Targeting somatostatin receptors using in situ-bioconjugated fluorescent nanoparticles

Author:

Sreenivasan Varun KA1,Kim Eun J2,Goodchild Ann K1,Connor Mark1,Zvyagin Andrei V3

Affiliation:

1. Macquarie University, NSW 2109, Australia

2. Department of Science Education – Chemical Education Major, Daegu University, Gyeonbuk, Republic of Korea

3. Macquarie University, NSW 2109, Australia.

Abstract

Aim: The author’s group report, for the first time, on the development of a quantum dot (QD)-based fluorescent somatostatin (somatotropin release-inhibiting factor [SRIF]) probe that enables specific targeting of somatostatin receptors. Receptor-mediated endocytosis of SRIF was imaged using this probe. Materials & methods: Biotinylated SRIF-analog (SRIF-B) and streptavidin (Sav)-coated QDs were used for the probe synthesis. A dye-labeled streptavidin complex was used to evaluate the effect of Sav binding on the activity of SRIF-B. Results: A preconjugated probe of the form SRIF-B:Sav-QD, was inactive and unable to undergo receptor-mediated endocytosis. An alternative in situ bioconjugation strategy, where SRIF-B and Sav-QD were added in two consecutive steps, enabled visualization of the receptor-mediated endocytosis. The process of Sav binding appeared to be responsible for the inactivity in the first case. Conclusion: The in situ two-step bioconjugation strategy allowed QDs to be targeted to somatostatin receptors. This strategy should enable flexible fluorescent tagging of SRIF for the investigation of molecular trafficking in cells and targeted delivery in live animals. Original submitted 14 November 2011; Revised submitted 27 February 2012; Published online 20 July 2012

Publisher

Future Medicine Ltd

Subject

Development,General Materials Science,Biomedical Engineering,Medicine (miscellaneous),Bioengineering

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