MAPK signaling to the early secretory pathway revealed by kinase/phosphatase functional screening

Author:

Farhan Hesso1,Wendeler Markus W.1,Mitrovic Sandra1,Fava Eugenio2,Silberberg Yael3,Sharan Roded3,Zerial Marino2,Hauri Hans-Peter1

Affiliation:

1. Biozentrum, Universität Basel, 4056 Basel, Switzerland

2. High-Throughput Technology Development Studio, Max Planck Institute of Molecular Cell Biology and Genetics, 01307 Dresden, Germany

3. The Blavatnik School of Computer Science, Tel Aviv University, 69978 Tel Aviv, Israel

Abstract

To what extent the secretory pathway is regulated by cellular signaling is unknown. In this study, we used RNA interference to explore the function of human kinases and phosphatases in controlling the organization of and trafficking within the secretory pathway. We identified 122 kinases/phosphatases that affect endoplasmic reticulum (ER) export, ER exit sites (ERESs), and/or the Golgi apparatus. Numerous kinases/phosphatases regulate the number of ERESs and ER to Golgi protein trafficking. Among the pathways identified, the Raf–MEK (MAPK/ERK [extracellular signal-regulated kinase] kinase)–ERK cascade, including its regulatory proteins CNK1 (connector enhancer of the kinase suppressor of Ras-1) and neurofibromin, controls the number of ERESs via ERK2, which targets Sec16, a key regulator of ERESs and COPII (coat protein II) vesicle biogenesis. Our analysis reveals an unanticipated complexity of kinase/phosphatase-mediated regulation of the secretory pathway, uncovering a link between growth factor signaling and ER export.

Publisher

Rockefeller University Press

Subject

Cell Biology

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