| Literature DB >> 27170716 |
Jorge Morales1, Muneaki Hashimoto1, Tom A Williams2, Hiroko Hirawake-Mogi1, Takashi Makiuchi1, Akiko Tsubouchi1, Naoko Kaga3, Hikari Taka3, Tsutomu Fujimura3, Masato Koike4, Toshihiro Mita1, Frédéric Bringaud5, Juan L Concepción6, Tetsuo Hashimoto7, T Martin Embley8, Takeshi Nara9.
Abstract
The remodelling of organelle function is increasingly appreciated as a central driver of eukaryotic biodiversity and evolution. Kinetoplastids including Trypanosoma and Leishmania have evolved specialized peroxisomes, called glycosomes. Glycosomes uniquely contain a glycolytic pathway as well as other enzymes, which underpin the physiological flexibility of these major human pathogens. The sister group of kinetoplastids are the diplonemids, which are among the most abundant eukaryotes in marine plankton. Here we demonstrate the compartmentalization of gluconeogenesis, or glycolysis in reverse, in the peroxisomes of the free-living marine diplonemid, Diplonema papillatum Our results suggest that peroxisome modification was already under way in the common ancestor of kinetoplastids and diplonemids, and raise the possibility that the central importance of gluconeogenesis to carbon metabolism in the heterotrophic free-living ancestor may have been an important selective driver. Our data indicate that peroxisome modification is not confined to the kinetoplastid lineage, but has also been a factor in the success of their free-living euglenozoan relatives.Entities:
Keywords: diplonemids; glycolysis; kinetoplastids; metabolic compartmentalization; organelle evolution; peroxisomes
Mesh:
Substances:
Year: 2016 PMID: 27170716 PMCID: PMC4874719 DOI: 10.1098/rspb.2016.0520
Source DB: PubMed Journal: Proc Biol Sci ISSN: 0962-8452 Impact factor: 5.349