AAV-delivered muscone-induced transgene system for treating chronic diseases in mice via inhalation

Author:

Wu XinORCID,Yu YuanhuanORCID,Wang MeiyanORCID,Dai Di,Yin Jianli,Liu WenjingORCID,Kong DeqiangORCID,Tang Shasha,Meng Meiyao,Gao Tian,Zhang Yuanjin,Zhou YangORCID,Guan Ningzi,Zhao ShangangORCID,Ye HaifengORCID

Abstract

AbstractGene therapies provide treatment options for many diseases, but the safe and long-term control of therapeutic transgene expression remains a primary issue for clinical applications. Here, we develop a muscone-induced transgene system packaged into adeno-associated virus (AAV) vectors (AAVMUSE) based on a G protein-coupled murine olfactory receptor (MOR215-1) and a synthetic cAMP-responsive promoter (PCRE). Upon exposure to the trigger, muscone binds to MOR215-1 and activates the cAMP signaling pathway to initiate transgene expression. AAVMUSE enables remote, muscone dose- and exposure-time-dependent control of luciferase expression in the livers or lungs of mice for at least 20 weeks. Moreover, we apply this AAVMUSE to treat two chronic inflammatory diseases: nonalcoholic fatty liver disease (NAFLD) and allergic asthma, showing that inhalation of muscone—after only one injection of AAVMUSE—can achieve long-term controllable expression of therapeutic proteins (ΔhFGF21 or ΔmIL-4). Our odorant-molecule-controlled system can advance gene-based precision therapies for human diseases.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

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