Hsp47 promotes biogenesis of multi-subunit neuroreceptors in the endoplasmic reticulum

Hsp47促进内质网中多亚基神经受体的生物合成

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作者:Ya-Juan Wang # ,Xiao-Jing Di # ,Pei-Pei Zhang ,Xi Chen ,Marnie P Williams ,Dong-Yun Han ,Raad Nashmi ,Brandon J Henderson ,Fraser J Moss ,Ting-Wei Mu

Abstract

Protein homeostasis (proteostasis) deficiency is an important contributing factor to neurological and metabolic diseases. However, how the proteostasis network orchestrates the folding and assembly of multi-subunit membrane proteins is poorly understood. Previous proteomics studies identified Hsp47 (Gene: SERPINH1), a heat shock protein in the endoplasmic reticulum lumen, as the most enriched interacting chaperone for gamma-aminobutyric acid type A (GABAA) receptors. Here, we show that Hsp47 enhances the functional surface expression of GABAA receptors in rat neurons and human HEK293T cells. Furthermore, molecular mechanism study demonstrates that Hsp47 acts after BiP (Gene: HSPA5) and preferentially binds the folded conformation of GABAA receptors without inducing the unfolded protein response in HEK293T cells. Therefore, Hsp47 promotes the subunit-subunit interaction, the receptor assembly process, and the anterograde trafficking of GABAA receptors. Overexpressing Hsp47 is sufficient to correct the surface expression and function of epilepsy-associated GABAA receptor variants in HEK293T cells. Hsp47 also promotes the surface trafficking of other Cys-loop receptors, including nicotinic acetylcholine receptors and serotonin type 3 receptors in HEK293T cells. Therefore, in addition to its known function as a collagen chaperone, this work establishes that Hsp47 plays a critical and general role in the maturation of multi-subunit Cys-loop neuroreceptors. Keywords: GABAA receptors; Hsp47; assembly; biochemistry; cell biology; chemical biology; epilepsy; folding; human; mouse; proteostasis.

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