Abstract
Mitochondrial trifunctional protein (MTP) is a hetero-octamer of four α and four β subunits that catalyzes the final three steps of mitochondrial long chain fatty acid β-oxidation. Human MTP deficiency causes Reye-like syndrome, cardiomyopathy, or sudden unexpected death. We used gene targeting to generate an MTP α subunit null allele and to produce mice that lack MTP α and β subunits. The Mtpa–/– fetuses accumulate long chain fatty acid metabolites and have low birth weight compared with the Mtpa+/– and Mtpa+/+ littermates. Mtpa–/– mice suffer neonatal hypoglycemia and sudden death 6–36 hours after birth. Analysis of the histopathological changes in the Mtpa–/– pups revealed rapid development of hepatic steatosis after birth and, later, significant necrosis and acute degeneration of the cardiac and diaphragmatic myocytes. This mouse model documents that intact mitochondrial long chain fatty acid oxidation is essential for fetal development and for survival after birth. Deficiency of MTP causes fetal growth retardation, neonatal hypoglycemia, and sudden death.
Authors
Jamal A. Ibdah, Hyacinth Paul, Yiwen Zhao, Scott Binford, Ken Salleng, Mark Cline, Dietrich Matern, Michael J. Bennett, Piero Rinaldo, Arnold W. Strauss
Heart enzymatic activitiesA in MTP knockout mice
Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)