Expression of Lipolytic Genes in the Adipose Tissue of Pregnant and Lactating Holstein Dairy Cattle J Dairy Sci, November 1, 2007; 90(11): 5237 - 5246. [Abstract] [Full Text] [PDF]
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