miR-122-5p Expression and Secretion in Melanoma Cells Is Amplified by the LPAR3 SH3-Binding Domain to Regulate Wnt1

miR-122-5p Expression and Secretion in Melanoma Cells Is Amplified by the LPAR3 SH3-Binding Domain to Regulate Wnt1

The lysophosphatidic acid receptor-3 (LPAR3) is a G protein-coupled receptor that mediates viability among malignant cells and aggressiveness among certain tumors. The study's objective was to determine the interplay between LPAR3 and miRNAs to impact key cellular signaling pathways. Using SK-M...

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Veröffentlicht in:Molecular cancer research 2019-01, Vol.17 (1), p.299-309
Hauptverfasser: Byrnes, Charnel C, Jia, Wei, Alshamrani, Ali A, Kuppa, Sudeepti S, Murph, Mandi M
Format: Artikel
Sprache:eng
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Animals
Binding Sites
Cell Proliferation - physiology
Hep G2 Cells
Humans
Melanoma - genetics
Melanoma - metabolism
Melanoma - pathology
Mice
Mice, Knockout
MicroRNAs - biosynthesis
MicroRNAs - genetics
MicroRNAs - metabolism
Protein Domains
Receptors, Lysophosphatidic Acid - metabolism
Wnt1 Protein - metabolism
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container_end_page 309
container_issue 1
container_start_page 299
container_title Molecular cancer research
container_volume 17
creator Byrnes, Charnel C
Jia, Wei
Alshamrani, Ali A
Kuppa, Sudeepti S
Murph, Mandi M
description The lysophosphatidic acid receptor-3 (LPAR3) is a G protein-coupled receptor that mediates viability among malignant cells and aggressiveness among certain tumors. The study's objective was to determine the interplay between LPAR3 and miRNAs to impact key cellular signaling pathways. Using SK-Mel-2 and SK-Mel-5 melanoma cells, wild-type and mutated receptors were stably expressed to explore molecular mechanisms. LPAR3 signaling induced miR-122-5p intracellularly and subsequently its inclusion into exosomes. This amplification resulted in less abundant Wnt1, maintenance of GSK3 inactivation and to a lesser extent, partial degradation of β-catenin. The surge in miR-122-5p and reduction in Wnt1 originated from signaling at the Src homology 3 (SH3) ligand-binding motif within the third intracellular loop of LPAR3, because mutant receptors did not increase miR-122-5p and had a weakened capacity to reduce Wnt1. In addition, a key mediator of melanoma survival signaling, the peroxisome proliferator-activated receptor gamma coactivator 1-α (PPARGC1A/PGC1), was involved in miR-122-5p transcription. In conclusion, this study highlights the powerful role miRNAs have in fine-tuning specific G protein-coupled receptor-mediated signaling events by altering the transcription of signaling transduction pathway components. This study also identifies that LPAR3 increases miR-122-5p expression, which occurs mechanistically through the SH3 domain and helps explain why miR-122-5p increases are detected in cancer patient serum. IMPLICATIONS: LPAR3 is partially responsible for the production and secretion of miR-122-5p, found in the serum of a wide variety of patients with cancer.
doi_str_mv 10.1158/1541-7786.MCR-18-0460
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source MEDLINE; American Association for Cancer Research; EZB-FREE-00999 freely available EZB journals; Free Full-Text Journals in Chemistry
subjects Animals
Binding Sites
Cell Proliferation - physiology
Hep G2 Cells
Humans
Melanoma - genetics
Melanoma - metabolism
Melanoma - pathology
Mice
Mice, Knockout
MicroRNAs - biosynthesis
MicroRNAs - genetics
MicroRNAs - metabolism
Protein Domains
Receptors, Lysophosphatidic Acid - metabolism
Wnt1 Protein - metabolism
title miR-122-5p Expression and Secretion in Melanoma Cells Is Amplified by the LPAR3 SH3-Binding Domain to Regulate Wnt1
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