Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia

Jonathan Bastos; Carleigh  O' Brien; Mónica Vara Pérez; Myrthe Mampay; Lynn Van Olst; Liam Barry-Carroll; Daliya Kancheva; Sophia Leduc; Ayla Line Lievens; Leen Ali; Vladislav Vlasov; Laura Meysman; Hadis Shakeri; Ria Roelandt; Hannah Van Hove; Karen De Vlaminck; Isabelle Scheyltjens; Fazeela  Yaqoob; Sonia I. Lombroso; Maria Breugelmans; Gilles Faron; Diego Gomez-Nicola; David Gate; F. Chris Bennett; Kiavash Movahedi

doi:10.1016/j.immuni.2025.04.006

Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia

Jonathan Bastos, Carleigh O' Brien, Mónica Vara Pérez, Myrthe Mampay, Lynn Van Olst, Liam Barry-Carroll, Daliya Kancheva, Sophia Leduc, Ayla Line Lievens, Leen Ali, Vladislav Vlasov, Laura Meysman, Hadis Shakeri, Ria Roelandt, Hannah Van Hove, Karen De Vlaminck, Isabelle Scheyltjens, Fazeela Yaqoob, Sonia I. Lombroso, Maria BreugelmansGilles Faron, Diego Gomez-Nicola, David Gate, F. Chris Bennett, Kiavash Movahedi

Onderzoeksoutput: Article › peer review

2 Citaten (Scopus)

Samenvatting

Microglia and border-associated macrophages (BAMs) are critical for brain health, and their dysfunction is associated to disease. Replacing brain macrophages holds substantial therapeutic promise but remains challenging. Here, we demonstrate that monocytes can efficiently replace all brain macrophages. Monocytes readily replaced embryonal BAMs upon their depletion and engrafted as monocyte-derived microglia (Mo-Microglia) upon more sustained niche availability. Mo-Microglia expanded comparably to their embryonic counterparts and showed similar longevity. However, monocytes were unable to replicate the distinct identity of embryonically derived BAMs and microglia. Using xenotransplantation, we found that human monocytes exhibited similar behavior, enabling identification of putative Mo-Microglia in Alzheimer's disease individuals. In mice and humans, monocyte ontogeny shaped their identity as brain macrophages. Importantly, mouse fetal liver monocytes exhibited a distinct epigenetic landscape and could develop a bona fide microglial identity. Our results illuminate brain macrophage development and highlight monocytes as an abundant progenitor source for brain macrophage replacement therapies.

Originele taal-2	English
Artikelnummer	E12
Pagina's (van-tot)	1269-1288
Aantal pagina's	19
Tijdschrift	Immunity
Volume	58
Nummer van het tijdschrift	5
DOI's	https://doi.org/10.1016/j.immuni.2025.04.006
Status	Published - 13 mei 2025

Bibliografische nota

Publisher Copyright:
© 2025 The Author(s)

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10.1016/j.immuni.2025.04.006

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Bastos, J., O' Brien, C., Vara Pérez, M., Mampay, M., Van Olst, L., Barry-Carroll, L., Kancheva, D., Leduc, S., Lievens, A. L., Ali, L., Vlasov, V., Meysman, L., Shakeri, H., Roelandt, R., Van Hove, H., De Vlaminck, K., Scheyltjens, I., Yaqoob, F., I. Lombroso, S., ... Movahedi, K. (2025). Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia. Immunity, 58(5), 1269-1288. Artikel E12. https://doi.org/10.1016/j.immuni.2025.04.006

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title = "Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia",

abstract = "Microglia and border-associated macrophages (BAMs) are critical for brain health, and their dysfunction is associated to disease. Replacing brain macrophages holds substantial therapeutic promise but remains challenging. Here, we demonstrate that monocytes can efficiently replace all brain macrophages. Monocytes readily replaced embryonal BAMs upon their depletion and engrafted as monocyte-derived microglia (Mo-Microglia) upon more sustained niche availability. Mo-Microglia expanded comparably to their embryonic counterparts and showed similar longevity. However, monocytes were unable to replicate the distinct identity of embryonically derived BAMs and microglia. Using xenotransplantation, we found that human monocytes exhibited similar behavior, enabling identification of putative Mo-Microglia in Alzheimer's disease individuals. In mice and humans, monocyte ontogeny shaped their identity as brain macrophages. Importantly, mouse fetal liver monocytes exhibited a distinct epigenetic landscape and could develop a bona fide microglial identity. Our results illuminate brain macrophage development and highlight monocytes as an abundant progenitor source for brain macrophage replacement therapies.",

author = "Jonathan Bastos and {O' Brien}, Carleigh and {Vara P{\'e}rez}, M{\'o}nica and Myrthe Mampay and {Van Olst}, Lynn and Liam Barry-Carroll and Daliya Kancheva and Sophia Leduc and Lievens, {Ayla Line} and Leen Ali and Vladislav Vlasov and Laura Meysman and Hadis Shakeri and Ria Roelandt and {Van Hove}, Hannah and {De Vlaminck}, Karen and Isabelle Scheyltjens and Fazeela Yaqoob and {I. Lombroso}, Sonia and Maria Breugelmans and Gilles Faron and Diego Gomez-Nicola and David Gate and Bennett, {F. Chris} and Kiavash Movahedi",

