A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states

John F. Tuddenham; Mariko Taga; Verena Haage; Victoria S. Marshe; Tina Roostaei; Charles White; Annie J. Lee; Masashi Fujita; Anthony Khairallah; Ya Zhang; Gilad Green; Bradley Hyman; Matthew Frosch; Sarah Hopp; Thomas G. Beach; Geidy E. Serrano; John Corboy; Naomi Habib; Hans Ulrich Klein; Rajesh Kumar Soni; Andrew F. Teich; Richard A. Hickman; Roy N. Alcalay; Neil Shneider; Julie Schneider; Peter A. Sims; David A. Bennett; Marta Olah; Vilas Menon; Philip L. De Jager

doi:10.1038/s41593-024-01764-7

A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states

John F. Tuddenham
, Mariko Taga
, Verena Haage
, Victoria S. Marshe
, Tina Roostaei
, Charles White
, Annie J. Lee
, Masashi Fujita
, Anthony Khairallah
, Ya Zhang
, Gilad Green
, Bradley Hyman
, Matthew Frosch
, Sarah Hopp
, Thomas G. Beach
, Geidy E. Serrano
, John Corboy
, Naomi Habib
, Hans Ulrich Klein
, Rajesh Kumar Soni

Andrew F. Teich, Richard A. Hickman, Roy N. Alcalay, Neil Shneider, Julie Schneider, Peter A. Sims, David A. Bennett, Marta Olah, Vilas Menon, Philip L. De Jager

Producción científica: Article › revisión exhaustiva

26 Citas (Scopus)

Resumen

Human microglia play a pivotal role in neurological diseases, but we still have an incomplete understanding of microglial heterogeneity, which limits the development of targeted therapies directly modulating their state or function. Here, we use single-cell RNA sequencing to profile 215,680 live human microglia from 74 donors across diverse neurological diseases and CNS regions. We observe a central divide between oxidative and heterocyclic metabolism and identify microglial subsets associated with antigen presentation, motility and proliferation. Specific subsets are enriched in susceptibility genes for neurodegenerative diseases or the disease-associated microglial signature. We validate subtypes in situ with an RNAscope–immunofluorescence pipeline and high-dimensional MERFISH. We also leverage our dataset as a classification resource, finding that induced pluripotent stem cell model systems capture substantial in vivo heterogeneity. Finally, we identify and validate compounds that recapitulate certain subtypes in vitro, including camptothecin, which downregulates the signature of disease-enriched subtypes and upregulates a signature previously associated with Alzheimer’s disease.

Idioma original	English (US)
Número de artículo	6129
Páginas (desde-hasta)	2521-2537
Número de páginas	17
Publicación	Nature Neuroscience
Volumen	27
N.º	12
DOI	https://doi.org/10.1038/s41593-024-01764-7
Estado	Published - dic 2024

ASJC Scopus subject areas

General Neuroscience

Acceder al documento

10.1038/s41593-024-01764-7

Otros archivos y enlaces

Citar esto

Tuddenham, J. F., Taga, M., Haage, V., Marshe, V. S., Roostaei, T., White, C., Lee, A. J., Fujita, M., Khairallah, A., Zhang, Y., Green, G., Hyman, B., Frosch, M., Hopp, S., Beach, T. G., Serrano, G. E., Corboy, J., Habib, N., Klein, H. U., ... De Jager, P. L. (2024). A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states. Nature Neuroscience, 27(12), 2521-2537. Artículo 6129. https://doi.org/10.1038/s41593-024-01764-7

Tuddenham, JF, Taga, M, Haage, V, Marshe, VS, Roostaei, T, White, C, Lee, AJ, Fujita, M, Khairallah, A, Zhang, Y, Green, G, Hyman, B, Frosch, M, Hopp, S, Beach, TG, Serrano, GE, Corboy, J, Habib, N, Klein, HU, Soni, RK, Teich, AF, Hickman, RA, Alcalay, RN, Shneider, N, Schneider, J, Sims, PA, Bennett, DA, Olah, M, Menon, V & De Jager, PL 2024, 'A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states', Nature Neuroscience, vol. 27, n.º 12, 6129, pp. 2521-2537. https://doi.org/10.1038/s41593-024-01764-7

@article{9b01be3227b54ab9a6d83ce341712f2b,

title = "A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states",

abstract = "Human microglia play a pivotal role in neurological diseases, but we still have an incomplete understanding of microglial heterogeneity, which limits the development of targeted therapies directly modulating their state or function. Here, we use single-cell RNA sequencing to profile 215,680 live human microglia from 74 donors across diverse neurological diseases and CNS regions. We observe a central divide between oxidative and heterocyclic metabolism and identify microglial subsets associated with antigen presentation, motility and proliferation. Specific subsets are enriched in susceptibility genes for neurodegenerative diseases or the disease-associated microglial signature. We validate subtypes in situ with an RNAscope–immunofluorescence pipeline and high-dimensional MERFISH. We also leverage our dataset as a classification resource, finding that induced pluripotent stem cell model systems capture substantial in vivo heterogeneity. Finally, we identify and validate compounds that recapitulate certain subtypes in vitro, including camptothecin, which downregulates the signature of disease-enriched subtypes and upregulates a signature previously associated with Alzheimer{\textquoteright}s disease.",

