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	<title>Institute for Basic Science study &#8211; Science</title>
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		<title>Study uncovers how astrocytes enable long-term memory</title>
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		<pubDate>Tue, 07 Jul 2026 22:40:09 +0000</pubDate>
				<category><![CDATA[Social Science]]></category>
		<category><![CDATA[ankyrin-2]]></category>
		<category><![CDATA[astrocyte gatekeepers]]></category>
		<category><![CDATA[astrocytes]]></category>
		<category><![CDATA[glial cells]]></category>
		<category><![CDATA[Institute for Basic Science study]]></category>
		<category><![CDATA[long-term memory]]></category>
		<category><![CDATA[memory consolidation]]></category>
		<category><![CDATA[memory persistence]]></category>
		<category><![CDATA[Nature Communications.]]></category>
		<category><![CDATA[neural circuit stabilization]]></category>
		<category><![CDATA[remote memory deficits]]></category>
		<category><![CDATA[scaffolding protein]]></category>
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					<description><![CDATA[For a memory to last a lifetime, the brain must do more than simply encode an experience—it must actively preserve it. Yet the biological machinery that decides whether a recollection fades within weeks or survives for decades has remained stubbornly opaque. A study published in Nature Communications now reveals that the key is not found [&#8230;]]]></description>
										<content:encoded><![CDATA[<p>For a memory to last a lifetime, the brain must do more than simply encode an experience—it must actively preserve it. Yet the biological machinery that decides whether a recollection fades within weeks or survives for decades has remained stubbornly opaque. A study published in <em>Nature Communications</em> now reveals that the key is not found in neurons alone but in astrocytes, the star-shaped glial cells long relegated to a support role. Researchers at the Institute for Basic Science in South Korea have demonstrated that these cells act as gatekeepers of memory persistence, orchestrating a molecular dialogue that stabilizes the neural circuits holding our most enduring memories.</p>
<p>The team, led by neuroscientist Koh Wuhyun, focused on ankyrin-2 (Ank2), a scaffolding protein expressed abundantly in astrocytes. To test its role, they engineered mice in which the <em>Ank2</em> gene was selectively deleted from these glial cells. Immediately after learning a task, the mutant mice performed identically to their normal littermates: recent memory was fully intact. Two weeks later, however, the picture had changed dramatically. The same animals showed profound deficits in remote memory, unable to recall what they had once known. The dissociation was striking, proving that the formation of a memory and its long-term maintenance rely on biologically distinct processes, and that astrocytes are central to the latter.</p>
<p>Microscopic analysis offered a structural explanation. Astrocytes lacking Ank2 exhibited drastically simplified architectures, their elaborate branches retracted. More critically, they formed far fewer physical contacts with engram neurons, the very cells that store a specific memory trace. These astrocyte-to-neuron contacts, induced by learning, are thought to stabilize synaptic ensembles over time. Without them, the circuit-level consolidation that anchors long-term potentiation (LTP)—the persistent strengthening of synapses widely considered a cellular correlate of memory—began to falter. Remarkably, baseline synaptic transmission remained normal, indicating a specific failure in the machinery of maintenance rather than general neuronal dysfunction.</p>
<p>At a molecular level, the study traced the defect to a signaling cascade involving brain-derived neurotrophic factor (BDNF). Astrocytes receive BDNF through the truncated receptor TrkB.T1, which couples to intracellular calcium release via IP3R2 channels. Ank2, the researchers discovered, is required for the stability of this calcium signaling hub. When Ank2 was absent, BDNF-stimulated calcium transients weakened, and the structural remodeling that normally follows learning ground to a halt. Direct infusion of BDNF into the hippocampus, which typically bolsters remote memory, became completely ineffective in the knockout animals, confirming that astrocytic Ank2 is indispensable for BDNF-dependent memory stabilization.</p>
<p>To establish causality in the opposite direction, the team built an optogenetic tool named Opto-T1, which uses light to selectively activate TrkB.T1 signaling in astrocytes. Stimulating this pathway induced robust astrocytic remodeling, reinforced LTP, and significantly extended the lifespan of remote memories, all without altering recent recall. It was a clean demonstration that astrocytes are not passive partners but active, sufficient drivers of memory perseverance. The finding flips the neuron-centric script, placing glia at the heart of cognitive endurance.</p>
<p>“Our findings show that astrocytes are not passive support cells, but active regulators that determine how long memories last,” Koh said. “By identifying Ank2 as a key regulator of astrocyte remodeling and BDNF signaling, we have uncovered a new mechanism that helps stabilize long-term memories and opens new avenues for understanding and potentially treating memory disorders.”</p>
<p>The implications travel well beyond basic neuroscience. Variants in the <em>ANK2</em> gene have been linked to autism spectrum disorder, intellectual disability, and epilepsy. The new work suggests that disrupted astrocyte-neuron coupling may be a common thread uniting these conditions, offering a fresh conceptual framework for how glial dysfunction could erode cognitive stability. Moreover, the findings raise the possibility that targeting astrocytic BDNF pathways could one day help sustain memories in the face of aging or neurodegenerative disease. As the population ages and the burden of memory-related disorders grows, the notion that astrocytes can be commandeered to reinforce fading recollections moves from speculative to tantalizingly concrete.</p>
<p>The study, published on July 7, 2026, in <em>Nature Communications</em>, marks a watershed in memory research. It reveals that the brain’s “support cells” are in fact arbiters of our cognitive past, sculpting the very contours of our personal histories. By shining a light—literally, via optogenetics—on the hidden work of astrocytes, the research opens a path toward therapies that might one day ensure our most precious memories are not merely formed, but faithfully kept.</p>
<p><strong>Subject of Research</strong>: Mice (Animals)<br />
<strong>Article Title</strong>: Astrocytic Ankyrin-2 Enables Memory Persistence in the Mouse Hippocampus<br />
<strong>News Publication Date</strong>: July 7, 2026<br />
<strong>Web References</strong>: <a href="https://dx.doi.org/10.1038/s41467-026-75009-5">https://dx.doi.org/10.1038/s41467-026-75009-5</a><br />
<strong>References</strong>: Nature Communications, 2026; DOI: 10.1038/s41467-026-75009-5<br />
<strong>Image Credits</strong>: Institute for Basic Science<br />
<strong>Keywords</strong>: memory persistence, astrocytes, ankyrin-2, BDNF, TrkB.T1, IP3R2, calcium signaling, long-term potentiation, hippocampus, optogenetics, engram, memory consolidation</p>
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