Literature DB >> 4073566

Mitochondrial alterations in embryos exposed to B-hydroxybutyrate in whole embryo culture.

W E Horton, T W Sadler.   

Abstract

The ketone body B-hydroxybutyrate (B-OHB) produces malformations and ultrastructural alterations in mitochondria of mouse embryos exposed for 24 hours to the compound in whole embryo culture. The present study was conducted to establish the time-course of the mitochondrial changes to determine whether the changes are reversible, and to relate these changes to the malformations produced by the compound. Since mitochondria also play a key role in the metabolism of ketone bodies, the capacity of the early somite embryo to metabolize B-OHB was investigated in an effort to link the morphological alterations in the mitochondria to a biochemical process. Early somite embryos were cultured 4, 8, or 24 hours in the presence of 32 mM DL-B-OHB and then cultured for an additional 24 hours in control serum. Finally, embryonic tissue during the teratogenic period was assessed for its capability to oxidize B-OHB using D-(3-14C)-B-OHB. The treated embryos showed progressive alterations in the mitochondria, beginning at 4 hours with a loss of matrix density and culminating at 24 hours with high-amplitude swelling, complete loss of matrix density, and disappearance of cristae. These alterations were reversible following removal of the embryos after 24 hours of exposure to B-OHB and culturing for an additional 24 hours in control serum. Metabolism studies demonstrated that the early somite embryo possesses a limited capacity to oxidatively metabolize B-OHB. The biochemical implications of these findings are discussed with respect to the possible role of ketone bodies in the mechanism of diabetes-induced congenital malformations.

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Year:  1985        PMID: 4073566     DOI: 10.1002/ar.1092130113

Source DB:  PubMed          Journal:  Anat Rec        ISSN: 0003-276X


  4 in total

Review 1.  Congenital malformations in offspring of diabetic mothers--animal and human studies.

Authors:  Ulf J Eriksson; Jonas Cederberg; Parri Wentzel
Journal:  Rev Endocr Metab Disord       Date:  2003-03       Impact factor: 6.514

2.  Recovery by mouse embryos following teratogenic exposure to ketosis.

Authors:  L Shum; T W Sadler
Journal:  Diabetologia       Date:  1991-05       Impact factor: 10.122

3.  Effects of oxygen concentration on embryonic development in rats: a light and electron microscopic study using whole-embryo culture techniques.

Authors:  A Miki; E Fujimoto; T Ohsaki; H Mizoguti
Journal:  Anat Embryol (Berl)       Date:  1988

Review 4.  The status of diabetic embryopathy.

Authors:  Ulf J Eriksson; Parri Wentzel
Journal:  Ups J Med Sci       Date:  2016-04-27       Impact factor: 2.384

  4 in total

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