Literature DB >> 7472652

Dietary methionine does not reduce penetrance in curly tail mice but causes a phenotype-specific decrease in embryonic growth.

H W van Straaten1, H Blom, M C Peeters, A M Rousseau, K J Cole, M J Seller.   

Abstract

The mouse mutation, curly tail, has incomplete penetrance and variable expression. Approximately 60% of the mice have a curly tail (CT), from which up to 20% may have lumbosacral spina bifida. Approximately 40% are normal, with a straight tail (ST). We tested whether L-methionine, which reduces the penetrance of neural tube defects in the Axd mouse mutant, has beneficial effects in the curly tail mutant. A single injection of L-methionine (200-1600 mg/kg body wt) on d 9 of pregnancy had no effect on the embryos, whereas there was a minor increase in penetrance at the highest dose. Chronic supplementation of L-methionine via the drinking water (1554 mg.kg body wt-1.d-1) did not shift penetrance. However, it decreased the weight of d 13 embryos from ST dams but not of those from CT dams. This phenotype-specific difference in response was evident and most unexpected. Mice from curly tail and other inbred strains were subjected to an L-methionine loading test and serum homocysteine assay. The different strains varied in their basal serum homocysteine concentrations, and they had proportionate significant increases after L-methionine loading. In CT and ST mice, basal serum homocysteine concentrations as well as the levels after loading were similar to each other and intermediate in the range of the mice tested. We conclude that L-methionine does not reduce penetrance in the curly tail mouse and that this strain reflects no derangement in L-methionine handling.

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Year:  1995        PMID: 7472652     DOI: 10.1093/jn/125.11.2733

Source DB:  PubMed          Journal:  J Nutr        ISSN: 0022-3166            Impact factor:   4.798


  3 in total

Review 1.  Curly tail: a 50-year history of the mouse spina bifida model.

Authors:  H W van Straaten; A J Copp
Journal:  Anat Embryol (Berl)       Date:  2001-04

2.  Over-expression of Grhl2 causes spina bifida in the Axial defects mutant mouse.

Authors:  Madeleine R Brouns; Sandra C P De Castro; Els A Terwindt-Rouwenhorst; Valentina Massa; Johan W Hekking; Caroline S Hirst; Dawn Savery; Chantal Munts; Darren Partridge; Wout Lamers; Eleonore Köhler; Henny W van Straaten; Andrew J Copp; Nicholas D E Greene
Journal:  Hum Mol Genet       Date:  2011-01-24       Impact factor: 6.150

3.  Dietary methionine effects on plasma homocysteine and HDL metabolism in mice.

Authors:  Wanda Velez-Carrasco; Martin Merkel; Christian O Twiss; Jonathan D Smith
Journal:  J Nutr Biochem       Date:  2007-08-17       Impact factor: 6.048

  3 in total

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