G-Quadruplex Binding of an NIR Emitting Osmium Polypyridyl Probe Revealed by Solution NMR and Time-Resolved Infrared Studies.

G-quadruplexes are emerging targets in cancer research and understanding how diagnostic probes bind to DNA G-quadruplexes in solution is critical to the development of new molecular tools. In this study the binding of an enantiopure NIR emitting [Os(TAP)2 (dppz)]2+ complex to different G-quadruplex structures formed by human telomer (hTel) and cMYC sequences in solution is reported. The combination of NMR and time-resolved infrared spectroscopic techniques reveals the sensitivity of the emission response to subtle changes in the binding environment of the complex. Similar behaviour is also observed for the related complex [Os(TAP)2 (dppp2)]2+ upon quadruplex binding.

c-kit2 G-quadruplex stabilized via a covalent probe: exploring G-quartet asymmetry.

Several sequences forming G-quadruplex are highly conserved in regulatory regions of genomes of different organisms and affect various biological processes like gene expression. Diverse G-quadruplex properties can be modulated via their interaction with small polyaromatic molecules such as pyrene. To investigate how pyrene interacts with G-rich DNAs, we incorporated deoxyuridine nucleotide(s) with a covalently attached pyrene moiety (Upy) into a model system that forms parallel G-quadruplex structures. We individually substituted terminal positions and positions in the pentaloop of the c-kit2 sequence originating from the KIT proto-oncogene with Upy and performed a detailed NMR structural study accompanied with molecular dynamic simulations. Our results showed that incorporation into the pentaloop leads to structural polymorphism and in some cases also thermal destabilization. In contrast, terminal positions were found to cause a substantial thermodynamic stabilization while preserving topology of the parent c-kit2 G-quadruplex. Thermodynamic stabilization results from π-π stacking between the polyaromatic core of the pyrene moiety and guanine nucleotides of outer G-quartets. Thanks to the prevalent overall conformation, our structures mimic the G-quadruplex found in human KIT proto-oncogene and could potentially have antiproliferative effects on cancer cells.

The use of Pantherpix pixel detector in radiotherapy QA.

There are various different detectors, which can be used for radiotherapy measurements, and more are about to be adopted. Hybrid pixel detectors (HPD) have been originally developed for the high energy physics. However, over the last few years they also expanded in the medical physics. Novel 2D detector Pantherpix is a HPD designed specifically for the radiotherapy. In this article, its properties are characterised and an assessment of its use in radiotherapy photon beams is provided. Properties such as response stability, response linearity, angular dependence and energy dependence were studied. In order to prove sufficient clinical quality for relative dosimetry, further measurements were undertaken (i.e. dose profiles and collimator scatter factors). Acquired results were compared with ion chamber and gafchromic film results. Namely the applicability of PhPix for cobalt beam therapy, which is still widely used (and will be used in near future) in economically less developed countries, is considered.