Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2

D. Vacondio; H. Nogueira Pinto; L. Coenen; I. A. Mulder; R. Fontijn; B. van het Hof; W. K. Fung; A. Jongejan; G. Kooij; N. Zelcer; A. J. Rozemuller; H. E. de Vries; N. M. de Wit

doi:https://doi.org/10.1038/s41419-023-06316-8

Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2

D. Vacondio, H. Nogueira Pinto, L. Coenen, I. A. Mulder, R. Fontijn, B. van het Hof, W. K. Fung, A. Jongejan, G. Kooij, N. Zelcer, A. J. Rozemuller, H. E. de Vries, N. M. de Wit

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Abstract

In Alzheimer’s disease (AD) more than 50% of the patients are affected by capillary cerebral amyloid-angiopathy (capCAA), which is characterized by localized hypoxia, neuro-inflammation and loss of blood-brain barrier (BBB) function. Moreover, AD patients with or without capCAA display increased vessel number, indicating a reactivation of the angiogenic program. The molecular mechanism(s) responsible for BBB dysfunction and angiogenesis in capCAA is still unclear, preventing a full understanding of disease pathophysiology. The Liver X receptor (LXR) family, consisting of LXRα and LXRβ, was reported to inhibit angiogenesis and particularly LXRα was shown to secure BBB stability, suggesting a major role in vascular function. In this study, we unravel the regulatory mechanism exerted by LXRα to preserve BBB integrity in human brain endothelial cells (BECs) and investigate its role during pathological conditions. We report that LXRα ensures BECs identity via constitutive inhibition of the transcription factor SNAI2. Accordingly, deletion of brain endothelial LXRα is associated with impaired DLL4-NOTCH signalling, a critical signalling pathway involved in vessel sprouting. A similar response was observed when BECs were exposed to hypoxia, with concomitant LXRα decrease and SNAI2 increase. In support of our cell-based observations, we report a general increase in vascular SNAI2 in the occipital cortex of AD patients with and without capCAA. Importantly, SNAI2 strongly associated with vascular amyloid-beta deposition and angiopoietin-like 4, a marker for hypoxia. In hypoxic capCAA vessels, the expression of LXRα may decrease leading to an increased expression of SNAI2, and consequently BECs de-differentiation and sprouting. Our findings indicate that LXRα is essential for BECs identity, thereby securing BBB stability and preventing aberrant angiogenesis. These results uncover a novel molecular pathway essential for BBB identity and vascular homeostasis providing new insights on the vascular pathology affecting AD patients. [Figure not available: see fulltext.].

Original language	English
Article number	781
Pages (from-to)	781
Journal	Cell Death & Disease
Volume	14
Issue number	11
DOIs	https://doi.org/10.1038/s41419-023-06316-8 https://doi.org/10.1038/s41419-023-06316-8
Publication status	Published - 1 Nov 2023

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Vacondio, D., Nogueira Pinto, H., Coenen, L., Mulder, I. A., Fontijn, R., van het Hof, B., Fung, W. K., Jongejan, A., Kooij, G., Zelcer, N., Rozemuller, A. J., de Vries, H. E., & de Wit, N. M. (2023). Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2. Cell Death & Disease, 14(11), 781. Article 781. https://doi.org/10.1038/s41419-023-06316-8, https://doi.org/10.1038/s41419-023-06316-8

@article{e53f075d311a4db2832906d6b3a2a474,

title = "Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2",

abstract = "In Alzheimer{\textquoteright}s disease (AD) more than 50% of the patients are affected by capillary cerebral amyloid-angiopathy (capCAA), which is characterized by localized hypoxia, neuro-inflammation and loss of blood-brain barrier (BBB) function. Moreover, AD patients with or without capCAA display increased vessel number, indicating a reactivation of the angiogenic program. The molecular mechanism(s) responsible for BBB dysfunction and angiogenesis in capCAA is still unclear, preventing a full understanding of disease pathophysiology. The Liver X receptor (LXR) family, consisting of LXRα and LXRβ, was reported to inhibit angiogenesis and particularly LXRα was shown to secure BBB stability, suggesting a major role in vascular function. In this study, we unravel the regulatory mechanism exerted by LXRα to preserve BBB integrity in human brain endothelial cells (BECs) and investigate its role during pathological conditions. We report that LXRα ensures BECs identity via constitutive inhibition of the transcription factor SNAI2. Accordingly, deletion of brain endothelial LXRα is associated with impaired DLL4-NOTCH signalling, a critical signalling pathway involved in vessel sprouting. A similar response was observed when BECs were exposed to hypoxia, with concomitant LXRα decrease and SNAI2 increase. In support of our cell-based observations, we report a general increase in vascular SNAI2 in the occipital cortex of AD patients with and without capCAA. Importantly, SNAI2 strongly associated with vascular amyloid-beta deposition and angiopoietin-like 4, a marker for hypoxia. In hypoxic capCAA vessels, the expression of LXRα may decrease leading to an increased expression of SNAI2, and consequently BECs de-differentiation and sprouting. Our findings indicate that LXRα is essential for BECs identity, thereby securing BBB stability and preventing aberrant angiogenesis. These results uncover a novel molecular pathway essential for BBB identity and vascular homeostasis providing new insights on the vascular pathology affecting AD patients. [Figure not available: see fulltext.].",

