Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow

Vionnie W.C. Yu; Borja Saez; Colleen Cook; Sutada Lotinun; Ana Pardo-Saganta; Ying Hua Wang; Stefania Lymperi; Francesca Ferraro; Marc H.G.P. Raaijmakers; Joy Y. Wu; Lan Zhou; Jayaraj Rajagopal; Henry M. Kronenberg; Roland Baron; D. T. Scadden

doi:10.1084/jem.20141843

Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow

Vionnie W.C. Yu, Borja Saez, Colleen Cook, Sutada Lotinun, Ana Pardo-Saganta, Ying Hua Wang, Stefania Lymperi, Francesca Ferraro, Marc H.G.P. Raaijmakers, Joy Y. Wu, Lan Zhou, Jayaraj Rajagopal, Henry M. Kronenberg, Roland Baron, D. T. Scadden

Research output: Contribution to journal › Article › peer-review

150 Scopus citations

Abstract

Production of the cells that ultimately populate the thymus to generate α/β T cells has been controversial, and their molecular drivers remain undefined. Here, we report that specific deletion of bone-producing osteocalcin (Ocn)-expressing cells in vivo markedly reduces T-competent progenitors and thymus-homing receptor expression among bone marrow hematopoietic cells. Decreased intrathymic T cell precursors and decreased generation of mature T cells occurred despite normal thymic function. The Notch ligand DLL4 is abundantly expressed on bone marrow Ocn⁺ cells, and selective depletion of DLL4 from these cells recapitulated the thymopoietic abnormality. These data indicate that specific mesenchymal cells in bone marrow provide key molecular drivers enforcing thymus-seeding progenitor generation and thereby directly link skeletal biology to the production of T cell- based adaptive immunity.

Original language	English (US)
Pages (from-to)	759-774
Number of pages	16
Journal	Journal of Experimental Medicine
Volume	212
Issue number	5
DOIs	https://doi.org/10.1084/jem.20141843
State	Published - May 4 2015

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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Yu, V. W. C., Saez, B., Cook, C., Lotinun, S., Pardo-Saganta, A., Wang, Y. H., Lymperi, S., Ferraro, F., Raaijmakers, M. H. G. P., Wu, J. Y., Zhou, L., Rajagopal, J., Kronenberg, H. M., Baron, R., & Scadden, D. T. (2015). Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow. Journal of Experimental Medicine, 212(5), 759-774. https://doi.org/10.1084/jem.20141843

Yu, VWC, Saez, B, Cook, C, Lotinun, S, Pardo-Saganta, A, Wang, YH, Lymperi, S, Ferraro, F, Raaijmakers, MHGP, Wu, JY, Zhou, L, Rajagopal, J, Kronenberg, HM, Baron, R & Scadden, DT 2015, 'Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow', Journal of Experimental Medicine, vol. 212, no. 5, pp. 759-774. https://doi.org/10.1084/jem.20141843

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title = "Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow",

abstract = "Production of the cells that ultimately populate the thymus to generate α/β T cells has been controversial, and their molecular drivers remain undefined. Here, we report that specific deletion of bone-producing osteocalcin (Ocn)-expressing cells in vivo markedly reduces T-competent progenitors and thymus-homing receptor expression among bone marrow hematopoietic cells. Decreased intrathymic T cell precursors and decreased generation of mature T cells occurred despite normal thymic function. The Notch ligand DLL4 is abundantly expressed on bone marrow Ocn+ cells, and selective depletion of DLL4 from these cells recapitulated the thymopoietic abnormality. These data indicate that specific mesenchymal cells in bone marrow provide key molecular drivers enforcing thymus-seeding progenitor generation and thereby directly link skeletal biology to the production of T cell- based adaptive immunity.",

author = "Yu, \{Vionnie W.C.\} and Borja Saez and Colleen Cook and Sutada Lotinun and Ana Pardo-Saganta and Wang, \{Ying Hua\} and Stefania Lymperi and Francesca Ferraro and Raaijmakers, \{Marc H.G.P.\} and Wu, \{Joy Y.\} and Lan Zhou and Jayaraj Rajagopal and Kronenberg, \{Henry M.\} and Roland Baron and Scadden, \{D. T.\}",

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doi = "10.1084/jem.20141843",

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AU - Lotinun, Sutada

AU - Pardo-Saganta, Ana

AU - Wang, Ying Hua

AU - Lymperi, Stefania

AU - Ferraro, Francesca

AU - Raaijmakers, Marc H.G.P.

AU - Wu, Joy Y.

AU - Zhou, Lan

AU - Rajagopal, Jayaraj

AU - Kronenberg, Henry M.

AU - Baron, Roland

AU - Scadden, D. T.

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AB - Production of the cells that ultimately populate the thymus to generate α/β T cells has been controversial, and their molecular drivers remain undefined. Here, we report that specific deletion of bone-producing osteocalcin (Ocn)-expressing cells in vivo markedly reduces T-competent progenitors and thymus-homing receptor expression among bone marrow hematopoietic cells. Decreased intrathymic T cell precursors and decreased generation of mature T cells occurred despite normal thymic function. The Notch ligand DLL4 is abundantly expressed on bone marrow Ocn+ cells, and selective depletion of DLL4 from these cells recapitulated the thymopoietic abnormality. These data indicate that specific mesenchymal cells in bone marrow provide key molecular drivers enforcing thymus-seeding progenitor generation and thereby directly link skeletal biology to the production of T cell- based adaptive immunity.

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Specific bone cells produce DLL4 to generate thymus-seeding progenitors from bone marrow

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