Subcellular localization of glyoxylate cycle key enzymes involved in oxalate biosynthesis of wood-destroying basidiomycete Fomitopsis palustris grown on glucose

Author:

Sakai Shunsuke1,Nishide Tatsunori1,Munir Erman2,Baba Kei'ichi1,Inui Hiroshi3,Nakano Yoshihisa3,Hattori Takefumi1,Shimada Mikio1

Affiliation:

1. Research Institute for Sustainable Humanosphere, Kyoto University, Uji, Kyoto 611-0011, Japan

2. University of North Sumatra, Jl. Bioteknologi No. 1 Kampus USU, Medan 20513, Indonesia

3. Department of Applied Biological Chemistry, University of Osaka Prefecture, Sakai, Osaka 599-8231, Japan

Abstract

This study investigated the subcellular localization of key enzymes of the glyoxylate cycle, i.e. isocitrate lyase (ICL; EC 4.1.3.1) and malate synthase (EC 2.3.3.9), that function constitutively in coordination with oxalate biosynthesis of glucose-grownFomitopsis palustris. The ICL purified previously fromF. palustrisis termed FPICL1. Subcellular fractionation analysis of the cell homogenate by the sucrose density-gradient method showed that both key enzymes were present in peroxisomes, whereas acetyl-CoA synthase (EC 6.2.1.1) and oxalate-producing oxaloacetate acetylhydrolase (EC 3.7.1.1) were cytosolic. The peroxisomal localization of FPICL1 was further confirmed by electron microscopic and immunocytochemical analysis with anti-FPICL1 antibody. In addition, the peroxisomal target signal, composed of SKL at the C terminus of the cDNA encoding FPICL1, was found, which also suggests that FPICL1 is peroxisomal. Accordingly, it is postulated that transportation of succinate from peroxisomes to mitochondria, and vice versa, for the transportation of isocitrate or citrate, occurs in glucose-grownF. palustrisfor the constitutive metabolic coordination of the TCA and glyoxylate cycles with oxalate biosynthesis.

Publisher

Microbiology Society

Subject

Microbiology

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