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The Cellular Approach to the Determination of Pyridoxine Requirements in Pregnant and Nonpregnant Rats1,2,

Judy A. Driskell3 and Avanelle Kirksey

Department of Foods and Nutrition, Purdue University, Lafayette, Indiana 47907

The cellular approach was used in evaluating the pyridoxine requirements of pregnant and nonpregnant rats. A plateau in hepatic DNA and RNA concentrations occurred at the 10 µg level of pyridoxine intake in nonpregnant animals. The DNA concentration of maternal and fetal livers also plateaued at the 10 µg level, whereas the DNA content of fetal brain did not plateau until 15 µg. RNA concentrations in fetal and maternal liver also plateaued at the 15 µg level. Hepatic polysomal activity maximized in animals fed the 10 µg level of pyridoxine; however, fetal brain ribosomal activity did not plateau until the level of intake was 20 µg. Total protein content was related to polysomal and ribosomal activities; a plateau in protein content in maternal and fetal liver occurred at the 15 µg level of pyridoxine intake and in fetal brain at 20 µg. Among the measurements used, alanine aminotransferase activities, protein and RNA content, and polysomal activities had the highest correlations with the level of pyridoxine intake. On the basis of these parameters, the pyridoxine requirement for nonpregnant rats appeared to be between 10 and 15 µg daily and between 15 and 20 µg for pregnant animals.


1 Journal Paper no. 4125 of the Purdue University Agricultural Experiment Station. Supported in part by The Nutrition Foundation and by an NDEA Title IV Fellowship.

2 These data were presented in part at the meeting of the American Institute of Nutrition, Atlantic City, New Jersey, April 1970, (Federation Proc. 29: 823 (abstr.)).

3 Present address: Department of Nutrition and Foods, Auburn University, Auburn, Ala.

Manuscript received 27 July 1970.





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