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Mechanics and fate stochasticity shape stem cell distribution in tissues

Created on 13 Jun 2026

Authors

Krämer, J. C., Hannezo, E., Elgeti, J.

Abstract

Balancing cellular loss in tissues requires fine balance of cell proliferation and differentiation. In differentiated tissues consisting of a single cell type, a mechanical regulation of proliferation has been proposed to underlie growth-control and homeostatic steady-states. Yet, how tissues containing different cell types with distinct proliferation rates, mechanical interactions, and spatial self-organization retain robust homeostasis of cell proportions remains poorly understood. Here, we combine particle-based mechanical models of proliferative tissues with a classical hierarchy of stem, progenitor, and differentiated cells, undergoing stochastic fate choices, and show that mechanical feedback alone is sufficient to stabilize populations. We derive analytically and computationally a phase diagram of possible stable states, in particular those maintained either via slow and rare stem cells with short-lived progenitors or no stem cells and long-lived progenitors. Our simulations uncover that mechanical control of growth is sufficient, in the absence of any codes of adhesion or extrinsic niche signals, to cause stable spatial structures, with small stem cell clusters forming and maintaining dynamical renewal units. Our results demonstrate how complex spatial structures can emerge in minimal stochastic and mechanical simulations with impact to understand the homeostasis of multi-cellular systems.

Preprint server: bioRxiv
The authors list and abstract were imported from bioRxiv on 13 Jun 2026.

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