Keyword search (4,164 papers available)

"Misic B" Authored Publications:

Title Authors PubMed ID
1 Mapping cerebral blood perfusion and its links to multi-scale brain organization across the human lifespan Farahani A; Liu ZQ; Ceballos EG; Hansen JY; Wennberg K; Zeighami Y; Dadar M; Gauthier CJ; Dagher A; Misic B; 40729400
PHYSICS
2 Benchmarking macaque brain gene expression for horizontal and vertical translation Luppi AI; Liu ZQ; Hansen JY; Cofre R; Niu M; Kuzmin E; Froudist-Walsh S; Palomero-Gallagher N; Misic B; 40020056
BIOLOGY
3 Correspondence between gene expression and neurotransmitter receptor and transporter density in the human brain Hansen JY; Markello RD; Tuominen L; Nørgaard M; Kuzmin E; Palomero-Gallagher N; Dagher A; Misic B; 36209794
CSBN
4 Numerical uncertainty in analytical pipelines lead to impactful variability in brain networks Kiar G; Chatelain Y; de Oliveira Castro P; Petit E; Rokem A; Varoquaux G; Misic B; Evans AC; Glatard T; 34724000
ENCS

 

Title:Mapping cerebral blood perfusion and its links to multi-scale brain organization across the human lifespan
Authors:Farahani ALiu ZQCeballos EGHansen JYWennberg KZeighami YDadar MGauthier CJDagher AMisic B
Link:https://pubmed.ncbi.nlm.nih.gov/40729400/
DOI:10.1371/journal.pbio.3003277
Publication:PLoS biology
Keywords:
PMID:40729400 Category: Date Added:2025-07-29
Dept Affiliation: PHYSICS
1 Montréal Neurological Institute, McGill University, Montréal, Québec, Canada.
2 Douglas Mental Health Institute, McGill University, Montréal, Québec, Canada.
3 Department of Physics, Concordia University, Montréal, Québec, Canada.
4 Montréal Heart Institute, Montréal, Québec, Canada.

Description:

Blood perfusion delivers oxygen and nutrients to all cells, making it a fundamental feature of brain organization. How cerebral blood perfusion maps onto micro-, meso- and macro-scale brain structure and function is therefore a key question in neuroscience. Here we analyze pseudo-continuous arterial spin labeling (ASL) data from [Formula: see text] healthy individuals in the HCP Lifespan studies (5-22 and 36-100 years) to reconstruct a high-resolution normative cerebral blood perfusion map. At the cellular and molecular level, cerebral blood perfusion co-localizes with granular layer IV, biological pathways for maintenance of cellular relaxation potential and mitochondrial organization, and with neurotransmitter and neuropeptide receptors involved in vasomodulation. At the regional level, blood perfusion aligns with cortical arealization and is greatest in regions with high metabolic demand and resting-state functional hubs. Looking across individuals, blood perfusion is dynamic throughout the lifespan, follows micro-architectural changes in development, and maps onto individual differences in physiological changes in aging. In addition, we find that cortical atrophy in multiple neurodegenerative diseases (late-onset Alzheimer's disease, TDP-43C, and dementia with Lewy bodies) is most pronounced in regions with lower perfusion, highlighting the utility of perfusion topography as an indicator of transdiagnostic vulnerability. Finally, we show that ASL-derived perfusion can be used to delineate arterial territories in a data-driven manner, providing insights into how the vascular system is linked to human brain function. Collectively, this work highlights how cerebral blood perfusion is central to, and interlinked with, multiple structural and functional systems in the brain.





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