Studies using Aplysia californica have demonstrated that transcription after nerve injury occurs during a rapid, transient first phase and a delayed, prolonged second phase. Although the second phase is especially important for regeneration, the mRNAs produced during this phase have not been identified. We characterized two such mRNAs following axotomy. One encodes a novel fasciclin-1 homologue, Aplysia fasciclin-like protein (apFasP), and the other encodes Aplysia beta-thymosin (ap beta T). In addition to mRNA synthesis, proteins required for regeneration must be available at the site of growth, and the transport and local translation of certain extrasomatic mRNAs aids in this process. We found ap beta T and apFasP proteins and mRNA at growth cones in vitro. However, only the mRNA for ap beta T was present in regenerating axons in vivo. This implies that the membrane protein apFasP is supplied by rapid transport from the soma, whereas the soluble ap beta T is synthesized locally.

• 出版日期2005-11-15