Paper
1 August 2007 Nanocluster: photothermal bubble as optical probes for cytometric and microscopic applications
Dmitri O. Lapotko, Ekaterina Y. Lukianova-Hleb, Jason H. Hafner
Author Affiliations +
Proceedings Volume 6734, International Conference on Lasers, Applications, and Technologies 2007: Laser Technologies for Medicine; 67340E (2007) https://doi.org/10.1117/12.753159
Event: International Conference on Lasers, Applications, and Technologies '07, 2007, Minsk, Belarus
Abstract
The ability to detect optical signals form a cellular target depends upon the amount of optical energy that can be generated by this target as the signal. Given that the sensitivity of optical detectors has some finite limit, further increase of the sensitivity of optical diagnostic methods requires increasing the energy of target-generated signal. Usually this energy is converted by the cellular target upon its optical excitation and is limited by many factors such as: cell and target damage thresholds, efficiency of excitation energy conversion, size of the target etc. All these put principal limitation on sensing small targets (like molecules) in living cells with any optical method because the energy that can be safely converted by the target into a signal is limited. To overcome this limitation and to improve the sensitivity of optical microscopy of living cells (and cytometry in general) we propose the concept of intracellular amplification of the optical signal. This concept includes two major steps. First, primary (pump) optical radiation interacts with the target (a probe molecule) to generate a transient target. Second, the transient target is sensed with additional optical radiation that does not interact strongly with primary target or the cell, and, hence, may have high enough energy to increase the signal from transient target even above the energy of pump radiation, which is limited by cell and target damage thresholds. We propose to use optical scattering from clusters of gold nanoparticles (the target) that are selectively formed in specific cells through antibody-receptor interaction and through endocytosis. To amplify this optical signal we propose to generate photothermal bubbles (the transient target) around those clusters. In experiments with water suspensions and with individual tumor K562 cells we have achieved optical signal amplification in individual cells (relatively to the scattering signal from intact cells): with gold nanorod intracellular clusters, 14.8 times, with photothermal bubbles, generated around those clusters, more than 100 times. Those signals were much higher than corresponding fluorescent signals and were obtained from living cells.
© (2007) COPYRIGHT Society of Photo-Optical Instrumentation Engineers (SPIE). Downloading of the abstract is permitted for personal use only.
Dmitri O. Lapotko, Ekaterina Y. Lukianova-Hleb, and Jason H. Hafner "Nanocluster: photothermal bubble as optical probes for cytometric and microscopic applications", Proc. SPIE 6734, International Conference on Lasers, Applications, and Technologies 2007: Laser Technologies for Medicine, 67340E (1 August 2007); https://doi.org/10.1117/12.753159
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Cited by 2 scholarly publications.
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KEYWORDS
Scattering

Nanoparticles

Light scattering

Target detection

Signal detection

Nanorods

Luminescence

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