Functional and structural insight into properdin control of complement alternative pathway amplification.

Pedersen DV, Roumenina L, Jensen RK, Gadeberg TA, Marinozzi C, Picard C, Rybkine T, Thiel S, Sørensen UB, Stover C, Fremeaux-Bacchi V, Andersen GR, EMBO J 36(8):1084-1099 (2017) Europe PMC

SASDB69 – E244K monomeric human Properdin

E244K Human Properdin

MW^experimental	50	kDa
MW^expected	49	kDa

log I(s) 1.66×10⁴ 1.66×10³ 1.66×10² 1.66×10¹

E244K Human Properdin small angle scattering data

s, nm^-1

Log plot Log-Log plot

ln I(s)

ln 1.67×10⁴ R_g: 4.1 nm 0 (4.1 nm)^-2 s²

(sR_g)²I(s)/I(0)

1.104 0 √3 sR_g

D_max: 15 nm

Data validation

Fits and models

log I(s)	s, nm^-1
+3 Δ/σ -3	s, nm^-1

Synchrotron SAXS data from solutions of recombinantly formed monomeric human E244K properdin in 10 mM HEPES pH 7.2, 150 mM NaCl, were collected EMBL-P12 bioSAXS beam line at the PETRAIII storage ring (Hamburg, Germany) equipped with a Pilatus 2M detector (I(s) vs s, where s = 4π sin θ/λ; 2θ is the scattering angle; λ = 0.124 nm). A solute concentration of 2.7 mg/ml was measured at 20°C. 20 successive 0.05 second frames were collected. The data were normalized to the intensity of the transmitted beam and radially averaged; the scattering of the solvent-blank was subtracted and scaled for protein concentration.

E244K Human Properdin (E244K FP)
Mol. type		Protein
Organism		Homo sapiens
Olig. state		Monomer
Mon. MW		49.3 kDa

UniProt		P27918
Sequence		FASTA