Arrestin-3 Scaffolding of the JNK3 Cascade Suggests a Mechanism for Signal Amplification

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2018 Dec 29

PMID 30591558

Citations 25

Authors

Nicole A Perry

Tamer S Kaoud

Oscar O Ortega

Ali I Kaya

David J Marcus

John M Pleinis

Sandra Berndt

Qiuyan Chen

Xuanzhi Zhan

Kevin N Dalby

Carlos F Lopez

T M Iverson

Vsevolod V Gurevich

Affiliations

Soon will be listed here.

Abstract

Scaffold proteins tether and orient components of a signaling cascade to facilitate signaling. Although much is known about how scaffolds colocalize signaling proteins, it is unclear whether scaffolds promote signal amplification. Here, we used arrestin-3, a scaffold of the ASK1-MKK4/7-JNK3 cascade, as a model to understand signal amplification by a scaffold protein. We found that arrestin-3 exhibited >15-fold higher affinity for inactive JNK3 than for active JNK3, and this change involved a shift in the binding site following JNK3 activation. We used systems biochemistry modeling and Bayesian inference to evaluate how the activation of upstream kinases contributed to JNK3 phosphorylation. Our combined experimental and computational approach suggested that the catalytic phosphorylation rate of JNK3 at Thr-221 by MKK7 is two orders of magnitude faster than the corresponding phosphorylation of Tyr-223 by MKK4 with or without arrestin-3. Finally, we showed that the release of activated JNK3 was critical for signal amplification. Collectively, our data suggest a "conveyor belt" mechanism for signal amplification by scaffold proteins. This mechanism informs on a long-standing mystery for how few upstream kinase molecules activate numerous downstream kinases to amplify signaling.

Citing Articles

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