Hox genes are crucial regulators of periosteal stem cell identity

Author:

Leclerc Kevin1,Remark Lindsey H.12,Ramsukh Malissa1,Josephson Anne Marie12,Palma Laura1,Parente Paulo E. L.1,Sambon Margaux1,Lee Sooyeon13,Lopez Emma Muiños14,Morgani Sophie M.1ORCID,Leucht Philipp12ORCID

Affiliation:

1. NYU Robert I. Grossman School of Medicine 1 Department of Orthopedic Surgery , , New York, NY 10016, USA

2. NYU Robert I. Grossman School of Medicine 2 Department of Cell Biology , , New York, NY 10016, USA

3. Institute of Comparative Molecular Endocrinology, Ulm University 3 , Ulm 89081, Germany

4. Clínica Universidad de Navarra 4 Cell Therapy Area , , Pamplona 31008, Spain

Abstract

ABSTRACT Periosteal stem and progenitor cells (PSPCs) are major contributors to bone maintenance and repair. Deciphering the molecular mechanisms that regulate their function is crucial for the successful generation and application of future therapeutics. Here, we pinpoint Hox transcription factors as necessary and sufficient for periosteal stem cell function. Hox genes are transcriptionally enriched in periosteal stem cells and their overexpression in more committed progenitors drives reprogramming to a naïve, self-renewing stem cell-like state. Crucially, individual Hox family members are expressed in a location-specific manner and their stem cell-promoting activity is only observed when the Hox gene is matched to the anatomical origin of the PSPC, demonstrating a role for the embryonic Hox code in adult stem cells. Finally, we demonstrate that Hoxa10 overexpression partially restores the age-related decline in fracture repair. Together, our data highlight the importance of Hox genes as key regulators of PSPC identity in skeletal homeostasis and repair.

Funder

National Institute on Aging

Musculoskeletal Transplant Foundation

National Center for Advancing Translational Sciences

New York Stem Cell Foundation

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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