Multiplexed sequential imaging in living cells with orthogonal fluorogenic RNA aptamer/dye pairs

Author:

Zheng Ru1,Wu Rigumula1,Liu Yuanchang1,Sun Zhining1,Xue Zhaolin1,Bagheri Yousef1,Khajouei Sima1,Mi Lan1,Tian Qian1,Pho Raymond2,Liu Qinge3,Siddiqui Sidrat1ORCID,Ren Kewei14,You Mingxu15ORCID

Affiliation:

1. Department of Chemistry, University of Massachusetts , Amherst , MA  01003 , USA

2. Department of Chemical Engineering, University of Massachusetts , Amherst , MA  01003 , USA

3. Department of Chemistry, Mount Holyoke College , Holyoke , MA  01075 , USA

4. School of Chemistry and Chemical Engineering, Nanjing University of Science and Technology , Nanjing  210094 , China

5. Molecular and Cellular Biology Program, University of Massachusetts , Amherst , MA  01003 , USA

Abstract

Abstract Detecting multiple targets in living cells is important in cell biology. However, multiplexed fluorescence imaging beyond two-to-three targets remains a technical challenge. Herein, we introduce a multiplexed imaging strategy, ‘sequential Fluorogenic RNA Imaging-Enabled Sensor’ (seqFRIES), which enables live-cell target detection via sequential rounds of imaging-and-stripping. In seqFRIES, multiple orthogonal fluorogenic RNA aptamers are genetically encoded inside cells, and then the corresponding cell membrane permeable dye molecules are added, imaged, and rapidly removed in consecutive detection cycles. As a proof-of-concept, we have identified in this study four fluorogenic RNA aptamer/dye pairs that can be used for highly orthogonal and multiplexed imaging in living bacterial and mammalian cells. After further optimizing the cellular fluorescence activation and deactivation kinetics of these RNA/dye pairs, the whole four-color semi-quantitative seqFRIES process can be completed in ∼20 min. Meanwhile, seqFRIES-mediated simultaneous detection of critical signalling molecules and mRNA targets was also achieved within individual living cells. We expect our validation of this new seqFRIES concept here will facilitate the further development and potential broad usage of these orthogonal fluorogenic RNA/dye pairs for multiplexed and dynamic live-cell imaging and cell biology studies.

Funder

Chan Zuckerberg Initiative Dynamic Imaging

NSF

Alfred P. Sloan Research Fellowship

Camille Dreyfus Teacher-Scholar Award

UMass Amherst

NIH

SLAS Graduate Education Fellowship

Paul Hatheway Terry Scholarship

Publisher

Oxford University Press (OUP)

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