Crystal structure and interaction studies of human DHTKD1 provide insight into a mitochondrial megacomplex in lysine catabolism

Bezerra, G.A.; Foster, W.R.; Bailey, H.J.; Hicks, K.G.; Sauer, S.W.; Dimitrov, B.; McCorvie, T.J.; Okun, J.G.; Rutter, J.; Koelker, S.; Yue, W.W.

doi:10.1107/S205225252000696X

Figure 1
Overall structure of hDHTKD1. (a) A schematic of hDHTKD1 domain organization, indicating disease-causing missense mutations with arrows. (b) Structure of the hDHTKD1 homodimer, where one subunit is coloured according to the domain organization from panel (a) and the other subunit is coloured grey. ThDP co-factors and Mg²⁺ ions are shown as sticks and spheres, respectively. (c) Sites of missense mutations are shown as black spheres on one hDHTKD1 protomer [same view as panel (b)]. (d) Structural superposition of hDHTKD1, ecOGDH (PDB code 2jgd) and msOGDH (PDB code 6r2b; Wagner et al., 2019

) highlighting their different inter-domain linkers (coloured purple, blue and light brown, respectively). (e) A magnified view of the dotted box in panel (d), showing how the hDHTKD1 inter-domain linker (purple) packs against two loop regions (black). Binding positions for the allosteric effectors AMP in the ecOGDH structure (PDB code 2jgd) and acetyl-CoA in the msOGDH structure (PDB code 2y0p; Wagner et al., 2011

) are shown as blue and brown meshes, respectively. (f) Overall architectures of the hDHTKD1 homodimer (left), the human (PDHA–PDHB)₂ heterotetramer (middle, PDB code 1ni4; Ciszak et al., 2003

) and the human (BCKDHA–BCKDHB)₂ heterotetramer (right, PDB code 1dtw; Ævarsson et al., 2000

) are shown. hDHTKD1 homodimer has a larger volume because of the insertions coloured red.

IUCrJ

Volume 7| Part 4| July 2020| Pages 693-706

ISSN: 2052-2525

https://doi.org/10.1107/S205225252000696X

BIOLOGY | MEDICINE

Open

access

Search IUCr Journals		doi		Advanced search
Author		volume	page