4.7 Article

Tumor-derived miR-378a-3p-containing extracellular vesicles promote osteolysis by activating the Dyrk1a/Nfatc1/Angptl2 axis for bone metastasis

CANCER LETTERS (2022)

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Journal

CANCER LETTERS
Volume 526, Issue -, Pages 76-90

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.canlet.2021.11.017

Keywords

Prostate cancer; Bone metastasis; Extracellular vesicle; miR-378a-3p; Osteolytic progression

Categories

Oncology

Funding

  1. Chinese Ministry of Science and Technology [2017YFA0102900]
  2. National Natural Science Foundation of China [81874097, 82072843, 81630073, 81872406, 81672850]
  3. Science and Technology Commission of Shanghai Municipality [20JC1417600, 19411967400]
  4. Peak Disciplines (Type IV) of In-stitutions of Higher Learning in Shanghai
  5. 111 project [B21024]
  6. KC Wong foundation

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The study revealed that tumor-derived EVs play a significant role in PCa bone metastasis by activating the Dyrk1a/Nfatc1/Angptl2 axis in BMMs to induce osteolytic progression. miR-378a-3p may serve as a potential predictor of metastatic PCa, and reducing its release or recruitment into EVs could be a therapeutic strategy against PCa metastasis.
Most prostate cancer (PCa)-related deaths are caused by progression to bone metastasis. Recently, the importance of extracellular vesicles (EVs) in pre-metastatic niche formation has been reported. However, whether and how tumor-derived EVs interact with bone marrow macrophages (BMMs) to release EV-delivered microRNAs to promote osteolysis and induce pre-metastatic niche formation for PCa bone metastasis remain unclear. Our in vitro and in vivo functional and mechanistic assays revealed that EV-mediated release of miR-378a-3p from tumor cells was upregulated in bone-metastatic PCa, maintaining low intracellular miR-378a-3p concentration to promote proliferation and MAOA-mediated epithelial-to-mesenchymal transition. Moreover, miR-378a-3p enrichment in tumor-derived EVs was induced by hnRNPA2B1 (a transfer chaperone) overexpression. After tumor-derived EVs were taken in by BMMs, enriched miR-378a-3p promoted osteolytic progression by inhibiting Dyrk1a to improve Nfatc1 (an osteolysis-related transcription factor) nuclear translocation, to activate the expression of downstream target gene Angptl2. As a feedback, increased Angptl2 secretion into the tumor environment promoted PCa progression. In conclusion, tumor-derived miR-378a-3p-containing EVs play a significant role in PCa bone metastasis by activating the Dyrk1a/Nfatc1/Angptl2 axis in BMMs to induce osteolytic progression, making miR-378a-3p a potential predictor of metastatic PCa. Reducing the release of miR-378a-3pcontaining EVs or inhibiting the recruitment of miR-378a-3p into EVs can be a therapeutic strategy against PCa metastasis.

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