Defining blood-induced microglia functions in neurodegeneration through multiomic profiling

Andrew S. Mendiola; Zhaoqi Yan; Karuna Dixit; Jeffrey R. Johnson; Mehdi Bouhaddou; Anke Meyer-Franke; Min Gyoung Shin; Yu Yong; Ayushi Agrawal; Eilidh MacDonald; Gayathri Muthukumar; Clairice Pearce; Nikhita Arun; Belinda Cabriga; Rosa Meza-Acevedo; Maria del Pilar S. Alzamora; Scott S. Zamvil; Alexander R. Pico; Jae Kyu Ryu; Nevan J. Krogan; Katerina Akassoglou

doi:10.1038/s41590-023-01522-0

Defining blood-induced microglia functions in neurodegeneration through multiomic profiling

Andrew S. Mendiola, Zhaoqi Yan, Karuna Dixit, Jeffrey R. Johnson, Mehdi Bouhaddou, Anke Meyer-Franke, Min Gyoung Shin, Yu Yong, Ayushi Agrawal, Eilidh MacDonald, Gayathri Muthukumar, Clairice Pearce, Nikhita Arun, Belinda Cabriga, Rosa Meza-Acevedo, Maria del Pilar S. Alzamora, Scott S. Zamvil, Alexander R. Pico, Jae Kyu Ryu, Nevan J. KroganKaterina Akassoglou

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

46 Scopus citations

Abstract

Blood protein extravasation through a disrupted blood–brain barrier and innate immune activation are hallmarks of neurological diseases and emerging therapeutic targets. However, how blood proteins polarize innate immune cells remains largely unknown. Here, we established an unbiased blood-innate immunity multiomic and genetic loss-of-function pipeline to define the transcriptome and global phosphoproteome of blood-induced innate immune polarization and its role in microglia neurotoxicity. Blood induced widespread microglial transcriptional changes, including changes involving oxidative stress and neurodegenerative genes. Comparative functional multiomics showed that blood proteins induce distinct receptor-mediated transcriptional programs in microglia and macrophages, such as redox, type I interferon and lymphocyte recruitment. Deletion of the blood coagulation factor fibrinogen largely reversed blood-induced microglia neurodegenerative signatures. Genetic elimination of the fibrinogen-binding motif to CD11b in Alzheimer’s disease mice reduced microglial lipid metabolism and neurodegenerative signatures that were shared with autoimmune-driven neuroinflammation in multiple sclerosis mice. Our data provide an interactive resource for investigation of the immunology of blood proteins that could support therapeutic targeting of microglia activation by immune and vascular signals.

Original language	English
Pages (from-to)	1173-1187
Number of pages	15
Journal	Nature Immunology
Volume	24
Issue number	7
DOIs	https://doi.org/10.1038/s41590-023-01522-0
State	Published - Jul 2023
Externally published	Yes

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Mendiola, A. S., Yan, Z., Dixit, K., Johnson, J. R., Bouhaddou, M., Meyer-Franke, A., Shin, M. G., Yong, Y., Agrawal, A., MacDonald, E., Muthukumar, G., Pearce, C., Arun, N., Cabriga, B., Meza-Acevedo, R., Alzamora, M. D. P. S., Zamvil, S. S., Pico, A. R., Ryu, J. K., ... Akassoglou, K. (2023). Defining blood-induced microglia functions in neurodegeneration through multiomic profiling. Nature Immunology, 24(7), 1173-1187. https://doi.org/10.1038/s41590-023-01522-0

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title = "Defining blood-induced microglia functions in neurodegeneration through multiomic profiling",

abstract = "Blood protein extravasation through a disrupted blood–brain barrier and innate immune activation are hallmarks of neurological diseases and emerging therapeutic targets. However, how blood proteins polarize innate immune cells remains largely unknown. Here, we established an unbiased blood-innate immunity multiomic and genetic loss-of-function pipeline to define the transcriptome and global phosphoproteome of blood-induced innate immune polarization and its role in microglia neurotoxicity. Blood induced widespread microglial transcriptional changes, including changes involving oxidative stress and neurodegenerative genes. Comparative functional multiomics showed that blood proteins induce distinct receptor-mediated transcriptional programs in microglia and macrophages, such as redox, type I interferon and lymphocyte recruitment. Deletion of the blood coagulation factor fibrinogen largely reversed blood-induced microglia neurodegenerative signatures. Genetic elimination of the fibrinogen-binding motif to CD11b in Alzheimer{\textquoteright}s disease mice reduced microglial lipid metabolism and neurodegenerative signatures that were shared with autoimmune-driven neuroinflammation in multiple sclerosis mice. Our data provide an interactive resource for investigation of the immunology of blood proteins that could support therapeutic targeting of microglia activation by immune and vascular signals.",

