Molecular pixelation: spatial proteomics of single cells by sequencing

Author:

Karlsson FilipORCID,Kallas Tomasz,Thiagarajan Divya,Karlsson MaxORCID,Schweitzer Maud,Navarro Jose FernandezORCID,Leijonancker Louise,Geny Sylvain,Pettersson Erik,Rhomberg-Kauert JanORCID,Larsson Ludvig,van Ooijen Hanna,Petkov Stefan,González-Granillo Marcela,Bunz Jessica,Dahlberg Johan,Simonetti MicheleORCID,Sathe Prajakta,Brodin PetterORCID,Barrio Alvaro Martinez,Fredriksson SimonORCID

Abstract

AbstractThe spatial distribution of cell surface proteins governs vital processes of the immune system such as intercellular communication and mobility. However, fluorescence microscopy has limited scalability in the multiplexing and throughput needed to drive spatial proteomics discoveries at subcellular level. We present Molecular Pixelation (MPX), an optics-free, DNA sequence-based method for spatial proteomics of single cells using antibody–oligonucleotide conjugates (AOCs) and DNA-based, nanometer-sized molecular pixels. The relative locations of AOCs are inferred by sequentially associating them into local neighborhoods using the sequence-unique DNA pixels, forming >1,000 spatially connected zones per cell in 3D. For each single cell, DNA-sequencing reads are computationally arranged into spatial proteomics networks for 76 proteins. By studying immune cell dynamics using spatial statistics on graph representations of the data, we identify known and new patterns of spatial organization of proteins on chemokine-stimulated T cells, highlighting the potential of MPX in defining cell states by the spatial arrangement of proteins.

Funder

The presented work was funded by the Wellcome Leap ΔTissue Program and Stiftelsen för Strategisk Forskning, SSF.

Brodin is supported by a Proof-of-Concept grant from Knut & Alice Wallenberg Foundation

Publisher

Springer Science and Business Media LLC

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