New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling

Cardiolipin interacts with many proteins of the mitochondrial inner membrane and, together with cytochrome C and creatine kinase, activates them. It can be considered as an integrating factor for components of the mitochondrial respiratory chain, which provides for an efficient transfer of electrons...

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Main Authors: Gregory A. Shilovsky, Oleg A. Zverkov, Alexandr V. Seliverstov, Vasily V. Ashapkin, Tatyana S. Putyatina, Lev I. Rubanov, Vassily A. Lyubetsky
Format: Article
Language:English
Published: Hindawi Limited 2019-01-01
Series:Oxidative Medicine and Cellular Longevity
Online Access:http://dx.doi.org/10.1155/2019/2901057
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spelling doaj-fc0b552bc1ce4746837b7486d59831d22020-11-25T02:13:01ZengHindawi LimitedOxidative Medicine and Cellular Longevity1942-09001942-09942019-01-01201910.1155/2019/29010572901057New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin RemodelingGregory A. Shilovsky0Oleg A. Zverkov1Alexandr V. Seliverstov2Vasily V. Ashapkin3Tatyana S. Putyatina4Lev I. Rubanov5Vassily A. Lyubetsky6Institute for Information Transmission Problems of the Russian Academy of Sciences (Kharkevich Institute), 127051, RussiaInstitute for Information Transmission Problems of the Russian Academy of Sciences (Kharkevich Institute), 127051, RussiaInstitute for Information Transmission Problems of the Russian Academy of Sciences (Kharkevich Institute), 127051, RussiaBelozersky Institute of Physico-Chemical Biology, Lomonosov Moscow State University, 119991, RussiaFaculty of Biology, Lomonosov Moscow State University, 119234, RussiaInstitute for Information Transmission Problems of the Russian Academy of Sciences (Kharkevich Institute), 127051, RussiaInstitute for Information Transmission Problems of the Russian Academy of Sciences (Kharkevich Institute), 127051, RussiaCardiolipin interacts with many proteins of the mitochondrial inner membrane and, together with cytochrome C and creatine kinase, activates them. It can be considered as an integrating factor for components of the mitochondrial respiratory chain, which provides for an efficient transfer of electrons and protons. The major, if not the only, factor of cardiolipin maturation is tafazzin. Variations of isoform proportions of this enzyme can cause severe diseases such as Barth syndrome. Using bioinformatic methods, we have found conserved C-terminal regions in many tafazzin isoforms and identified new mammalian species that acquired exon 5 as well as rare occasions of intron retention between exons 8 and 9. The regions in the C-terminal part arise from frameshifts relative to the full-length TAZ transcript after skipping exon 9 or retention of the intron between exons 10 and 11. These modifications demonstrate specific distribution among the orders of mammals. The dependence of the species maximum lifespan, body weight, and mitochondrial metabolic rate on the modifications has been demonstrated. Arguably, unconventional tafazzin isoforms provide for the optimal balance between the increased biochemical activity of mitochondria (resulting from specific environmental or nutritional conditions) and lifespan maintenance; and the functional role of such isoforms is linked to the modification of the primary and secondary structures at their C-termini.http://dx.doi.org/10.1155/2019/2901057
collection DOAJ
language English
format Article
sources DOAJ
author Gregory A. Shilovsky
Oleg A. Zverkov
Alexandr V. Seliverstov
Vasily V. Ashapkin
Tatyana S. Putyatina
Lev I. Rubanov
Vassily A. Lyubetsky
spellingShingle Gregory A. Shilovsky
Oleg A. Zverkov
Alexandr V. Seliverstov
Vasily V. Ashapkin
Tatyana S. Putyatina
Lev I. Rubanov
Vassily A. Lyubetsky
New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
Oxidative Medicine and Cellular Longevity
author_facet Gregory A. Shilovsky
Oleg A. Zverkov
Alexandr V. Seliverstov
Vasily V. Ashapkin
Tatyana S. Putyatina
Lev I. Rubanov
Vassily A. Lyubetsky
author_sort Gregory A. Shilovsky
title New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
title_short New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
title_full New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
title_fullStr New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
title_full_unstemmed New C-Terminal Conserved Regions of Tafazzin, a Catalyst of Cardiolipin Remodeling
title_sort new c-terminal conserved regions of tafazzin, a catalyst of cardiolipin remodeling
publisher Hindawi Limited
series Oxidative Medicine and Cellular Longevity
issn 1942-0900
1942-0994
publishDate 2019-01-01
description Cardiolipin interacts with many proteins of the mitochondrial inner membrane and, together with cytochrome C and creatine kinase, activates them. It can be considered as an integrating factor for components of the mitochondrial respiratory chain, which provides for an efficient transfer of electrons and protons. The major, if not the only, factor of cardiolipin maturation is tafazzin. Variations of isoform proportions of this enzyme can cause severe diseases such as Barth syndrome. Using bioinformatic methods, we have found conserved C-terminal regions in many tafazzin isoforms and identified new mammalian species that acquired exon 5 as well as rare occasions of intron retention between exons 8 and 9. The regions in the C-terminal part arise from frameshifts relative to the full-length TAZ transcript after skipping exon 9 or retention of the intron between exons 10 and 11. These modifications demonstrate specific distribution among the orders of mammals. The dependence of the species maximum lifespan, body weight, and mitochondrial metabolic rate on the modifications has been demonstrated. Arguably, unconventional tafazzin isoforms provide for the optimal balance between the increased biochemical activity of mitochondria (resulting from specific environmental or nutritional conditions) and lifespan maintenance; and the functional role of such isoforms is linked to the modification of the primary and secondary structures at their C-termini.
url http://dx.doi.org/10.1155/2019/2901057
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