Literature DB >> 29543430

Newly Identified Aplysia SPTR-Gene Family-Derived Peptides: Localization and Function.

Guo Zhang1, Wang-Ding Yuan1, Ferdinand S Vilim2, Elena V Romanova3, Ke Yu1, Si-Yuan Yin1, Zi-Wei Le1, Ying-Yu Xue1, Ting-Ting Chen1, Guo-Kai Chen1, Song-An Chen1, Elizabeth C Cropper2, Jonathan V Sweedler3, Klaudiusz R Weiss2, Jian Jing1,2.   

Abstract

When individual neurons in a circuit contain multiple neuropeptides, these peptides can target different sets of follower neurons. This endows the circuit with a certain degree of flexibility. Here we identified a novel family of peptides, the Aplysia SPTR-Gene Family-Derived peptides (apSPTR-GF-DPs). We demonstrated apSPTR-GF-DPs, particularly apSPTR-GF-DP2, are expressed in the Aplysia CNS using immunohistochemistry and MALDI-TOF MS. Furthermore, apSPTR-GF-DP2 is present in single projection neurons, e.g., in the cerebral-buccal interneuron-12 (CBI-12). Previous studies have demonstrated that CBI-12 contains two other peptides, FCAP/CP2. In addition, CBI-12 and CP2 promote shortening of the protraction phase of motor programs. Here, we demonstrate that FCAP shortens protraction. Moreover, we show that apSPTR-GF-DP2 also shortens protraction. Surprisingly, apSPTR-GF-DP2 does not increase the excitability of retraction interneuron B64. B64 terminates protraction and is modulated by FCAP/CP2 and CBI-12. Instead, we show that apSPTR-GF-DP2 and CBI-12 increase B20 excitability and B20 activity can shorten protraction. Taken together, these data indicate that different CBI-12 peptides target different sets of pattern-generating interneurons to exert similar modulatory actions. These findings provide the first definitive evidence for SPTR-GF's role in modulation of feeding, and a form of molecular degeneracy by multiple peptide cotransmitters in single identified neurons.

Entities:  

Keywords:  Aplysia; SPTR-Gene Family-Derived peptides; feeding; neuromodulation; neuropeptides; projection interneuron

Mesh:

Substances:

Year:  2018        PMID: 29543430      PMCID: PMC6093785          DOI: 10.1021/acschemneuro.7b00513

Source DB:  PubMed          Journal:  ACS Chem Neurosci        ISSN: 1948-7193            Impact factor:   4.418


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