Article

The multifunctional adaptor protein HIP-55 couples Smad7 to accelerate TGF-β type I receptor degradation

Yang Sun1,2,3,4, Zi-jian Li1,2,3,4
1 Department of Cardiology and Institute of Vascular Medicine, Peking University Third Hospital
2 Key Laboratory of Cardiovascular Molecular Biology and Regulatory Peptides, Ministry of Health
3 Key Laboratory of Molecular Cardiovascular Sciences, Ministry of Education
4 Beijing Key Laboratory of Cardiovascular Receptors Research, Beijing 100191, China
Correspondence to: Zi-jian Li: lizijian@bjmu.edu.cn,
DOI: 10.1038/s41401-021-00741-1
Received: 29 April 2021
Accepted: 5 July 2021
Advance online: 30 July 2021

Abstract

Transforming growth factor β (TGF-β) is a multifunctional polypeptide that plays critical roles in regulating a broad range of cellular functions and physiological processes. TGF-β signalling dysfunction contributes to many disorders, such as cardiovascular diseases, cancer and immunological diseases. The homoeostasis of negative feedback regulation is critical for signal robustness, duration and specificity, which precisely control physiological and pathophysiological processes. However, the underlying mechanism by which the negative regulation of TGF-β signalling is integrated and coordinated is still unclear. Here, we reveal that haematopoietic progenitor kinase-interacting protein of 55 kDa (HIP-55) was upregulated upon TGF-β stimulation, while the loss of HIP-55 caused TGF-β signalling overactivation and the abnormal accumulation of downstream extracellular matrix (ECM) genes. HIP-55 interacts with Smad7 and competes with Smad7/Axin complex formation to inhibit the Axin-mediated degradation of Smad7. HIP-55 further couples Smad7 to TβRI but not TβRII, driving TβRI degradation. Altogether, our findings demonstrate a new mechanism by which the effector and negative feedback functions of HIP-55 are coupled and may provide novel strategies for the treatment of TGF-β signalling-related human diseases.
Keywords: TGF-β type I receptor; degradation; HIP-55; Smad7; TGF-β signalling-related human diseases

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