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year = "2025",

month = may,

day = "13",

doi = "10.1016/j.immuni.2025.04.006",

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Bastos, J, O' Brien, C, Vara Pérez, M , Mampay, M, Van Olst, L, Barry-Carroll, L, Kancheva, D , Leduc, S , Lievens, AL , Ali, L , Vlasov, V , Meysman, L , Shakeri, H, Roelandt, R, Van Hove, H, De Vlaminck, K, Scheyltjens, I, Yaqoob, F, I. Lombroso, S, Breugelmans, M , Faron, G, Gomez-Nicola, D, Gate, D, Bennett, FC & Movahedi, K 2025, 'Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia', Immunity, vol. 58, nr. 5, E12, blz. 1269-1288. https://doi.org/10.1016/j.immuni.2025.04.006

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T1 - Monocytes can efficiently replace all brain macrophages and fetal liver monocytes can generate bona fide SALL1+ microglia

AU - Bastos, Jonathan

AU - O' Brien, Carleigh

AU - Vara Pérez, Mónica

AU - Mampay, Myrthe

AU - Van Olst, Lynn

AU - Barry-Carroll, Liam

AU - Kancheva, Daliya

AU - Leduc, Sophia

AU - Lievens, Ayla Line

AU - Ali, Leen

AU - Vlasov, Vladislav

AU - Meysman, Laura

AU - Shakeri, Hadis

AU - Roelandt, Ria

AU - Van Hove, Hannah

AU - De Vlaminck, Karen

AU - Scheyltjens, Isabelle

AU - Yaqoob, Fazeela

AU - I. Lombroso, Sonia

AU - Breugelmans, Maria

AU - Faron, Gilles

AU - Gomez-Nicola, Diego

AU - Gate, David

AU - Bennett, F. Chris

AU - Movahedi, Kiavash

PY - 2025/5/13

Y1 - 2025/5/13

N2 - Microglia and border-associated macrophages (BAMs) are critical for brain health, and their dysfunction is associated to disease. Replacing brain macrophages holds substantial therapeutic promise but remains challenging. Here, we demonstrate that monocytes can efficiently replace all brain macrophages. Monocytes readily replaced embryonal BAMs upon their depletion and engrafted as monocyte-derived microglia (Mo-Microglia) upon more sustained niche availability. Mo-Microglia expanded comparably to their embryonic counterparts and showed similar longevity. However, monocytes were unable to replicate the distinct identity of embryonically derived BAMs and microglia. Using xenotransplantation, we found that human monocytes exhibited similar behavior, enabling identification of putative Mo-Microglia in Alzheimer's disease individuals. In mice and humans, monocyte ontogeny shaped their identity as brain macrophages. Importantly, mouse fetal liver monocytes exhibited a distinct epigenetic landscape and could develop a bona fide microglial identity. Our results illuminate brain macrophage development and highlight monocytes as an abundant progenitor source for brain macrophage replacement therapies.

AB - Microglia and border-associated macrophages (BAMs) are critical for brain health, and their dysfunction is associated to disease. Replacing brain macrophages holds substantial therapeutic promise but remains challenging. Here, we demonstrate that monocytes can efficiently replace all brain macrophages. Monocytes readily replaced embryonal BAMs upon their depletion and engrafted as monocyte-derived microglia (Mo-Microglia) upon more sustained niche availability. Mo-Microglia expanded comparably to their embryonic counterparts and showed similar longevity. However, monocytes were unable to replicate the distinct identity of embryonically derived BAMs and microglia. Using xenotransplantation, we found that human monocytes exhibited similar behavior, enabling identification of putative Mo-Microglia in Alzheimer's disease individuals. In mice and humans, monocyte ontogeny shaped their identity as brain macrophages. Importantly, mouse fetal liver monocytes exhibited a distinct epigenetic landscape and could develop a bona fide microglial identity. Our results illuminate brain macrophage development and highlight monocytes as an abundant progenitor source for brain macrophage replacement therapies.

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U2 - 10.1016/j.immuni.2025.04.006

DO - 10.1016/j.immuni.2025.04.006

M3 - Article

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SN - 1074-7613

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EP - 1288

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JF - Immunity

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