Controllable gap junctions by vitamin B12 and light

Duo Cui, Shuzhang Liu, Xinyu Huang, Xiaohan Alex Tang, Min Zheng, Zonglin He, Rui Xu, Chenbo Sun, Yingjie Xu, Renjun Tu*, Peng Zou*, Ting Xie*, Fei Sun*

*Corresponding author for this work

Research output: Contribution to journalJournal Articlepeer-review

Abstract

Gap junctions mediate rapid signal transduction between contiguous cells, which are indispensable for multicellular organisms to coordinate cellular activities across numerous physiological processes. However, precise control of gap junctions remains elusive. Herein, we present CarGAP, a single-component chemo-optogenetic tool that utilizes the C-terminal adenosylcobalamin (AdoB12) binding domain of a photoreceptor protein (i.e., CarHC) to achieve reversible control over both vertebrate and invertebrate gap junctions with spatiotemporal precision. The vertebrate CarGAP (i.e., Cx-CarGAP), created by genetically fusing connexins with CarHC in mammalian cells, can efficiently block the gap junction channels through AdoB12-induced protein oligomerization and subsequently reinstate them via green light-induced protein disassembly. We further introduced the CarGAP system (i.e., Inx-CarGAP) to the Drosophila ovary, enabling reversible control over the heterotypic gap junctions formed by innexin2 (Inx2) and innexin4 (Inx4, also known as zero population growth, Zpg), thereby uncovering the roles of gap junctions in stem cell-niche interactions. This study illustrates CarGAP as a generalizable chemo-optogenetic tool for interrogating the functions of gap junctions in various biological contexts.

Original languageEnglish
Pages (from-to)e2518037122
JournalProceedings of the National Academy of Sciences of the United States of America
Volume122
Issue number52
Early online date23 Dec 2025
DOIs
Publication statusPublished - 30 Dec 2025

Keywords

  • chemogenetics
  • gap junction
  • stem cell niche

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