Nature Communications 2015-01-01

In vivo model with targeted cAMP biosensor reveals changes in receptor-microdomain communication in cardiac disease.

Julia U Sprenger, Ruwan K Perera, Julia H Steinbrecher, Stephan E Lehnart, Lars S Maier, Gerd Hasenfuss, Viacheslav O Nikolaev

文献索引:Nat. Commun. 6 , 6965, (2015)

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摘要

3',5'-cyclic adenosine monophosphate (cAMP) is an ubiquitous second messenger that regulates physiological functions by acting in distinct subcellular microdomains. Although several targeted cAMP biosensors are developed and used in single cells, it is unclear whether such biosensors can be successfully applied in vivo, especially in the context of disease. Here, we describe a transgenic mouse model expressing a targeted cAMP sensor and analyse microdomain-specific second messenger dynamics in the vicinity of the sarcoplasmic/endoplasmic reticulum calcium ATPase (SERCA). We demonstrate the biocompatibility of this targeted sensor and its potential for real-time monitoring of compartmentalized cAMP signalling in adult cardiomyocytes isolated from a healthy mouse heart and from an in vivo cardiac disease model. In particular, we uncover the existence of a phosphodiesterase-dependent receptor-microdomain communication, which is affected in hypertrophy, resulting in reduced β-adrenergic receptor-cAMP signalling to SERCA.


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  • 氯化钠
  • 牛磺酸
  • 佛司可林
  • 无水氯化钙
  • 腺苷3',5'-环单磷酸...
  • 硫酸镁
  • 碳酸氢钠
  • 氯化钠-35cl
  • 巯基乙醇
  • 磷酸二氢钾

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