Literature DB >> 26621635

The c-Ring of the F1FO-ATP Synthase: Facts and Perspectives.

Salvatore Nesci1, Fabiana Trombetti1, Vittoria Ventrella1, Alessandra Pagliarani2.   

Abstract

The F1FO-ATP synthase is the only enzyme in nature endowed with bi-functional catalytic mechanism of synthesis and hydrolysis of ATP. The enzyme functions, not only confined to energy transduction, are tied to three intrinsic features of the annular arrangement of c subunits which constitutes the so-called c-ring, the core of the membrane-embedded FO domain: (i) the c-ring constitution is linked to the number of ions (H(+) or Na(+)) channeled across the membrane during the dissipation of the transmembrane electrochemical gradient, which in turn determines the species-specific bioenergetic cost of ATP, the "molecular currency unit" of energy transfer in all living beings; (ii) the c-ring is increasingly involved in the mitochondrial permeability transition, an event linked to cell death and to most mitochondrial dysfunctions; (iii) the c subunit species-specific amino acid sequence and susceptibility to post-translational modifications can address antibacterial drug design according to the model of enzyme inhibitors which target the c subunits. Therefore, the simple c-ring structure not only allows the F1FO-ATP synthase to perform the two opposite tasks of molecular machine of cell life and death, but it also amplifies the enzyme's potential role as a drug target.

Entities:  

Keywords:  Bioenergetic cost; Drug-binding region; F1FO-ATP synthase; Mitochondrial permeability transition; c-Ring, mitochondria

Mesh:

Substances:

Year:  2015        PMID: 26621635     DOI: 10.1007/s00232-015-9860-3

Source DB:  PubMed          Journal:  J Membr Biol        ISSN: 0022-2631            Impact factor:   1.843


  74 in total

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