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[Press Release] Piecing the Puzzle Together: How Different Brain Regions Contribute to Visual Object Memory

Update:2024年8月26日更新
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Chiba, August 21, 2024

 

Piecing the Puzzle Together: How Different Brain Regions Contribute to Visual Object Memory 

 

Animal experiments shed light on the functions and layout of brain networks involved in memory in primates 

 

While the anterior ventral temporal cortex is known to be crucial for visual object memory, the way in which it is regulated by higher cognitive areas in the brain remains unclear. Researchers from Japan have now addressed this gap through extensive experiments on macaques engaged in visual memory tasks, examining both large-scale brain networks and individual neuron activity. Their findings clarify the functions of different brain regions and could facilitate the development of neurological treatments.

 

Visual object memory refers to our brain's ability to store, recognize, and recall visual information about objects we perceive. This capability is essential for interacting with the world, influencing learning, problem-solving, navigation, and social interactions. Without effective visual object memory, these activities would be nearly impossible. Consequently, many neuroscientists have been making dedicated attempts to uncover the mechanisms behind this critical aspect of cognition in both humans and animals.

 

Numerous studies on primates engaged in memory tasks have established that the anterior ventral temporal cortex (aVTC) is crucial for visual object memory. Neurons in this region can represent complex visual objects, suggesting that they can function in visual object memory even without direct visual input, relying instead on regulatory signals from higher cognitive areas. Despite this understanding, the specifics of this "top-down" regulation and the broader functional network that includes aVTC remain unclear.

 

In an effort to answer these questions, a research team from Japan conducted an in-depth investigation to shed light on this elusive issue. Led by Senior Research Scientist Toshiyuki Hirabayashi from the National Institutes for Quantum Science and Technology (QST), they conducted various types of experiments on macaques performing visual memory tasks. Their latest paper was published in Nature Communications on July 10, 2024 and was co-authored by Takafumi Minamimoto from the Advanced Neuroimaging Center, QST. 

 

First, the researchers ran functional positron emission tomography scans on macaques during a visual recall task, which enabled them to pinpoint brain regions with higher activity by measuring minute changes in blood flow. They combined these measurements with functional magnetic resonance imaging data, taken previously over a large population of macaques, which quantified the connectivity between different brain areas. In this way, they identified specific nodes within the aVTC and the orbitofrontal cortex (OFC) as essential members of the network governing visual object memory. 

 

To cement these findings, they conducted chemogenetic silencing experiments. Simply put, they genetically modified the OFC of macaques using a viral vector to introduce custom-designed receptors to the neurons. These receptors prevent the firing of the neurons, but only in the presence of a very specific designer drug. The team observed that the monkeys performed significantly worse in the visual recall tasks when the OFC was chemically silenced, which did not impair their visual perception in any way. 

 

Nonetheless, the researchers wanted to take their analysis one step further, and so, they explored the small-scale details governing visual object memory in the aVTC and OFC. “Both the macroscale identification of brain network nodes and the subsequent microscale, cellular-level understanding of causal information flow along the identified nodes are required for a comprehensive understanding of the network mechanisms underpinning object memory,” remarks Hirabayashi. To this end, they conducted single-neuron recordings in the aVTC of the same macaques used in previous experiments, assessing the memory-related activity and higher-order modulation in these neurons. They found that the memory-related activity of individual aVTC neurons, but not perception-related activity, was specifically attenuated by OFC silencing. This was consistent with the behavioral results obtained earlier. Furthermore, similar changes in neuronal activity occurred when the monkeys made a mnemonic error in the task prior to OFC silencing, suggesting the behavioral relevance of the memory-related activity in individual aVTC neurons, which was supported by top-down inputs from the OFC.

 

Together, these analyses helped the team obtain a detailed understanding of the mechanisms underpinning short-term visual object memory in primates. Given that our brains share many functional and structural characteristics with those of these animals, the findings of this study can ultimately help in understanding ourselves better as well. Worth noting, this could have important implications in medicine. As Hirabayashi explains, “The discovered network mechanisms in non-human primates could provide a mechanistic understanding of related memory deficits that occur in human dementia.” Adding further, he says, “The artificial neuromodulation of the currently discovered network in patients with dementia might restore their visual memory functions.

 

Let us hope this work serves as a stepping stone towards a more comprehensive understanding of the most complex object known in the known universe—the human brain. 

 

brain-wide network

 

Image title: Newfound brain-wide network and its role in visual object memory

Image caption: Diagram of the ventral fronto-temporal network operations necessary for visual object memory. During perception (left), neurons in the anterior ventral temporal cortex (aVTC) are primarily activated by bottom-up visual input, while the effect of top-down regulation from the orbitofrontal cortex (OFC) remains minimal. During memory retention without visual input (right), top-down signals from the OFC upregulate the aVTC neurons, which represent behaviorally relevant item information.

Image source: Toshiyuki Hirabayashi from National Institutes for Quantum Science and Technology

License type: Original content

Usage restrictions: Cannot be reused without permission

 

 

Reference

Title of original paper:

Multiscale chemogenetic dissection of fronto-temporal top-down regulation for object memory in primates

Journal

Nature Communications

DOI:

10.1038/s41467-024-49570-w

 

 

About National Institutes for Quantum Science and Technology, Japan

The National Institutes for Quantum Science and Technology (QST) was established in April 2016 to promote quantum science and technology in a comprehensive and integrated manner. The new organization was formed from the merger of the National Institute of Radiological Sciences (NIRS) with certain operations that were previously undertaken by the Japan Atomic Energy Agency (JAEA). QST is committed to advancing quantum science and technology, creating world-leading research and development platforms, and exploring new fields, thereby achieving significant academic, social, and economic impacts.

 

 

 

Website: https://www.qst.go.jp/site/qst-english/

 

 

About Senior Research Scientist Toshiyuki Hirabayashi from National Institutes for Quantum Science and Technology, Japan

Dr. Toshiyuki Hirabayashi is a Senior Research Scientist in the Advanced Neuroimaging Center at the National Institutes for Quantum Science and Technology (QST), Japan. He obtained his Ph.D. from the University of Tokyo School of Medicine in 2006. He then joined his alma mater as a research associate in 2007, becoming a university lecturer by 2013. In 2015, he became a senior researcher at the National Institute of Radiological Sciences (NIRS), which later became QST. Dr. Hirabayashi’s research interests include functional neural circuits, memory retrieval, and fMRI/electrophysiology with chemogenetics in macaques. In 2014, he was awarded a Japan Neuroscience Society Young Investigator Award. 

 

 

Media contact:

International Affairs and Public Relations Section

Department of International Affairs and Public Relations

Tel: +81-43-206-3026 Email: info@qst.go.jp