author = "D. Vacondio and {Nogueira Pinto}, H. and L. Coenen and Mulder, {I. A.} and R. Fontijn and {van het Hof}, B. and Fung, {W. K.} and A. Jongejan and G. Kooij and N. Zelcer and Rozemuller, {A. J.} and {de Vries}, {H. E.} and {de Wit}, {N. M.}",

note = "Funding Information: The authors wish to thank Dr. Couraud (Institute Cochin, Universit{\'e} Paris Descartes, Paris, France) for providing the human BEC line hCMEC/D3, Dr. Dirk Geerts and Peter. J. M. Stroeken for providing the construct for the knockdowns development. The Advanced Optical Microscopy core facility in O | 2 (AO | 2 M) for their expertise and help with the microscopy applications ( http://www.ao2m.amsterdam ). This work was supported by grants to NMdW from ZonMw Onderzoeksprogramma Dementie (project nr: 10510022110005). This work was supported by an out-of-the-box grant from the ACS institute of the AUMC. NZ is supported by a Vici grant from the Netherlands Organization for Scientific Research (NWO; 016.176.643).” Funding Information: The authors wish to thank Dr. Couraud (Institute Cochin, Universit{\'e} Paris Descartes, Paris, France) for providing the human BEC line hCMEC/D3, Dr. Dirk Geerts and Peter. J. M. Stroeken for providing the construct for the knockdowns development. The Advanced Optical Microscopy core facility in O | 2 (AO | 2 M) for their expertise and help with the microscopy applications (http://www.ao2m.amsterdam). This work was supported by grants to NMdW from ZonMw Onderzoeksprogramma Dementie (project nr: 10510022110005). This work was supported by an out-of-the-box grant from the ACS institute of the AUMC. NZ is supported by a Vici grant from the Netherlands Organization for Scientific Research (NWO; 016.176.643).” Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = nov,

day = "1",

doi = "https://doi.org/10.1038/s41419-023-06316-8",

language = "English",

volume = "14",

pages = "781",

journal = "Cell Death & Disease",

issn = "2041-4889",

publisher = "Nature Publishing Group",

number = "11",

}

Vacondio, D, Nogueira Pinto, H, Coenen, L , Mulder, IA , Fontijn, R, van het Hof, B, Fung, WK, Jongejan, A, Kooij, G , Zelcer, N , Rozemuller, AJ , de Vries, HE & de Wit, NM 2023, 'Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2', Cell Death & Disease, vol. 14, no. 11, 781, pp. 781. https://doi.org/10.1038/s41419-023-06316-8, https://doi.org/10.1038/s41419-023-06316-8

TY - JOUR

T1 - Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2

AU - Vacondio, D.

AU - Nogueira Pinto, H.

AU - Coenen, L.

AU - Mulder, I. A.

AU - Fontijn, R.

AU - van het Hof, B.

AU - Fung, W. K.

AU - Jongejan, A.

AU - Kooij, G.

AU - Zelcer, N.

AU - Rozemuller, A. J.

AU - de Vries, H. E.

AU - de Wit, N. M.

N1 - Funding Information: The authors wish to thank Dr. Couraud (Institute Cochin, Université Paris Descartes, Paris, France) for providing the human BEC line hCMEC/D3, Dr. Dirk Geerts and Peter. J. M. Stroeken for providing the construct for the knockdowns development. The Advanced Optical Microscopy core facility in O | 2 (AO | 2 M) for their expertise and help with the microscopy applications ( http://www.ao2m.amsterdam ). This work was supported by grants to NMdW from ZonMw Onderzoeksprogramma Dementie (project nr: 10510022110005). This work was supported by an out-of-the-box grant from the ACS institute of the AUMC. NZ is supported by a Vici grant from the Netherlands Organization for Scientific Research (NWO; 016.176.643).” Funding Information: The authors wish to thank Dr. Couraud (Institute Cochin, Université Paris Descartes, Paris, France) for providing the human BEC line hCMEC/D3, Dr. Dirk Geerts and Peter. J. M. Stroeken for providing the construct for the knockdowns development. The Advanced Optical Microscopy core facility in O | 2 (AO | 2 M) for their expertise and help with the microscopy applications (http://www.ao2m.amsterdam). This work was supported by grants to NMdW from ZonMw Onderzoeksprogramma Dementie (project nr: 10510022110005). This work was supported by an out-of-the-box grant from the ACS institute of the AUMC. NZ is supported by a Vici grant from the Netherlands Organization for Scientific Research (NWO; 016.176.643).” Publisher Copyright: © 2023, The Author(s).

