Structural basis for trypanosomal haem acquisition and susceptibility to the host innate immune system

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Abstract

Sleeping sickness is caused by trypanosome parasites, which infect humans and livestock in Sub-Saharan Africa. Haem is an important growth factor for the parasites and is acquired from the host by receptor-mediated uptake of haptoglobin (Hp)-haemoglobin (Hb) complexes. The parasite Hp-Hb receptor (HpHbR) is also a target for a specialized innate immune defence executed by trypanosome-killing lipoprotein particles containing an Hp-related protein in complex with Hb. Here we report the structure of the multimeric complex between human Hp-Hb and Trypanosoma brucei brucei HpHbR. Two receptors forming kinked three-helical rods with small head regions bind to Hp and the 2-subunits of Hb (2Hb),with one receptor at each end of the dimeric Hp-Hb complex.The Hb 2-subunit haem group directly associates with the receptors, which allows for sensing of haem-containing Hp-Hb.The HpHbR-binding region of Hp is conserved in Hp-related protein, indicating an identical recognition of Hp-Hb and trypanolytic particles by HpHbR in human plasma

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Stødkilde, K., Torvund-Jensen, M., Moestrup, S. K., & Andersen, C. B. F. (2014). Structural basis for trypanosomal haem acquisition and susceptibility to the host innate immune system. Nature Communications, 5. https://doi.org/10.1038/ncomms6487

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