Figure 1.

A minimal model for protein synthesis as a trigger for long-term memory formation. The model summarized in this figure makes a large number of assumptions for simplicity’s sake: that these events occur locally at a dendritic spine, and that the process is NMDA receptor-dependent. The model does not specify molecules or mechanisms, and it ignores the need for altered gene expression. In this model a memory-causing event such as a set of appropriately contingent environmental signals leads to NMDA receptor activation and the subsequent formation of a memory engram. NMDA receptor activation recruits signal transduction mechanisms to precipitate an altered rate of synthesis of a subset of synaptic proteins. This altered protein synthesis is in addition to “housekeeping” protein synthesis that contributes to ongoing maintenance of the dendritic spine (blue pathway). Also, the spine maintains constitutive synthesis of effector proteins that when complexed with the appropriate partners can increase synaptic strength (the green pathway). The targets of the signal for altered protein synthesis (the red pathway) comprise the appropriate partners for the green pathway, in order to increase synaptic strength. Thus, the altered synthesis of the appropriate proteins is the trigger for synaptic potentiation, and the “new” proteins interact with other proteins already present to effect the change. The effector protein complex is the readout of the altered protein synthesis. The red pathway becomes quasi-constitutive by a positive feedback mechanism. Thus, the triggering mechanism can perpetuate itself by one of two possible mechanisms. First, it might promote its own re-synthesis at a new higher rate locally in order to perpetuate the altered spectrum (or rate) of synthesis of a subset of local effector proteins. This mechanism is what is illustrated in this figure. Alternatively and minimally, the complex might perpetuate itself by an increased rate of recruitment to the locale of a protein synthesized globally throughout the cell. One of these two mechanisms is the maintenance mechanism at the molecular level. The self-perpetuating structural/functional change is a component of the engram, and serves as a molecular basis for memory storage.