Aspartate Aminotransferase in Synaptic and Nonsynaptic Mitochondria: Differential Effect of Compounds That Influence Transient Hetero-enzyme Complex (metabolon) Formation

Overview

Journal Neurochem Int

Specialties Chemistry
Neurology

Date 2006 Mar 4

PMID 16513215

Citations 19

Authors

Mary C McKenna

Irene B Hopkins

Steven L Lindauer

Penelope Bamford

Affiliations

Soon will be listed here.

Abstract

The enzyme aspartate aminotransferase (AAT) has a number of key roles in astrocytes and neurons in brain. An understanding of the regulation of AAT is important since AAT is involved in many aspects of glutamate metabolism including the synthesis of neurotransmitter glutamate. Mitochondrial AAT binds to a protein and lipids on the inner mitochondrial membrane and also forms a number of transient hetero-enzyme complexes with other enzymes. These complexes serve to facilitate metabolism by essentially channeling substrates and cofactors to other enzymes within the complex. The association and dissociation of transiently formed hetero-enzyme complexes may modulate enzyme activity in "real time" since these complexes are dynamically influenced by changes in the concentration of a number of key metabolites. The influence of several effectors that modulate AAT activity, either directly, or by altering the binding of AAT to mitochondrial lipids, or the association/dissociation into transient hetero-enzyme complexes was determined. The addition of palmitate, malate, citrate, glutamate, bovine serum albumin and Mg(2+) modulated AAT activity differently in synaptic and nonsynaptic mitochondria from brain. These findings suggest that AAT activity and also glutamate metabolism, may be regulated in part, by metabolites that influence binding of the enzyme to lipids or proteins in the inner mitochondrial membrane and/or the association/dissociation of transient hetero-enzyme complexes. This may have a role in the compartmentation of glutamate metabolism in brain.

Citing Articles

In the Brain, It Is Not All about Sugar.

Antunes B, Mateus T, Morais V NeuroSci. 2024; 5(2):209-221.

PMID: 39483499 PMC: 11493208. DOI: 10.3390/neurosci5020016.

Revealing the contribution of astrocytes to glutamatergic neuronal transmission.

Cuellar-Santoyo A, Ruiz-Rodriguez V, Mares-Barbosa T, Patron-Soberano A, Howe A, Portales-Perez D Front Cell Neurosci. 2023; 16:1037641.

PMID: 36744061 PMC: 9893894. DOI: 10.3389/fncel.2022.1037641.

Hormone-Glutamine Metabolism: A Critical Regulatory Axis in Endocrine-Related Cancers.

Xu F, Shi J, Qin X, Zheng Z, Chen M, Lin Z Int J Mol Sci. 2022; 23(17).

PMID: 36077501 PMC: 9456462. DOI: 10.3390/ijms231710086.

Neurometabolite Levels and Relevance to Central Sensitization in Chronic Orofacial Pain Patients: A Magnetic Resonance Spectroscopy Study.

Terumitsu M, Takado Y, Fukuda K, Kato E, Tanaka S J Pain Res. 2022; 15:1421-1432.

PMID: 35599974 PMC: 9122062. DOI: 10.2147/JPR.S362793.

Novel Probable Glance at Inflammatory Scenario Development in Autistic Pathology.

Harutyunyan A, Harutyunyan H, Yenkoyan K Front Psychiatry. 2022; 12:788779.

PMID: 35002805 PMC: 8727757. DOI: 10.3389/fpsyt.2021.788779.