PY - 2023/11/1

Y1 - 2023/11/1

N2 - In Alzheimer’s disease (AD) more than 50% of the patients are affected by capillary cerebral amyloid-angiopathy (capCAA), which is characterized by localized hypoxia, neuro-inflammation and loss of blood-brain barrier (BBB) function. Moreover, AD patients with or without capCAA display increased vessel number, indicating a reactivation of the angiogenic program. The molecular mechanism(s) responsible for BBB dysfunction and angiogenesis in capCAA is still unclear, preventing a full understanding of disease pathophysiology. The Liver X receptor (LXR) family, consisting of LXRα and LXRβ, was reported to inhibit angiogenesis and particularly LXRα was shown to secure BBB stability, suggesting a major role in vascular function. In this study, we unravel the regulatory mechanism exerted by LXRα to preserve BBB integrity in human brain endothelial cells (BECs) and investigate its role during pathological conditions. We report that LXRα ensures BECs identity via constitutive inhibition of the transcription factor SNAI2. Accordingly, deletion of brain endothelial LXRα is associated with impaired DLL4-NOTCH signalling, a critical signalling pathway involved in vessel sprouting. A similar response was observed when BECs were exposed to hypoxia, with concomitant LXRα decrease and SNAI2 increase. In support of our cell-based observations, we report a general increase in vascular SNAI2 in the occipital cortex of AD patients with and without capCAA. Importantly, SNAI2 strongly associated with vascular amyloid-beta deposition and angiopoietin-like 4, a marker for hypoxia. In hypoxic capCAA vessels, the expression of LXRα may decrease leading to an increased expression of SNAI2, and consequently BECs de-differentiation and sprouting. Our findings indicate that LXRα is essential for BECs identity, thereby securing BBB stability and preventing aberrant angiogenesis. These results uncover a novel molecular pathway essential for BBB identity and vascular homeostasis providing new insights on the vascular pathology affecting AD patients. [Figure not available: see fulltext.].

AB - In Alzheimer’s disease (AD) more than 50% of the patients are affected by capillary cerebral amyloid-angiopathy (capCAA), which is characterized by localized hypoxia, neuro-inflammation and loss of blood-brain barrier (BBB) function. Moreover, AD patients with or without capCAA display increased vessel number, indicating a reactivation of the angiogenic program. The molecular mechanism(s) responsible for BBB dysfunction and angiogenesis in capCAA is still unclear, preventing a full understanding of disease pathophysiology. The Liver X receptor (LXR) family, consisting of LXRα and LXRβ, was reported to inhibit angiogenesis and particularly LXRα was shown to secure BBB stability, suggesting a major role in vascular function. In this study, we unravel the regulatory mechanism exerted by LXRα to preserve BBB integrity in human brain endothelial cells (BECs) and investigate its role during pathological conditions. We report that LXRα ensures BECs identity via constitutive inhibition of the transcription factor SNAI2. Accordingly, deletion of brain endothelial LXRα is associated with impaired DLL4-NOTCH signalling, a critical signalling pathway involved in vessel sprouting. A similar response was observed when BECs were exposed to hypoxia, with concomitant LXRα decrease and SNAI2 increase. In support of our cell-based observations, we report a general increase in vascular SNAI2 in the occipital cortex of AD patients with and without capCAA. Importantly, SNAI2 strongly associated with vascular amyloid-beta deposition and angiopoietin-like 4, a marker for hypoxia. In hypoxic capCAA vessels, the expression of LXRα may decrease leading to an increased expression of SNAI2, and consequently BECs de-differentiation and sprouting. Our findings indicate that LXRα is essential for BECs identity, thereby securing BBB stability and preventing aberrant angiogenesis. These results uncover a novel molecular pathway essential for BBB identity and vascular homeostasis providing new insights on the vascular pathology affecting AD patients. [Figure not available: see fulltext.].

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U2 - https://doi.org/10.1038/s41419-023-06316-8

DO - https://doi.org/10.1038/s41419-023-06316-8

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SN - 2041-4889

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SP - 781

JO - Cell Death & Disease

JF - Cell Death & Disease

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M1 - 781

ER -

Liver X receptor alpha ensures blood-brain barrier function by suppressing SNAI2

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