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September 4th, 2025
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University of Wisconsin-Madison
developmental biology
bioRxiv

Vcam1 in endothelial and stromal cells regulates hematopoietic stem cell contact with the niche

Santis Larrain, O.Open in Google Scholar•Alhaj Kadour, A.Open in Google Scholar•Agarwala, S.Open in Google Scholar•Li, W.Open in Google Scholar•Blaser, B. W.Open in Google Scholar•Lasarev, M. R.Open in Google Scholar•Alexandridis, R.Open in Google Scholar•Veltri, A.Open in Google Scholar•Enkhbayar, K.Open in Google Scholar•Hagedorn, E. J.Open in Google Scholaret al.

Hematopoietic stem and progenitor cells (HSPCs) are essential for differentiation into all blood cell types. In mammals, the interaction between HSPCs and the fetal liver niche during development is critical for stem cell maturation. Integrin alpha 4 (Itga4) on HSPCs and vascular cell adhesion molecule (Vcam1) on niche cells are critical for HSPC colonization of the fetal liver (FL). Itga4 and Vcam1 also function in the zebrafish equivalent of the FL, the caudal hematopoietic tissue (CHT), however, the specific niche cells that express Vcam1 remain unclear. Using multiple approaches, including fluorescent in situ hybridization, we found Vcam1 is expressed in endothelial cells (ECs) and mesenchymal stromal cells (MSCs), but not macrophages. Time-lapse live imaging of itga4 mutants showed the Itga4-Vcam1 axis is required for HSPC retention in the CHT niche, but not homing or lodgment. Our results show that Itga4 on HSPCs and Vcam1 on ECs and MSCs are involved in retention in the CHT niche.

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