Hemochromatosis neural archetype reveals iron disruption in motor circuits

Robert Loughnan; Jonathan Ahern; Mary Boyle; Terry L Jernigan; Donald J Hagler; John R Iversen; Oleksandr Frei; Diana M Smith; Ole Andreassen; Noah Zaitlen; Leo Sugrue; Wesley K Thompson; Anders Dale; Andrew J Schork; Chun Chieh Fan

doi:10.1126/sciadv.adp4431

Hemochromatosis neural archetype reveals iron disruption in motor circuits

Robert Loughnan, Jonathan Ahern, Mary Boyle, Terry L Jernigan, Donald J Hagler, John R Iversen, Oleksandr Frei, Diana M Smith, Ole Andreassen, Noah Zaitlen, Leo Sugrue, Wesley K Thompson, Anders Dale, Andrew J Schork, Chun Chieh Fan

1 Citationer (Scopus)

Abstract

Our understanding of brain iron regulation and its disruption in disease is limited. Excess iron affects motor circuitry, contributing to Parkinson's disease (PD) risk. The molecular mechanisms regulating central iron levels, beyond a few well-known genes controlling peripheral iron, remain unclear. We generated scores based on the archetypal brain iron accumulation observed in magnetic resonance imaging scans of individuals with excessive dietary iron absorption and hemochromatosis risk. Genome-wide analysis revealed that this score is highly heritable, identifying loci associated with iron homeostasis, and driven by peripheral iron levels. Our score predicted gait abnormalities and showed a U-shaped relationship with PD risk, identifying individuals with threefold increased risk. These results establish a hormetic relationship between brain iron and PD risk, where central iron levels are strongly determined by genetics via peripheral iron. This framework combining forward and reverse genetics is a powerful study design to understand genomic drivers underlying high dimensional phenotypes.

Originalsprog	Engelsk
Artikelnummer	eadp4431
Tidsskrift	Science Advances
Vol/bind	10
Udgave nummer	47
Sider (fra-til)	eadp4431
DOI	https://doi.org/10.1126/sciadv.adp4431
Status	Udgivet - 22 nov. 2024

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Loughnan, R., Ahern, J., Boyle, M., Jernigan, T. L., Hagler, D. J., Iversen, J. R., Frei, O., Smith, D. M., Andreassen, O., Zaitlen, N., Sugrue, L., Thompson, W. K., Dale, A., Schork, A. J., & Fan, C. C. (2024). Hemochromatosis neural archetype reveals iron disruption in motor circuits. Science Advances, 10(47), eadp4431. Artikel eadp4431. https://doi.org/10.1126/sciadv.adp4431

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title = "Hemochromatosis neural archetype reveals iron disruption in motor circuits",

abstract = "Our understanding of brain iron regulation and its disruption in disease is limited. Excess iron affects motor circuitry, contributing to Parkinson's disease (PD) risk. The molecular mechanisms regulating central iron levels, beyond a few well-known genes controlling peripheral iron, remain unclear. We generated scores based on the archetypal brain iron accumulation observed in magnetic resonance imaging scans of individuals with excessive dietary iron absorption and hemochromatosis risk. Genome-wide analysis revealed that this score is highly heritable, identifying loci associated with iron homeostasis, and driven by peripheral iron levels. Our score predicted gait abnormalities and showed a U-shaped relationship with PD risk, identifying individuals with threefold increased risk. These results establish a hormetic relationship between brain iron and PD risk, where central iron levels are strongly determined by genetics via peripheral iron. This framework combining forward and reverse genetics is a powerful study design to understand genomic drivers underlying high dimensional phenotypes.",

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AU - Ahern, Jonathan

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AU - Iversen, John R

AU - Frei, Oleksandr

AU - Smith, Diana M

AU - Andreassen, Ole

AU - Zaitlen, Noah

AU - Sugrue, Leo

AU - Thompson, Wesley K

AU - Dale, Anders

AU - Schork, Andrew J

AU - Fan, Chun Chieh

PY - 2024/11/22

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N2 - Our understanding of brain iron regulation and its disruption in disease is limited. Excess iron affects motor circuitry, contributing to Parkinson's disease (PD) risk. The molecular mechanisms regulating central iron levels, beyond a few well-known genes controlling peripheral iron, remain unclear. We generated scores based on the archetypal brain iron accumulation observed in magnetic resonance imaging scans of individuals with excessive dietary iron absorption and hemochromatosis risk. Genome-wide analysis revealed that this score is highly heritable, identifying loci associated with iron homeostasis, and driven by peripheral iron levels. Our score predicted gait abnormalities and showed a U-shaped relationship with PD risk, identifying individuals with threefold increased risk. These results establish a hormetic relationship between brain iron and PD risk, where central iron levels are strongly determined by genetics via peripheral iron. This framework combining forward and reverse genetics is a powerful study design to understand genomic drivers underlying high dimensional phenotypes.

AB - Our understanding of brain iron regulation and its disruption in disease is limited. Excess iron affects motor circuitry, contributing to Parkinson's disease (PD) risk. The molecular mechanisms regulating central iron levels, beyond a few well-known genes controlling peripheral iron, remain unclear. We generated scores based on the archetypal brain iron accumulation observed in magnetic resonance imaging scans of individuals with excessive dietary iron absorption and hemochromatosis risk. Genome-wide analysis revealed that this score is highly heritable, identifying loci associated with iron homeostasis, and driven by peripheral iron levels. Our score predicted gait abnormalities and showed a U-shaped relationship with PD risk, identifying individuals with threefold increased risk. These results establish a hormetic relationship between brain iron and PD risk, where central iron levels are strongly determined by genetics via peripheral iron. This framework combining forward and reverse genetics is a powerful study design to understand genomic drivers underlying high dimensional phenotypes.

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KW - Parkinson Disease/metabolism

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KW - Genome-Wide Association Study

KW - Magnetic Resonance Imaging

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KW - Female

KW - Middle Aged

KW - Genetic Predisposition to Disease

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Hemochromatosis neural archetype reveals iron disruption in motor circuits

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