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Publication : 14-3-3ζ is crucial for the conversion of labile short-term object recognition memory into stable long-term memory.

First Author  Navarro-Lobato I Year  2021
Journal  J Neurosci Res Volume  99
Issue  9 Pages  2305-2317
PubMed ID  34115908 Mgi Jnum  J:347779
Mgi Id  MGI:7625792 Doi  10.1002/jnr.24894
Citation  Navarro-Lobato I, et al. (2021) 14-3-3zeta is crucial for the conversion of labile short-term object recognition memory into stable long-term memory. J Neurosci Res 99(9):2305-2317
abstractText  The consolidation of new memories into long-lasting memories is multistage process characterized by distinct temporal dynamics. However, our understanding on the initial stage of transformation of labile memory of recent experience into stable memory remains elusive. Here, with the use of rats and mice overexpressing a memory enhancer called regulator of G protein signaling 14 of 414 amino acids (RGS14(414) ) as a tool, we show that the expression of RGS14(414) in male rats' perirhinal cortex (PRh), which is a brain area crucial for object recognition memory (ORM), enhanced the ORM to the extent that it caused the conversion of labile short-term ORM (ST-ORM) expected to last for 40 min into stable long-term ORM (LT-ORM) traceable after a delay of 24 hr, and that the temporal window of 40 to 60 min after object exposure not only was key for this conversion but also was the time frame when a surge in 14-3-3zeta protein was observed. A knockdown of 14-3-3zeta gene abrogated both the increase in 14-3-3zeta protein and the formation of LT-ORM. Furthermore, this 14-3-3zeta upregulation increased brain-derived growth factor (BDNF) levels in the time frame of 60 min and 24 hr and 14-3-3zeta knockdown decreased the BDNF levels, and a deletion of BDNF gene produced loss in mice ability to form LT-ORM. Thus, within 60 min of object exposure, 14-3-3zeta facilitated the conversion of labile ORM into stable ORM, whereas beyond the 60 min, it mediated the consolidation of the stable memory into long-lasting ORM by regulating BDNF signaling.
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