The RNA binding proteins LARP4A and LARP4B promote sarcoma and carcinoma growth and metastasis

Author:

Coleman Jennifer C.,Tattersall Luke,Yianni Val,Knight Laura,Yu Hongqiang,Hallett Sadie,Johnson Philip,Caetano Ana,Cosstick Charlie,Ridley Anne,Gartland Alison,Conte Maria R,Grigoriadis Agamemnon E.ORCID

Abstract

SUMMARYRNA-binding proteins (RBPs) are emerging as important regulators of pathogenesis, including cancer. Here we reveal that the recently characterised RBPs LARP4A and LARP4B are differentially overexpressed in primary osteosarcoma and osteosarcoma lung metastases, as well as in prostate cancer. Depletion of LARP4A and LARP4B inhibited primary tumour growth and metastatic spread in xenograft studies, as well as inhibiting cell proliferation, motility and migration. Transcriptomic profiling combined with high content multiparametric cell cycle analysis unveiled a central role for LARP4B, but not LARP4A, in regulating cell cycle progression in osteosarcoma and prostate cancer cell lines, potentially through modulating the post-transcriptional regulation of RNA targets that include key cell cycle proteins such as Cyclins B1 and E2, Aurora B and E2F1. Our work assigns new functions to LARP4A and LARP4B as pro-tumorigenic proteins in bone and prostate cancer, highlights their similarities while indicating distinct functional aspects, and adds significantly to the rapidly increasing roles of RBPs in different cancer models. Uncovering clear biological roles for these paralogous proteins provides new avenues for identifying novel tissue-specific targets and potential druggable intervention.

Publisher

Cold Spring Harbor Laboratory

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