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Human proteins identified that explain inter-individual differences in functional brain connectivity

Date:
October 31, 2024
Source:
University of Alabama at Birmingham
Summary:
A long-standing goal of neuroscience is to understand how molecules and cellular structures on a microscale give rise to communication between brain regions at the macroscale. A study now identifies, for the first time, hundreds of brain proteins that explain inter-individual differences in functional connectivity and structural covariation in the human brain.
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A long-standing goal of neuroscience is to understand how molecules and cellular structures on a microscale give rise to communication between brain regions at the macroscale. A study published in Nature Neuroscience now identifies, for the first time, hundreds of brain proteins that explain inter-individual differences in functional connectivity and structural covariation in the human brain.

"A central goal of neuroscience is to develop an understanding of the brain that ultimately describes the mechanistic basis of human cognition and behavior," said Jeremy Herskowitz, Ph.D., associate professor in the University of Alabama at Birmingham Department of Neurology and co-corresponding author of the study with Chris Gaiteri, Ph.D., SUNY Upstate Medical University, Syracuse, New York. "This study demonstrates the feasibility of integrating data from vastly different biophysical scales to provide a molecular understanding of human brain connectivity."

Bridging the gap from the molecular scale of proteins and mRNA to the brain-wide neuroimaging scale of functional and structural magnetic resonance imaging -- a span of about seven orders of magnitude -- was made possible by the Religious Orders Study and Rush Memory and Aging Project, or ROSMAP, at Rush University, Chicago, Illinois.

ROSMAP enrolls Catholic nuns, priests and brothers age 65 or older, who are without known dementia at time of enrollment. Participants receive medical and psychological evaluations each year and agree to donate their brains after death.

Herskowitz, Gaiteri and colleagues studied postmortem brain samples and data from a unique cohort of 98 ROSMAP participants. Their data types included resting state fMRI, structural MRI, genetics, dendritic spine morphometry, proteomics and gene expression measurements from the superior frontal gyrus and inferior temporal gyrus of the brain.

"Based on the stability of functional connectivity patterns within individuals, we hypothesized that it is possible to combine postmortem molecular and subcellular data with antemortem neuroimaging data from the same individuals to prioritize molecular mechanisms underlying brain connectivity," Herskowitz said.

The average age of the ROSMAP participants at time of MRI scan and at death were 88 +/- 6 years and 91 +/- 6 years, respectively, with an average time interval between the MRI scan and age at death of 3 +/- 2 years. The average postmortem interval to brain sampling was 8.5 +/- 4.6 hours. In the study, the researchers performed detailed characterization of each omic, cellular and neuroimaging data type, then integrated the different data types using computational clustering algorithms.

The key to the research was using an intermediate scale measurement -- dendritic spine morphometry, the shapes, sizes and densities of the spines -- to link the molecular scale with the brain-wide neuroimaging scale. The integration of dendritic spine morphometry to contextualize the proteomic and transcriptomic signals was critical for detecting protein association with functional connectivity. "Initially, the protein and RNA measures could not explain the person-to-person variability in functional connectivity; however, it all clicked once we integrated the dendritic spine morphology to bridge the gap from molecules to inter-brain region communication," Herskowitz said.

A dendrite is a branched extension from a neuron body that receives impulses from other neurons. Each dendrite can have thousands of small protrusions called spines. The head of each spine can form a contact point called a synapse to receive an impulse sent from the axon of another neuron. Dendritic spines can rapidly change shape or volume while forming new synapses, part of the process called brain plasticity, and the head of the spine structurally supports postsynaptic density. Spines can be divided into shape subclasses based on their three-dimensional structure as thin, mushroom, stubby or filopodia. This summer, in a different study, Herskowitz and colleagues used ROSMAP samples to show that preservation of memory in the very old was maintained by the quality, as measured by dendritic spine head diameter, not the quantity of synapses in the brain.

In this latest study, the hundreds of proteins the researchers identified that explain inter-individual differences in functional connectivity and structural covariation were enriched for proteins involved in synapses, energy metabolism and RNA processing. "By integrating data at the genetic, molecular, subcellular and tissue levels, we linked specific biochemical changes at synapses to connectivity between brain regions," Herskowitz said.

"Overall, this study indicates that acquiring data across the major perspectives in human neuroscience from the same set of brains is foundational for understanding how human brain function is supported at multiple biophysical scales," Herskowitz said. "While future research is necessary for fully determining the scope and components of multi-scale brain synchrony, we have established a robustly defined initial set of molecules whose effects likely resonate across biophysical scales."

Besides Herskowitz and Gaiteri, co-authors of the study, "Multiscale Integration Identifies Synaptic Proteins Associated with Human Brain Connectivity," are Bernard Ng, Shinya Tasaki and David A. Bennett, Rush University Medical Center, Chicago, Illinois; Kelsey M. Greathouse, Courtney K. Walker, Audrey J. Weber, Ashley B. Adamson, Julia P. Andrade, Emily H. Poovey, Kendall A. Curtis and Hamad M. Muhammad, UAB Department of Neurology and Center for Neurodegeneration and Experimental Therapeutics; Ada Zhang, SUNY Upstate Medical University; Sydney Covitz, Matt Cieslak, Jakob Seidlitz, Ted Satterthwaite and Jacob Vogel, University of Pennsylvania, Philadelphia, Pennsylvania; and Nicholas T. Seyfried, Emory University School of Medicine, Atlanta, Georgia.

Support came from National Institutes of Health grants AG061800, AG061798, AG057911, AG067635, AG054719, AG063755, AG068024, NS061788, AG10161, AG72975, AG15819, AG17917, AG46152 and AG61356.

At UAB, Neurology is a department in the Marnix E. Heersink School of Medicine.


Story Source:

Materials provided by University of Alabama at Birmingham. Original written by Jeff Hansen. Note: Content may be edited for style and length.


Journal Reference:

  1. Bernard Ng, Shinya Tasaki, Kelsey M. Greathouse, Courtney K. Walker, Ada Zhang, Sydney Covitz, Matt Cieslak, Audrey J. Weber, Ashley B. Adamson, Julia P. Andrade, Emily H. Poovey, Kendall A. Curtis, Hamad M. Muhammad, Jakob Seidlitz, Ted Satterthwaite, David A. Bennett, Nicholas T. Seyfried, Jacob Vogel, Chris Gaiteri, Jeremy H. Herskowitz. Integration across biophysical scales identifies molecular and cellular correlates of person-to-person variability in human brain connectivity. Nature Neuroscience, 2024; DOI: 10.1038/s41593-024-01788-z

Cite This Page:

University of Alabama at Birmingham. "Human proteins identified that explain inter-individual differences in functional brain connectivity." ScienceDaily. ScienceDaily, 31 October 2024. <www.sciencedaily.com/releases/2024/10/241031124556.htm>.
University of Alabama at Birmingham. (2024, October 31). Human proteins identified that explain inter-individual differences in functional brain connectivity. ScienceDaily. Retrieved November 20, 2024 from www.sciencedaily.com/releases/2024/10/241031124556.htm
University of Alabama at Birmingham. "Human proteins identified that explain inter-individual differences in functional brain connectivity." ScienceDaily. www.sciencedaily.com/releases/2024/10/241031124556.htm (accessed November 20, 2024).

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