author = "Mendiola, {Andrew S.} and Zhaoqi Yan and Karuna Dixit and Johnson, {Jeffrey R.} and Mehdi Bouhaddou and Anke Meyer-Franke and Shin, {Min Gyoung} and Yu Yong and Ayushi Agrawal and Eilidh MacDonald and Gayathri Muthukumar and Clairice Pearce and Nikhita Arun and Belinda Cabriga and Rosa Meza-Acevedo and Alzamora, {Maria del Pilar S.} and Zamvil, {Scott S.} and Pico, {Alexander R.} and Ryu, {Jae Kyu} and Krogan, {Nevan J.} and Katerina Akassoglou",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = jul,

doi = "10.1038/s41590-023-01522-0",

language = "English",

volume = "24",

pages = "1173--1187",

journal = "Nature Immunology",

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Mendiola, AS, Yan, Z, Dixit, K, Johnson, JR, Bouhaddou, M, Meyer-Franke, A, Shin, MG, Yong, Y, Agrawal, A, MacDonald, E, Muthukumar, G, Pearce, C, Arun, N, Cabriga, B, Meza-Acevedo, R, Alzamora, MDPS, Zamvil, SS, Pico, AR, Ryu, JK, Krogan, NJ & Akassoglou, K 2023, 'Defining blood-induced microglia functions in neurodegeneration through multiomic profiling', Nature Immunology, vol. 24, no. 7, pp. 1173-1187. https://doi.org/10.1038/s41590-023-01522-0

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T1 - Defining blood-induced microglia functions in neurodegeneration through multiomic profiling

AU - Mendiola, Andrew S.

AU - Yan, Zhaoqi

AU - Dixit, Karuna

AU - Johnson, Jeffrey R.

AU - Bouhaddou, Mehdi

AU - Meyer-Franke, Anke

AU - Shin, Min Gyoung

AU - Yong, Yu

AU - Agrawal, Ayushi

AU - MacDonald, Eilidh

AU - Muthukumar, Gayathri

AU - Pearce, Clairice

AU - Arun, Nikhita

AU - Cabriga, Belinda

AU - Meza-Acevedo, Rosa

AU - Alzamora, Maria del Pilar S.

AU - Zamvil, Scott S.

AU - Pico, Alexander R.

AU - Ryu, Jae Kyu

AU - Krogan, Nevan J.

AU - Akassoglou, Katerina

PY - 2023/7

Y1 - 2023/7

N2 - Blood protein extravasation through a disrupted blood–brain barrier and innate immune activation are hallmarks of neurological diseases and emerging therapeutic targets. However, how blood proteins polarize innate immune cells remains largely unknown. Here, we established an unbiased blood-innate immunity multiomic and genetic loss-of-function pipeline to define the transcriptome and global phosphoproteome of blood-induced innate immune polarization and its role in microglia neurotoxicity. Blood induced widespread microglial transcriptional changes, including changes involving oxidative stress and neurodegenerative genes. Comparative functional multiomics showed that blood proteins induce distinct receptor-mediated transcriptional programs in microglia and macrophages, such as redox, type I interferon and lymphocyte recruitment. Deletion of the blood coagulation factor fibrinogen largely reversed blood-induced microglia neurodegenerative signatures. Genetic elimination of the fibrinogen-binding motif to CD11b in Alzheimer’s disease mice reduced microglial lipid metabolism and neurodegenerative signatures that were shared with autoimmune-driven neuroinflammation in multiple sclerosis mice. Our data provide an interactive resource for investigation of the immunology of blood proteins that could support therapeutic targeting of microglia activation by immune and vascular signals.

AB - Blood protein extravasation through a disrupted blood–brain barrier and innate immune activation are hallmarks of neurological diseases and emerging therapeutic targets. However, how blood proteins polarize innate immune cells remains largely unknown. Here, we established an unbiased blood-innate immunity multiomic and genetic loss-of-function pipeline to define the transcriptome and global phosphoproteome of blood-induced innate immune polarization and its role in microglia neurotoxicity. Blood induced widespread microglial transcriptional changes, including changes involving oxidative stress and neurodegenerative genes. Comparative functional multiomics showed that blood proteins induce distinct receptor-mediated transcriptional programs in microglia and macrophages, such as redox, type I interferon and lymphocyte recruitment. Deletion of the blood coagulation factor fibrinogen largely reversed blood-induced microglia neurodegenerative signatures. Genetic elimination of the fibrinogen-binding motif to CD11b in Alzheimer’s disease mice reduced microglial lipid metabolism and neurodegenerative signatures that were shared with autoimmune-driven neuroinflammation in multiple sclerosis mice. Our data provide an interactive resource for investigation of the immunology of blood proteins that could support therapeutic targeting of microglia activation by immune and vascular signals.

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U2 - 10.1038/s41590-023-01522-0

DO - 10.1038/s41590-023-01522-0

M3 - Article

AN - SCOPUS:85161413442

SN - 1529-2908

VL - 24

SP - 1173

EP - 1187

JO - Nature Immunology

JF - Nature Immunology

IS - 7

ER -

Defining blood-induced microglia functions in neurodegeneration through multiomic profiling

Abstract

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