author = "Tuddenham, \{John F.\} and Mariko Taga and Verena Haage and Marshe, \{Victoria S.\} and Tina Roostaei and Charles White and Lee, \{Annie J.\} and Masashi Fujita and Anthony Khairallah and Ya Zhang and Gilad Green and Bradley Hyman and Matthew Frosch and Sarah Hopp and Beach, \{Thomas G.\} and Serrano, \{Geidy E.\} and John Corboy and Naomi Habib and Klein, \{Hans Ulrich\} and Soni, \{Rajesh Kumar\} and Teich, \{Andrew F.\} and Hickman, \{Richard A.\} and Alcalay, \{Roy N.\} and Neil Shneider and Julie Schneider and Sims, \{Peter A.\} and Bennett, \{David A.\} and Marta Olah and Vilas Menon and \{De Jager\}, \{Philip L.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.",

year = "2024",

month = dec,

doi = "10.1038/s41593-024-01764-7",

language = "English (US)",

volume = "27",

pages = "2521--2537",

journal = "Nature Neuroscience",

issn = "1097-6256",

publisher = "Nature Research",

number = "12",

}

TY - JOUR

T1 - A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states

AU - Tuddenham, John F.

AU - Taga, Mariko

AU - Haage, Verena

AU - Marshe, Victoria S.

AU - Roostaei, Tina

AU - White, Charles

AU - Lee, Annie J.

AU - Fujita, Masashi

AU - Khairallah, Anthony

AU - Zhang, Ya

AU - Green, Gilad

AU - Hyman, Bradley

AU - Frosch, Matthew

AU - Hopp, Sarah

AU - Beach, Thomas G.

AU - Serrano, Geidy E.

AU - Corboy, John

AU - Habib, Naomi

AU - Klein, Hans Ulrich

AU - Soni, Rajesh Kumar

AU - Teich, Andrew F.

AU - Hickman, Richard A.

AU - Alcalay, Roy N.

AU - Shneider, Neil

AU - Schneider, Julie

AU - Sims, Peter A.

AU - Bennett, David A.

AU - Olah, Marta

AU - Menon, Vilas

AU - De Jager, Philip L.

PY - 2024/12

Y1 - 2024/12

N2 - Human microglia play a pivotal role in neurological diseases, but we still have an incomplete understanding of microglial heterogeneity, which limits the development of targeted therapies directly modulating their state or function. Here, we use single-cell RNA sequencing to profile 215,680 live human microglia from 74 donors across diverse neurological diseases and CNS regions. We observe a central divide between oxidative and heterocyclic metabolism and identify microglial subsets associated with antigen presentation, motility and proliferation. Specific subsets are enriched in susceptibility genes for neurodegenerative diseases or the disease-associated microglial signature. We validate subtypes in situ with an RNAscope–immunofluorescence pipeline and high-dimensional MERFISH. We also leverage our dataset as a classification resource, finding that induced pluripotent stem cell model systems capture substantial in vivo heterogeneity. Finally, we identify and validate compounds that recapitulate certain subtypes in vitro, including camptothecin, which downregulates the signature of disease-enriched subtypes and upregulates a signature previously associated with Alzheimer’s disease.

AB - Human microglia play a pivotal role in neurological diseases, but we still have an incomplete understanding of microglial heterogeneity, which limits the development of targeted therapies directly modulating their state or function. Here, we use single-cell RNA sequencing to profile 215,680 live human microglia from 74 donors across diverse neurological diseases and CNS regions. We observe a central divide between oxidative and heterocyclic metabolism and identify microglial subsets associated with antigen presentation, motility and proliferation. Specific subsets are enriched in susceptibility genes for neurodegenerative diseases or the disease-associated microglial signature. We validate subtypes in situ with an RNAscope–immunofluorescence pipeline and high-dimensional MERFISH. We also leverage our dataset as a classification resource, finding that induced pluripotent stem cell model systems capture substantial in vivo heterogeneity. Finally, we identify and validate compounds that recapitulate certain subtypes in vitro, including camptothecin, which downregulates the signature of disease-enriched subtypes and upregulates a signature previously associated with Alzheimer’s disease.

UR - https://www.scopus.com/pages/publications/85207279082

UR - https://www.scopus.com/pages/publications/85207279082#tab=citedBy

U2 - 10.1038/s41593-024-01764-7

DO - 10.1038/s41593-024-01764-7

M3 - Article

C2 - 39406950

AN - SCOPUS:85207279082

SN - 1097-6256

VL - 27

SP - 2521

EP - 2537

JO - Nature Neuroscience

JF - Nature Neuroscience

IS - 12

M1 - 6129

ER -

A cross-disease resource of living human microglia identifies disease-enriched subsets and tool compounds recapitulating microglial states

Resumen

ASJC Scopus subject areas

Acceder al documento

Otros archivos y enlaces

Huella

Citar esto