Abstract

Multicellular organisms contain diverse tissues built from multiple cell types. It remains unclear how large numbers of interacting cells can precisely coordinate their gene expression during tissue self-organization. We develop a generalized model of multicellular gene expression that includes intracellular and intercellular gene interactions in tissue-like collectives. Motivated by modern transcriptomics, we represent multistable cellular phenotypes by mapping the binarized transcriptional patterns of individual cells onto Hopfield networks. We incorporate spatial cell-cell signaling by coupling transcriptional states of adjacent cells on a square lattice. We show that tuning the intercellular signaling strength results in a cascade of transitions toward different collective states with emergent single-cell phenotypes. Despite an enormous number of possible tissue states, we find that intercellular signaling tends to stabilize a small number of compositionally and spatially simple tissue types. These results establish a theoretical framework to investigate how cell collectives self-organize into distinct stable patterns.

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