Optical and Structural Characterization of a Chronic Myeloid Leukemia DNA Biosensor.

Cordeiro M, Otrelo-Cardoso AR, Svergun DI, Konarev PV, Lima JC, Santos-Silva T, Baptista PV, ACS Chem Biol 13(5):1235-1242 (2018) Europe PMC

SASDCG5 – Light encoded DNA biosensor: e13C DNA

e13C

MW^I(0)	7	kDa
MW^expected	6	kDa
V^Porod	8	nm³

log I(s) 1.06×10¹ 1.06×10⁰ 1.06×10^-1 1.06×10^-2

s, nm^-1

Log plot Log-Log plot

ln I(s)

ln 1.07×10¹ R_g: 1.3 nm 0 (1.3 nm)^-2 s²

(sR_g)²I(s)/I(0)

1.104 0 √3 sR_g

p(r)	R_g: 1.3 nm 0 D_max: 5 nm

Data validation

Experimental data range

p(r) fit to data

Metric

Value

s_min D_max / π

0.6

N_Shannon

Worse

Better

Metric

Value

p_cormap

χ²

0.851
0.833

Worse

Better

Fits and models

log I(s)	s, nm^-1
+3 Δ/σ -3	s, nm^-1

Synchrotron SAXS data from solutions of Light encoded DNA biosensor: e13C DNA in 154 mM NaCl, pH 8.3 were collected at the BM29 beam line at the ESRF (Grenoble, France) using a Pilatus 1M detector at a sample-detector distance of 3 m and at a wavelength of λ = 0.1 nm (I(s) vs s, where s = 4πsinθ/λ and 2θ is the scattering angle). Solute concentrations ranging between 0.3 and 2 mg/ml were measured at 5°C. 20 successive 0.050 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 the different curves were scaled for protein concentration. The low angle data collected at lower concentration were merged with the highest concentration high angle data to yield the final composite scattering curve. The model depicts the averaged spatial representation of the DNA (DAMFILT occupancy and volume-corrected bead model).

e13C
Mol. type		DNA
Olig. state		Monomer
Mon. MW		6.2 kDa
Sequence		FASTA