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p53 loss activates prometastatic secretory vesicle biogenesis in the Golgi

Xiaochao Tan, Priyam Banerjee, Lei Shi, Guan-Yu Xiao, B. Leticia Rodriguez, Caitlin L. Grzeskowiak, Xin Liu, Yu Jiang, Don L. Gibbons, William K. Russell, Chad J. Creighton, Jonathan M. Kurie

2021Science Advances33 citationsDOIOpen Access PDF

Abstract

Cancer cells exhibit hyperactive secretory states that maintain cancer cell viability and remodel the tumor microenvironment. However, the oncogenic signals that heighten secretion remain unclear. Here, we show that p53 loss activates prometastatic secretory vesicle biogenesis in the Golgi. p53 loss up-regulates the expression of a Golgi scaffolding protein, progestin and adipoQ receptor 11 (PAQR11), which recruits an adenosine diphosphate ribosylation factor 1-containing protein complex that loads cargos into secretory vesicles. PAQR11-dependent secretion of a protease, PLAU, prevents anoikis and initiates autocrine activation of a PLAU receptor/signal transducer and activator of transcription-3-dependent pathway that up-regulates PAQR11 expression, thereby completing a feedforward loop that amplifies prometastatic effector protein secretion. Pharmacologic inhibition of PLAU receptor impairs the growth and metastasis of p53-deficient cancers. Blockade of PAQR11-dependent secretion inhibits immunosuppressive processes in the tumor microenvironment. Thus, Golgi reprogramming by p53 loss is a key driver of hypersecretion in cancer.

Topics & Concepts

Cell biologyGolgi apparatusSecretionTumor microenvironmentBiologyAutocrine signallingCancer cellSecretory pathwayReceptorCancer researchCancerEndocrinologyBiochemistryTumor cellsGeneticsEndoplasmic reticulumMechanisms of cancer metastasisCellular transport and secretionS100 Proteins and Annexins
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