A simple schematic on parallel optical detection of two-fluorophore barcode for single-molecule nanopore sensing is presented. The chosen two fluorophores, ATTO-532 and DY-521-XL, emitting in well-separated spectrum range can be excited at the same wavelength. A beam splitter was employed to separate signals from the two fluorophores and guide them to the same CCD camera. Based on a conventional microscope, sources of background in the nanopore sensing system, including membranes, compounds in buffer solution, and a detection cell was characterized. By photoluminescence excitation measurements, it turned out that silicon membrane has a negligible photoluminescence under the examined excitation from 440 nm to 560 nm, in comparison with a silicon nitrite membrane. Further, background signals from the detection cell were suppressed. Brownian motion of 450 bps DNA labelled with single ATTO-532 or DY-521-XL was successfully recorded by our optical system.
Direct measurements of the optical absorption cross section (σ) and exciton lifetime are performed on a single silicon quantum dot fabricated by electron beam lithography (EBL), reactive ion etching (RIE) and oxidation. For this aim, single photon counting using, an avalanche photodiode detector (APD) is applied to record photoluminescence (PL) intensity traces under pulsed excitation. The PL decay is found to be of a mono-exponential character with a lifetime of 6.5 μs. By recording the photoluminescence rise time at different photon fluxes the absorption cross could be extracted yielding a value of 1.46×10-14cm2 under 405 nm excitation wavelength. The PL quantum efficiency is found to be about 9% for the specified single silicon quantum dot.
Access to the requested content is limited to institutions that have purchased or subscribe to SPIE eBooks.
You are receiving this notice because your organization may not have SPIE eBooks access.*
*Shibboleth/Open Athens users─please
sign in
to access your institution's subscriptions.
To obtain this item, you may purchase the complete book in print or electronic format on
SPIE.org.
INSTITUTIONAL Select your institution to access the SPIE Digital Library.
PERSONAL Sign in with your SPIE account to access your personal subscriptions or to use specific features such as save to my library, sign up for alerts, save searches, etc.