4.4 Article

Exosomal circKDM4A Induces CUL4B to Promote Prostate Cancer Cell Malignancy in a miR-338-3p-Dependent Manner

Journal

BIOCHEMICAL GENETICS
Volume 61, Issue 1, Pages 390-409

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10528-022-10251-2

Keywords

Exosomes; circKDM4A; miR-338-3p; CUL4B

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It has been found that circKDM4A is abnormally expressed in serum exosomes of prostate cancer patients. Treatment with exosomes promotes proliferation, migration, and invasion of prostate cancer cells while inhibiting apoptosis, and these effects are attenuated after circKDM4A knockdown. Moreover, circKDM4A acts as a sponge for miR-338-3p and interacts with CUL4B in prostate cancer cells. CircKDM4A regulates the effect of exosome-induced malignancy in prostate cancer cells by interacting with miR-338-3p and CUL4B.
Circular RNA lysine demethylase 4A (circKDM4A) is also named circ_0012098 and its abnormal expression has been confirmed in serum exosomes of prostate cancer (PC) patients. However, whether PC progression involves the exosomal circ_0012098 remains unknown. RNA expression of circKDM4A, microRNA-338-3p (miR-338-3p) and cullin 4B (CUL4B) was detected by quantitative real-time polymerase chain reaction. Protein expression was checked by Western blot. The positive expression rate of nuclear proliferation marker (ki-67) was analyzed by immunohistochemistry assay. Dual-luciferase reporter assay and RNA immunoprecipitation assay were used to identify the interaction between miR-338-3p and circKDM4A or CUL4B. Mouse model assay was performed to determine the effect of exosomal circKDM4A on tumorigenesis in vivo. CircKDM4A expression was significantly upregulated in the serum exosomes from PC patients compared with the exosomes from healthy volunteers. Exosomes treatment promoted the proliferation, migration and invasion of PC cells but inhibited apoptosis; however, these effects were attenuated after circKDM4A knockdown. Meanwhile, circKDM4A depletion restored exosome-increased circKDM4A expression. Additionally, circKDM4A acted as a miR-338-3p sponge, and miR-338-3p bound to CUL4B in PC cells. CircKDM4A regulated the effect of exosome-induced PC cell malignancy by interacting with miR-338-3p and CUL4B. Moreover, circKDM4A silencing relieved exosome-induced tumor growth in vivo. Exosomal circKDM4A promoted PC malignant progression by the miR-338-3p/CUL4B axis, providing a therapeutic target for PC.

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